TY  - JOUR
A1  - Kroner-Weigl, Niklas
A1  - Chu, Jin
A1  - Rudert, Maximilian
A1  - Alt, Volker
A1  - Shukunami, Chisa
A1  - Docheva, Denitsa
T1  - Dexamethasone is not sufficient to facilitate tenogenic differentiation of dermal fibroblasts in a 3D organoid model
JF  - Biomedicines
N2  - Self-assembling three-dimensional organoids that do not rely on an exogenous scaffold but maintain their native cell-to-cell and cell-to-matrix interactions represent a promising model in the field of tendon tissue engineering. We have identified dermal fibroblasts (DFs) as a potential cell type for generating functional tendon-like tissue. The glucocorticoid dexamethasone (DEX) has been shown to regulate cell proliferation and facilitate differentiation towards other mesenchymal lineages. Therefore, we hypothesized that the administration of DEX could reduce excessive DF proliferation and thus, facilitate the tenogenic differentiation of DFs using a previously established 3D organoid model combined with dose-dependent application of DEX. Interestingly, the results demonstrated that DEX, in all tested concentrations, was not sufficient to notably induce the tenogenic differentiation of human DFs and DEX-treated organoids did not have clear advantages over untreated control organoids. Moreover, high concentrations of DEX exerted a negative impact on the organoid phenotype. Nevertheless, the expression profile of tendon-related genes of untreated and 10 nM DEX-treated DF organoids was largely comparable to organoids formed by tendon-derived cells, which is encouraging for further investigations on utilizing DFs for tendon tissue engineering.
KW  - 3D organoids
KW  - dermal fibroblasts
KW  - dexamethasone
KW  - scaffold-free
KW  - tenogenic differentiation
KW  - tendon tissue engineering
Y1  - 2023
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-311234
SN  - 2227-9059
VL  - 11
IS  - 3
ER  - 
TY  - THES
A1  - George, Enrico
T1  - Temporäre Hemiepiphyseodese bei idiopathischen Beinachsenfehlstellungen - klinische und radiologische Gegenüberstellung der VaWiKo® EPI-PLATTE und PediatrOS™ FlexTack™ - eine retrospektive Studie
T1  - Temporary hemiepiphysiodesis with idiopathic leg axis malalignment - clinical and radiological comparison of the VaWiKo® EPI-PLATTE and PediatrOS™ FlexTack™ - a retrospective study
N2  - Beinachsenfehlstellungen im Kindesalter zählen zu den häufigsten Wachstums- und Entwicklungsstörungen der unteren Extremitäten. Eine daraus resultierende Prädisposition für degenerative Erkrankungen begründet die Bedeutung der operativen Korrektur bei noch geöffneten Wachstumsfugen mittels temporärer Hemiepiphyseodese. 
Zur Beurteilung des Therapieerfolges wurden insgesamt 140 Beinachsen mit idiopathischen Achsfehlstellungen retrospektiv betrachtet. In den Jahren 2017 bis 2021 wurden mit der VaWiKo® EPI-PLATTE und der PediatrOS™ FlexTack™ zwei unterschiedliche Implantate zur temporären Hemiepiphyseodese in der kinderorthopädischen Klinik des Marienstift Arnstadt verwendet. Entsprechend der verwendeten Implantate erfolgte die Einteilung in zwei Patientengruppen, die sowohl klinisch als auch radiologisch jeweils prä- und postoperativ gegenübergestellt wurden.
Bei Patienten/-innen mit einer Beinachsenkorrektur durch die VaWiKo® EPI-PLATTE ergab sich durchschnittlich eine signifikant kürzere Explantationsdauer (EP 26,05 min; FT 35,60 min) sowie eine kürzere Durchleuchtungszeit in Winkelminuten (EP 0,03; FT 0,07) im Rahmen der Explantation. Dem gegenüber steht die signifikant kürzere stationäre Aufenthaltsdauer in Tagen bei der Im- und Explantation der PediatrOS™ FlexTack™. (EP 5,43/ 3,73; FT 4,52/ 3,35). In Bezug auf die zur Wachstumskorrektur benötigten Zeit in Tagen resultiert in der Varus-Gruppe ein signifikanter Unterschied zugunsten der PediatrOS™ FlexTack™, (EP 517; FT 299) wohingegen sich in der Valgus-Gruppe kein signifikanter Unterschied zwischen beiden Implantaten zeigte (EP 343; FT 334). Zusammenfassend traten zwei Komplikationen auf, die jeweils Kinder aus der PediatrOS™ FlexTack™-Gruppe betrafen.
