TY  - THES
A1  - Winnerlein, Martin
T1  - Molecular Beam Epitaxy and Characterization of the Magnetic Topological Insulator (V,Bi,Sb)\(_2\)Te\(_3\)
T1  - Molekularstrahlepitaxie und Charakterisierung des magnetischen topologischen Isolators (V,Bi,Sb)\(_2\)Te\(_3\)
N2  - The subject of this thesis is the fabrication and characterization of magnetic topological
insulator layers of (V,Bi,Sb)\(_2\)Te\(_3\) exhibiting the quantum anomalous Hall
effect. A major task was the experimental realization of the quantum anomalous
Hall effect, which is only observed in layers with very specific structural,
electronic and magnetic properties. These properties and their influence on the
quantum anomalous Hall effect are analyzed in detail.
First, the optimal conditions for the growth of pure Bi\(_2\)Te\(_3\) and Sb\(_2\)Te\(_3\) crystal
layers and the resulting structural quality are studied. The crystalline quality of
Bi\(_2\)Te\(_3\) improves significantly at higher growth temperatures resulting in a small
mosaicity-tilt and reduced twinning defects. The optimal growth temperature is
determined as 260\(^{\circ}\)C, low enough to avoid desorption while maintaining a high
crystalline quality.
The crystalline quality of Sb\(_2\)Te\(_3\) is less dependent on the growth temperature.
Temperatures below 230\(^{\circ}\)C are necessary to avoid significant material desorption,
though. Especially for the nucleation on Si(111)-H, a low sticking coefficient is
observed preventing the coalescence of islands into a homogeneous layer.
The influence of the substrate type, miscut and annealing sequence on the growth
of Bi\(_2\)Te\(_3\) layers is investigated. The alignment of the layer changes depending on
the miscut angle and annealing sequence: Typically, layer planes align parallel to
the Si(111) planes. This can enhance the twin suppression due to transfer of the
stacking order from the substrate to the layer at step edges, but results in a step
bunched layer morphology. For specific substrate preparations, however, the layer
planes are observed to align parallel to the surface plane. This alignment avoids
displacement at the step edges, which would cause anti-phase domains. This results
in narrow Bragg peaks in XRD rocking curve scans due to long-range order in
the absence of anti-phase domains. Furthermore, the use of rough Fe:InP(111):B
substrates leads to a strong reduction of twinning defects and a significantly reduced
mosaicity-twist due to the smaller lattice mismatch.
Next, the magnetically doped mixed compound V\(_z\)(Bi\(_{1−x}\)Sb\(_x\))\(_{2−z}\)Te\(_3\) is studied in
order to realize the quantum anomalous Hall effect. The addition of V and Bi to
Sb\(_2\)Te\(_3\) leads to efficient nucleation on the Si(111)-H surface and a closed, homogeneous
layer. Magneto-transport measurements of layers reveal a finite anomalous
Hall resistivity significantly below the von Klitzing constant. The observation of
the quantum anomalous Hall effect requires the complete suppression of parasitic
bulklike conduction due to defect induced carriers. This can be achieved by optimizing
the thickness, composition and growth conditions of the layers.
The growth temperature is observed to strongly influence the structural quality.
Elevated temperatures result in bigger islands, improved crystallographic orientation
and reduced twinning. On the other hand, desorption of primarily Sb is
observed, affecting the thickness, composition and reproducibility of the layers.
At 190\(^{\circ}\)C, desorption is avoided enabling precise control of layer thickness and
composition of the quaternary compound while maintaining a high structural
quality.
It is especially important to optimize the Bi/Sb ratio in the (V,Bi,Sb)\(_2\)Te\(_3\) layers,
since by alloying n-type Bi\(_2\)Te\(_3\) and p-type Sb\(_2\)Te\(_3\) charge neutrality is achieved at
a specific mixing ratio. This is necessary to shift the Fermi level into the magnetic
exchange gap and fully suppress the bulk conduction. The Sb content x furthermore
influences the in-plane lattice constant a significantly. This is utilized to
accurately determine x even for thin films below 10 nm thickness required for the
quantum anomalous Hall effect. Furthermore, x strongly influences the surface
morphology: with increasing x the island size decreases and the RMS roughness
increases by up to a factor of 4 between x = 0 and x = 1.
A series of samples with x varied between 0.56-0.95 is grown, while carefully
maintaining a constant thickness of 9 nm and a doping concentration of 2 at.% V.
Magneto-transport measurements reveal the charge neutral point around x = 0.86
at 4.2 K. The maximum of the anomalous Hall resistivity of 0.44 h/e\(^2\) is observed
at x = 0.77 close to charge neutrality. Reducing the measurement temperature
to 50 mK significantly increases the anomalous Hall resistivity. Several samples
in a narrow range of x between 0.76-0.79 show the quantum anomalous Hall effect
with the Hall resistivity reaching the von Klitzing constant and a vanishing
longitudinal resistivity. Having realized the quantum anomalous Hall effect as the
first group in Europe, this breakthrough enabled us to study the electronic and
magnetic properties of the samples in close collaborations with other groups.
In collaboration with the Physikalisch-Technische Bundesanstalt high-precision
measurements were conducted with detailed error analysis yielding a relative de-
viation from the von Klitzing constant of (0.17 \(\pm\) 0.25) * 10\(^{−6}\). This is published
as the smallest, most precise value at that time, proving the high quality of the
provided samples. This result paves the way for the application of magnetic topological
insulators as zero-field resistance standards.
Non-local magneto-transport measurements were conducted at 15 mK in close
collaboration with the transport group in EP3. The results prove that transport
happens through chiral edge channels. The detailed analysis of small anomalies in
transport measurements reveals instabilities in the magnetic phase even at 15 mK.
Their time dependent nature indicates the presence of superparamagnetic contributions
in the nominally ferromagnetic phase.
Next, the influence of the capping layer and the substrate type on structural properties
and the impact on the quantum anomalous Hall effect is investigated. To
this end, a layer was grown on a semi-insulating Fe:InP(111)B substrate using the
previously optimized growth conditions. The crystalline quality is improved significantly
with the mosaicity twist reduced from 5.4\(^{\circ}\) to 1.0\(^{\circ}\). Furthermore, a layer
without protective capping layer was grown on Si and studied after providing sufficient
time for degradation. The uncapped layer on Si shows perfect quantization,
while the layer on InP deviates by about 5%. This may be caused by the higher
crystalline quality, but variations in e.g. Sb content cannot be ruled out as the
cause. Overall, the quantum anomalous Hall effect seems robust against changes
in substrate and capping layer with only little deviations.
Furthermore, the dependence of the quantum anomalous Hall effect on the thickness
of the layers is investigated. Between 5-8 nm thickness the material typically
transitions from a 2D topological insulator with hybridized top and bottom surface
states to a 3D topological insulator. A set of samples with 6 nm, 8 nm, and
9 nm thickness exhibits the quantum anomalous Hall effect, while 5 nm and 15 nm
thick layers show significant bulk contributions. The analysis of the longitudinal
and Hall conductivity during the reversal of magnetization reveals distinct differences
between different thicknesses. The 6 nm thick layer shows scaling consistent
with the integer quantum Hall effect, while the 9 nm thick layer shows scaling expected
for the topological surface states of a 3D topological insulator. The unique
scaling of the 9 nm thick layer is of particular interest as it may be a result of
axion electrodynamics in a 3D topological insulator.
Subsequently, the influence of V doping on the structural and magnetic properties
of the host material is studied systematically. Similarly to Bi alloying, increased
V doping seems to flatten the layer surface significantly. With increasing V content,
Te bonding partners are observed to increase simultaneously in a 2:3 ratio
as expected for V incorporation on group-V sites. The linear contraction of the
in-plane and out-of-plane lattice constants with increasing V doping is quantitatively
consistent with the incorporation of V\(^{3+}\) ions, possibly mixed with V\(^{4+}\)
ions, at the group-V sites. This is consistent with SQUID measurements showing
a magnetization of 1.3 \(\mu_B\) per V ion.
Finally, magnetically doped topological insulator heterostructures are fabricated
and studied in magneto-transport. Trilayer heterostructures with a non-magnetic
(Bi,Sb)\(_2\)Te\(_3\) layer sandwiched between two magnetically doped layers are predicted
to host the axion insulator state if the two magnetic layers are decoupled and in
antiparallel configuration. Magneto-transport measurements of such a trilayer heterostructure
with 7 nm undoped (Bi,Sb)\(_2\)Te\(_3\) between 2 nm thick layers doped with
1.5 at.% V exhibit a zero Hall plateau representing an insulating state. Similar results
in the literature were interpreted as axion insulator state, but in the absence
of a measurement showing the antiparallel magnetic orientation other explanations
for the insulating state cannot be ruled out.
Furthermore, heterostructures including a 2 nm thin, highly V doped layer region
show an anomalous Hall effect of opposite sign compared to previous samples. A
dependency on the thickness and position of the doped layer region is observed,
which indicates that scattering at the interfaces causes contributions to the anomalous
Hall effect of opposite sign compared to bulk scattering effects.
Many interesting phenomena in quantum anomalous Hall insulators as well as axion
insulators are still not unambiguously observed. This includes Majorana bound
states in quantum anomalous Hall insulator/superconductor hybrid systems and
the topological magneto-electric effect in axion insulators. The limited observation
temperature of the quantum anomalous Hall effect of below 1 K could be increased
in 3D topological insulator/magnetic insulator heterostructures which utilize the
magnetic proximity effect.
The main achievement of this thesis is the reproducible growth and characterization
of (V,Bi,Sb)2Te3 layers exhibiting the quantum anomalous Hall effect. The
detailed study of the structural requirements of the quantum anomalous Hall effect
and the observation of the unique axionic scaling behavior in 3D magnetic
topological insulator layers leads to a better understanding of the nature of this
new quantum state. The high-precision measurements of the quantum anomalous
Hall effect reporting the smallest deviation from the von Klitzing constant
are an important step towards the realization of a zero-field quantum resistance
standard.
N2  - Das Thema dieser Arbeit ist die Herstellung und Charakterisierung von Schichten
des magnetischen topologischen Isolators (V,Bi,Sb)\(_2\)Te\(_3\), die den Quanten anomalen
Hall-Effekt zeigen. Die Hauptaufgabe war die experimentelle Realisierung
des Quanten anomalen Hall-Effekts, welcher nur in Schichten mit bestimmten
strukturellen, elektronischen und magnetischen Eigenschaften beobachtet wird.
Diese Eigenschaften wurden ermittelt und ihr Einfluss genau analysiert.
Als Erstes wurden die optimalen Bedingungen für das Wachstum von reinen
Bi\(_2\)Te\(_3\) und Sb\(_2\)Te\(_3\) Kristallschichten und die resultierende strukturelle Qualität
untersucht. Die kristalline Qualität von Bi\(_2\)Te\(_3\) verbessert sich signifikant bei hohen
Wachstumstemperaturen, welche die Neigung der Domänen verringern und
Zwillingsdefekte reduzieren. Als optimale Wachstumstemperatur wurde 260\(^{\circ}\)C
ermittelt, ausreichend niedrig um Desorption zu vermeiden während eine hohe
Kristallqualität erhalten bleibt.
Die Wachstumstemperatur von Sb\(_2\)Te\(_3\) hat einen geringeren Einfluss auf die Kristallqualität.
Temperaturen unter 230\(^{\circ}\)C sind allerdings nötig um erhebliche Desorption
zu vermeiden. Ein geringer Haftkoeffizient wurde besonders bei der Nukleation
auf der Si(111)-H Oberfläche beobachtet und verhindert das Zusammenwachsen
von Inseln zu einer homogenen Schicht.
Der Einfluss des Substrattyps, der Fehlorientierung der Oberfläche und der Ausheizsequenz
auf das Wachstum von Bi\(_2\)Te\(_3\) Schichten wurde untersucht. Die Ausrichtung
der Schicht ändert sich je nach Winkel der Fehlorientierung und der
Ausheilsequenz: Typischerweise orientieren sich die Ebenen der Schicht parallel zu
den Si(111) Ebenen, was aufgrund des Transfers der Stapelfolge vom Substrat zur
Schicht an den Stufenkanten die Unterdrückung von Zwillingsdefekte verbessert.
Andererseits führt diese Orientierung zu Anti-Phasen-Domänen durch die Verschiebung
an den Stufenkanten und zu einer gestuften Oberflächenmorphologie.
Für bestimmte Substratpräparationen richtet sich die Schicht jedoch parallel zur
Oberfläche aus. Diese Orientierung verhindert Verschiebungen an Stufenkanten
und damit Anti-Phasen-Domänen. Dies führt aufgrund der langreichweitigen Ordnung
zu sehr schmalen Bragg-Reflexen in XRD rocking curve Diffraktogrammen.
Weiterhin führen raue Fe:InP(111):B Substrate zu einer starken Unterdrückung
von Zwillingsdefekten und aufgrund der besseren Gitteranpassung zu einer deutlich
verringerten Verdrehung der Domänen.
Als Nächstes wurde das magnetisch dotierte V\(_z\)(Bi\(_{1−x}\)Sb\(_x\))\(_{2−z}\)Te\(_3\) untersucht mit
dem Ziel den Quanten anomalen Hall-Effekt zu realisieren. Die Zugabe von V und
Bi zu Sb\(_2\)Te\(_3\) führt zu einer effizienten Nukleation auf der Si(111)-H Oberfläche
und einer geschlossenen, homogenen Schicht. Magnetotransport Messungen der
Schichten ergeben einen messbaren anomalen Hall-Widerstand deutlich unter der
von-Klitzing-Konstanten. Die Beobachtung des Quanten anomalen Hall-Effekts
setzt eine vollständige Unterdrückung der defekt-induzierten, parasitären Leitfähigkeit
im Inneren der Schicht voraus. Dies kann durch die Optimierung der
Dicke, Zusammensetzung und Wachstumsbedingungen der Schicht erreicht werden.
Beobachtungen zeigen, dass die Wachstumstemperatur die strukturelle Qualität
stark beeinflusst. Erhöhte Temperaturen erzielen größere Inseln, eine verbesserte
kristalline Orientierung und weniger Zwillingsdefekte. Andererseits wird Desorption
von überwiegend Sb beobachtet, was sich auf die Dicke, Zusammensetzung
und Reproduzierbarkeit der Schichten auswirkt. Bei 190\(^{\circ}\)C kann Desorption vermieden
werden, was eine präzise Kontrolle über Schichtdicke und Zusammensetzung
des quaternären Verbunds ermöglicht, während eine hohe strukturelle Qualität
erhalten bleibt.
Es ist besonders wichtig das Bi/Sb Verhältnis zu optimieren, da durch das Legieren
des n-Typ Bi\(_2\)Te\(_3\) mit dem p-Typ Sb\(_2\)Te\(_3\) bei einem bestimmten Verhältnis Ladungsneutralität
erzielt wird. Dies ist nötig um die Leitung im Inneren der Schicht
vollständig zu unterdrücken und die Fermikante in die magnetische Austauschlücke
zu schieben. Der Sb Gehalt x beeinflusst außerdem die Gitterkonstante a in der
Ebene deutlich, im Gegensatz zur Gitterkonstante c in Wachstumsrichtung. Mit
Hilfe dieses Zusammenhangs kann x selbst in dünnen Schichten unter 10 nm Dicke,
wie sie für den Quantum anomalen Hall-Effekt benötigt werden, genau bestimmt
werden. Der Sb Gehalt x beeinflusst weiterhin die Oberflächenmorphologie deutlich:
mit steigenden x verringert sich die Inselgröße und die RMS Rauigkeit wächst
um bis zu einem Faktor 4 zwischen x = 0 und x = 1.
Eine Probenserie mit x zwischen 0,56−0,95 wurde hergestellt, wobei darauf geachtet
wurde eine konstante Dicke von 9 nm und eine Dotierkonzentration von 2 at.%
V beizubehalten. Magnetotransport Messungen bei 4,2K zeigen Ladungsneutra-
lität bei x = 0,86. Der maximale anomale Hall-Widerstand von 0,44 h/e\(^2\) wird
bei x = 0,77 nahe der Ladungsneutralität beobachtet. Wird die Messtemperatur
auf 50 mK reduziert, steigt der anomale Hall-Widerstand signifikant an. Mehrere
Proben mit x in einem schmalen Bereich von 0,76−0,79 zeigen den Quanten
anomalen Hall-Effekt mit einem Hall-Widerstand, der die von-Klitzing-Konstante
erreicht, und verschwindendem longitudinalen Widerstand. Die Realisierung des
Quantum anomalen Hall-Effekts als erste Gruppe in Europa ermöglichte es uns
die elektrischen und magnetischen Eigenschaften der Proben in Zusammenarbeit
mit anderen Gruppen zu untersuchen.
In Kollaboration mit der Physikalisch-Technische Bundesanstalt wurden Hochpräzisionsmessungen
mit detaillierter Fehleranalyse durchgeführt und eine relative
Abweichung von der von-Klitzing-Konstante von (0,17\(\pm\)0,25)*10\(^{−6}\) erzielt. Dieser
Wert wurde als kleinster und genauester Wert publiziert, was die hohe Qualität
der zur Verfügung gestellten Proben zeigt. Dieses Ergebnis ebnet den Weg für die
Anwendung von magnetischen topologischen Isolatoren als Widerstand Standards
ohne Magnetfeld.
In enger Zusammenarbeit mit der Transport Gruppe in der EP3 wurden nichtlokale
Magnetotransport Messungen bei 15mK durchgeführt. Das Ergebnis beweist,
dass Transport durch chirale Randkanäle erfolgt. Die detaillierte Analyse
kleiner Anomalien in Transport Messungen offenbart Instabilitäten in der magnetischen
Phase selbst bei 15 mK. Der zeitabhängige Charakter dieser Anomalien
weist auf superparamagnetische Anteile in der nominell ferromagnetischen Phase
hin.
Als nächstes wurde der Einfluss der Deckschicht und des Substrattyps auf die
strukturellen Eigenschaften und die Auswirkungen auf den Quanten anomalen
Hall-Effekt untersucht. Dazu wurde eine Schicht auf halbisolierendem Fe:InP(111)B
Substrat unter den zuvor optimierten Wachstumsbedingungen gewachsen. Dies
führt zu einer deutlich erhöhten kristallinen Qualität mit einem verringerten Verdrehungswinkel
von 5,4\(^{\circ}\) auf 1,0\(^{\circ}\). Weiterhin wurde eine Schicht ohne schützende
Deckschicht auf Si gewachsen und, nachdem ausreichend Zeit für mögliche Degradation
vergangen war, gemessen. Die Schicht auf Si ohne Deckschicht zeigt perfekte
Quantisierung, während die Schicht auf InP eine Abweichung von etwa 5%
aufweist. Ursache könnte die höhere kristalline Qualität sein, Variationen in z.B.
Sb Gehalt könnten jedoch auch eine Rolle spielen. Insgesamt scheint der Quanten
anomale Hall-Effekt robust gegenüber Änderungen des Substrats und der
Deckschicht zu sein.
Des Weiteren wurde die Abhängigkeit des Quanten anomalen Hall-Effekts von
der Schichtdicke untersucht. Zwischen 5−8 nm Dicke wechselt das Material typischerweise
von einem 2D topologischen Isolator mit hybridisierten oberen und
unteren Oberflächenzustand zu einem 3D topologischen Isolator. Eine Probenreihe
mit 6 nm, 8 nm und 9 nm Schichtdicke zeigt den Quanten anomalen Hall-
Effekt, während 5 nm und 15 nm dicke Schichten deutliche Beiträge aus dem Volumen
haben. Die Analyse der longitudinalen- und Hall-Leitfähigkeit während der
Umkehrung der Magnetisierung offenbart eindeutige Unterschiede. Die 6 nm dicke
Schicht zeigt ein Skalierungsverhalten konsistent mit dem ganzzahligen Quanten-
Hall-Effekt, die 9 nm dicke Schicht dagegen zeigt das erwartete Skalierungsverhalten
für die topologischen Oberflächenzustände eines 3D topologischen Isolators.
Das besondere Skalierungsverhalten der 9 nm dicken Schicht ist von besonderem
Interesse, da es der axionischen Elektrodynamik in einem 3D topologischen Isolator
entspringen könnte.
Anschließend wird der Einfluss von V Dotierung auf die strukturellen und magnetischen
Eigenschaften der Schichten systematisch untersucht. Ähnlich wie das
Legieren mit Bi, scheint V Dotieren die Oberfläche deutlich zu glätten. Mit steigenden
V Gehalt erhöht sich die Zahl der Te Bindungspartner simultan im 2:3 Verhältnis,
wie erwartet für den Einbau von V auf Gruppe-V Plätzen. Die lineare Kontraktion
der Gitterkonstanten in der Ebene und senkrecht dazu mit steigender V
Dotierung ist quantitativ konsistent mit dem Einbau von V\(^{3+}\) Ionen, möglicherweise
gemischt mit V\(^{4+}\) Ionen, auf Gruppe-V Plätzen. Dies ist konsistent mit
SQUID Messungen die eine Magnetisierung von 1,3 \(\mu_B\) pro V Ion zeigen.