Sowohl die PediatrOS™ FlexTack™ als auch die VaWiKo® EPI-PLATTE konnten die gewünschte Beinachsenkorrektur erzielen. Die in der Literatur mit der PediatrOS™ FlexTack™ in Verbindung gebrachten kürzeren Implantations- und Durchleuchtungszeiten sowie die kürzeren Therapiedauern des Genu valgum konnten im Vergleich zur VaWiKo® EPI-PLATTE nicht bestätigt werden.
N2  - In the study, the VaWiKo® EPI-PLATTE (EP) and PediatrOS™ FlexTack™ (FT) were opposed as implants for temporary hemiepiphysiodesis to establish a direct comparability and therefore being able to show possible therapeutic consequences. The aim of the study was to make a prospectively preoperative statement on the selection of the implant to be chosen in view of the co-factors.

In the years from 2017 to 2021, a total of eighty children with idiopathic leg axis malpositions were surgically treated in the Department of Paediatric Orthopaedics at Marienstift Arnstadt. According to the implants used, the patients were divided into two groups of 40 children each. To evaluate the success of the therapy, the resulting 140 leg axes were examined retrospectively. To verify the leg axis malalignment, the intermalleolar distance was used clinically on the one hand and the MAD/mLDFW/mMPTW and aFTW were used radiologically with full length x-rays taken pre- and postoperatively on the other.

Of the 80 patients, 29 (36.25%) were female and 51 (63.75%) male. A total of 140 leg axis malpositions were corrected, 12 (8.57%) were varus and 128 (91.43%) valgus axes. The average age at the time of surgery was 12.74 years. The mean preoperative intermalleolar distance of 11.83 cm in the 55 patients with bilateral valgus deformity showed no significant difference between the two groups (p=0.294). The mean MAD in the valgus group was -16.52 mm preoperatively (p=0.966) and 3.60 mm postoperatively (p=0.125). The preoperatively measured mLDFW, mMPTW and aFTW did not show any significant difference in the comparison of the VaWiKo® EPI-PLATTE and PediatrOS™ FlexTack™, so that a homogeneous patient population was there. Patients with leg axis correction using the VaWiKo® EPI-PLATTE had a significantly shorter explantation time (p=0,006) and a shorter fluoroscopy time in angular minutes (p=0,005) during explantation. These contrasts with the significantly shorter inpatient length of stay in days during implantation and explantation of the PediatrOS™ FlexTack™. (EP 5.43/ 3.73; FT 4.52/ 3.35). In relation to the time required for growth correction in days, there was a significant difference in favour of the PediatrOS™ FlexTack™ in the varus group (EP 517; FT 299), whereas there was no significant difference between the two implants in the valgus group (EP 343; FT 334). Two complications occurred, each affecting children in the PediatrOS™ FlexTack™ group. 

Both the PediatrOS™ FlexTack™ and the VaWiKo® EPI-PLATTE were able to achieve the desired leg axis correction. The VaWiKo® EPI-PLATTE was more convincing with shorter explantation times and fluoroscopy times an no documented complications compared to the PediatrOS™ FlexTack™. The PediatrOS™ FlexTack™ impressed with a shorter therapy duration in the correction of varus deformities.
KW  - Epiphyseodese
KW  - Temporäre Hemiepiphyseodese
Y1  - 2023
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-327338
ER  - 
TY  - THES
A1  - Reck, Alexander Reiner
T1  - Die operative Korrektur der Madelung'schen Deformität
T1  - Surgical correction of Madelung's deformity
N2  - Im Rahmen dieser retrospektiven Studie zur Madelung-Deformität wurden 23 Hände von 16 Patienten, welche in einem Zeitraum von 17,5 Jahren mit einer Radiuskorrekturosteotomie (RKO) oder eine Physiolyse mit Vickers-Band-Entfernung (PHY) behandelt wurden, nachuntersucht und bezüglich des OP-Outcomes verglichen. Die Gruppe RKO umfasste 14 Hände mit einem Durchschnittsalter von 22 Jahren und einer durchschnittlichen Follow-Up-Zeitraum von 7 Jahren. Die Gruppe PHY bestand aus 9 Händen mit einem Durchschnittsalter von 13 Jahren und einem mittleren Follow-Up-Zeitraum von 5 Jahren.
In unserem Kollektiv konnte die Radiuskorrektur eine Verbesserung bezüglich der Schmerzen, des subjektiven Gesundheitsstatus, der Beweglichkeit und der radiologischen Ausprägung der Deformität herbeiführen. Die vorliegenden Ergebnisse stützen damit die aus der bisherigen Literatur ableitbare Vermutung, dass dieses Verfahren zur Therapie der Madelung-Deformität geeignet ist. Die Physiolyse mit Vickers-Band-Entfernung konnte die Progredienz der Erkrankung in unserer Stichprobe nicht suffizient aufhalten, wie es anhand der bisherigen Literatur allerdings zu erwarten gewesen wäre. Infolgedessen kam es in der Gruppe PHY zu einer Zunahme der Schmerzen und der Ausprägung der Deformität sowie einer Verschlechterung des Gesundheitsstatus. Der Grund hierfür lag wahrscheinlich im, verglichen mit der bisherigen Literatur, relativ hohen Durchschnittsalter der Gruppe. Es lässt sich schlussfolgern, dass die Physiolyse mit Vickers-Band-Entfernung ihre Wirkung vor allem im Kindesalter voll entfaltet.
Im Einklang mit der bisherigen Literatur konnte keine Korrelation zwischen den aktuellen radiologischen und klinischen Befunden beobachtet werden. Jedoch zeigte sich ein augenscheinlicher Zusammenhang zwischen der Veränderung der radiologischen Parameter und der Veränderung des klinischen Befindens, was einen Nutzen der McCarroll-Parameter im Rahmen der OP-Planung nahelegt.
N2  - In this retrospective study, 23 hands of 16 patients suffering from Madelung's deformity that were treated with radius corrective osteotomy (RKO) or physiolysis with removal of the Vickers-ligament(PHY) over a period of 17.5 years were followed up for comparison of the surgical outcome of these two groups. The RKO group included 14 hands with an average age of 22 years and an average follow-up period of 7 years. The PHY group consisted of 9 hands with a mean age of 13 years and a mean follow-up period of 5 years. In our collective, radius corrective osteotomy was able to bring about an improvement in terms of pain, subjective health status, mobility, and radiological severity of the deformity. The present results thus support the assumption derivable from the previous literature that this procedure is suitable for the therapy of the Madelung deformity. Physiolysis with Vickers ligament removal was not able to sufficiently halt the progression of the disease in our sample, although this would have been expected from the previous literature. As a result, there was an increase in pain and severity of deformity and a worsening of health status in the PHY group. The reason for this was probably the relatively high average age of our sample compared to the previous literature. This leads to the conclusion that physiolysis with Vickers ligament excision is most effective in children. Consistent with previous literature, no correlation was observed between the current radiological and clinical findings. However, there appeared to be a correlation between the alteration of radiological characteristics and the alteration of clinical outcomes, pointing to the usefulness of McCarroll's parameters for surgical planning.
KW  - Handdeformität
KW  - Operation
KW  - Korrektur
KW  - Handgelenk
KW  - Madelung-Deformität
KW  - Madelung
KW  - Radiuskorrekturosteotomie
KW  - Vickers-Band
KW  - Physiolyse
KW  - Madelung's deformity
KW  - Madelung deformity
KW  - osteotomy
KW  - physiolysis
KW  - surgical correction
KW  - Madelung, Otto Wilhelm
Y1  - 2023
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-326604
ER  - 
TY  - JOUR
A1  - Dhaliwal, Anand
A1  - Zamora, Tomas
A1  - Nedopil, Alexander J.
A1  - Howell, Stephen M.
A1  - Hull, Maury L.
T1  - Six commonly used postoperative radiographic alignment parameters do not predict clinical outcome scores after unrestricted caliper-verified kinematically aligned TKA
JF  - Journal of Personalized Medicine
N2  - Background: Unrestricted caliper-verified kinematically aligned (KA) TKA restores patient’s prearthritic coronal and sagittal alignments, which have a wide range containing outliers that concern the surgeon practicing mechanical alignment (MA). Therefore, knowing which radiographic parameters are associated with dissatisfaction could help a surgeon decide whether to rely on them as criteria for revising an unhappy patient with a primary KA TKA using MA principles. Hence, we determined whether the femoral mechanical angle (FMA), hip–knee–ankle angle (HKAA), tibial mechanical angle (TMA), tibial slope angle (TSA), and the indicators of patellofemoral tracking, including patella tilt angle (PTA) and the lateral undercoverage of the trochlear resection (LUCTR), are associated with clinical outcome scores. Methods: Forty-three patients with a CT scan and skyline radiograph after a KA TKA with PCL retention and medial stabilized design were analyzed. Linear regression determined the strength of the association between the FMA, HKA angle, PTS, PTA, and LUCTR and the forgotten joint score (FJS), Oxford knee score (OKS), and KOOS Jr score obtained at a mean of 23 months. Results: There was no correlation between the FMA (range 2° varus to −10° valgus), HKAA (range 10° varus to −9° valgus), TMA (range 10° varus to −0° valgus), TSA (range 14° posterior to −4° anterior), PTA (range, −10° medial to 14° lateral), and the LUCTR resection (range 2 to 9 mm) and the FJS (median 83), the OKS (median 44), and the KOOS Jr (median 85) (r = 0.000 to 0.079). Conclusions: Surgeons should be cautious about using postoperative FMA, HKAA, TMA, TSA, PTA, and LUCTR values within the present study’s reported ranges to explain success and dissatisfaction after KA TKA.