Schließlich werden magnetisch dotierte topologische Isolator Heterostrukturen hergestellt
und in Magnetotransport Messungen charakterisiert. Der Axion-Isolator
Zustand wurde in dreischichtigen Heterostrukturen mit einer nichtmagnetischen
(Bi,Sb)\(_2\)Te\(_3\) Lage zwischen zwei magnetischen Schichten vorhergesagt, falls die
beiden magnetischen Lagen entkoppelt sind und in antiparalleler Ausrichtung vorliegen.
Magnetotransport Messungen solcher dreischichtigen Heterostrukturen mit
7 nm undotiertem (Bi,Sb)\(_2\)Te\(_3\) zwischen jeweils 2 nm dicken dotierten Schichten
mit 1,5 at.% V zeigen ein Null Hall-Plateau, das einen isolierenden Zustand repräsentiert.
Ähnliche Ergebnisse in der Literatur wurden als Axion-Isolator Zustand
interpretiert, jedoch können andere Erklärungen ohne eine direkten Messung der
antiparallelen magnetischen Orientierung nicht ausgeschlossen werden.
Weiterhin zeigen Heterostrukturen mit einer 2 nm dünnen, hoch V dotierten Schicht
einen anomalen Hall-Effekt mit entgegengesetzten Vorzeichen im Vergleich zu
vorhergehenden Proben. Die Abhängigkeit von der Dicke und Position dieser
Schicht könnte darauf hindeuten, dass Streuprozesse an den Grenzflächen einen
Beitrag zum anomalen Hall-Effekt entgegengesetzt zu den Volumenstreuprozessen
verursachen.
Viele interessante Phänomene in Quanten anomalen Hall Isolatoren sowie Axion-
Isolatoren sind noch nicht eindeutig beobachtet worden. Dies schließt gebundene
Majorana-Zustände in Quanten anomalen Hall Isolator/Supraleiter Hybridsystemen
und den topologischen magneto-elektrischen Effekt in Axion-Isolatoren ein.
Die limitierte Beobachtungstemperatur des Quanten anomalen Hall-Effekts von
unter 1 K könnte in Heterostrukturen aus 3D topologischen Isolator und magnetischen
Isolator Schichten welche den magnetischen Proximity-Effekt nutzen erhöht
werden.
Das wichtigste Ergebnis dieser Arbeit ist das reproduzierbare Wachstum und
die Charakterisierung von (V,Bi,Sb)\(_2\)Te\(_3\) Schichten die den Quanten anomalen
Hall-Effekt zeigen. Die detaillierte Untersuchung der strukturellen Voraussetzungen
und die Beobachtung des besonderen axionischen Skalierungsverhaltens in
3D magnetischen Isolatorschichten führt zu einem besseren Verständnis dieses
neuen Quantenzustands. Die Hochpräzisionsmessungen des Quanten anomalen
Hall-Effekts mit der geringsten Abweichung von der von-Klitzing-Konstanten sind
ein wichtiger Schritt zur Realisierung eines Widerstand-Standards basierend auf
Quantisierung ohne magnetischem Feld.
KW  - Bismutverbindungen
KW  - Topologischer Isolator
KW  - Molekularstrahlepitaxie
KW  - Quanten anomalen Hall-Effekt
KW  - Quantum anomalous Hall effect
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-211666
ER  - 
TY  - THES
A1  - Kerner, Florian Tobias
T1  - Reactions of rhodium(I) with diynes and studies of the photophysical behavior of the luminescent products
T1  - Reaktionen von Rhodium(I) mit Diinen und Untersuchung der photophysikalischen Eigenschaften der lumineszenten Produkte
N2  - Chapter 1 deals with the reaction of [Rh(acac)(PMe3)2] with para-substituted 1,4-diphenylbuta-1,3-diynes at room temperature, in which a complex containing a bidentate organic fulvene moiety, composed of two diynes, σ-bound to the rhodium center is formed in an all-carbon [3+2] type cyclization reaction. In addition, a complex containing an organic indene moiety, composed of three diynes, attached to the rhodium center in a bis-σ-manner is formed in a [3+2+3] cyclization process. 
Reactions at 100 °C reveal that the third diyne inserts between the rhodium center and the bis-σ-bound organic fulvene moiety. Furthermore, the formation of a 2,5- and a 2,4-bis(arylethynyl)rhodacyclopentadiene is observed. The unique [3+2] cyclization product was used for the synthesis of a highly conjugated organic molecule, which is hard to access or even inaccessible by conventional methods. Thus, at elevated temperatures, reaction of the [3+2] product with para-tolyl isocyanate led to the formation of a purple organic compound containing the organic fulvene structure and one equivalent of para-tolyl isocyanate.
The blue and green [3+2+3] complexes show an unusually broad absorption from 500 – 1000 nm with extinction coefficients ε of up to 11000 M-1 cm-1. The purple organic molecule shows an absorption spectrum similar to those of known diketopyrrolopyrroles.
Additionally, the reaction of [Rh(acac)(PMe3)2] with para-tolyl isocyanate was investigated. A cis-phosphine complex of the form cis-[Rh(acac)(PMe3)2(isocyanate)2] with an isocyanate dimer bound to the rhodium center by one carbon and one oxygen atom was isolated.
Replacing the trimethylphosphine ligands in [Rh(acac)(PMe3)2] with the stronger σ-donating NHC ligand Me2Im (1,3-dimethylimidazolin-2-ylidene), again, drastically alters the reaction. Similar [3+2] and [3+2+3] products to those discussed above could not be unambiguously assigned, but cis- and trans-π-complexes, which are in an equilibrium with the two starting materials, were formed.
Chapters 2 is about the influence of the backbone of the α,ω-diynes on the formation and photophysical properties of 2,5-bis(aryl)rhodacyclopentadienes. Therefore, different α,ω-diynes were reacted with [Rh(acac)(PMe3)2] and [Rh(acac)(P(p-tolyl)3)2] in equimolar amounts. In general, a faster consumption of the rhodium(I) starting material is observed while using preorganized α,ω-diynes with electron withdrawing substituents in the backbone. The isolated PMe3-substituted rhodacyclopentadienes exhibit fluorescence, despite the presence of the heavy atom rhodium, with lifetimes τF of < 1 ns and photoluminescence quantum yields Φ of < 0.01 as in previously reported P(p-tolyl)-substituted 2,5-bis(arylethynyl)rhodacyclopentadienes. However, an isolated P(p-tolyl)-substituted 2,5-bis(aryl)rhodacyclopentadiene shows multiple lifetimes and different absorption and excitation spectra leading to the conclusion that different species may be present.
Reaction of [Rh(acac)(Me2Im)2] with dimethyl 4,4'-(naphthalene-1,8-diylbis(ethyne-2,1-diyl))dibenzoate, results in the formation of a mixture trans- and cis-NHC-substituted 2,5-bis(aryl)rhodacyclopentadienes.
In chapter 3 the reaction of various acac- and diethyldithiocarbamate-substituted rhodium(I) catalysts bearing (chelating)phosphines with α,ω-bis(arylethynyl)alkanes (α,ω-diynes), yielding luminescent dimers and trimers, is described. The photophysical properties of dimers and trimers of the α,ω-diynes were investigated and compared to para-terphenyl, showing a lower quantum yield and a larger apparent Stokes shift.
Furthermore, a bimetallic rhodium(I) complex of the form [Rh2(ox)(P(p-tolyl)3)4] (ox: oxalate) was reacted with a CO2Me-substituted α,ω-tetrayne forming a complex in which only one rhodium(I) center reacts with the α,ω-tetrayne. The photophysical properties of this mixed rhodium(I)/(III) species shows only negligible differences compared to the P(p-tolyl)- and CO2Me-substituted 2,5-bis(arylethynyl)rhodacyclopentadiene, previously synthesized by Marder and co-workers.
N2  - Kapitel 1 beschäftigt sich mit der Umsetzung von [Rh(acac)(PMe3)2] mit zwei Äquivalenten para-substituierten 1,4-Diphenylbuta-1,3-diins bei Raumtemperatur. Dabei bildete sich ein Komplex, welcher eine organische Fulveneinheit, bestehend aus zwei Diinen und verbunden über zwei σ-Bindungen mit dem Rhodiumzentralatom, besitzt. Diese Verbindung bildet sich in einer „all-carbon“ [3+2] ähnlichen Zyklisierungsreaktion. Ebenso konnte aus derselben Reaktion ein Komplex mit einer Indeneinheit, bestehend aus drei Diinen, welche durch zwei σ-Bindungen mit dem Rhodiumzentralatom verbunden sind, isoliert und charakterisiert werden. Diese Verbindung bildet sich in einer „all-carbon“ [3+2+3] ähnlichen Zyklisierungsreaktion. Experimente bei 100 °C zeigen, dass sich das zusätzliche dritte Diin zwischen dem Rhodiumzentralatom und der organischen Fulveneinheit einfügt. Zusätzlich konnte die Bildung von 2,4- und 2,5-Bis(arylethinyl)rhodazyklopentadienen bei 100°C beobachtet werden. Diese seltene [3+2] Zyklisierungsreaktion kann benutzt werden um konjugierte, organische Moleküle darzustellen, welche sonst nur schwer oder gar nicht mit bisher bekannten Synthesemethoden zugänglich sind. In der Umsetzung des [3+2] Komplexes mit para-Tolylisocyanat bei 80 °C konnte ein violetter, rein organischer Feststoff erhalten werden, bestehend aus der organischen Fulveneinheit und einem Äquivalent para-Tolylisocyanat. Die blauen und grünen [3+2+3] Komplexe zeigen unter anderem eine ungewöhnliche breite Absorption von 500 – 1000 nm mit einem Extinktionskoeffizienten von bis zu 11000 M-1 cm-1. Die violette, rein organische Verbindung zeigt ein Absorptionsspektrum ähnlich zu bereits bekannten Diketopyrrolopyrrolen. Auch wurde die Reaktion von [Rh(acac)(PMe3)2] mit para-Tolylisocyanat untersucht. Es konnte ein cis-phosphan Komplex, bei dem ein para-Tolylisocyanat-Dimer über ein Kohlenstoff- und ein Sauerstoffatom an das Rhodiumzentralatom koordiniert, isoliert und charakterisiert werden. Substitution des Trimethylphosphans im Rh(I)-Präkursors durch einen NHC Liganden, nämlich Me2Im (1,3-dimethylimidazolin-2-yliden) führt zu einem unterschiedlichen Reaktionsverlauf. Ähnliche [3+2] und [3+2+3] Komplexe konnten nicht zweifelsfrei bestätigt werden, dafür konnte aber gezeigt werden, dass sich in der Reaktion bildende cis- und trans-Komplexe im Gleichgewicht mit den verwendeten Startmaterialien befinden.
Im zweiten Kapitel dieser Arbeite wurde der Einfluss des Rückgrats von α,ω-bis(arylethynyl)alkanen (α,ω-Diine) auf die Bildung und die photophysikalischen Eigenschaften von 2,5-Bis(aryl)rhodazyklopentadienen untersucht. Dazu wurden mehrere α,ω-Diine mit unterschiedlichem Rückgrat synthetisiert und diese mit [Rh(acac)(PMe3)2] und [Rh(acac)(P(p-tolyl)3)2] in äquimolaren Mengen reagiert. Es konnte ein schnellerer Verbrauch des Rh(I)-Präkursors bei der Verwendung von vororganisierten α,ω-Diinen mit elektronenziehenden Substituenten am Rückgrat festgestellt werden. Die PMe3-substituierten Rhodazyklopentadiene zeigen Fluoreszenz, trotz der Anwesenheit eines Schwermetalls. Lebenszeiten von τF < 1 ns und Quantenausbeuten von Φ < 0.01, ähnlich wie in P(p-tolyl)-substituierten 2,5-Bis(arylethynyl)rhodazyklopentadienen wurden beobachtet. Bei einem isolierten P(p-tolyl)-substituierten 2,5-Bis(aryl)rhodazyklopentadien konnten mehrere Lebenszeiten, wie auch unterschiedliche Absorptions- und Anregungsspektren detektiert werden, was zu der Schlussfolgerung führt, dass in Lösung mehrere Spezies vorhanden sind. Die Reaktion von [Rh(acac)(Me2Im)2] mit Dimethyl 4,4'-(naphthalen-1,8-diylbis(ethyn-2,1-diyl))dibenzoat führt zur Bildung einer Mischung aus trans- und cis-NHC-substituierter 2,5-Bis(aryl)rhodazyklopentadienen.
Im dritten Kapitel, wurde die Bildung lumineszenter Dimere und Trimere aus der Umsetzung von verschiedenen α,ω-Diinen mit katalytischen Mengen verschiedener acac- und diethyldithiocarbamat-substituierter Rhodium(I)-Katalysatoren mit (chelatisierenden) phosphanen untersucht. Anschließend wurden die photophysikalischen Eigenschaften der Dimere und Trimere untersucht und mit para-Terphenyl verglichen. Dabei wurden ähnliche Lebenszeiten, eine geringere Quantenausbeute wie auch größere Stokes-Verschiebungen der Dimere und Trimere im Vergleich zu para-Terphenyl gefunden. Auch wurde die Reaktion zwischen einem bimetallischen Rhodium Komplex [Rh2(ox)(P(p-tolyl)3)4] (ox: oxalat) und einem CO2Me-substituiertem α,ω-bis(arylbutadiynyl)alkan (α,ω-Tetrain) untersucht. In dieser Umsetzung reagierte nur eine der beiden möglichen Rhodium(I)-zentren mit dem α,ω-Tetrain unter Bildung eines 2,5-Bis(arylethynyl)rhodazyklopentadiens. Die photophysikalischen Eigenschaften dieser gemischten Rhodium(I)/(III)-Spezies zeigt nur marginale unterschiede, verglichen mit einem mononuklearen P(p-tolyl)- und CO2Me-substituiertem 2,5-Bis(arylethynyl)rhodazyklopentadiens, welches zuvor im Arbeitskreis Marder schon synthetisiert wurde.
KW  - Übergangsmetallkomplexe
KW  - Rhodium
KW  - Übergangsmetallkomplex
KW  - Zyklisierung
KW  - Transitionmetal
KW  - Cyclization
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-209107
ER  - 
TY  - THES
A1  - Kreß, Luisa Sophia
T1  - Determination of cytokine and axon guidance molecule profiles in patients with small fiber neuropathy
T1  - Bestimmung von Zytokin- und Axon Guidance Molekül-Profilen bei Patienten mit Kleinfaserneuropathie
N2  - The pathophysiological mechanisms of pain in small fiber neuropathy (SFN) are unclear. Based on experimental and clinical studies, sensitized nociceptors in the skin are reported to be involved in pain development. These nociceptors may be sensitized by cutaneous and systemic pain mediators e.g. pro- and anti-inflammatory cytokines. The aim of our study was, to measure the systemic and local gene expression of pro- and anti-inflammatory cytokines in white blood cells (WBC) as well as in primary fibroblasts and keratinocytes obtained from human skin of patients with SFN. Furthermore, gene expression levels of axon guidance molecules and their receptors, as potential regulators of the intraepidermal nerve fiber density (IENFD), were investigated. 55 patients and 31 healthy controls were prospectively recruited. Participants underwent extensive clinical phenotyping and blood sampling, 6-mm skin punch biopsies were taken from the right lateral calf and the upper thigh. Systemic relative gene expression levels (ΔG) of the interleukin (IL)-1β, IL-2, IL-6, IL-8, and tumor necrosis factor (TNF) was measured in WBC. Skin punch biopsies were taken to determine the IENFD and to obtain primary fibroblast and keratinocyte cell cultures. Skin cells were then used for investigation of ΔG in axon guidance molecules netrin 1 (NTN1) and ephrin A4 (EPHA4) as well as their receptors Unc5b receptor, and ephrin A4 (EFNA4) as well as cytokines IL-1β, IL-4, IL-6, IL-8, IL-10, TNF, and transforming growth factor (TGF). Systemically, gene expression of IL-2, IL-8, and TNF was higher in SFN patients compared to healthy controls. In keratinocytes, higher expression levels of NTN1 and TGF were found when comparing the SFN patients to the controls. In fibroblasts higher gene expression was shown in NTN1, Unc5b, IL-6, and IL-8 when comparing patients to healthy controls. The systemically and local elevated levels of pro-inflammatory, algesic cytokines in SFN patients compared to healthy controls, confirms a potential pathophysiological role in the development of neuropathic pain. Data also indicate fibroblasts and keratinocytes to influence subepidermal and intraepidermal nerve fiber growth through the expression of NTN1 and Unc5b. Thus, skin cells may contribute to the development of neuropathic pain through local denervation.
N2  - Der Pathomechanismus von Schmerz bei Small fiber Neuropathie (SFN) ist unklar. Auf Grundlage tierexperimenteller und klinischer Studien wird die Einwirkung kutaner und systemischer Schmerzmediatoren auf sensibilisierte Nozizeptoren in der Haut als mögliche Ursache diskutiert. In diesem Zusammenhang gab es Hinweise auf die Bedeutung von pro- und anti-inflammatorischen Zytokinen in der Pathophysiologie neuropathischer Schmerzen. Ziel der Studie war es, die systemische und lokale Genexpression pro- und anti-inflammatorischer Zytokine in Leukozyten sowie kutanen Fibroblasten und Keratinozyten von Patienten mit SFN zu messen. Ferner wurde untersucht, inwieweit die Expression repellierender Axon Guidance Moleküle und ihrer Rezeptoren in Hautzellen die intraepidermale Nervenfaserdichte (IENFD) regulieren könnte. Insgesamt konnten 55 SFN PatientInnen und 31 gesunde KontrollprobandInnen prospektiv rekrutiert werden. Nach ausführlicher klinischer Phänotypisierung und Blutentnahme wurden bei allen StudienteilnehmerInnen 6-mm Hautstanzbiopsien am lateralen Unter- und Oberschenkel entnommen. Die Messung der systemisch relativen Genexpression (ΔG) der Zytokine Interleukin (IL)-1β, IL-2, IL-6, IL-8 und des tumor necrose factors (TNF) erfolgte aus Leukozyten. Aus den Hautstanzbiopsien, die u.a. zur Bestimmung der IENFD verwendet wurden, wurden außerdem Primärzellkulturen von Keratinozyten und Fibroblasten angelegt, aus denen die lokale ΔG von Axon Guidance Molekülen Netrin 1 (NTN1) und Ephrin A4 (EPHA4), deren Rezeptoren Unc5b, und Ephrin A4 receptor (EFNA4) sowie der Zytokine IL-1β, IL-4, IL-6, IL-8, IL-10, TNF und des transforming growth factors (TGF) erfolgte. Systemisch zeigte sich eine höhere Genexpression für IL-2, IL-8 und TNF bei SFN Patienten im Vergleich zu gesunden Kontrollen. In Keratinozyten konnten höhere Expressionen von NTN1 und TGF-β1 bei Vergleich der Patientengruppe mit der Kontrollgruppe nachgewiesen werden. In Fibroblasten zeigte sich im Gruppenvergleich eine höhere Genexpression für NTN1, Unc5b sowie für IL-6 und IL-8. Die systemisch und lokal bei SFN Patienten nachgewiesene höhere Expression algetischer, pro-inflammatorischer Zytokine verglichen mit Kontrollen unterstützt eine mögliche pathophysiologische Rolle bei der Entstehung von neuropathischen Schmerzen. Ferner weisen die Daten darauf hin, dass Fibroblasten und Keratinozyten durch die Expression von NTN1 und Unc5b Einfluss auf das subepidermale und intraepidermale Nervenfaserwachstum nehmen und durch lokale Denervierung bei der Entstehung neuropathischer Schmerzen mitwirken könnten.
KW  - Neuropathischer Schmerz
KW  - Pathomechanismus
KW  - Cytokine
KW  - small fiber neuropathy
KW  - axon guidance molecules
KW  - pathophysilogical mechanisms
KW  - cytokines
KW  - skin cells
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-209113
ER  - 
TY  - THES
A1  - Koschitzki, Kim Christine Cornelia
T1  - Evaluation of preclinical animal models in bone tissue engineering and their success in clinical translation
T1  - Evaluierung von vorklinischen Tiermodellen für Bone Tissue Engineering und von ihrem Erfolg in der klinischen Umsetzung
N2  - Autologous bone still represents today’s gold standard for the treatment of critical size bone defects and fracture non-unions despite associated disadvantages regarding limitations in availability, donor site morbidity, costs and efficacy. Bone tissue engineered constructs would present a promising alternative to currently available treatments. However, research on preclinical animal studies still fails to provide clinical applicable results able to allow the replacement of currently applied methods. It seems that the idea of bone tissue engineering, which has now been integral part of academic studies for over 30 years, got somehow stuck at an intermediate level, in between intense preclinical research and striven stages of initial clinical trial phases. A clear discrepancy exists between the number of studies with preclinical animal models for bone tissue engineering and the number of clinically approved bone tissue engineered constructs available to patients.