KW  - total knee arthroplasty
KW  - kinematic alignment
KW  - reoperation
KW  - revision
KW  - phenotype
Y1  - 2022
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-288186
SN  - 2075-4426
VL  - 12
IS  - 9
ER  - 
TY  - JOUR
A1  - Nedopil, Alexander J.
A1  - Howell, Stephen M.
A1  - Hull, Maury L.
T1  - Measurement of tibial orientation helps select the optimal insert thickness to personalize PCL tension in a medial ball-in-socket TKA
JF  - Journal of Personalized Medicine
N2  - As the conformity of a medial ball-in-socket total knee arthroplasty (TKA) provides intrinsic anterior-posterior (A-P) stability, surgeons cannot rely on the manual examination of sagittal laxity to identify the optimal insert thickness. Instead, the present study determined whether measuring tibial axial orientation in extension and 90° flexion with an insert goniometer could identify the optimal thickness that, when implanted, provides high postoperative function. In twenty-two patients that underwent unrestricted caliper-verified kinematic alignment (KA) with a PCL retaining implant, two surgeons measured tibial orientation in extension and 90° flexion with 10, 11, 12, and 13 mm thick insert goniometers. Each TKA had one insert thickness that restored either the maximum external tibial orientation in extension, the maximum internal tibial orientation at 90° flexion, or both relative to 1 mm thinner and thicker inserts. In addition, the 6-month median [interquartile range] Forgotten Joint Score of 73 (54–87) and Oxford Knee Score of 42 (38–45) indicated high satisfaction and function. In conclusion, surgeons using a medial ball-in-socket TKA design can measure external tibial orientation in extension and internal tibial orientation at 90° flexion with an insert goniometer. Furthermore, implanting an insert with the thickness that provided the maximum orientation values resulted in high postoperative function, thereby personalizing PCL tension.
KW  - posterior cruciate ligament
KW  - tibial rotation
KW  - medial pivot
KW  - total knee arthroplasty
KW  - kinematic alignment
Y1  - 2022
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-286232
SN  - 2075-4426
VL  - 12
IS  - 9
ER  - 
TY  - JOUR
A1  - Nedopil, Alexander J.
A1  - Howell, Stephen M.
A1  - Hull, Maury L.
T1  - A TKA insert with a lateral flat articular surface maximizes external and internal tibial orientations without anterior lift-off relative to low- and ultracongruent surfaces
JF  - Journal of Personalized Medicine
N2  - Background: In total knee arthroplasty (TKA), inserts can have different levels of medial and lateral congruency determined by the acuteness of the upslopes of the anterior and posterior articular surfaces. The present study evaluated an insert with different levels of lateral congruency and a medial ball-in-socket congruency to test the hypothesis that a lateral flat (F) insert maximizes external tibial orientation at extension and internal orientation at 90° flexion and lowers the incidence of anterior lift-off relative to low-congruent (LC) and ultracongruent (UC) lateral inserts. Methods: Two surgeons treated 23 patients with unrestricted caliper-verified kinematic alignment (KA) and posterior cruciate ligament (PCL) retention. They randomly trialed inserts with a medial radial dial that functioned as a built-in goniometer by measuring the tibial orientation relative to a sagittal line on the femoral trial component. Anterior lift-off of the insert from the baseplate indicated PCL tightness. Results: The F insert’s mean of 9° of external tibial orientation was higher than that of the LC (5°, p < 0.0001) and UC inserts (2°, p < 0.0001). The −13° of internal tibial orientation at 90° flexion was higher than that of the LC (−9°, p < 0.0001) and UC inserts (−7°, p < 0.0001). The 0% incidence of anterior lift-off was less than that of the LC (26%) and UC inserts (57%) (p < 0.0001). Conclusions: Surgeons and implant manufacturers should know that adding congruency to the lateral articular surface limits external tibial orientation in extension and internal tibial orientation at 90° flexion and overtightens the PCL. These rotational limitations and flexion space tightness can adversely affect patellofemoral tracking and knee flexion.