The aim of this thesis was hence to evaluate preclinical animal models for bone tissue engineering as well as the perception of scientists and clinicians towards these models. Moreover, the general role of bone tissue engineering and its clinical need assessed by scientists and surgeons was investigated. A survey was conducted questioning both scientific and clinical opinions on currently available study designs and researchers’ satisfaction with preclinical animal models. Additionally, a literature research was conducted, resulting in 167 papers from the last 10 years that report current designs of preclinical orthotopic animal studies in bone tissue engineering. Thereby, the focus lied on the description of the models regarding animal species, strain, age, gender and defect design. The outcome of the literature search was evaluated and compared to the outcome obtained from the survey.
The survey data revealed that both scientists and surgeons generally remain positive about the future role of bone tissue engineering and its step to clinical translation, at least in the distant future, where it then might replace the current gold standard, autologous bone. Moreover, most of the participants considered preclinical animal models as relevant and well developed but the results as not yet realizable in the clinics. Surgeons thereby demonstrated a slightly more optimistic perception of currently conducted research with animal models compared to scientists. However, a rather inconsistent description of present preclinical study designs could be discerned when evaluating the reported study designs in the survey and the papers of the literature search.
Indeed, defining an appropriate animal species, strain, age, gender, observation time, observation method and surgical design often depends on different indications and research questions and represents a highly challenging task for the establishment of a preclinical animal model. The existing lack of valid guidelines for preclinical testing of bone tissue engineering leads hence to a lack of well standardized preclinical animal models. Moreover, still existing knowledge gaps regarding aspects that affect the process of fracture healing, such as vascularization or immunological aspects, were found to hinder clinical translation of bone tissue engineered constructs. 
Using literature review and survey, this thesis points out critical issues that need to be addressed to allow clinical translation of bone tissue engineered constructs. It can be concluded that currently existing study designs with preclinical animal models cannot live up to the claim of providing suitable results for clinical implementation. The here presented comprehensive summary of currently used preclinical animal models for bone tissue engineering reveals a missing consensus on the usage of models such as an apparent lack of reporting and standardization regarding the study designs described in both papers from the literature review and the survey. It thereby indicates a crucial need to improve preclinical animal models in order to allow clinical translation. Despite the fact that participants of the survey generally revealed a positive perception towards the use of bone tissue engineered constructs and affirmed the clinical need for such novel designs, the missing standardization constitutes a main weak point for the provision of reliable study outcome and the translational success of the models. The optimization of reproducibility and reliability, as well as the further understanding of ongoing mechanisms in bone healing in order to develop effective tissue engineered constructs, need to form the basis of all study designs. The study outcomes might then fulfill the requirements of maybe today's and hopefully tomorrow's aging population.
N2  - Über die letzten 30 Jahre hat die Rolle von Bone Tissue Engineering vielversprechenden Fortschritt gemacht und immer neue Ansätze werden etabliert. Somit stellt Bone Tissue Engineering eine aussichtsvolle Alternative zu dem heutigen Goldstandard (autogene Knochenersatzmaterialien) dar, nachdem diese häufig mit Nachteilen einhergehen: limitierte Verfügbarkeit, Morbidität durch Zweiteingriffe, ungenügend Stabilität und Kosten. Die klinische Umsetzung findet jedoch nicht so schnell statt, wie ursprünglich erhofft und es scheint, als würde die vorklinische Forschung auf der Stelle treten. Das Ausbleiben von reproduzierbaren und standardisierten vorklinischen Studien verhindert dabei eine "bench to bedside" Translation. 
Ziel dieser Doktorarbeit war es, derzeitige präklinische Tiermodelle für Bone Tissue Engineering zu evaluieren und dabei zu untersuchen, woran es liegen könnte, dass die Lücke zwischen vorklinischen Studienergebnissen und klinischer Umsetzung noch immer existiert. Es wurde ein Fragebogen erstellt, anhand dessen die generelle Meinung gegenüber Bone Tissue Engineering und die Effizienz derzeitiger präklinischer Studienmodelle aus sowohl klinischer, als auch wissenschaftlicher Sicht hinterfragt wurde. Hier wurde außerdem auf die Beurteilung der Zufriedenstellung solcher Modelle seitens der Forscher eingegangen. 
Darüber hinaus erfolgte eine systemische Literatursuche auf der Online-Plattform “Pubmed” mit dem Ziel Studien der letzten zehn Jahre über präklinische orthotopische Tiermodelle in Bone Tissue Engineering zusammenzufassen und die verschiedenen Studiendesigns zu evaluieren. Der Fokus lag dabei auf der Beschreibung der Tiermodelle bezüglich Tierart, Geschlecht, Alter und Defektdesign. Ergebnisse der Literatursuche wurden anschließend evaluiert und mit den Antworten aus dem Fragebogen verglichen und diskutiert. 
Es hat sich anhand des Fragebogens gezeigt, dass sowohl Wissenschaftler, als auch Chirurgen positiv gestimmt sind, was die zukünftige Anwendung von Bone Tissue Engineering in den Kliniken betrifft. Jedoch beurteilten die meisten Teilnehmer des Fragebogens die präklinischen Tiermodelle zwar als relevant und gut entwickelt, deren Ergebnisse als klinisch allerdings nicht anwendbar. Dabei fiel die Einschätzung präklinischer Forschung mit Tiermodellen unter den Chirurgen etwas optimistischer aus als unter den Forschern. Die Evaluierung der Studien aus dem Fragebogens und der Literatursuche zeigte jedoch auch, dass die darin beschriebenen Tiermodelle einen eher uneinheitlichen Studienaufbau aufweisen. Tatsächlich stellt die Etablierung eines fundierten Studiendesigns im Anbetracht der zahlreichen Möglichkeiten eine immense Herausforderung dar. Die Festlegung eines Versuchsaufbaus hängt dabei von der Wahl der Tierart, dessen Geschlecht und Alter, des chirurgischen Ablaufs, sowie der technischen und zeitlichen Beobachtungsmöglichkeit ab. Es stellte sich heraus, dass für viele Studien eine diesbezüglich notwendige Standardisierung kaum existiert und dadurch Studienergebnisse entstehen, die schwer reproduzierbar sind und somit den Ansprüchen einer klinischen Umsetzung nicht gerecht werden können. Hinzu kommen außerdem die noch immer bestehenden Wissenslücken in Bezug auf Knochenheilung beeinflussende Faktoren wie Vaskularisation und Abläufe des Immunsystems. 
Abschließend lässt sich sagen, dass die durchgeführte Evaluierung von Studien mit präklinischen Tiermodellen eine fehlende Standardisierung derzeit existierender Studiendesigns darlegt und eine klinische Umsetzung der daraus resultierenden Studienergebnissen somit noch nicht möglich ist. Auch wenn die Teilnehmer des Fragebogens den Bedarf an neuen, klinisch anerkannten Methoden für Knochenaufbauten nahelegten und eine generell positive Einstellung gegenüber dem potentiellen Gebrauch von Bone Tissue Engineering Konstrukte in den Kliniken zeigten, ist die Ablösung von autologem Knochen durch solch neuartige Designs nicht realisierbar, solange die Reproduzierbarkeit der Daten aus präklinischen Tiermodellstudien fehlt. Zusammen mit wegweisenden Richtlinien und fundiertem Wissen über grundliegende Mechanismen im Knochenheilungsprozess, sollte sie die Basis eines jeden Studienaufbaus mit präklinischen Tiermodellen darstellen, um schließlich zu den Ergebnissen zu gelangen, die es für eine klinische Umsetzung von Bone Tissue Engineering bedarf.
KW  - bone
KW  - tissue
KW  - engineering
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-207593
ER  - 
TY  - THES
A1  - Yang, Tao
T1  - Functional insights into the role of a bacterial virulence factor and a host factor in Neisseria gonorrhoeae infection
T1  - Funktionelle Einblicke in die Rolle eines bakteriellen Virulenzfaktors und eines Wirtsfaktors bei der Infektion mit Neisseria gonorrhoeae
N2  - Neisseria gonorrhoeae (GC) is a human specific pathogenic bacterium. Currently, N. gonorrhoeae developed resistance to virtually all the available antibiotics used for treatment. N. gonorrhoeae starts infection by colonizing the cell surface, followed by invasion of the host cell, intracellular persistence, transcytosis and exit into the subepithelial space. Subepithelial bacteria can reach the bloodstream and disseminate to other tissues causing systemic infections, which leads to serious conditions such as arthritis and pneumonia. A number of studies have well established the host-pathogen interactions during the initial adherence and invasion steps. However, the mechanism of intracellular survival and traversal is poorly understood so far. Hence, identification of novel bacterial virulence factors and host factors involved in the host-pathogen interaction is a crucial step in understanding disease development and uncovering novel therapeutic approaches. Besides, most of the previous studies about N. gonorrhoeae were performed in the conventional cell culture. Although they have provided insights into host-pathogen interactions, much information about the native infection microenvironment, such as cell polarization and barrier function, is still missing. 
This work focused on determining the function of novel bacterial virulence factor NGFG_01605 and host factor (FLCN) in gonococcal infection. NGFG_01605 was identified by Tn5 transposon library screening. It is a putative U32 protease. Unlike other proteins in this family, it is not secreted and has no ex vivo protease activity. NGFG_01605 knockout decreases gonococcal survival in the epithelial cell. 3D models based on T84 cell was developed for the bacterial transmigration assay. NGFG_01605 knockout does not affect gonococcal transmigration. 
The novel host factor FLCN was identified by shRNA library screening in search for factors that affected gonococcal adherence and/or internalization. We discovered that FLCN did not affect N. gonorrhoeae adherence and invasion but was essential for bacterial survival. Since programmed cell death is a host defence mechanism against intracellular pathogens, we further explored apoptosis and autophagy upon gonococcal infection and determined that FLCN did not affect apoptosis but inhibited autophagy. Moreover, we found that FLCN inhibited the expression of E-cadherin. Knockdown of E- cadherin decreased the autophagy flux and supported N. gonorrhoeae survival. Both non-polarized and polarized cells are present in the cervix, and additionally, E-cadherin represents different polarization properties on these different cells. Therefore, we established 3-D models to better understand the functions of FLCN. We discovered that FLCN was critical for N. gonorrhoeae survival in the 3-D environment as well, but not through inhibiting autophagy. Furthermore, FLCN inhibits the E-cadherin expression and disturbs its polarization in the 3-D models. Since N. gonorrhoeae can cross the epithelial cell barriers through both cell-cell junctions and transcellular migration, we further explored the roles FLCN and E-cadherin played in transmigration. FLCN delayed N. gonorrhoeae transmigration, whereas the knockdown of E-cadherin increased N. gonorrhoeae transmigration. 
In summary, we revealed roles of the NGFG_01605 and FLCN-E-cadherin axis play in N. gonorrhoeae infection, particularly in relation to intracellular survival and transmigration. This is also the first study that connects FLCN and human-specific pathogen infection.
N2  - Neisseria gonorrhoeae (GC) ist ein humanpathogenes Bakterium. Gegen jedes kommerziell erhältliche Antibiotikum konnten bereits Resistenzen entdeckt werden. Die Infektion von Neisserien startet mit der Kolonisierung der Zelloberfläche, gefolgt von der Invasion in die Zelle, intrazellulärer Persistenz, Transzytose und Verlassen des subepithelen Raums. Subepithele Bakterien können den Blutfluss erreichen und sich somit auf andere Gewebe verbreiten und dadurch schwerwiegende Erkrankungen wie Arthritis und Lungenentzündungen verursachen. Zahlreiche Studien haben die Interaktion zwischen Wirtszelle und Pathogen zwischen Adhärenz und Invasion gut charakterisiert. Allerdings ist der Mechanismus des intrazellulären Überlebens und der Transmigration weitestgehend unbekannt. Um neue therapeutische Ansätze zu definieren ist es deshalb wichtig weitere bakterielle und zelluläre Faktoren verantwortlich für Interaktionen zwischen Wirt und Pathogen zu identifizieren.
Außerdem wurden Studien über N. gonorrhoeae bisher in konventioneller Zellkultur durchgeführt. Auch wenn diese weitere Einsichten in Wirt-Pathogen Interaktionen geben, ist viel Information in der nativen Infektionsumgebung, wie Zellpolarisierung oder Barrierefunktionen, bisher nicht bekannt.

Diese Arbeit fokussiert sich auf die Bestimmung eines neuen bakteriellen Virulenzfaktors, NGFG_01605, und Wirtsfaktoren (FLCN) in der Infektion von Gonokokken. NGFG_01605 wurde über Screening einer Transposonsammlung identifiziert und ist eine vermeintliche U32 Protease. Im Gegensatz zu anderen Proteinen dieser Familie, wird diese Protease nicht sekretiert und hat keine ex vivo Proteaseaktivität. Der Knockout von NGFG_01605 vermindert die Überlebensrate von Gonokokken in Epithelzellen. 3D-Modelle basierend auf T84-Zellen wurden für die Analyse der bakteriellen Transmigration entwickelt. Der Knockout von NGFG_01605 hat keinen Einfluss auf die Transmigration.

Bei der Suche neuer Wirtsfaktoren, die für die Adhärenz und/oder Internalisierung wichtig sind, wurde FLCN durch ein Screening einer shRNA Sammlung entdeckt. Wir konnten zeigen, dass dieser Faktor zwar nicht für die Adhärenz oder Invasion von N. gonorrhoeae, aber für das Überleben der Bakterien in der Wirtszelle essenziell ist. Da der programmierte Zelltod ein typischer Abwehrmechanismus gegen intrazelluläre Bakterien ist, haben wir Apoptose und Autophagie weiter untersucht und konnten zeigen, dass FLCN zwar keinen Effekt auf Apoptose hat, aber Autophagie inhibiert.
Außerdem konnten wir zeigen, dass FLCN die Expression von E-cadherin inhibiert. Auch der Knockdown von E-cadherin verringerte Autophagie und erhöhte das Überleben von N. gonorrhoeae. Im Gebärmutterhals sind sowohl polarisierte als auch nicht-polarisierte Zellen präsent. E-cadherin hat zudem unterschiedliche Einflüsse auf diese unterschiedlichen Zellen. Aus diesem Grund haben wir ein 3D-Modell entwickelt, um die Funktionen von FLCN besser zu verstehen. Wir entdeckten, dass FLCN zwar auch im 3D Modell wichtig für das Überleben ist, aber nicht durch Inhibition von Autophagie. Außerdem inhibiert FLCN die Expression und Verteilung von E-cadherin in 3D-Modellen. Da N. gonorrhoeae die Epithelzellbarierre durch sowohl Zell-Zell-Kontakte als auch transzelluläre Migration überwinden kann, untersuchten wir daraufhin die Rollen von FLCN und E-cadherin in der transzellulären Migration. Diese wird durch FLCN verspätet und durch Knockdown von E-cadherin erhöht.

Zusammengefasst, haben wir die Rolle von NGFG_01605 und den Zusammenhang von FLCN und E-cadherin während der Infektion von N. gonorrhoeae untersucht. Unser Fokus war hierbei das intrazelluläre Überleben sowie zelluläre Transmigration. Diese Arbeit ist die Erste, die FLCN und humanpathogenspezifische Infektion miteinander in Verbindung bringt.
KW  - Folliculin
KW  - autophagy
KW  - polarized epithelium
KW  - protease
KW  - Gonococcal invasion
KW  - autophagocytose
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-208959
ER  - 
TY  - INPR
A1  - Wohlgemuth, Matthias
A1  - Mitric, Roland
T1  - Excitation energy transport in DNA modelled by multi-chromophoric field-induced surface hopping
T2  - Physical Chemistry Chemical Physics
N2  - Absorption of ultraviolet light is known as a major source of carcinogenic mutations of DNA. The underlying processes of excitation energy dissipation are yet not fully understood. In this work we provide a new and generally applicable route for studying the excitation energy transport in multi-chromophoric complexes at an atomistic level. The surface-hopping approach in the frame of the extended Frenkel exciton model combined with QM/MM techniques allowed us to simulate the photodynamics of the alternating (dAdT)10 : (dAdT)10 double-stranded DNA. In accordance with recent experiments, we find that the excited state decay is multiexponential, involving a long and a short component which are due to two distinct mechanisms: formation of long-lived delocalized excitonic and charge transfer states vs. ultrafast decaying localized states resembling those of the bare nucleobases. Our simulations explain all stages of the ultrafast photodynamics including initial photoexcitation, dynamical evolution out of the Franck-Condon region, excimer formation and nonradiative relaxation to the ground state.
KW  - Photodynamics
KW  - DNA
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-209467
ET  - submitted version
ER  - 
TY  - THES
A1  - Klein, Thomas
T1  - Establishing an in vitro disease model for Fabry Disease using patient specific induced pluripotent stem cell-derived sensory neurons
T1  - Etablierung eines in vitro Krankheitsmodells für M. Fabry mittels patienteneigener sensibler Neurone, generiert über induzierte pluripotente Stammzellen
N2  - Fabry disease (FD) is an X-linked lysosomal storage disorder caused by deficiency of the α-galactosidase A (GLA), leading to intracellular accumulations of globotriaosylceramide (Gb3). Acral burning pain, which can be triggered by heat, fever or physical activity is an early hallmark of FD and greatly reduces patients’ quality of life. The pathophysiology of FD pain is unknown and research is hindered by the limited in vivo availability of suitable human biomaterial. To overcome this obstacle, we generated induced pluripotent stem cells (iPSC) from one female and two male patients with a differing pain phenotype, and developed a refined differentiation protocol for sensory neurons to increase reliability and survival of these neurons, serving as an in vitro disease model. Neurons were characterized for the correct neuronal subtype using immunocytochemistry, gene expression analysis, and for their functionality using electrophysiological measurements. 
iPSC and sensory neurons from the male patients showed Gb3 accumulations mimicking the disease phenotype, whereas no Gb3 depositions were detected in sensory neurons derived from the female cell line, likely caused by a skewed X-chromosomal inactivation in favor of healthy GLA. Using super-resolution imaging techniques we showed that Gb3 is localized in neuronal lysosomes of male patients and in a first experiment using dSTORM microscopy we were able to visualize the neuronal membrane in great detail. To test our disease model, we treated the neurons with enzyme replacement therapy (ERT) and analyzed its effect on the cellular Gb3 load, which was reduced in the male FD-lines, compared to non-treated cells. We also identified time-dependent differences of Gb3 accumulations, of which some seemed to be resistant to ERT. We also used confocal Ca2+ imaging to investigate spontaneous neuronal network activity, but analysis of the dataset proofed to be difficult, nonetheless showing a high potential for further investigations. We revealed that neurons from a patient with pain pain are more easily excitable, compared to cells from a patient without pain and a healthy control. 
We provide evidence for the potential of patient-specific iPSC to generate a neuronal in vitro disease model, showing the typical molecular FD phenotype, responding to treatment, and pointing towards underlying electrophysiological mechanisms causing different pain phenotypes. Our sensory neurons are suitable for state-of-the-art microscopy techniques, opening new possibilities for an in-depth analysis of cellular changes, caused by pathological Gb3 accumulations. Taken together, our system can easily be used to investigate the effect of the different mutations of GLA on a functional and a molecular level in affected neurons.
N2  - Morbus Fabry (M. Fabry) ist eine X-chromosomal vererbte lysosomale Speichererkrankung, die durch die Defizienz von α-Galaktosidase A (GLA) verursacht wird. Diese führt zu pathologischen Ablagerungen von Globotriaosylceramid (Gb3) in Zellen. Akraler, brennender Schmerz, der durch Hitze, Fieber oder Sport ausgelöst werden kann, ist ein frühes Krankheitsmerkmal und reduziert die Lebensqualität der Patienten deutlich. Die Pathophysiologie von M. Fabry ist unklar und die Forschung ist durch die limitierte Verfügbarkeit von humanem Biomaterial nur eingeschränkt möglich. Um dieses Problem zu bewältigen haben wir induzierte pluripotente Stammzellen (iPSC) von einer weiblichen Patientin und zwei männlichen Patienten mit unterschiedlichen Schmerzphänotypen generiert. Mit diesen Zellen konnten wir ein verbessertes Protokoll zur Herstellung sensibler Neurone etablieren um diese als in vitro Krankheitsmodell zu nutzen. Die Neurone wurden mittels Immunozytochemie, Genexpressionsanalyse und elektrophysiologischer Messungen auf die korrekte Zellidentität und deren Funktionalität getestet.
Gb3 Ablagerungen konnten als Krankheitsmerkmal in iPSC und sensiblen Neuronen der männlichen Patienten, nicht aber in Zellen der weiblichen Patientin und der Kontrollperson nachgewiesen werden. Das Fehlen von pathologischen Ablagerungen in Zellen der weiblichen Betroffenen ist vermutlich auf eine verschobene X-Inaktivierung zu Gunsten des gesunden GLA zurückzuführen. Nichtsdestotrotz ist es uns durch die Nutzung hochauflösender Mikroskopietechniken gelungen, bei männlichen Patienten Gb3 in neuronalen Lysosomen nachzuweisen und die Membran in großem Detail abzubilden. Die Behandlung der Neurone mit der Enzymersatztherapie (ERT) als Nachweis für die Funktionalität des Krankheitsmodells führte zu einer Reduktion der Gb3 Ablagerungen bei männlichen Zellen, im Vergleich zu unbehandelten Zellen. Zudem konnten wir unterschiedliche Arten von Gb3 Akkumulationen identifizieren, von denen einige scheinbar behandlungsresistent sind. Erste Versuche mit Ca2+ Imaging zeigten spontane, neuronale Netzwerkaktivität, die noch weitergehend analysiert werden müssen. Mittels Patch-Clamp Analysen konnten wir zeigen, dass Neurone des Patienten mit Schmerzen leichter erregbar sind als Zellen des Patienten ohne Schmerzen, was einen Hinweis auf die mögliche Beteiligung gestörter Ionenkanäle gibt.
Wir konnten zeigen, dass patientenspezifische iPSC geeignet sind um ein neuronales in vitro Krankheitsmodell zu erstellen. Dieses Modell zeigt den typischen molekularen Phänotypen des M. Fabry, spricht auf ERT an und liefert erste Hinweise auf pathologische elektrophysiologische Krankheitsursachen, die zu unterschiedlichen Schmerzphänotypen führen können. Zelluläre Veränderungen durch Gb3 Ablagerungen können nun mittels neuester Mikroskopietechniken anhand der von uns generierten Neurone untersucht werden um ein besseres Verständnis der zugrundeliegenden Pathophysiologie zu bekommen. Zusammenfassend bietet unser System eine neue Möglichkeit den neuronalen Einfluss verschiedener GLA Mutationen auf einer funktionellen und molekularen Ebene zu untersuchen und die Diversität von M. Fabry aufzuschlüsseln.
KW  - Induzierte pluripotente Stammzelle
KW  - iPSC
KW  - disease model
KW  - fabry disease
KW  - pain
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199705
ER  - 
TY  - THES
A1  - Klepsch, Maximilian Andreas
T1  - Small RNA-binding complexes in Chlamydia trachomatis identified by Next-Generation Sequencing techniques
T1  - Identifizierung von kleinen RNA-bindenden Komplexen in Chlamydia trachomatis mittels Hochdurchsatz- Sequenziertechniken
N2  - Chlamydia infect millions worldwide and cause infertility and blinding trachoma. Chlamydia trachomatis (C. trachomatis) is an obligate intracellular gram-negative pathogen with a significantly reduced genome. This bacterium shares a unique biphasic lifecycle in which it alternates between the infectious, metabolically inert elementary bodies (EB) and the non-infections, metabolically active replicative reticular bodies (RB).
One of the challenges of working with Chlamydia is its difficult genetic accessibility. In the present work, the high-throughput method TagRNA-seq was used to differentially label transcriptional start sites (TSS) and processing sites (PSS) to gain new insights into the transcriptional landscape of C. trachomatis in a coverage that has never been achieved before. Altogether, 679 TSSs and 1067 PSSs were detected indicating its high transcriptional activity and the need for transcriptional regulation. Furthermore, the analysis of the data revealed potentially new non-coding ribonucleic acids (ncRNA) and a map of transcriptional processing events. Using the upstream sequences, the previously identified σ66 binding motif was detected.
In addition, Grad-seq for C. trachomatis was established to obtain a global interactome of the RNAs and proteins of this intracellular organism. The Grad-Seq data suggest that many of the newly annotated RNAs from the TagRNA-seq approach are present in complexes. Although Chlamydia lack the known RNA-binding proteins (RBPs), e.g. Hfq and ProQ, observations in this work reveal the presence of a previously unknown RBP. 
Interestingly, in the gradient analysis it was found that the σ66 factor forms a complex with the RNA polymerase (RNAP). On the other hand, the σ28 factor is unbound. This is in line with results from previous studies showing that most of the genes are under control of σ66. The ncRNA IhtA is known to function via direct base pairing to its target RNA of HctB, and by doing so is influencing the chromatin condensation in Chlamydia. This study confirmed that lhtA is in no complex. On the other hand, the ncRNA ctrR0332 was found to interact with the SNF2 protein ctl0077, a putative helicase. Both molecules co-sedimented in the gradient and were intact after an aptamer-based RNA pull-down. The SWI2/SNF2 class of proteins are nucleosome remodeling complexes. The prokaryotic RapA from E. coli functions as transcription regulator by stimulating the RNAP recycling. This view might imply that the small ncRNA (sRNA) ctrR0332 is part of the global regulation network in C. trachomatis controlling the transition between EBs and RBs via interaction with the SNF2 protein ctl0077.
The present work is the first study describing a global interactome of RNAs and proteins in C. trachomatis providing the basis for future interaction studies in the field of this pathogen.
N2  - Chlamydien verursachen jährlich Millionen Neuinfektionen weltweit und können zu Spätschäden wie Unfruchtbarkeit und Erblindung führen. Chlamydien sind obligat intrazelluläre, gram-negative Pathogene mit einem stark reduzierten Genom. Sie besitzen einen einzigartigen biphasischen Lebenszyklus, bei dem der Erreger zwischen den metabolisch inaktiven, infektiösen Elementarkörperchen (EBs) und den nicht infektiösen, metabolisch aktiven und replikativen Retikularkörperchen (RBs) alterniert.
Eine Problemantik beim Arbeiten mit Chlamydien ist die Schwierigkeit der gezielten genetischen Manipulation des Pathogens. 
In der vorliegenden Arbeit wurde die Hochdurchsatz-Sequenziermethode TagRNA-Seq genutzt, um die transkriptionelle Organisation von Chlamydia trachomatis (C. trachomatis) zu analysieren und besser zu verstehen. Transkriptionelle Start Stellen (TSS) und Prozessierungsstellen (PSS) werden dabei unterschiedlich markiert, sodass eine zuverlässigere und genauere Auflösung erreicht wird als bisher durch in anderen Studien verwendete Methoden. Insgesamt konnten so 679 TSSs und 1067 PSSs detektiert werden. Es konnte gezeigt werden, dass das Transkriptom von C. trachomatis weitaus aktiver ist als bisher angenommen und eine Regulation auf transkriptioneller Ebene bedarf. Die Methode erlaubte zudem die Identifizierung von potenziell neuen nicht-kodierende RNAs sowie die Kartierung von transkriptionellen Prozessierungsereignissen. Unter Verwendung der 5’-upstreamliegenden Sequenzen konnte außerdem das in anderen Bakterien bereits bekannte σ66-Bindemotiv detektiert werden.
In der vorliegenden Arbeit wurde zudem die Methode Grad-Seq in C. trachomatis etabliert, um ein globales Interaktom für RNAs (engl. ribonucleic acid) und Proteine des intrazellulären Organismus zu erstellen. 
Für viele der im TagRNA-Seq Ansatz identifizierten und neu annotierten RNAs konnte so eine Komplexbildung beobachtet werden. Dies deutet auf das Vorhandensein eines bislang unbekanntes RNA-Bindeprotein (RBP) hin, da Chlamydien keines der bekannten RBPs, z.B. Hfq oder ProQ, besitzen.
Die Gradienten-Analyse ergab, dass der σ66-Faktor in einem Komplex mit der RNA-Polymerase (RNAP) vorliegt und dass der σ28-Faktor ungebunden ist. Diese Beobachtung entspricht den Ergebnissen vorheriger Studien, die zeigten das die meisten Gene durch σ66 kontrolliert werden. Die Daten bestätigen außerdem, dass IhtA, eine ncRNA (engl. non-coding ribonucleic acid), die über direkte Basenpaarbindung mit ihrem Ziel-RNA von hctB interagiert, nicht in einem Komplex vorliegt. Für die ncRNA ctrR0332 hingegen konnte das SNF2-Protein ctl0077 als Interaktionspartner identifiziert werden. Beide Moleküle co-sedimentieren im Gradienten und konnten mittels eines Aptamer-basierenden RNA Pull-Downs in intakter Form isoliert werden. Die Klasse der SWI2/SNF2-Proteine gehört zu den Nukleosomen-Remodeling-Komplexen. In Prokaryoten konnte für das in E. coli vorkommende RapA, welches ebenfalls zu den SWI2/SNF2-Proteinen zählt, die Funktion eines Transkriptionsregulators nachgewiesen werden, indem die RNAP-Wiederverwertung stimuliert wird. Dies könnte bedeuten, dass die ncRNA ctrR0332 ebenfalls Teil eines globalen Regulationsnetzwerks ist, welches durch Interaktion mit dem SNF2-Protein ctl0077 die Transition zwischen dem RB- und EB-Stadium reguliert. 
In der vorliegenden Arbeit konnte erstmals ein globales Interaktom von RNAs und Proteinen in C. trachomatis erstellt werden, welches als Grundlage für zukünftige Interaktionsstudien des Pathogens genutzt werden kann.
KW  - High throughput screening
KW  - Small RNA
KW  - Chlamydia trachomatis
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199741
ER  - 
TY  - INPR
A1  - Humeniuk, Alexander
A1  - Bužančić, Margarita
A1  - Hoche, Joscha
A1  - Cerezo, Javier
A1  - Mitric, Roland
A1  - Santoro, Fabrizio
A1  - Bonačić-Koutecky, Vlasta
T1  - Predicting fluorescence quantum yields for molecules in solution: A critical assessment of the harmonic approximation and the choice of the lineshape function
T2  - The Journal of Chemical Physics
N2  - For the rational design of new fluorophores, reliable predictions of fluorescence quantum yields from first principles would be of great help. However, efficient computational approaches for predicting transition rates usually assume that the vibrational structure is harmonic. While the harmonic approximation has been used successfully to predict vibrationally resolved spectra and radiative rates, its reliability for non-radiative rates is much more questionable. Since non-adiabatic transitions convert large amounts of electronic energy into vibrational energy, the highly excited final vibrational states deviate greatly from harmonic oscillator eigenfunctions. We employ a time-dependent formalism to compute radiative and non-radiative rates for transitions and study the dependence on model parameters. For several coumarin dyes we compare different adiabatic and vertical harmonic models (AS, ASF, AH, VG, VGF, VH), in order to dissect the
importance of displacements, frequency changes and Duschinsky rotations. In addition we analyze the effect of different broadening functions (Gaussian, Lorentzian or Voigt). Moreover, to assess the qualitative influence of anharmonicity on the internal conversion rate, we develop a simplified anharmonic model. We adress the reliability of these models considering the potential errors introduced by the harmonic approximation and the phenomenological width of the broadening function.
KW  - fluorescence quantum yield
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199305
UR  - https://doi.org/10.1063/1.5143212
N1  - Accepted Manuscript.
N1  - This article may be downloaded for personal use only. Any other use requires prior permission of the author and AIP Publishing. This article appeared in A. Humeniuk et al. J. Chem. Phys. 152, 054107 (2020); https://doi.org/10.1063/1.5143212 and may be found at https://doi.org/10.1063/1.5143212.
ER  - 
TY  - THES
A1  - Maimari, Theopisti
T1  - The influence of N-terminal peptides of G-protein coupled receptor kinase (GRK) 2, 3 and 5 on β-adrenergic signaling
T1  - Der Einfluss von N-terminalen Peptiden der G-Protein gekoppelten Rezeptorkinasen (GRK) 2, 3 und 5 in der β-adrenergen Signaltransduktion
N2  - G protein coupled receptor kinases (GRK) phosphorylate and thereby desensitize G protein coupled receptors (GPCR) including β-adrenergic receptors (βAR), which are critical regulators of cardiac function. We identified the Raf kinase inhibitor protein (RKIP) as an endogenous inhibitor of GRK2 that leads to increased cardiac contractility via βAR activation. RKIP binds to the N-terminus (aa1-185) of GRK2, which is important for the GRK2/receptor interaction. Thereby it interferes with the GRK2/receptor interaction without interference with cytosolic GRK2 target activation. In this project, the RKIP/GRK interface was investigated to develop strategies that simulate the effects of RKIP on βAR. 
RKIP binding to different isoforms of GRK expressed in the heart was analyzed by protein interaction assays using full-length and N-termini of GRK2, GRK3 and GRK5: 1-53, 54-185 and 1-185. Co-immunoprecipitation (Co-IPs) and pull-down assays revealed that RKIP binds to the peptides of GRK2 and GRK3 but not to the ones of GRK5, which suggests the existence of several binding sites of RKIP within the N-termini of GRK2 and GRK3. To analyze whether the peptides of GRK2 and GRK3 are able to simulate the RKIP mediated interference of the GRK2/receptor interaction, we analyzed the β2-AR phosphorylation in the absence and presence of the peptides. Interestingly, N-termini (aa1-185) of GRK2 and GRK3 reduced β2AR phosphorylation to a comparable extent as RKIP. In line with reduced receptor phosphorylation, the peptides also reduced isoproterenol-stimulated receptor internalization as shown by [3H] CGP-12177 radioligand binding assay and fluorescence microscopy compared to control cells. Subsequently, these peptides increased downstream signaling of β2AR, i.e. the phosphorylation of the PKA substrate phosducin. In an attempt to elucidate the mechanism behind the observed effects, Co-IPs were performed in order to investigate whether the peptides bind directly to the β2-AR and block its phosphorylation by GRK2. Indeed, GRK2 1-185 and GRK3 1-185 could bind the receptor, suggesting that this way GRK2 is prevented from inhibiting the receptor. To investigate the physiological effect of GRK2 1-185, GRK3 1-185 and GRK5 1-185, their effect on neonatal mouse cardiomyocyte contractility and hypertrophy was analyzed. After long-term isoproterenol stimulation, in the presence of GRK2 1 185 and GRK3 1-185 the cross-sectional area of the cardiomyocytes showed no significant increase in comparison to the unstimulated control cells. In addition, upon isoproterenol stimulation, GRK2 1-185 and GRK3 1-185 increased the beat rate in cardiomyocytes, mimicking RKIP while the base impedance, an indicator of viability, remained stable.
The N-termini (1-185) of GRK2 and GRK3 simulated RKIP’s function and had a significant influence on β2AR phosphorylation, on its downstream signaling and internalization, could bind β2-AR, increased beat rate and did not significantly induce hypertrophy, suggesting that they may serve as a model for the generation of new and more specific targeting strategies for GRK mediated receptor regulation.
N2  - G-Protein gekoppelte Rezeptorkinasen (GRK) phosphorylieren und desensitisieren G-Protein gekoppelte Rezeptoren (GPCR), einschließlich β-adrenerge Rezeptoren (βAR), welche wichtige Regulatoren der Herzfunktion sind. Raf Kinase Inhibitor Protein (RKIP) ist ein endogener Inhibitor von GRK2, der zur Aktivierung von βAR führt und dadurch zur Steigerung der Herzkontraktilität. RKIP bindet N-terminal (1-185) an GRK2; der GRK2 N-Terminus ist wichtig für die GRK2/Rezeptor Interaktion. Durch diese Bindung wird GRK2 inhibiert und derer Interaktion mit den Rezeptor gestört, allerdings bleiben die zytosolische GRK2 Substrate unbeeinflusst. In diesem Projekt wurde die Interaktion zwischen RKIP und GRK untersucht, um neue Targeting Strategien zu entwickeln, die die positiven Effekte von RKIP auf βAR Signalwege simulieren.
Die Bindung von RKIP an verschiedene, im Herzen lokalisierte GRK-Isoformen wurde über protein interaction assays untersucht:  mit GRK2, GRK3 und GRK5 und mit deren N-terminalen Peptiden  1-53, 54-185, 1-185. Die Co-Immunopräzipitationen (Co-IPs) und die pull-down Versuche haben gezeigt, dass RKIP sowohl GRK2 und GRK3 als auch deren N-Termini bindet, GRK5 und dessen N-termini hingegen nicht. Daraus lässt sich schlussfolgern, dass sich mehrere RKIP Bindungsstellen an dem GRK2 N-Terminus befinden. Um zu analysieren, ob die GRK2- und GRK3-Peptide eine ähnliche Wirkung wie RKIP auf die Interaktion von GRK2 und Rezeptor aufweisen, wurde die Rezeptorphosphorylierung ermittelt. Es konnte gezeigt werden, dass GRK2 1-185 und GRK3 1-185 die Phosphorylierung des βAR reduzieren können. Radioligandbindungsassays mit [3H] CGP-12177 und Fluoreszenzmikroskopie zeigten zudem, dass GRK2 1-185 und GRK3 1-185 auch die Internalisierungsrate des βAR senken können. Anschließend hatten GRK2 1-185 und GRK3 1-185 einen positiven Effekt auf einem βAR downstream Signalmolekül. Hierbei handelte es sich um die Phosphorylierung von Phosducin, was ein PKA-Substrat ist. Um die Wirkungsweise der N-termini zu erläutern, wurde untersucht, ob diese direkt den β2AR binden und somit die GRK2 vermittelte Phosphorylierung hindern. Interessanterweise konnte gezeigt werden, dass GRK2 1-185 und GRK3  1- 185 den β2AR binden und dementsprechend einen Einfluss auf die Phosphorylierung haben. Des Weiteren, wurden die Effekte der Peptide auf  Kontraktilität und Hypertrophie in neonatalen Mauskardiomyozyten analysiert. In Anwesenheit von GRK2 1-185 und GRK3 1-185 war die Querschnittsfläche der Mauskardiomyozyten nicht signifikant größer im Vergleich zu den unstimulierten Kontrollzellen.  Außerdem wurde eine signifikante Erhöhung der Kontraktilität in den Mauskardiomyozyten mit GRK2 1-185 und GRK3 1-185 beobachtet.  
Insgesamt, konnten GRK2 1-185 und GRK3 1-185 RKIPs Funktion simulieren: sie hatten einen signifikanten Effekt auf β2AR-Phosphorylierung, Internalisierung und downstream Signaling. Zudem konnten sie die Kontraktilität erhöhen und hatten keinen Einfluss auf Hypertrophie. Somit könnten sie als Prototyp für die Entwicklung neuer Targeting Strategien für die GRK-vermittelte Rezeptor Regulation, genutzt werden.
KW  - G protein-coupled receptor kinase
KW  - Raf kinase inhibitor protein
KW  - Inhibition
KW  - Heart failure
KW  - Peptides
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199322
ER  - 
TY  - THES
A1  - Kurz, Andreas
T1  - Correlative live and fixed cell superresolution microscopy
T1  - Korrelative hochauflösende Mikroskopie an lebenden und fixierten Zellen
N2  - Over the last decade life sciences have made an enormous leap forward. The development of complex analytical instruments, in particular in fluorescence microscopy, has played a decisive role in this. Scientist can now rely on a wide range of imaging techniques that offer different advantages in terms of optical resolution, recording speed or living cell compatibility. With the help of these modern microscopy techniques, multi-protein complexes can be resolved, membrane receptors can be counted, cellular pathways analysed or the internalisation of receptors can be tracked. However, there is currently no universal technique for comprehensive experiment execution that includes dynamic process capture and super resolution imaging on the same target object. In this work, I built a microscope that combines two complementary imaging techniques and enables correlative experiments in living and fixed cells. With an image scanning based laser spot confocal microscope, fast dynamics in several colors with low photodamage of the cells can be recorded. This novel system also has an improved resolution of 170 nm and was thoroughly characterized in this work. The complementary technique is based on single molecule localization microscopy, which can achieve a structural resolution down to 20-30 nm. Furthermore I implemented a microfluidic pump that allows direct interaction with the sample placed on the microscope. Numerous processes such as living cell staining, living cell fixation, immunostaining and buffer exchange can be observed and performed directly on the same cell. Thus, dynamic processes of a cell can be frozen and the structures of interest can be stained and analysed with high-resolution microscopy. Furthermore, I have equipped the detection path of the single molecule technique with an adaptive optical element. With the help of a deformable mirror, imaging functions can be shaped and information on the 3D position of the individual molecules can be extracted.