KW  - total knee arthroplasty
KW  - kinematic alignment
KW  - implant design
KW  - PCL retention
KW  - congruency
Y1  - 2022
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-286142
SN  - 2075-4426
VL  - 12
IS  - 8
ER  - 
TY  - JOUR
A1  - Wang, Chenglong
A1  - Stöckl, Sabine
A1  - Li, Shushan
A1  - Herrmann, Marietta
A1  - Lukas, Christoph
A1  - Reinders, Yvonne
A1  - Sickmann, Albert
A1  - Grässel, Susanne
T1  - Effects of extracellular vesicles from osteogenic differentiated human BMSCs on osteogenic and adipogenic differentiation capacity of naïve human BMSCs
JF  - Cells
N2  - Osteoporosis, or steroid-induced osteonecrosis of the hip, is accompanied by increased bone marrow adipogenesis. Such a disorder of adipogenic/osteogenic differentiation, affecting bone-marrow-derived mesenchymal stem cells (BMSCs), contributes to bone loss during aging. Here, we investigated the effects of extracellular vesicles (EVs) isolated from human (h)BMSCs during different stages of osteogenic differentiation on the osteogenic and adipogenic differentiation capacity of naïve (undifferentiated) hBMSCs. We observed that all EV groups increased viability and proliferation capacity and suppressed the apoptosis of naïve hBMSCs. In particular, EVs derived from hBMSCs at late-stage osteogenic differentiation promoted the osteogenic potential of naïve hBMSCs more effectively than EVs derived from naïve hBMSCs (naïve EVs), as indicated by the increased gene expression of COL1A1 and OPN. In contrast, the adipogenic differentiation capacity of naïve hBMSCs was inhibited by treatment with EVs from osteogenic differentiated hBMSCs. Proteomic analysis revealed that osteogenic EVs and naïve EVs contained distinct protein profiles, with pro-osteogenic and anti-adipogenic proteins encapsulated in osteogenic EVs. We speculate that osteogenic EVs could serve as an intercellular communication system between bone- and bone-marrow adipose tissue, for transporting osteogenic factors and thus favoring pro-osteogenic processes. Our data may support the theory of an endocrine circuit with the skeleton functioning as a ductless gland.
KW  - extracellular vesicles
KW  - mesenchymal stem cells
KW  - osteogenic potential
KW  - osteogenic differentiation
KW  - adipogenic differentiation
KW  - ECM remodeling
KW  - bone regeneration
Y1  - 2022
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-286112
SN  - 2073-4409
VL  - 11
IS  - 16
ER  - 
TY  - JOUR
A1  - Stratos, Ioannis
A1  - Behrendt, Ann-Kathrin
A1  - Anselm, Christian
A1  - Gonzalez, Aldebarani
A1  - Mittlmeier, Thomas
A1  - Vollmar, Brigitte
T1  - Inhibition of TNF-α restores muscle force, inhibits inflammation, and reduces apoptosis of traumatized skeletal muscles
JF  - Cells
N2  - Background: Muscle injuries are common in humans and are often associated with irrecoverable damage and disability. Upon muscle injury, TNF-α signaling pathways modulate the healing process and are predominantly associated with tissue degradation. In this study we assumed that TNF-α inhibition could reduce the TNF-α-associated tissue degradation after muscle injury. Materials and methods: Therefore, the left soleus muscle of 42 male Wistar rats was injured using a standardized open muscle injury model. All rats were treated immediately after injury either with infliximab (single i.p. injection; 10 mg/kg b.w.) or saline solution i.p. Final measurements were conducted at day one, four, and 14 post injury. The muscle force, the muscle cell proliferation, the muscle cell coverage as well as the myofiber diameter served as read out parameters of our experiment. Results: Systemic application of infliximab could significantly reduce the TNF-α levels in the injured muscle at day four upon trauma compared to saline treated animals. The ratio of muscle weight to body weight was increased and the twitch muscle force showed a significant rise 14 days after trauma and TNF-α inhibition. Quantification of myofiber diameter in the penumbra zone showed a significant difference between both groups at day one and four after injury, indicated by muscle hypertrophy in the infliximab group. Planimetric analysis of the injured muscle at day 14 revealed increased muscle tissue fraction in the infliximab group compared to the control animals. Muscle cell proliferation did not differ between both groups. Conclusions: These data provide evidence that the TNF-α blockade positively regulates the restauration of skeletal muscles upon injury.
KW  - muscle injury
KW  - regeneration
KW  - infliximab
KW  - tumor necrosis factor alpha
Y1  - 2022
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-286094
SN  - 2073-4409
VL  - 11
IS  - 15
ER  - 
TY  - THES
A1  - Paulus [verh. Rehling], Sofia
T1  - CRISPR/Cas9-basierte Etablierung Alkalischer Phosphatase-defizienter odontogener Zelllinien zur Analyse der dentalen Aspekte der Hypophosphatasie
T1  - CRISPR/Cas9-based establishment of alkaline phosphatase deficient odontogenous cell lines to analyze dental aspects of Hypophosphatasia
N2  - Die Hypophosphatasie (HPP) ist eine seltene Erberkrankung, welche durch compound-heterozygote oder dominant negative heterozygote Mutationen des ALPL Gens zu einem Funktionsverlust der gewebeunspezifischen Alkalischen Phosphatase (TNAP) führt. Die daraus resultierenden Mineralisierungsstörungen betreffen sowohl den Knochen als auch in milderen Ausprägungsformen die Zähne und den Zahnhalteapparat. Das zahnmedizinische Leitsymptom und in vielen Fällen das erste Anzeichen der HPP ist dabei der vorzeitige Verlust der Milchzähne ohne physiologische Wurzelresorption. Im Rahmen dieser Arbeit wurden verschiedene TNAP defiziente immortalisierte Zellen des parodontalen Ligaments (PDL) mittels der CRISPR/Cas9 Methode generiert und anschließend fünf Zelllinien charakterisiert. Die dabei entstandenen Mutationen variierten von einer moderaten heterozygoten Punktmutation zu einer schwerwiegenden homozygoten Deletion eines einzelnen Nukleotids, welche in einem vorzeitigen Stopcodon resultierte. Analysen der ALPL Expression (qPCR), TNAP Aktivitätsmessungen (CSPD Assay) und TNAP Färbungen zeigten einen signifikanten Rückgang in allen TNAP-defizienten Zelllinien mit einer starken Korrelation zwischen der Restaktivität und dem Ausmaß der Mutation, welche in Einklang mit der komplexen Genotyp-Phänotyp Korrelation bei HPP zu bringen ist. Das Potential der osteogenen Differenzierung der hTERT PDL Zellen wurde in der homozygot mutierten Zelllinie komplett unterdrückt. Mögliche Mechanismen des vorzeitigen Zahnverlustes bei HPP Patienten ist die geminderte Formation und Mineralisation des Wurzelzements und die fehlerhafte Insertion der parodontalen Fasern. Die hier erstmalig etablierten Zellkulturmodelle liefern ein valides spenderunabhängiges in vitro Modell der HPP, welches dazu beitragen kann, die molekularbiologischen Zusammenhänge der dentalen Aspekte der Hypophosphatasie zu ergründen und daraus gegebenenfalls neue Therapieansätze abzuleiten.
N2  - Hypophosphatasia (HPP) is a rare inherited disorder caused by loss-of-function mutations in the ALPL gene encoding the Tissue Nonspecific Alkaline Phosphatase (TNAP). Besides skeletal symptoms, some patients also present dental abnormalities like for example the premature loss of deciduous teeth. Here we generated and characterized five different TNAP-deficient periodontal ligament (PDL) derived cell lines using the method of CRISPR-Cas9. The mutations varied from a moderate heterozygous point mutation to a severe homozygous deletion leading to a premature stop codon. Analysis of the ALPL expression and TNAP activity measurements  in CSPD Assays and TNAP stainings revealed a decrease for all TNAP-deficient cell lines with a strong correlation between the residual activity and the extend of the mutation. The already limited differentiation capacity of immortalized hTERT (human telomerase reverse transcriptase) PDL cells is completely abolished in the homozygously mutated cell line. Putative key mechanisms for the premature exfoliation in HPP are the restricted formation and mineralization of the cementum and the impaired insertion of elastic dental fibers. The newly generated TNAP-deficient cell lines provide a promising and donor independent in vitro model to gain better understanding of the molecular mechanisms of dental problems in HPP.