N2  - Im letzten Jahrzehnt hat der Bereich der Lebenswissenschaften einen enormen Sprung nach vorne gemacht. Maßgeblich dafür waren die Entwicklung von komplexen Analysegeräten insbesondere in der Fluoreszenz Mikroskopie. Die Anwender können nun auf eine Vielzahl von Bildgebungstechniken zurückgreifen die unterschiedliche Vorzüge hinsichtlich optischer Auflösung, Aufnahmegeschwindigkeit oder Lebend Zell Kompatibilität bieten. Mithilfe dieser modernen Mikroskopietechniken lassen sich beispielsweise Multiproteinkomplexe auflösen, Membranrezeptoren zählen, zelluläre Signalwege analysieren oder die Internalisierung von Rezeptoren verfolgen. Für eine umfassende Experimentdurchführung, die Erfassung dynamischer Prozesse sowie superhochauflösende Bildgebung an ein und demselben Zielobjekt beinhalten, gibt es derzeit keine einheitliche Technik. In dieser Arbeit habe ich ein Mikroskop aufgebaut, das zwei komplementäre Bildgebungstechniken vereint und korrelative Experimente von lebend zu fixierten Zellen ermöglicht. Mit einem Image Scanning basierten Konfokal Mikroskop können schnelle Dynamiken in mehreren Farben mit geringer Photoschädigung der Zellen aufgenommen werden. Dieses neuartige System weist zudem eine Auflösungsverbesserung von 170 nm auf und wurde im Rahmen der Arbeit ausführlich charakterisiert. Die komplementäre Technik basiert auf der Einzel-Molekül Lokalisations Mikroskopie, mit der sich eine strukturelle Auflösung von bis zu 20 nm erreichen lässt. Desweiteren habe ich eine Mikrofluidpumpe implementiert, die eine direkte Interaktion mit der auf dem Mikroskop platzierten Probe erlaubt. Zahlreiche Prozesse wie Lebend-Zell Färbung, Lebend-Zell Fixierung, Immuno-Färbung und Puffertausch können damit direkt an der gleichen Zelle beobachtet und durchgeführt werden. So können dynamische Prozesse einer Zelle sozusagen eingefroren werden und die Strukturen von Interesse gefärbt und mit höchstauflösender Mikroskopie analysiert werden. Desweiteren habe ich den Detektionspfad der Einzel-Molekül Technik mit einem adaptiven optischen Element ausgestattet. Mithilfe eines deformierbaren Spiegels lässt sich so Abbildungsfunktion formen und Information zur 3D Position der einzelnen Moleküle gewinnen.
KW  - Einzelmolekülmikroskopie
KW  - Adaptive Optik
KW  - Image-Scanning Microscope
KW  - Correlative microscopy
KW  - Adaptive Optics
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199455
ER  - 
TY  - THES
A1  - Hagmann, Hanns Antony
T1  - The impact of the CRISPR/Cas system on the interaction of Neisseria meningitidis with human host cells
T1  - Der Einfluss des CRISPR/Cas-Systems auf die Interaktion von Neisseria meningitidis mit menschlichen Wirtszellen
N2  - Neisseria meningitidis, a commensal β-proteobacterium residing exclusively in the human nasopharynx, is a leading cause of sepsis and epidemic meningitis worldwide. While comparative genome analysis was able to define hyperinvasive lineages that are responsible for most of the cases of invasive meningococcal disease (IMD), the genetic basis of their virulence remains unclear. Recent studies demonstrate that the type II C CRISPR/Cas system of meningococci is associated with carriage and less invasive lineages. CRISPR/Cas, an adaptive defence system against foreign DNA, was shown to be involved in gene regulation in Francisella novicida. This study shows that knockout strains of N. meningitidis lacking the Cas9 protein are impaired in the adhesion to human nasopharyngeal cells in a strain-dependant manner, which constitutes a central step in the pathogenesis of IMD. Consequently, this study indicates that the meningococcal CRISPR/Cas system fulfils functions beyond the defence of foreign DNA and is involved in the regulation of meningococcal virulence.
N2  - Neisseria meningitidis, ein ß-Proteobakterium, welches als Kommensale ausschließlich den humanen Nasopharynx besiedelt, ist ein weltweit führender Verursacher von Sepsis und epidemischer Meningitis. Auch wenn mittels vergleichender Genomanalysen hyperinvasive Stämme definiert werden konnten, welche für die meisten Fälle von invasiven Meningokokkenerkrankungen verantwortlich sind, bleibt die genetische Grundlage ihrer Virulenz ungeklärt. In vorangegangenen Studien konnte gezeigt werden, dass das Typ II-C CRISPR/Cas-System der Meningokokken assoziiert ist mit Trägerstämmen. CRISPR/Cas ist ein adaptives Verteidigungssystem der Bakterien gegen fremde DNA, das darüber hinaus Aufgaben in der Genregulation von Francisella novicida erfüllt. Diese Arbeit zeigt, dass knockout Stämme von N. meningitidis, denen das Cas9-Protein fehlt, in Abhängigkeit von ihrem genetischen Hintergrund die Fähigkeit verlieren an Zellen des menschlichen Nasopharynx zu adhärieren. Die Adhäsion an den Wirtszellen stellt einen zentralen
Schritt in der Pathogenese der invasiven Meningokokkenerkrankungen dar. Die Ergebnisse dieser Arbeit deuten darauf hin, dass das CRISPR/Cas-System in Meningokokken neben seiner Funktion als bakterielles Immunsystem an der Regulation der bakteriellen Virulenz beteiligt sein könnte.
KW  - CRISPR/Cas-Methode
KW  - Neisseria meningitidis
KW  - Bacteria-Host Cell Interaction
KW  - Regulation of Gene Expression
KW  - Cas9
KW  - Type II-C CRISPR/Cas
KW  - Adhesion and Invasion
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199490
ER  - 
TY  - THES
A1  - Reichenbach, Juliane Renate
T1  - Paternal age effects on sperm DNA methylation and its impact on the next generation
T1  - Der väterliche Alterseffekt auf das Spermienmethylom und seine Auswirkungen auf die nächste Generation
N2  - The effect of late parenthood on the offspring´s physical and mental health status has recently become an increasingly important topic of discussion. Studies on neurodevelopmental disorders in children of older parents (Naserbakht et al., 2011) outline the negative consequences of aging fathers as unpredictable compared to the better-understood unfavorable maternal influences (Cedars  et al. 2015). This may be due to the fact that lifelong production of male gametes becomes more susceptible to error, not only for somatic mutations. Non-genomic mechanisms such as epigenetic methylation also alter DNA dynamically throughout life (Jones et al., 2015) and influence the aging human sperm DNA (Jenkins et al., 2014). These methylation changes may be transmitted to the next generation via epigenetic inheritance mechanisms (Milekic et al., 2015), which may negatively impact the sensitive epigenetic regulation of cell differentiation in the embryonic period (Curley et al., 2011; Spiers et al., 2015). Accordingly, Nardone et al. (2014) reported several hypomethylated regions in autistic patients, illustrating potential epigenetic influences on the multifactorial pathogenesis of neuropsychiatric disorders. In the present study, the methylation status of five gene regions in the sperm DNA of males of different ages was analyzed by two techniques - pyrosequencing and deep bisulfite sequencing. Two gene regions, FOXK1 and DMPK, showed a highly significant age-related methylation loss and FOXK1 a reduced methylation variation at the level of single alleles. In addition, the examined gene region of FOXK1 showed significant methylation changes in the fetal cord blood DNA of the respective offspring of the sperm donor. This fact suggests a transfer of age-related methylation loss to the next generation. Interestingly, a methylation analysis at the level of single alleles showed that the methylation loss was inherited exclusively by the father. FOXK1 is a transcription factor that plays an important role in the epigenetic regulation of the cell cycle during embryonic neuronal development (Huang et al., 2004; Wijchers et al., 2006). For this reason, the methylation status of FOXK1 in the blood of autistic patients and an age- and sex-matched control group was investigated. While both groups showed age-associated FOXK1 methylation loss, a faster dynamics of methylation change was observed in the autistic group. Although further studies are needed to uncover inheritance mechanisms of epigenetic information, the present results show an evident influence of age-related methylation changes on offspring. When advising future fathers, it is important to consider how the paternal epigenome is altered by aging and can have a negative impact on the developing embryo.
N2  - Die Auswirkungen einer späten Elternschaft auf die körperliche und geistige Gesundheit der Nachkommen wurde in letzter Zeit zunehmend diskutiert. Studien zu neurologischen Entwicklungsstörungen bei Kindern älterer Eltern (Naserbakht et al. 2011) skizzieren insbesondere die negativen Folgen alternder Väter (Cedars et al. 2015). Dies ist möglicherweise darauf zurückzuführen, dass die lebenslange Produktion männlicher Gameten im Laufe des Lebens nicht nur für somatische Mutationen fehleranfälliger wird. Auch nicht-genomische Mechanismen wie die epigenetische Methylierung verändert die DNA im Laufe des Lebens dynamisch (Jones et al. 2015) und beeinflussen die alternde menschliche Spermien-DNA (Jenkins et al. 2014). Möglicherweise werden diese Methylierungsveränderungen über epigenetische Vererbungsmechanismen an die nächste Generation übertragen (Milekic et al. 2015), was sich negativ auf die empfindliche epigenetische Regulation der Zelldifferenzierung in der Embryonalperiode auswirken kann (Curley et al. 2011; Spiers et al. 2015). Mögliche epigenetische Einflüsse auf die multifaktorielle Pathogenese neuropsychiatrischer Erkrankungen veranschaulichend, zeigten Nardone et al. (2014) mehrere hypomethylierte Regionen bei autistischen Patienten auf. In der vorliegenden Arbeit wurde der Methylierungsstatus von fünf Genregionen in der Spermien-DNA von Männern unterschiedlichen Alters durch zwei Techniken analysiert – das Pyrosequencing und das Deep Bisulfite Sequencing. Zwei Genregionen, FOXK1 und DMPK, zeigten einen hochgradig signifikanten altersbedingten Methylierungsverlust und FOXK1 auf der Ebene einzelner Allele eine verringerte Methylierungsvariation. Darüber hinaus zeigte die untersuchte Genregion von FOXK1 signifikante Methylierungsveränderungen in der Nabelschnurblut-DNA der jeweiligen Nachkommen der Samenspender. Diese Tatsache spricht für eine Übertragung des altersbedingten Methylierungsverlustes auf die nächste Generation.
Anhand einer Methylierungsanalyse auf der Ebene einzelner Allele konnte interessanterweise gezeigt werden, dass der Methylierungsverlust ausschließlich durch den Vater vererbt wurde. FOXK1 ist ein Transkriptionsfaktor, der eine wichtige Rolle bei der epigenetischen Regulation des Zellzyklus während der embryonalen neuronalen Entwicklung spielt (Huang et al. 2004; Wijchers et al. 2006). Aus diesem Grund wurde der Methylierungsstatus von FOXK1 im Blut autistischer Patienten und einer alters- und geschlechtsentsprechenden Kontrollgruppe untersucht. Während beide Gruppen einen altersassoziierten FOXK1-Methylierungverlust zeigten, wurde in der autistischen Gruppe eine schnellere Dynamik der Methylierungsänderung beobachtet. Obwohl weitere Studien erforderlich sind, um Vererbungsmechanismen epigenetischer Information aufzudecken, zeigen die vorliegenden Ergebnisse einen offensichtlichen Einfluss altersbedingter Methylierungsveränderungen auf die Nachkommen. Bei der Beratung zukünftiger Väter ist es wichtig zu berücksichtigen, wie das väterliche Epigenom durch das Altern verändert wird und negative Auswirkungen auf den sich entwickelnden Embryo haben kann.
KW  - Epigenetik
KW  - Vater
KW  - Spermium
KW  - Autismus
KW  - Methylierung
KW  - paternal age
KW  - epigenetics
KW  - sperm
KW  - methylation
KW  - reproduction
KW  - autism
KW  - Väterliches Alter
KW  - Epigenetik
KW  - Spermien
KW  - Methylierung
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199805
ER  - 
TY  - JOUR
A1  - Blättner, Sebastian
A1  - Das, Sudip
A1  - Paprotka, Kerstin
A1  - Eilers, Ursula
A1  - Krischke, Markus
A1  - Kretschmer, Dorothee
A1  - Remmele, Christian W.
A1  - Dittrich, Marcus
A1  - Müller, Tobias
A1  - Schuelein-Voelk, Christina
A1  - Hertlein, Tobias
A1  - Mueller, Martin J.
A1  - Huettel, Bruno
A1  - Reinhardt, Richard
A1  - Ohlsen, Knut
A1  - Rudel, Thomas
A1  - Fraunholz, Martin J.
T1  - Staphylococcus aureus Exploits a Non-ribosomal Cyclic Dipeptide to Modulate Survival within Epithelial Cells and Phagocytes
JF  - PLoS Pathogens
N2  - Community-acquired (CA) Staphylococcus aureus cause various diseases even in healthy individuals. Enhanced virulence of CA-strains is partly attributed to increased production of toxins such as phenol-soluble modulins (PSM). The pathogen is internalized efficiently by mammalian host cells and intracellular S. aureus has recently been shown to contribute to disease. Upon internalization, cytotoxic S. aureus strains can disrupt phagosomal membranes and kill host cells in a PSM-dependent manner. However, PSM are not sufficient for these processes. Here we screened for factors required for intracellular S. aureus virulence. We infected escape reporter host cells with strains from an established transposon mutant library and detected phagosomal escape rates using automated microscopy. We thereby, among other factors, identified a non-ribosomal peptide synthetase (NRPS) to be required for efficient phagosomal escape and intracellular survival of S. aureus as well as induction of host cell death. By genetic complementation as well as supplementation with the synthetic NRPS product, the cyclic dipeptide phevalin, wild-type phenotypes were restored. We further demonstrate that the NRPS is contributing to virulence in a mouse pneumonia model. Together, our data illustrate a hitherto unrecognized function of the S. aureus NRPS and its dipeptide product during S. aureus infection.
KW  - cell death
KW  - cytotoxicity
KW  - Staphylococcus aureus
KW  - host cells
KW  - neutrophils
KW  - macrophages
KW  - transposable elements
KW  - epithelial cells
Y1  - 2016
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-180380
VL  - 12
IS  - 9
ER  - 
TY  - INPR
A1  - Titov, Evgenii
A1  - Humeniuk, Alexander
A1  - Mitric, Roland
T1  - Comparison of moving and fixed basis sets for nonadiabatic quantum dynamics at conical intersections
T2  - Chemical Physics
N2  - We assess the performance of two different types of basis sets for nonadiabatic quantum dynamics at conical intersections. The basis sets of both types are generated using Ehrenfest trajectories of nuclear coherent states. These trajectories can either serve as a moving (time-dependent) basis or be employed to sample a fixed (time-independent) basis. We demonstrate on the example of two-state two-dimensional and three-state five-dimensional models that both basis set types can yield highly accurate results for population transfer at intersections, as compared with reference quantum dynamics. The details of wave packet evolutions are discussed for the case of the two-dimensional model. The fixed basis is found to be superior to the moving one in reproducing nonlocal spreading and maintaining correct shape of the wave packet upon time evolution. Moreover, for the models considered, the fixed basis set outperforms the moving one in terms of computational efficiency.
KW  - Nonadiabatic quantum dynamics
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199225
UR  - https://doi.org/10.1016/j.chemphys.2019.110526
N1  - Submitted version
ER  - 
TY  - INPR
A1  - Lindner, Joachim O.
A1  - Sultangaleeva, Karina
A1  - Röhr, Merle I. S.
A1  - Mitric, Roland
T1  - metaFALCON: A program package for automatic sampling of conical intersection seams using multistate metadynamics
T2  - Journal of Chemical Theory and Computation
N2  - The multistate metadynamics for automatic exploration of conical intersection seams and systematic location of minimum energy crossing points in molecular systems and its implementation into the software package metaFALCON is presented. Based on a locally modified energy gap between two Born–Oppenheimer electronic states as a collective variable, multistate metadynamics trajectories are driven toward an intersection point starting from an arbitrary ground state geometry and are subsequently forced to explore the conical intersection seam landscape. For this purpose, an additional collective variable capable of distinguishing structures within the seam needs to be defined and an additional bias is introduced into the off-diagonal elements of an extended (multistate) electronic Hamiltonian. We demonstrate the performance of the algorithm on the examples of the 1,3-butadiene, benzene, and 9H-adenine molecules, where multiple minimum energy crossing points could be systematically located using the Wiener number or Cremer–Pople parameters as collective variables. Finally, with the example of 9H-adenine, we show that the multistate metadynamics potential can be used to obtain a global picture of a conical intersection seam. Our method can be straightforwardly connected with any ab initio or semiempirical electronic structure theory that provides energies and gradients of the respective electronic states and can serve for systematic elucidation of the role of conical intersections in the photophysics and photochemistry of complex molecular systems, thus complementing nonadiabatic dynamics simulations.
KW  - Computational Chemistry
KW  - Metadynamics
KW  - Hydrogen
KW  - Hydrocarbons
KW  - Chemical Structure
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199258
UR  - https://doi.org/10.1021/acs.jctc.9b00029
N1  - This document is the Accepted Manuscript version of a Published Work that appeared in final form in Journal of Chemical Theory and Computation, copyright © American Chemical Society after peer review and technical editing by the publisher. To access the final edited and published work see Journal of Chemical Theory and Computation 2019, 15, 6, 3450-3460. https://doi.org/10.1021/acs.jctc.9b00029.
ER  - 
TY  - JOUR
A1  - Hansmann, T.
A1  - Heinzmann, J.
A1  - Wrenzycki, C.
A1  - Zechner, U.
A1  - Niemann, H.
A1  - Haaf, T.
T1  - Characterization of Differentially Methylated Regions in 3 Bovine Imprinted Genes: A Model for Studying Human Germ-Cell and Embryo Development
JF  - Cytogenetic and Genome Research
N2  - Correct imprinting is crucial for normal fetal and placental development in mammals. Experimental evidence in animal models and epidemiological studies in humans suggest that assisted reproductive technologies (ARTs) can interfere with imprinted gene regulation in gametogenesis and early embryogenesis. Bos taurus is an agriculturally important species in which ARTs are commonly employed. Because this species exhibits a similar preimplantation development and gestation length as humans, it is increasingly being used as a model for human germ-cell and embryo development. However, in contrast to humans and mice, there is relatively little information on bovine imprinted genes. Here, we characterized the bovine intergenic IGF2-H19 imprinting control region (ICR) spanning approximately 3 kb. We identified a 300-bp differentially methylated region (DMR) approximately 6 kb upstream of the H19 promoter, containing a CpG island with CTCF-binding site and high sequence similarity with the human intergenic ICR. Additional differentially methylated CpG islands lie –6 kb to –3 kb upstream of the promoter, however these are less conserved. Both classical bisulfite sequencing and bisulfite pyrosequencing demonstrated complete methylation of the IGF2-H19 ICR in sperm, complete demethylation in parthenogenetic embryos having only the female genome, and differential methylation in placental and somatic tissues. In addition, we established pyrosequencing assays for the previously reported bovine SNRPN and PEG3 DMRs. The observed methylation patterns were consistent with genomic imprinting in all analyzed tissues/cell types. The identified IGF2-H19 ICR and the developed quantitative methylation assays may prove useful for further studies on the relationship between ARTs and imprinting defects in the bovine model.
KW  - bovine
KW  - differentially methylated region
KW  - IGF2-H19
KW  - imprinting control region
Y1  - 2010
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199051
SN  - 1424-8581
SN  - 1424-859X
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 132
IS  - 4
ER  - 
TY  - JOUR
A1  - Kraft, Peter
A1  - Drechsler, Christiane
A1  - Gunreben, Ignaz
A1  - Heuschmann, Peter Ulrich
A1  - Kleinschnitz, Christoph
T1  - Regulation of Blood Coagulation Factors XI and XII in Patients with Acute and Chronic Cerebrovascular Disease: A Case-Control Study
JF  - Cerebrovascular Diseases
N2  - Background: Animal models have implicated an integral role for coagulation factors XI (FXI) and XII (FXII) in thrombus formation and propagation of ischemic stroke (IS). However, it is unknown if these molecules contribute to IS pathophysiology in humans, and might be of use as biomarkers for IS risk and severity. This study aimed to identify predictors of altered FXI and FXII levels and to determine whether there are differences in the levels of these coagulation factors between acute cerebrovascular events and chronic cerebrovascular disease (CCD). Methods: In this case-control study, 116 patients with acute ischemic stroke (AIS) or transitory ischemic attack (TIA), 117 patients with CCD, and 104 healthy volunteers (HVs) were enrolled between 2010 and 2013 at our University hospital. Blood sampling was undertaken once in the CCD and HV groups and on days 0, 1, and 3 after stroke onset in patients with AIS or TIA. Correlations between serum FXI and FXII levels and demographic and clinical parameters were tested by linear regression and analysis of variance. Results: The mean age of AIS/TIA patients was 70 ± 12. Baseline clinical severity measured with NIHSS and Barthel Index was 4.8 ± 6.0 and 74 ± 30, respectively. More than half of the patients had an AIS (58%). FXI levels were significantly correlated with different leukocyte subsets (p < 0.05). In contrast, FXII serum levels showed no significant correlation (p > 0.1). Neither FXI nor FXII levels correlated with CRP (p > 0.2). FXII levels were significantly higher in patients with CCD compared with those with AIS/TIA (mean ± SD 106 ± 26% vs. 97 ± 24%; univariate analysis: p < 0.05); these differences did not reach significance in multivariate analysis adjusted for sex and age. FXI levels did not differ significantly between study groups. Sex and age were significantly associated with FXI and/or FXII levels in patients with AIS/TIA (p < 0.05). In contrast, no statistical significant influence was found for treatment modality (thrombolysis or not), pre-treatment with platelet inhibitors, and severity of stroke. Conclusions: In this study, there was no differential regulation of FXI and FXII levels between disease subtypes but biomarker levels were associated with patient and clinical characteristics. FXI and FXII levels might be no valid biomarker for predicting stroke risk.
KW  - biomarker
KW  - factor XI
KW  - factor XII
KW  - ischemic stroke
KW  - chronic cerebrovascular disease
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199076
SN  - 1015-9770
SN  - 1421-9786
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 38
IS  - 5
ER  - 
TY  - JOUR
A1  - Zahnert, Thomas
A1  - Löwenheim, Hubert
A1  - Beutner, Dirk
A1  - Hagen, Rudolf
A1  - Ernst, Arneborg
A1  - Pau, Hans-Wilhelm
A1  - Zehlicke, Thorsten
A1  - Kühne, Hilke
A1  - Friese, Natascha
A1  - Tropitzsch, Anke
A1  - Lüers, Jan-Christoffer
A1  - Mlynski, Robert
A1  - Todt, Ingo
A1  - Hüttenbrink, Karl-Bernd
T1  - Multicenter Clinical Trial of Vibroplasty Couplers to Treat Mixed/Conductive Hearing Loss: First Results
JF  - Audiology and Neurotology
N2  - Objective: To evaluate the safety and effectiveness of round window (RW), oval window (OW), CliP and Bell couplers for use with an active middle ear implant. Methods: This is a multicenter, long-term, prospective trial with consecutive enrollment, involving 6 university hospitals in Germany. Bone conduction, air conduction, implant-aided warble-tone thresholds and Freiburger monosyllable word recognition scores were compared with unaided preimplantation results in 28 moderate-to-profound hearing-impaired patients after 12 months of follow-up. All patients had previously undergone failed reconstruction surgeries (up to 5 or more). In a subset of patients, additional speech tests at 12 months postoperatively were used to compare the aided with the unaided condition after implantation with the processor switched off. An established quality-of-life questionnaire for hearing aids was used to determine patient satisfaction. Results: Postoperative bone conduction remained stable. Mean functional gain for all couplers was 37 dB HL (RW = 42 dB, OW = 35 dB, Bell = 38 dB, CliP = 27 dB). The mean postoperative Freiburger monosyllable score was 71% at 65 dB SPL. The postimplantation mean SRT<sub>50</sub> (speech reception in quiet for 50% understanding of words in sentences) improved on average by 23 dB over unaided testing and signal-to-noise ratios also improved in all patients. The International Outcome Inventory for Hearing Aids (IOI-HA)quality-of-life questionnaire was scored very positively by all patients. Conclusion: A significant improvement was seen with all couplers, and patients were satisfied with the device at 12 months postoperatively. These results demonstrate that an active implant is an advantage in achieving good hearing benefit in patients with prior failed reconstruction surgery.
KW  - conductive hearing loss
KW  - mixed hearing loss
KW  - vibroplasty
KW  - couplers
KW  - middle ear implant
Y1  - 2016
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199129
SN  - 1420-3030
SN  - 1421-9700
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 21
IS  - 4
ER  - 
TY  - JOUR
A1  - Schwarzmeier, Hanna
A1  - Leehr, Elisabeth Johanna
A1  - Böhnlein, Joscha
A1  - Seeger, Fabian Reinhard
A1  - Roesmann, Kati
A1  - Gathmann, Bettina
A1  - Herrmann, Martin J.
A1  - Siminski, Niklas
A1  - Junghöfer, Markus
A1  - Straube, Thomas
A1  - Grotegerd, Dominik
A1  - Dannlowski, Udo
T1  - Theranostic markers for personalized therapy of spider phobia: Methods of a bicentric external cross‐validation machine learning approach
JF  - International Journal of Methods in Psychiatric Research
N2  - Objectives
Embedded in the Collaborative Research Center “Fear, Anxiety, Anxiety Disorders” (CRC‐TRR58), this bicentric clinical study aims at identifying biobehavioral markers of treatment (non‐)response by applying machine learning methodology with an external cross‐validation protocol. We hypothesize that a priori prediction of treatment (non‐)response is possible in a second, independent sample based on multimodal markers.

Methods
One‐session virtual reality exposure treatment (VRET) with patients with spider phobia was conducted on two sites. Clinical, neuroimaging, and genetic data were assessed at baseline, post‐treatment and after 6 months. The primary and secondary outcomes defining treatment response are as follows: 30% reduction regarding the individual score in the Spider Phobia Questionnaire and 50% reduction regarding the individual distance in the behavioral avoidance test.

Results
N = 204 patients have been included (n = 100 in Würzburg, n = 104 in Münster). Sample characteristics for both sites are comparable.

Discussion
This study will offer cross‐validated theranostic markers for predicting the individual success of exposure‐based therapy. Findings will support clinical decision‐making on personalized therapy, bridge the gap between basic and clinical research, and bring stratified therapy into reach. The study is registered at ClinicalTrials.gov (ID: NCT03208400).
KW  - machine learning
KW  - spider phobia
KW  - theranostic markers
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-213430
VL  - 29
IS  - 2
ER  - 
TY  - THES
A1  - Brandt, Gregor A.
T1  - Gait Initiation in Parkinson's Disease: The Interplay of Dopamine and Postural Control
T1  - Der erste Schritt bei M. Parkinson: Der Zusammenhang zwischen Dopamin und posturaler Kontrolle
N2  - Deterioration of gait and alterations of physiological gait initiation contribute significantly to the burden of disease in Parkinson's disease. This paper systematically investigates disease-specific alterations during the postural phases of gait initiation and demonstrates the influence of dopaminergic networks by assessing levodopa mediated improvements in motor performance and correlation of motor behavior with loss of striatal and cortical dopaminergic neurons. Particular attention is given to known confounders such as initial stance and anthropometrics.
N2  - Störungen des Gangbildes und Veränderungen der physiologischen Bewegungsabläufe während des ersten Schrittes tragen einen signifikanten Teil zur Krankheitslast der Parkinsonerkrankung bei. Diese Veröffentlichung untersucht systematisch die krankheitsspezifischen Veränderungen der posturalen Phase des ersten Schrittes und demonstriert den Einfluss dopaminerger Netzwerke durch Untersuchungen Levodopa-induzierter Verbesserungen des Bewegungsablaufs und Korrelationen des Bewegungsverhaltens mit dem Verlust striataler und kortikaler dopaminerger Neuronen. Besondere Sorgfalt wurde bekannten modifizierenden Faktoren wie initaler Standbreite und anthropometrischen Größen zu Teil.
KW  - Parkinson-Krankheit
KW  - Parkinson's Disease
KW  - Gait initiation
KW  - Motor Control
KW  - Dopamine
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-214636
ER  - 
TY  - THES
A1  - Vollmuth, Nadine
T1  - Role of the proto-oncogene c-Myc in the development of Chlamydia trachomatis
T1  - Die Rolle des proto-onkogenes c-Myc in der Entwicklung von Chlamydia trachomatis
N2  - Chlamydia trachomatis, an obligate intracellular human pathogen, is the world’s leading cause of infection related blindness and the most common, bacterial sexually transmitted disease. In order to establish an optimal replicative niche, the pathogen extensively interferes with the physiology of the host cell. Chlamydia switches in its complex developmental cycle between the infectious non-replicative elementary bodies (EBs) and the non-infectious replicative reticulate bodies (RBs). The transformation to RBs, shortly after entering a host cell, is a crucial process in infection to start chlamydial replication. Currently it is unknown how the transition from EBs to RBs is initiated. In this thesis, we could show that, in an axenic media approach, L glutamine uptake by the pathogen is crucial to initiate the EB to RB transition. L-glutamine is converted to amino acids which are used by the bacteria to synthesize peptidoglycan. Peptidoglycan inturn is believed to function in separating dividing Chlamydia. The glutamine metabolism is reprogrammed in infected cells in a c-Myc-dependent manner, in order to accomplish the increased requirement for L-glutamine. Upon a chlamydial infection, the proto-oncogene c-Myc gets upregulated to promote host cell glutaminolysis via glutaminase GLS1 and the L-glutamine transporter SLC1A5/ASCT2. Interference with this metabolic reprogramming leads to limited growth of C. trachomatis. Besides the active infection, Chlamydia can persist over a long period of time within the host cell whereby chronic and recurrent infections establish. C. trachomatis acquire a persistent state during an immune attack in response to elevated interferon-γ (IFN-γ) levels. It has been shown that IFN-γ activates the catabolic depletion of L-tryptophan via indoleamine 2,3-dioxygenase (IDO), resulting in the formation of non-infectious atypical chlamydial forms. In this thesis, we could show that IFN-γ depletes the key metabolic regulator c-Myc, which has been demonstrated to be a prerequisite for chlamydial development and growth, in a STAT1-dependent manner. Moreover, metabolic analyses revealed that the pathogen de routs the host cell TCA cycle to enrich pyrimidine biosynthesis. Supplementing pyrimidines or a-ketoglutarate helps the bacteria to partially overcome the persistent state. Together, the results indicate a central role of c-Myc induced host glutamine metabolism reprogramming and L-glutamine for the development of C. trachomatis, which may provide a basis for anti-infectious strategies. Furthermore, they challenge the longstanding hypothesis of L-tryptophan shortage as the sole reason for IFN-γ induced persistence and suggest a pivotal role of c-Myc in the control of the C. trachomatis dormancy.
N2  - Chlamydia trachomatis, ein obligat intrazellul¨ares humanes Pathogen, ist weltweit fu¨hrende Ursache fu¨r infektionsbedingte Erblindung und die h¨aufigste, bakterielle sexuell u¨bertragbare Krankheit. Um eine optimale Replikationsnische zu etablieren, interagiert das Pathogen in tensiv mit der Physiologie der Wirtszelle. Chlamydien wechseln in ihrem komplexen Entwick lungszyklus zwischen den infekti¨osen nicht replizierenden Elementark¨orperchen (EBs) und den nicht infekti¨osen replizierenden Retikulark¨orperchen (RBs), und diese Umwandlung in RBs kurz nach dem Eintritt in die Wirtszelle ist ein entscheidender Prozess in der Infektion, um die Replikation des Bakteriums einzuleiten. Derzeit ist noch nicht bekannt, wodurch diese Transformation von EBs zu RBs eingeleitet wird. In dieser Arbeit konnte gezeigt werden, dass bei einer zellfreien Kultivierung des Pathogens die Aufnahme von Glutamin durch den Erreger entscheidend ist, um den ¨Ubergang von EB zu RB zu initiieren. Vor kurzem wurde Peptidoglykan in den Septen von sich replizierenden Chlamydien nachgewiesen. Fu¨r die Syn these des Peptidoglykans nutzen die Bakterien das aufgenommene Glutamin. Der Glutamin metabolismus wird in infizierten Zellen c-Myc abh¨angig umprogrammiert, um den erh¨ohten Bedarf an Glutamin zu bew¨altigen. Bei einer Chlamydieninfektion wird das Proto-Onkogen c-Myc zur F¨orderung der Glutaminolyse der Wirtszelle u¨ber die Glutaminase GLS1 und den Glutamin Transporter SLC1A5/ASCT2 hochreguliert. Ein Eingreifen in diese metabolische Neuprogrammierung fu¨hrt zu einem reduzierten Wachstum von C. trachomatis. Neben der aktiven Infektion k¨onnen Chlamydien u¨ber einen sehr langen Zeitraum in der Wirtszelle persistieren, wodurch es zur Etablierung von chronischen und wiederkehrenden Infektionen kommt. C. trachomatis verf¨allt bei einem Immunangriff in Persistenz, wenn sie auf das freigesetzte Interferon-γ treffen. Es ist bekannt, dass Interferon-γ den Katabolismus von Tryptophan mittels indoleamine 2,3-dioxygenase (IDO) aktiviert, was zur Bildung von nicht infekti¨osen atypischen Chlamydienformen fu¨hrt. In dieser Arbeit konnte gezeigt werden, dass Interferon-γ den zentralen Stoffwechselregulator c-Myc, der sich fu¨r die Entwicklung und das Wachstum von Chlamydien als essentiell erwiesen hat, in Abh¨angigkeit von STAT1 herunter reguliert. Daru¨ber hinaus zeigte die Analyse des Metabolismus, dass das Pathogen den TCA Zyklus der Wirtszelle umleitet, um die Pyrimidinbiosynthese zu unterstu¨tzen. Die Zugabe von Pyrimidinen oder α-Ketoglutarat hilft den Bakterien den Status der Persistenz teilweise zu u¨berwinden. Zusammengenommen deuten die Ergebnisse auf eine zentrale Rolle der c-Myc induzierten Umprogrammierung des Glutaminmetabolismus und des Glutamins selbst fu¨r die Entwicklung von C. trachomatis hin. Diese Befunde k¨onnten eine Basis fu¨r Strategien gegen eine Infektion darstellen. Weiterhin stellen sie die seit langem bestehende Hypothese des Trypotphanmangels als alleiniger Grund fu¨r die von Interferon-γ induzierte Persistenz in Frage und legen eine zentrale Rolle von c-Myc bei der Kontrolle der C. trachomatis Dormanz nahe.
KW  - Chlamydia trachomatis
KW  - Persistence
KW  - trachomatis
KW  - chlamydia
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-203655
ER  - 
TY  - JOUR
A1  - Kotseva, Kornelia
A1  - De Backer, Guy
A1  - De Bacquer, Dirk
A1  - Rydén, Lars
A1  - Hoes, Arno
A1  - Grobbee, Diederick
A1  - Maggioni, Aldo
A1  - Marques-Vidal, Pedro
A1  - Jennings, Catriona
A1  - Abreu, Ana
A1  - Aguiar, Carlos
A1  - Badariene, Jolita
A1  - Bruthans, Jan
A1  - Castro Conde, Almudena
A1  - Cifkova, Renata
A1  - Crowley, Jim
A1  - Davletov, Kairat
A1  - Deckers, Jaap
A1  - De Smedt, Delphine
A1  - De Sutter, Johan
A1  - Dilic, Mirza
A1  - Dolzhenko, Marina
A1  - Dzerve, Vilnis
A1  - Erglis, Andrejs
A1  - Fras, Zlatko
A1  - Gaita, Dan
A1  - Gotcheva, Nina
A1  - Heuschmann, Peter
A1  - Hasan-Ali, Hosam
A1  - Jankowski, Piotr
A1  - Lalic, Nebojsa
A1  - Lehto, Seppo
A1  - Lovic, Dragan
A1  - Mancas, Silvia
A1  - Mellbin, Linda
A1  - Milicic, Davor
A1  - Mirrakhimov, Erkin
A1  - Oganov, Rafael
A1  - Pogosova, Nana
A1  - Reiner, Zeljko
A1  - Stöerk, Stefan
A1  - Tokgözoğlu, Lâle
A1  - Tsioufis, Costas
A1  - Vulic, Dusko
A1  - Wood, David
T1  - Lifestyle and impact on cardiovascular risk factor control in coronary patients across 27 countries: Results from the European Society of Cardiology ESC-EORP EUROASPIRE V registry
JF  - European Journal of Preventive Cardiology
N2  - Aims
The aim of this study was to determine whether the Joint European Societies guidelines on secondary cardiovascular prevention are followed in everyday practice.
	
Design
A cross-sectional ESC-EORP survey (EUROASPIRE V) at 131 centres in 81 regions in 27 countries.
	
Methods
Patients (<80 years old) with verified coronary artery events or interventions were interviewed and examined ≥6 months later.
	
Results
A total of 8261 patients (females 26%) were interviewed. Nineteen per cent smoked and 55% of them were persistent smokers, 38% were obese (body mass index ≥30 kg/m2), 59% were centrally obese (waist circumference: men ≥102 cm; women ≥88 cm) while 66% were physically active <30 min 5 times/week. Forty-two per cent had a blood pressure ≥140/90 mmHg (≥140/85 if diabetic), 71% had low-density lipoprotein cholesterol ≥1.8 mmol/L (≥70 mg/dL) and 29% reported having diabetes. Cardioprotective medication was: anti-platelets 93%, beta-blockers 81%, angiotensin-converting enzyme inhibitors/angiotensin receptor blockers 75% and statins 80%.
	
Conclusion
A large majority of coronary patients have unhealthy lifestyles in terms of smoking, diet and sedentary behaviour, which adversely impacts major cardiovascular risk factors. A majority did not achieve their blood pressure, low-density lipoprotein cholesterol and glucose targets. Cardiovascular prevention requires modern preventive cardiology programmes delivered by interdisciplinary teams of healthcare professionals addressing all aspects of lifestyle and risk factor management, in order to reduce the risk of recurrent cardiovascular events.
KW  - EUROASPIRE
KW  - lifestyle
KW  - cardiovascular risk factors
KW  - secondary prevention
KW  - guidelines
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-205526
SN  - 2047-4873
SN  - 2047-4881
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 26
IS  - 8
ER  - 
TY  - CHAP
A1  - Schmitz, Barbara
T1  - King and God : conceptions of rule and God in 3 Maccabees
T2  - Figures who shape scriptures, scriptures that shape figures
N2  - In 3 Maccabees, kingship as a form of rule is addressed on two levels: On the political level the question about a good king is addressed against the background of Hellenistic understandings of kingship, using the example of Ptolemy IV Philopator. This king is portrayed at the beginning of 3 Maccabees as a successful, positive, Hellenistic ruler, but one whose good rule goes off the rails. This analysis of the ideal of Hellenistic rule (cf. 3 Macc. 3:12-29; 6:24-28; 7:1-9) is then taken to a theological level: the God of Israel is portrayed as the true good king, the Soter who saves his people in their time of greatest trial (6:29, 32; 7:16). By these means the many divine epithets that are a striking feature of 3 Maccabees are incorporated into the narrative (cf. 2:2-3). Thereby 3 Maccabees not only thematises the conflict with a Hellenistic king who exploits his power in diverse ways but also focuses in a concentrated way the notion of a good (Hellenistic) king into the notion of God as king and ruler.
KW  - Maccabees
KW  - Hellenistic kingship
KW  - Xenophon
KW  - Cyropaidia
KW  - Isocrates
KW  - God in 3 Macc
Y1  - 2018
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-205149
ER  - 
TY  - CHAP
A1  - Schmitz, Barbara
T1  - Aspects of Worship in the Letter of Aristeas
T2  - Various Aspects of Worship in Deuterocanonical and Cognate Literature
N2  - Although the Letter of Aristeas mentions the translation of the Jewish nomos into Greek, it is striking that worship is not a fundamental theme of this writing. Nevertheless, six passages present acts of worship, which recount worship from different perspectives: Aristeas prays to God and explains his “Greek” idea of worship (Let. Aris. 17), whereas in Let. Aris. 132-140 the high priest explains the Jewish concept of worship. Sacrifices and prayers at the temple in Jerusalem for the Ptolemaic royal house are told in Let. Aris. 45, while at the Ptolemaic court in Alexandria one of the Jewish scholars prays at the beginning of the symposium (Let. Aris. 184-186). Then the daily prayer of the Jewish scholars are recounted in Let. Aris. 305-306 and finally the Ptolemaic king performs a proskynesis before the law at the end of the letter and thereby accepts the translation (Let. Aris. 317).
KW  - Aristeas
KW  - Letter of Aristeas
KW  - worship
KW  - proskynesis
Y1  - 2017
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-205150
VL  - 2016/2017
ER  - 
TY  - JOUR
A1  - Figueiredo, Ludmilla
A1  - Krauss, Jochen
A1  - Steffan-Dewenter, Ingolf
A1  - Cabral, Juliano Sarmento
T1  - Understanding extinction debts: spatio-temporal scales, mechanisms and a roadmap for future research
JF  - Ecography
N2  - Extinction debt refers to delayed species extinctions expected as a consequence of ecosystem perturbation. Quantifying such extinctions and investigating long‐term consequences of perturbations has proven challenging, because perturbations are not isolated and occur across various spatial and temporal scales, from local habitat losses to global warming. Additionally, the relative importance of eco‐evolutionary processes varies across scales, because levels of ecological organization, i.e. individuals, (meta)populations and (meta)communities, respond hierarchically to perturbations. To summarize our current knowledge of the scales and mechanisms influencing extinction debts, we reviewed recent empirical, theoretical and methodological studies addressing either the spatio–temporal scales of extinction debts or the eco‐evolutionary mechanisms delaying extinctions. Extinction debts were detected across a range of ecosystems and taxonomic groups, with estimates ranging from 9 to 90% of current species richness. The duration over which debts have been sustained varies from 5 to 570 yr, and projections of the total period required to settle a debt can extend to 1000 yr. Reported causes of delayed extinctions are 1) life‐history traits that prolong individual survival, and 2) population and metapopulation dynamics that maintain populations under deteriorated conditions. Other potential factors that may extend survival time such as microevolutionary dynamics, or delayed extinctions of interaction partners, have rarely been analyzed. Therefore, we propose a roadmap for future research with three key avenues: 1) the microevolutionary dynamics of extinction processes, 2) the disjunctive loss of interacting species and 3) the impact of multiple regimes of perturbation on the payment of debts. For their ability to integrate processes occurring at different levels of ecological organization, we highlight mechanistic simulation models as tools to address these knowledge gaps and to deepen our understanding of extinction dynamics.