KW  - Hypophosphatasie
KW  - TNAP
KW  - Alkalische Phosphatase
KW  - CRISPR/Cas-Methode
KW  - CRISPR/Cas9
Y1  - 2023
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-243491
ER  - 
TY  - THES
A1  - Seiler, Jonas
T1  - Die Expression des Vitamin-D-Rezeptors und der 24-Hydroxylase in Knochenmetastasen unterschiedlicher Entität
T1  - Vitamin-D-receptor- and CYP24A1- expression in bone metastases of different primary origin
N2  - Knochenmetastasen sind unter den drei häufigsten Manifestationsorten metastatischer Absiedelungen von fortgeschrittenen Tumorerkrankungen. Dabei sind insbesondere Patientinnen und Patienten mit Prostata- und Mammakarzinom von Knochenmetastasen betroffen. Diese Knochenmetastasen führen häufig zu einer deutlichen Verschlechterung der Lebensqualität und zu einer Begrenzung der Therapieoptionen auf lediglich palliative Ansätze. 
Die biologisch aktive Form von Vitamin D3, 1,25(OH)2-Vitamin D3, zeigt in präklinischen Studien antiproliferative und differenzierende Effekte auf Tumorzellen (101, 102, 104), die haupsächlich durch die Bindung an den Vitamin D-Rezeptor (VDR) vermittelt werden. Darüberhinaus konnte präklinisch gezeigt werden, dass eine niedrige Expression des VDRs, ligandenunabhängig, die Knochenmetastasierung und das Tumorwachstum begünstigt (118). Eine niedrige VDR-Expression ist in Primärtumoren in klinischen Studien mit aggressiven Tumoreigenschaften assoziiert (111, 113, 115) und kann zudem mit einer erhöhten/früheren ossären Metastasierung einhergehen (167). Zudem gibt es Hinweise auf einen dysregulierten 1,25(OH)2-Vitamin D3-Katabolismus durch eine erhöhte Expression des 1,25(OH)2-Vitamin D3 katabolisierenden Enzyms CYP24A1/24-Hydroxylase in primärem Tumorzellen (70, 121, 122). Durch die Untersuchungen der Primärtumoren ist damit zu hypothetisieren, dass die Expression des VDRs und von CYP24A1 bei der Tumorprogression und Knochenmetastasierung von Bedeutung sein könnte. Entsprechende Untersuchungen des VDRs und der 24-Hydroxylase in Knochenmetastasen fehlen allerdings. Deshalb wurde in dieser Arbeit die Expression des VDRs und von CYP24A1 in Knochenmetastasen unterschiedlicher Primärtumoren von 66 Patientinnen und Patienten untersucht und mögliche Assoziationen mit aggressiven Tumoreigenschaften analysiert. 
Der VDR konnte sowohl im Zytoplasma als auch im Nukleus nachgewiesen werden, während CYP24A1 nur im Zytoplasma lokalisiert war. Dabei wiesen insgesamt 71 % der Knochenmetastasen eine hohe VDR-Expression im Nukleus und 56 % im Zytoplasma auf. 59 % der Knochenmetastasen wiesen eine hohe Expression des VDRs insgesamt auf. CYP24A1 war ebenso in 59 % der Knochenmetastasen hoch exprimiert. Bei der Auswertung des Zusammenhangs zwischen den TNM-Stadien und des Gradings zeigte sich ein nicht signifikanter Trend von schlecht differenzierten Tumoren hin zu einer niedrigeren nukleären VDR-Expression (p=0.07, siehe Abbildung 33). Bezüglich der T-Stadien zeigten sich keine Unterschiede der Expression des VDRs und von CYP24A1 in den Knochenmetastasen zwischen lokal fortgeschrittenen und kleinen Primärtumoren. Weiterhin hatten Patientinnen und Patienten mit Lymphknotenmetastasen tendenziell eine verminderte VDR- und auch CYP24A1-Expression in den Knochenmetastasen im Vergleich zu Patienten und Patientinnen ohne Lymphknotenmetastasen (pVDR=0.15, pCYP24A1=0.06, siehe Abbildung 35). Außerdem hatten Patientinnen und Patienten mit multiple metastasierten Tumoren eine signifikant niedrigere nukleäre VDR- und auch CYP24A1-Expression im Vergleich zu Patientinnen und Patienten mit ausschließlich ossärer Metastasierung (pVDR=0.03, pCYP24A1=0.01, Abbildung 36). Die Proteinexpression des VDRs- und von CYP24A1 korrelierten signifikant (p=0.001). 