KW  - Anthropocene
KW  - biotic interaction
KW  - extinction dynamics
KW  - mechanistic modelling
KW  - time lag
KW  - transient dynamics
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-204859
VL  - 42
IS  - 12
ER  - 
TY  - JOUR
A1  - Ataee, Mohammad Sadegh
A1  - Maghsoudi, Yasser
A1  - Latifi, Hooman
A1  - Fadaie, Farhad
T1  - Improving estimation accuracy of growing stock by multi-frequency SAR and multi-spectral data over Iran's heterogeneously-structured broadleaf Hyrcanian forests
JF  - Forests
N2  - Via providing various ecosystem services, the old-growth Hyrcanian forests play a crucial role in the environment and anthropogenic aspects of Iran and beyond. The amount of growing stock volume (GSV) is a forest biophysical parameter with great importance in issues like economy, environmental protection, and adaptation to climate change. Thus, accurate and unbiased estimation of GSV is also crucial to be pursued across the Hyrcanian. Our goal was to investigate the potential of ALOS-2 and Sentinel-1's polarimetric features in combination with Sentinel-2 multi-spectral features for the GSV estimation in a portion of heterogeneously-structured and mountainous Hyrcanian forests. We used five different kernels by the support vector regression (nu-SVR) for the GSV estimation. Because each kernel differently models the parameters, we separately selected features for each kernel by a binary genetic algorithm (GA). We simultaneously optimized R\(^2\) and RMSE in a suggested GA fitness function. We calculated R\(^2\), RMSE to evaluate the models. We additionally calculated the standard deviation of validation metrics to estimate the model's stability. Also for models over-fitting or under-fitting analysis, we used mean difference (MD) index. The results suggested the use of polynomial kernel as the final model. Despite multiple methodical challenges raised from the composition and structure of the study site, we conclude that the combined use of polarimetric features (both dual and full) with spectral bands and indices can improve the GSV estimation over mixed broadleaf forests. This was partially supported by the use of proposed evaluation criterion within the GA, which helped to avoid the curse of dimensionality for the applied SVR and lowest over estimation or under estimation.
KW  - GSV
KW  - nu SVR
KW  - uneven-aged mountainous
KW  - polarimetery
KW  - multi-spectral
KW  - optimization
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-197212
SN  - 1999-4907
VL  - 10
IS  - 8
ER  - 
TY  - INPR
A1  - Lisinetskaya, Polina G.
A1  - Mitric, Roland
T1  - Collective Response in DNA-Stabilized Silver Cluster Assemblies from First-Principles Simulations
T2  - The Journal of Physical Chemistry Letters
N2  - We investigate fluorescence resonant energy transfer and concurrent electron dynamics in a pair of DNA-stabilized silver clusters. For this purpose we introduce a methodology for the simulation of collective optoelectronic properties of coupled molecular aggregates starting from first-principles quantum chemistry, which can be further applied to a broad range of coupled molecular systems to study their electro-optical response. Our simulations reveal the existence of low-energy coupled excitonic states, which enable ultrafast energy transport between subunits, and give insight into the origin of the fluorescence signal in coupled DNA-stabilized silver clusters, which have been recently experimentally detected. Hence, we demonstrate the possibility of constructing ultrasmall energy transmission lines and optical converters based on these hybrid molecular systems.
KW  - Metal clusters
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-198729
UR  - https://doi.org/10.1021/acs.jpclett.9b03136
N1  - This document is the unedited Author’s version of a  Submitted Work that was subsequently accepted for  publication in Journal of Physical Chemistry A, copyright © American Chemical Society after peer review. To access the final edited and published work see The Journal of Physical Chemistry Letters 2019, 10, 24, 7884-7889. https://doi.org/10.1021/acs.jpclett.9b03136.
ER  - 
TY  - INPR
A1  - Röder, Anja
A1  - Petersen, Jens
A1  - Issler, Kevin
A1  - Fischer, Ingo
A1  - Mitric, Roland
A1  - Poisson, Lionel
T1  - Exploring the Excited-State Dynamics of Hydrocarbon Radicals, Biradicals and Carbenes using Time-Resolved Photoelectron Spectroscopy and Field-Induced Surface Hopping Simulations
T2  - The Journal of Physical Chemistry A
N2  - Reactive hydrocarbon molecules like radicals, biradicals and carbenes are not only key players in combustion processes and interstellar and atmospheric chemistry, but some of them are also important intermediates in organic synthesis. These systems typically possess many low-lying, strongly coupled electronic states. After light absorption, this leads to rich photodynamics characterized by a complex interplay of nuclear and electronic motion, which is still not comprehensively understood and not easy to investigate both experimentally and theoretically. In order to elucidate trends and contribute to a more general understanding, we here review our recent work on excited-state dynamics of open-shell hydrocarbon species using time-resolved photoelectron spectroscopy and field-induced surface hopping simulations, and report new results on the excited-state dynamics of the tropyl and the 1-methylallyl radical. The different dynamics are compared, and the difficulties and future directions of time-resolved photoelectron spectroscopy and excited state dynamics simulations of open-shell hydrocarbon molecules are discussed.
KW  - Excited state dynamics
KW  - Hydrocarbon radicals
KW  - time-resolved photoelectron spectroscopy
KW  - field-induced surface hopping
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-198734
UR  - https://doi.org/10.1021/acs.jpca.9b06346
N1  - This document is the unedited Author’s version of a  Submitted Work that was subsequently accepted for  publication in Journal of Physical Chemistry A, copyright © American Chemical Society after peer review. To access the final edited and published work see Journal of Physical Chemistry A 2019, 123, 50, 10643-10662. https://doi.org/10.1021/acs.jpca.9b06346.
ER  - 
TY  - INPR
A1  - Titov, Evgenii
A1  - Humeniuk, Alexander
A1  - Mitric, Roland
T1  - Exciton localization in excited-state dynamics of a tetracene trimer: A surface hopping LC-TDDFTB study
T2  - Physical Chemistry Chemical Physics
N2  - Excitons in the molecular aggregates of chromophores are key participants in important processes such as photosynthesis or the functioning of organic photovoltaic devices. Therefore, the exploration of exciton dynamics is crucial. Here we report on exciton localization during excited-state dynamics of the recently synthesized tetracene trimer [Liu et al., Org. Lett., 2017, 19, 580]. We employ the surface hopping approach to nonadiabatic molecular dynamics in conjunction with the long-range corrected time-dependent density functional tight binding (LC-TDDFTB) method [Humeniuk and Mitrić, Comput. Phys. Commun., 2017, 221, 174]. Utilizing a set of descriptors based on the transition density matrix, we perform comprehensive analysis of exciton dynamics. The obtained results reveal an ultrafast exciton localization to a single tetracene unit of the trimer during excited-state dynamics, along with exciton transfer between units.
KW  - Exciton dynamics
Y1  - 2018
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-198680
UR  - https://doi.org/10.1039/C8CP05240A
N1  - Accepted Manuscript
ER  - 
TY  - INPR
A1  - Auerhammer, Nina
A1  - Schulz, Alexander
A1  - Schmiedel, Alexander
A1  - Holzapfel, Marco
A1  - Hoche, Joscha
A1  - Röhr, Merle I. S.
A1  - Mitric, Roland
A1  - Lambert, Christoph
T1  - Dynamic exciton localisation in a pyrene-BODIPY-pyrene dye conjugate
T2  - Physical Chemistry Chemical Physics
N2  - The photophysics of a molecular triad consisting of a BODIPY dye and two pyrene chromophores attached in 2-position are investigated by steady state and fs-time resolved transient absorption spectroscopy as well as by field induced surface hopping (FISH) simulations. While the steady state measurements indicate moderate chromophore interactions within the triad, the time resolved measurements show upon pyrene excitation a delocalised excited state which localises onto the BODIPY chromophore with a time constant of 0.12 ps. This could either be interpreted as an internal conversion process within the excitonically coupled chromophores or as an energy transfer from the pyrenes to the BODIPY dye. The analysis of FISH-trajectories reveals an oscillatory behaviour where the excitation hops between the pyrene units and the BODIPY dye several times until finally they become localised on the BODIPY chromophore within 100 fs. This is accompanied by an ultrafast nonradiative relaxation within the excitonic manifold mediated by the nonadiabatic coupling. Averaging over an ensemble of trajectories allowed us to simulate the electronic state population dynamics and determine the time constants for the nonradiative transitions that mediate the ultrafast energy transfer and exciton localisation on BODIPY.
KW  - Exciton localization dynamics
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-198718
UR  - https://doi.org/10.1039/C9CP00908F
N1  - Accepted manuscript
ER  - 
TY  - JOUR
A1  - Bauer, Boris
A1  - Goebeler, Matthias
A1  - Weissbrich, Benedikt
A1  - Kerstan, Andreas
T1  - Kerinokeratosis papulosa of childhood
JF  - Dermatology
N2  - Background: Kerinokeratosis papulosa (KP) is considered an extremely rare genodermatosis presenting usually as waxy papules on the trunk in childhood. 
Objective: To describe and analyze the clinical, histological and potential etiopathological aspects of KP. 
Methods: The dermatoscopic features of a new case of KP of childhood are investigated. The presence of human papillomavirus (HPV) DNA in lesional skin was studied by polymerase chain reaction. Furthermore, all cases of KP of childhood reported so far were reviewed. 
Results: As a diagnostic tool, we describe for the first time a dermatoscopic feature, namely a cribriform pattern of KP, in an 11-year-old boy. In addition, we detected HPV (type 57) in his KP lesions. 
Conclusions: Dermatoscopic examination might be a useful tool to distinguish KP from other skin lesions, e.g. common warts. The detection of HPV type 57 might hint to an etiological role of HPV for KP.
KW  - Waxy papulosis of childhood
KW  - Human papillomavirus
KW  - EVER1
KW  - EVER2
KW  - Kerinokeratosis papulosa
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-198997
SN  - 1018-8665
SN  - 1421-9832
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 231
IS  - 1
SP  - 1
EP  - 4
ER  - 
TY  - JOUR
A1  - Schmid, Michael
A1  - Steinlein, Claus
A1  - Winking, Heinz
T1  - Multicolor Spectral Analyses of Mitotic and Meiotic Mouse Chromosomes Involved in Multiple Robertsonian Translocations. I. The CD/Cremona Hybrid Strain
JF  - Cytogenetic and Genome Research
N2  - Multicolor spectral analysis (spectral karyotyping) was applied to mitotic and male diakinetic chromosomes of hybrid mice carrying a unique system of 18 autosomal Robertsonian translocation chromosomes with alternating arm homologies. Only the autosomes 19 and the XY sex chromosomes are excluded from these Robertsonian translocations. The translocations, previously identified by conventional banding analyses, could be verified by spectral karyotyping. Besides the Robertsonian translocations, no other interchromosomal rearrangements were detected. In diakineses of male meiosis, the 18 metacentric Robertsonian translocation chromosomes form a very large meiotic ‘superring'. The predictable, specific order of the chromosomes along this ‘superring' was completely confirmed by multicolor spectral analysis. In the majority of diakineses analyzed, the free autosomal bivalent 19 and the XY sex bivalent form a conspicuous complex which tightly associates with the 12;14 Robertsonian translocation chromosome in the ‘superring'.
KW  - meiotic ‘superring’
KW  - mouse
KW  - Robertsonian translocation chromosomes
KW  - spectral karyotyping
Y1  - 2016
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199013
SN  - 1424-8581
SN  - 1424-859X
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 147
IS  - 4
ER  - 
TY  - JOUR
A1  - Schmid, Michael
A1  - Steinlein, Claus
T1  - Chromosome Banding in Amphibia. XXXIII. Demonstration of 5-Methylcytosine-Rich Heterochromatin in Anura
JF  - Cytogenetic and Genome Research
N2  - An experimental approach using monoclonal anti-5-methylcytosine (5-MeC) antibodies and indirect immunofluorescence was elaborated for detecting 5-MeC-rich chromosome regions in anuran chromosomes. This technique was applied to mitotic metaphases of 6 neotropical frog species belonging to 6 genera and 4 families. The hypermethylation patterns were compared with a variety of banding patterns obtained by conventional banding techniques. The hypermethylated DNA sequences are species-specific and located exclusively in constitutive heterochromatin. They are found in centromeric, pericentromeric, telomeric, and interstitial positions of the chromosomes and adjacent to nucleolus organizer regions. 5-MeC-rich DNA sequences can be embedded both in AT- and GC-rich repetitive DNA. The experimental parameters that have major influence on the reproducibility and quality of the anti-5-MeC antibody labeling are discussed.
KW  - Anura
KW  - heterochromatin
KW  - hypermethylated DNA
KW  - immunofluorescence
KW  - 5-Methylcytosine
Y1  - 2016
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199022
SN  - 1424-8581
SN  - 1424-859X
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 148
IS  - 1
ER  - 
TY  - JOUR
A1  - Schneider, Eberhard
A1  - El Hajj, Nady
A1  - Müller, Fabian
A1  - Navarro, Bianca
A1  - Haaf, Thomas
T1  - Epigenetic Dysregulation in the Prefrontal Cortex of Suicide Completers
JF  - Cytogenetic and Genome Research
N2  - The epigenome is thought to mediate between genes and the environment, particularly in response to adverse life experiences. Similar to other psychiatric diseases, the suicide liability of an individual appears to be influenced by many genetic factors of small effect size as well as by environmental stressors. To identify epigenetic marks associated with suicide, which is considered the endpoint of complex gene-environment interactions, we compared the cortex DNA methylation patterns of 6 suicide completers versus 6 non-psychiatric sudden-death controls, using Illumina 450K methylation arrays. Consistent with a multifactorial disease model, we found DNA methylation changes in a large number of genes, but no changes with large effects reaching genome-wide significance. Global methylation of all analyzed CpG sites was significantly (0.25 percentage point) lower in suicide than in control brains, whereas the vast majority (97%) of the top 1,000 differentially methylated regions (DMRs) were higher methylated (0.6 percentage point) in suicide brains. Annotation analysis of the top 1,000 DMRs revealed an enrichment of differentially methylated promoters in functional categories associated with transcription and expression in the brain. In addition, we performed a comprehensive literature research to identify suicide genes that have been replicated in independent genetic association, brain methylation and/or expression studies. Although, in general, there was no significant overlap between different published data sets or between our top 1,000 DMRs and published data sets, our methylation screen strengthens a number of candidate genes (APLP2, BDNF, HTR1A, NUAK1, PHACTR3, MSMP, SLC6A4, SYN2, and SYNE2) and supports a role for epigenetics in the pathophysiology of suicide.
KW  - Cortex
KW  - DNA methylation
KW  - Suicidal behavior
KW  - Transcription regulation
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199032
SN  - 1424-8581
SN  - 1424-859X
VL  - 146
IS  - 1
ER  - 
TY  - JOUR
A1  - Schmid, Michael
A1  - Steinlein, Claus
A1  - Haaf, Thomas
A1  - Mijares-Urrutia, Abraham
T1  - Nascent ZW Sex Chromosomes in Thecadactylus rapicauda (Reptilia, Squamata, Phyllodactylidae)
JF  - Cytogenetic and Genome Research
N2  - The chromosomes of the turnip-tailed gecko Thecadactylus rapicauda from the Falcón State in northern Venezuela were examined by means of conventional staining, a variety of banding techniques and in situ hybridization with an 18S + 28S rDNA probe. In female specimens, C-banding analyses detected a cryptic W sex chromosome-associated interstitial heterochromatic segment which is absent in the Z sex chromosome. These ZW sex chromosomes are considered to be in a nascent stage of morphological differentiation and are absent in T. rapicauda collected in Guatemala. The amount, location and fluorochrome affinities of constitutive heterochromatin, the position of the nucleolus organizer region, and the genome sizes of female and male individuals were determined. The previously published cytogenetic data on T. rapicauda are discussed.
KW  - ZW sex chromosomes
KW  - Gecko
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-199041
SN  - 1424-8581
SN  - 1424-859X
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 143
IS  - 4
ER  - 
TY  - JOUR
A1  - Bura, Thomas
A1  - Beaupré, Serge
A1  - Légaré, Marc-André
A1  - Ibraikulov, Olzhas A.
A1  - Leclerc, Nicolas
A1  - Leclerc, Mario
T1  - Theoretical calculations for highly selective Direct Heteroarylation Polymerization: new nitrile-substituted Dithienyl-Diketopyrrolopyrrole-based polymers
JF  - Molecules
N2  - Direct Heteroarylation Polymerization (DHAP) is becoming a valuable alternative to classical polymerization methods being used to synthesize π-conjugated polymers for organic electronics applications. In previous work, we showed that theoretical calculations on activation energy (Ea) of the C–H bonds were helpful to rationalize and predict the selectivity of the DHAP. For readers’ convenience, we have gathered in this work all our previous theoretical calculations on Ea and performed new ones. Those theoretical calculations cover now most of the widely utilized electron-rich and electron-poor moieties studied in organic electronics like dithienyl-diketopyrrolopyrrole (DT-DPP) derivatives. Theoretical calculations reported herein show strong modulation of the Ea of C–H bond on DT-DPP when a bromine atom or strong electron withdrawing groups (such as fluorine or nitrile) are added to the thienyl moiety. Based on those theoretical calculations, new cyanated dithienyl-diketopyrrolopyrrole (CNDT-DPP) monomers and copolymers were prepared by DHAP and their electro-optical properties were compared with their non-fluorinated and fluorinated analogues.
KW  - DHAP
KW  - selectivity
KW  - theoretical calculations
KW  - conjugated polymers
KW  - organic electronics
Y1  - 2018
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-197648
SN  - 1420-3049
VL  - 23
IS  - 9
ER  - 
TY  - JOUR
A1  - Papenfort, Kai
A1  - Vogel, Jörg
T1  - Small RNA functions in carbon metabolism and virulence of enteric pathogens
JF  - Frontiers in Cellular and Infection Microbiology
N2  - Enteric pathogens often cycle between virulent and saprophytic lifestyles. To endure these frequent changes in nutrient availability and composition bacteria possess an arsenal of regulatory and metabolic genes allowing rapid adaptation and high flexibility. While numerous proteins have been characterized with regard to metabolic control in pathogenic bacteria, small non-coding RNAs have emerged as additional regulators of metabolism. Recent advances in sequencing technology have vastly increased the number of candidate regulatory RNAs and several of them have been found to act at the interface of bacterial metabolism and virulence factor expression. Importantly, studying these riboregulators has not only provided insight into their metabolic control functions but also revealed new mechanisms of post-transcriptional gene control. This review will focus on the recent advances in this area of host-microbe interaction and discuss how regulatory small RNAs may help coordinate metabolism and virulence of enteric pathogens.
KW  - sRNA
KW  - carbon metabolism
KW  - Hfq
KW  - CsrA
KW  - virulence
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-197520
SN  - 2235-2988
VL  - 4
IS  - 91
ER  - 
TY  - JOUR
A1  - Jungwirth, Gerhard
A1  - Yu, Tao
A1  - Moustafa, Mahmoud
A1  - Rapp, Carmen
A1  - Warta, Rolf
A1  - Jungk, Christine
A1  - Sahm, Felix
A1  - Dettling, Steffen
A1  - Zweckberger, Klaus
A1  - Lamszus, Katrin
A1  - Senft, Christian
A1  - Loehr, Mario
A1  - Keßler, Almuth F.