Somit konnte mit dieser Arbeit die Proteinexpression des VDRs und von CYP24A1 in Knochenmetastasen durch Immunhistologie nachgewiesen werden. Insgesamt wurde der VDR und CYP24A1 von Knochenmetastasen diverser Entität unterschiedlich stark exprimiert. Jedoch könnten insbesondere Patienten mit VDR-exprimierenden Knochenmetastasen von einer Vitamin D3-Supplementierung profitieren, die häufig einen 25-OH-Vitamin D3 Mangel  zeigen (165, 166). Ebenso könnte eine Untersuchung auf einen niedrigen VDR-Status in Primärtumoren dabei helfen, Krebspatienten mit einem hohen Metastasierungsrisiko zu identifizieren. Allerdings sind weitere und größere Studien inbesondere mit Evaluation des gesamten Vitamin D-Metabolismus und -Signalwegs notwendig, um diesen Zusammenhang weiter zu untersuchen.
N2  - Bone metastases are among the three most frequent sites of metastatic manifestation of late-stage cancers, particularly of prostate and breast cancers. Bone metastases often reduce patient’s quality of life due to skeletal-related events. Additionally, bone metastatic tumor treatment is predominantly restricted to palliative measures.
In preclinical studies, the biologically active form of vitamin D3, 1,25(OH)2-vitamin D3, has been demonstrated to have antiproliferative and differentiating effects on cancer cells (101, 102, 104), which are mostly mediated by binding to the vitamin D receptor (VDR). Moreover, the VDR expression itself may affect cancer growth and the metastatic potential to bone. For example, preclinically, it has been shown that VDR knockdown promotes bone metastases manifestation and growth (118). Furthermore, low VDR expression is associated to aggressive cancer characteristics in primary cancers (111, 113, 115) and also linked to earlier bone metastasis manifestation in breast cancer (120). In addition, there is evidence that 1,25(OH)2-vitamin D3- catabolism is altered in cancer cells. Thus, inactivation of local 1,25(OH)2-vitamin D3-levels in cancer cells may be increased (70, 121, 122). VDR and CYP24A1 expression could therefore be important concerning cancer progression and bone metastases manifestation and growth. However, there are currently no reports of studies investigating VDR expression and vitamin D-metabolism in bone metastases. The aim of this study was hence to assess VDR and CYP24A1 (vitamin D-catabolizing enzyme) expression in bone metastases of 66 patients secondary to prostate-, breast-, kidney-, lung-, follicular thyroid- and colorectal cancers using immunohistochemistry (132).
While the VDR was localised in the nucleus and cytoplasm, CYP24A1 was identified in the cytoplasm only. A high VDR nuclear protein expression was detected in 47/66 (71 %) and cytoplasmatic in 37/66 (56 %). 39/66 (59 %) of bone metastases had a high total VDR expression. CYP24A1 was also strongly expressed in 39/66 (59 %) of bone metastases. Expression levels were correlated to patient data and cancer characteristics. There was a non-significant trend of high-grade cancers towards low nuclear VDR expression (p=0.07, see figure 33). Additionally, patients with lymph node metastases (N-stage) tended to have a reduced bone metastatic VDR and CYP24A1 expression compared to patients without lymph node metastases (pVDR=0.15, pCYP24A1=0.06, see figure 35). There was no difference of VDR and CYP24A1 expression in bone metastases between locally advanced and small primary cancers (T-stage). Interestingly, patients with further metastases other than bone metastases had reduced nuclear VDR and CYP24A1 levels compared to patients without other distant metastases (pVDR=0.03, pCYP24A1=0.01, see figure 36). Nuclear VDR and CYP24A1 expression showed a significant positive correlation (p=0.001).
In conclusion, this study demonstrated that the VDR and CYP24A1 are widely expression in bone metastases of various origin. Therefore, patients with VDR-expressing bone metastases could, in particular, benefit from vitamin D3-supplementation, as vitamin D deficiency is frequent in patients with bone metastases (165, 166). Additionally, screening for a low VDR status in primary cancers could help to identify cancer patients at a high risk of metastasis. However, further and larger studies, that evaluate the entire vitamin D metabolism and signalling pathway, are needed to investigate this association.
KW  - Vitamin D3
KW  - Vitamin D
KW  - Vitamin D-Rezeptor
KW  - Knochenmetastasen
KW  - CYP24A1
KW  - vitamin d
KW  - vitamin d receptor
KW  - bone metastases
KW  - vdr
KW  - Knochenmetastase
KW  - Metastase
Y1  - 2023
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-321827
ER  -