A1  - Ketter, Ralf
A1  - Westphal, Manfred
A1  - Debus, Juergen
A1  - von Deimling, Andreas
A1  - Simon, Matthias
A1  - Unterberg, Andreas
A1  - Abdollahi, Amir
A1  - Herold-Mende, Christel
T1  - Identification of KIF11 as a Novel Target in Meningioma
JF  - Cancers
N2  - Kinesins play an important role in many physiological functions including intracellular vesicle transport and mitosis. The emerging role of kinesins in different cancers led us to investigate the expression and functional role of kinesins in meningioma. Therefore, we re-analyzed our previous microarray dataset of benign, atypical, and anaplastic meningiomas (n = 62) and got evidence for differential expression of five kinesins (KIFC1, KIF4A, KIF11, KIF14 and KIF20A). Further validation in an extended study sample (n = 208) revealed a significant upregulation of these genes in WHO°I to °III meningiomas (WHO°I n = 61, WHO°II n = 88, and WHO°III n = 59), which was most pronounced in clinically more aggressive tumors of the same WHO grade. Immunohistochemical staining confirmed a WHO grade-associated upregulated protein expression in meningioma tissues. Furthermore, high mRNA expression levels of KIFC1, KIF11, KIF14 and KIF20A were associated with shorter progression-free survival. On a functional level, knockdown of kinesins in Ben-Men-1 cells and in the newly established anaplastic meningioma cell line NCH93 resulted in a significantly inhibited tumor cell proliferation upon siRNA-mediated downregulation of KIF11 in both cell lines by up to 95% and 71%, respectively. Taken together, in this study we were able to identify the prognostic and functional role of several kinesin family members of which KIF11 exhibits the most promising properties as a novel prognostic marker and therapeutic target, which may offer new treatment options for aggressive meningiomas.
KW  - meningioma
KW  - KIF
KW  - kinesin
KW  - KIF11
KW  - NCH93
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-197402
SN  - 2072-6694
VL  - 11
IS  - 4
ER  - 
TY  - JOUR
A1  - Lamatsch, D. K.
A1  - Trifonov, V.
A1  - Schories, S.
A1  - Epplen, J. T.
A1  - Schmid, M.
A1  - Schartl, M.
T1  - Isolation of a Cancer-Associated Microchromosome in the Sperm-Dependent Parthenogen Poecilia formosa
JF  - Cytogenetic and Genome Research
N2  - In the asexual all-female fish species Poecilia formosa, the Amazon molly, supernumerary chromosomes have frequently been found in both laboratory-reared and wild-caught individuals. While wild-caught individuals with B chromosomes are phenotypically indifferent from conspecifics, individuals carrying B chromosomes from recent introgression events in the laboratory show phenotypic changes. Former analyses showed that the expression of a pigment cell locus is associated with the presence of these B chromosomes. In addition, they contain a so far unidentified locus that confers a higher susceptibility to tumor formation in the presence of pigmentation pattern. Isolation by microdissection and hybridization to metaphase chromosomes revealed that they contain one or several sequences with similarity to a highly repetitive pericentromeric and subtelomeric sequence in A chromosomes. Isolation of one particular sequence by AFLP showed that the B chromosomes contain at least 1 copy of an A-chromosomal region which is highly conserved in the whole genus Poecilia, i.e. more than 5 million years old. We propose it to be a single copy sequence.
KW  - paternal introgression
KW  - AFLP
KW  - asexual reproduction
KW  - B chromosomes
KW  - gynogenesis
KW  - microdissection
KW  - telomeres
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-196785
SN  - 1424-8581
SN  - 1424-859X
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 135
IS  - 2
ER  - 
TY  - JOUR
A1  - Dengler, Julius
A1  - Maldaner, Nicolai
A1  - Gläsker, Sven
A1  - Endres, Matthias
A1  - Wagner, Martin
A1  - Malzahn, Uwe
A1  - Heuschmann, Peter U.
A1  - Vajkoczy, Peter
T1  - Outcome of Surgical or Endovascular Treatment of Giant Intracranial Aneurysms, with Emphasis on Age, Aneurysm Location, and Unruptured Aneuryms - A Systematic Review and Meta-Analysis
JF  - Cerebrovascular Diseases
N2  - Background: Designing treatment strategies for unruptured giant intracranial aneurysms (GIA) is difficult as evidence of large clinical trials is lacking. We examined the outcome following surgical or endovascular GIA treatment focusing on patient age, GIA location and unruptured GIA. Methods: Medline and Embase were searched for studies reporting on GIA treatment outcome published after January 2000. We calculated the proportion of good outcome (PGO) for all included GIA and for unruptured GIA by meta-analysis using a random effects model. Results: We included 54 studies containing 64 study populations with 1,269 GIA at a median follow-up time (FU-T) of 26.4 months (95% CI 10.8-42.0). PGO was 80.9% (77.4-84.4) in the analysis of all GIA compared to 81.2% (75.3-86.1) in the separate analysis of unruptured GIA. For each year added to patient age, PGO decreased by 0.8%, both for all GIA and unruptured GIA. For all GIA, surgical treatment resulted in a PGO of 80.3% (95% CI 76.0-84.6) compared to 84.2% (78.5-89.8, p = 0.27) after endovascular treatment. In unruptured GIA, PGO was 79.7% (95% CI 71.5-87.8) after surgical treatment and 84.9% (79.1-90.7, p = 0.54) after endovascular treatment. PGO was lower in high quality studies and in studies presenting aggregate instead of individual patient data. In unruptured GIA, the OR for good treatment outcome was 5.2 (95% CI 2.0-13.0) at the internal carotid artery compared to 0.1 (0.1-0.3, p < 0.1) in the posterior circulation. Patient sex, FU-T and prevalence of ruptured GIA were not associated with PGO. Conclusions: We found that the chances of good outcome after surgical or endovascular GIA treatment mainly depend on patient age and aneurysm location rather than on the type of treatment conducted. Our analysis may inform future research on GIA.
KW  - surgical aneurysm treatment
KW  - giant intracranial aneurysm
KW  - endovascular treatment
Y1  - 2016
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-196792
SN  - 1015-9770
SN  - 1421-9786
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 41
IS  - 3-4
ER  - 
TY  - JOUR
A1  - Schneider, Eberhard
A1  - El Hajj, Nady
A1  - Haaf, Thomas
T1  - Epigenetic Information from Ancient DNA Provides New Insights into Human Evolution
BT  - Commentary on Gokhman D et al. (2014): Reconstructing the DNA 
Methylation Maps of the Neanderthal and the Denisovan. Science 344:523–527
JF  - Brain, Behavior and Evolution
N2  - No abstract available.
KW  - human evolution
KW  - Neanderthal
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-196800
SN  - 0006-8977
SN  - 1421-9743
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 84
IS  - 3
ER  - 
TY  - JOUR
A1  - Stieb, Sara Mae
A1  - Kelber, Christina
A1  - Wehner, Rüdiger
A1  - Rössler, Wolfgang
T1  - Antennal-Lobe Organization in Desert Ants of the Genus Cataglyphis
JF  - Brain, Behavior and Evolution
N2  - Desert ants of the genus Cataglyphis possess remarkable visual navigation capabilities. Although Cataglyphis species lack a trail pheromone system, Cataglyphis fortis employs olfactory cues for detecting nest and food sites. To investigate potential adaptations in primary olfactory centers of the brain of C. fortis, we analyzed olfactory glomeruli (odor processing units) in their antennal lobes and compared them to glomeruli in different Cataglyphis species. Using confocal imaging and 3D reconstruction, we analyzed the number, size and spatial arrangement of olfactory glomeruli in C. fortis, C.albicans, C.bicolor, C.rubra, and C.noda. Workers of all Cataglyphis species have smaller numbers of glomeruli (198–249) compared to those previously found in olfactory-guided ants. Analyses in 2 species of Formica – a genus closely related to Cataglyphis – revealed substantially higher numbers of olfactory glomeruli (c. 370), which is likely to reflect the importance of olfaction in these wood ant species. Comparisons between Cataglyphis species revealed 2 special features in C. fortis. First, with c. 198 C. fortis has the lowest number of glomeruli compared to all other species. Second, a conspicuously enlarged glomerulus is located close to the antennal nerve entrance. Males of C. fortis possess a significantly smaller number of glomeruli (c. 150) compared to female workers and queens. A prominent male-specific macroglomerulus likely to be involved in sex pheromone communication occupies a position different from that of the enlarged glomerulus in females. The behavioral significance of the enlarged glomerulus in female workers remains elusive. The fact that C. fortis inhabits microhabitats (salt pans) that are avoided by all other Cataglyphis species suggests that extreme ecological conditions may not only have resulted in adaptations of visual capabilities, but also in specializations of the olfactory system.
KW  - olfactory glomeruli
KW  - plasticity
KW  - ant
KW  - antennal lobe
KW  - glomerulus
KW  - insects
KW  - interspecific comparison
KW  - macroglomerulus
KW  - olfaction
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-196815
SN  - 0006-8977
SN  - 1421-9743
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 77
IS  - 3
ER  - 
TY  - JOUR
A1  - Schraven, Sebastian P.
A1  - Dalhoff, Ernst
A1  - Wildenstein, Daniela
A1  - Hagen, Rudolf
A1  - Gummer, Anthony W.
A1  - Mlynski, Robert
T1  - Alternative Fixation of an Active Middle Ear Implant at the Short Incus Process
JF  - Audiology and Neurotology
N2  - Introduction: Since 1996, the preferred approach for positioning the active middle-ear implant Vibrant Soundbridge© is a mastoidectomy and a posterior tympanotomy. With this device, placement of the floating mass transducer (FMT) on the long incus process is the standard method for treatment of mild-to-severe sensorineural hearing loss in the case of normal middle-ear anatomy. The aim of this study was to determine the vibrational effectiveness of FMT placement at the short incus process. Materials and Methods: An extended antrotomy and a posterior tympanotomy were performed in 5 fresh human temporal bones. As a control for normal middle-ear function, the tympanic membrane was stimulated acoustically and the vibration of the stapes footplate and the round-window (RW) membrane were (sequentially) measured by laser Doppler vibrometry. Vibration responses for coupling of an FMT to the long incus process (standard coupling) were compared to those for coupling to the short incus process. Results: Apart from narrow frequency bands near 3 and 9 kHz for the stapes footplate and RW membrane, respectively, the velocity responses presented no significant differences between standard coupling of the FMT and coupling to the short incus process. Conclusion: Coupling the FMT to the short incus process may be a viable alternative in cases where the surgical approach is limited to an extended antrotomy. A reliable technique for attachment to the short incus process has yet to be developed.
KW  - middle-ear surgery
KW  - active middle-ear implant
KW  - floating mass transducer
KW  - incus
KW  - Laser Doppler vibrometer
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-196823
SN  - 1420-3030
SN  - 1421-9700
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 19
IS  - 1
ER  - 
TY  - JOUR
A1  - de Zeeuw, Dick
A1  - Akizawa, Tadao
A1  - Agarwal, Rajiv
A1  - Audhya, Paul
A1  - Bakris, George L.
A1  - Chin, Melanie
A1  - Krauth, Melissa
A1  - Lambers Heerspink, Hiddo J.
A1  - Meyer, Colin J.
A1  - McMurray, John J.
A1  - Parving, Hans-Henrik
A1  - Pergola, Pablo E.
A1  - Remuzzi, Giuseppe
A1  - Toto, Robert D.
A1  - Vaziri, Nosratola D.
A1  - Wanner, Christoph
A1  - Warnock, David G.
A1  - Wittes, Janet
A1  - Chertow, Glenn M.
T1  - Rationale and Trial Design of Bardoxolone Methyl Evaluation in Patients with Chronic Kidney Disease and Type 2 Diabetes: The Occurrence of Renal Events (BEACON)
JF  - American Journal of Nephrology
N2  - Background: Chronic kidney disease (CKD) associated with type 2 diabetes mellitus constitutes a global epidemic complicated by considerable renal and cardiovascular morbidity and mortality, despite the provision of inhibitors of the renin-angiotensin-aldosterone system (RAAS). Bardoxolone methyl, a synthetic triterpenoid that reduces oxidative stress and inflammation through Nrf2 activation and inhibition of NF-κB was previously shown to increase estimated glomerular filtration rate (eGFR) in patients with CKD associated with type 2 diabetes mellitus. To date, no antioxidant or anti-inflammatory therapy has proved successful at slowing the progression of CKD. Methods: Herein, we describe the design of Bardoxolone Methyl Evaluation in Patients with Chronic Kidney Disease and Type 2 Diabetes: the Occurrence of Renal Events (BEACON) trial, a multinational, multicenter, double-blind, randomized, placebo-controlled Phase 3 trial designed to determine whether long-term administration of bardoxolone methyl (on a background of standard therapy, including RAAS inhibitors) safely reduces renal and cardiac morbidity and mortality. Results: The primary composite endpoint is time-to-first occurrence of either end-stage renal disease or cardiovascular death. Secondary endpoints include the change in eGFR and time to occurrence of cardiovascular events. Conclusion: BEACON will be the first event-driven trial to evaluate the effect of an oral antioxidant and anti-inflammatory drug in advanced CKD.
KW  - clinical trial
KW  - diabetes mellitus
KW  - glomerular filtration rate
KW  - trial design
KW  - bardoxolone methyl
KW  - Nrf2
KW  - end-stage renal disease
KW  - cardiovascular death
KW  - chronic kidney disease
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-196832
SN  - 0250-8095
SN  - 1421-9670
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 37
IS  - 3
ER  - 
TY  - JOUR
A1  - Mayr, Stefan
A1  - Kuenzer, Claudia
A1  - Gessner, Ursula
A1  - Klein, Igor
A1  - Rutzinger, Martin
T1  - Validation of earth observation time-series: a review for large-area and temporally dense land surface products
JF  - Remote Sensing
N2  - Large-area remote sensing time-series offer unique features for the extensive investigation of our environment. Since various error sources in the acquisition chain of datasets exist, only properly validated results can be of value for research and downstream decision processes. This review presents an overview of validation approaches concerning temporally dense time-series of land surface geo-information products that cover the continental to global scale. Categorization according to utilized validation data revealed that product intercomparisons and comparison to reference data are the conventional validation methods. The reviewed studies are mainly based on optical sensors and orientated towards global coverage, with vegetation-related variables as the focus. Trends indicate an increase in remote sensing-based studies that feature long-term datasets of land surface variables. The hereby corresponding validation efforts show only minor methodological diversification in the past two decades. To sustain comprehensive and standardized validation efforts, the provision of spatiotemporally dense validation data in order to estimate actual differences between measurement and the true state has to be maintained. The promotion of novel approaches can, on the other hand, prove beneficial for various downstream applications, although typically only theoretical uncertainties are provided.
KW  - accuracy
KW  - error estimation
KW  - global
KW  - intercomparison
KW  - remote sensing
KW  - uncertainty
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-193202
SN  - 2072-4292
VL  - 11
IS  - 22
ER  - 
TY  - JOUR
A1  - Grebinyk, Anna
A1  - Prylutska, Svitlana
A1  - Buchelnikov, Anatoliy
A1  - Tverdokhleb, Nina
A1  - Grebinyk, Sergii
A1  - Evstigneev, Maxim
A1  - Matyshevska, Olga
A1  - Cherepanov, Vsevolod
A1  - Prylutskyy, Yuriy
A1  - Yashchuk, Valeriy
A1  - Naumovets, Anton
A1  - Ritter, Uwe
A1  - Dandekar, Thomas
A1  - Frohme, Marcus
T1  - C60 fullerene as an effective nanoplatform of alkaloid Berberine delivery into leukemic cells
JF  - Pharmaceutics
N2  - A herbal alkaloid Berberine (Ber), used for centuries in Ayurvedic, Chinese, Middle-Eastern, and native American folk medicines, is nowadays proved to function as a safe anticancer agent. Yet, its poor water solubility, stability, and bioavailability hinder clinical application. In this study, we have explored a nanosized carbon nanoparticle—C60 fullerene (C60)—for optimized Ber delivery into leukemic cells. Water dispersions of noncovalent C60-Ber nanocomplexes in the 1:2, 1:1, and 2:1 molar ratios were prepared. UV–Vis spectroscopy, dynamic light scattering (DLS), and atomic force microscopy (AFM) evidenced a complexation of the Ber cation with the negatively charged C60 molecule. The computer simulation showed that π-stacking dominates in Ber and C\(_{60}\) binding in an aqueous solution. Complexation with C\(_{60}\) was found to promote Ber intracellular uptake. By increasing C\(_{60}\) concentration, the C\(_{60}\)-Ber nanocomplexes exhibited higher antiproliferative potential towards CCRF-CEM cells, in accordance with the following order: free Ber < 1:2 < 1:1 < 2:1 (the most toxic). The activation of caspase 3/7 and accumulation in the sub-G1 phase of CCRF-CEM cells treated with C\(_{60}\)-Ber nanocomplexes evidenced apoptosis induction. Thus, this study indicates that the fast and easy noncovalent complexation of alkaloid Ber with C\(_{60}\) improved its in vitro efficiency against cancer cells.
KW  - C60 fullerene
KW  - Berberine
KW  - noncovalent nanocomplex
KW  - UV–Vis
KW  - DLS and AFM measurements
KW  - drug release
KW  - leukemic cells
KW  - uptake
KW  - cytotoxicity
KW  - apoptosis
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-193216
SN  - 1999-4923
VL  - 11
IS  - 11
ER  - 
TY  - JOUR
A1  - Teichmann, Christoph
T1  - Corporate Groups within the Legal Framework of the European Union: The Group-Related Aspects of the SUP Proposal and the EU Freedom of Establishment
JF  - European Company and Financial Law Review
N2  - No abstract available.
KW  - EU
KW  - corporate groups
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-194513
SN  - 1613-2556
SN  - 1613-2548
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 12
IS  - 2
SP  - 202
EP  - 229
ER  - 
TY  - JOUR
A1  - Li, Shan
A1  - Li, Xin
A1  - Link, Roman
A1  - Li, Ren
A1  - Deng, Liping
A1  - Schuldt, Bernhard
A1  - Jiang, Xiaomei
A1  - Zhao, Rongjun
A1  - Zheng, Jingming
A1  - Li, Shuang
A1  - Yin, Yafang
T1  - Influence of cambial age and axial height on the spatial patterns of xylem traits in Catalpa bungei, a ring-porous tree species native to China
JF  - Forests
N2  - Studying how cambial age and axial height affects wood anatomical traits may improve our understanding of xylem hydraulics, heartwood formation and axial growth. Radial strips were collected from six different heights (0–11.3 m) along the main trunk of three Manchurian catalpa (Catalpa bungei) trees, yielding 88 samples. In total, thirteen wood anatomical vessel and fiber traits were observed usinglight microscopy (LM) and scanning electron microscopy (SEM), and linear models were used to analyse the combined effect of axial height, cambial age and their interaction. Vessel diameter differed by about one order of magnitude between early- and latewood, and increased significantly with both cambial age and axial height in latewood, while it was positively affected by cambial age and independent of height in earlywood. Vertical position further had a positive effect on earlywood vessel density, and negative effects on fibre wall thickness, wall thickness to diameter ratio and length. Cambial age had positive effects on the pit membrane diameter and vessel element length, while the annual diameter growth decreased with both cambial age and axial position. In contrast, early- and latewood fiber diameter were unaffected by both cambial age and axial height. We further observed an increasing amount of tyloses from sapwood to heartwood, accompanied by an increase of warty layers and amorphous deposits on cell walls, bordered pit membranes and pit apertures. This study highlights the significant effects of cambial age and vertical position on xylem anatomical traits, and confirms earlier work that cautions to take into account xylem spatial position when interpreting wood anatomical structures, and thus, xylem hydraulic functioning.
KW  - wood anatomy
KW  - vertical and radial variation
KW  - earlywood
KW  - latewood
KW  - growth ring width
KW  - tyloses
KW  - pit membrane diameter
KW  - vessel lumen diameter
KW  - fibre length
Y1  - 2019
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-196297
SN  - 1999-4907
VL  - 10
IS  - 8
ER  - 
TY  - JOUR
A1  - Camacho, J.P.M.
A1  - Schmid, M.
A1  - Cabrero, J.
T1  - B Chromosomes and Sex in Animals
JF  - Sexual Development
N2  - Supernumerary (B) chromosomes are dispensable elements found in many eukaryote genomes in addition to standard (A) chromosomes. In many respects, B chromosomes resemble sex chromosomes, so that a common ancestry for them has frequently been suggested. For instance, B chromosomes in grasshoppers, and other insects, show a pycnotic cycle of condensation-decondensation during meiosis remarkably similar to that of the X chromosome. In some cases, B chromosome size is even very similar to that of the X chromosome. These resemblances have led to suggest the X as the B ancestor in many cases. In addition, sex chromosome origin from B chromosomes has also been suggested. In this article, we review the existing evidence for both evolutionary pathways, as well as sex differences for B frequency at adult and embryo progeny levels, B chromosome effects or B chromosome transmission. In addition, we review cases found in the literature showing sex-ratio distortion associated with B chromosome presence, the most extreme case being the paternal sex ratio (PSR) chromosomes in some Hymenoptera. We finally analyse the possibility of B chromosome regularisation within the host genome and, as a consequence of it, whether B chromosomes can become regular members of the host genome.
KW  - A chromosomes
KW  - B chromosomes
KW  - sex ratio
KW  - X chromosome
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-196321
SN  - 1661-5425
SN  - 1661-5433
N1  - This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.
VL  - 5
IS  - 3
ER  -