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Glioblastomas are characterized by an aggressive local growth pattern, a marked degree of invasiveness and poor prognosis. Tumor invasiveness is facilitated by the increased activity of proteolytic enzymes which are involved in destruction of the extracellular matrix of the surrounding healthy brain tissue. Elevated levels of matrix metalloproteinases (MMPs) were found in glioblastoma (GBM) cell-lines, as well as in GBM biopsies as compared with low-grade astrocytoma (LGA) and normal brain samples, indicating a role in malignant progression. A careful review of the available literature revealed that both the expression and role of several of the 23 human MMP proteins is controversely discussed and for some there are no data available at all. We therefore screened a panel of 15 LGA and 15 GBM biopsy samples for those MMPs for which there is either no, very limited or even contradictory data available. Hence, this is the first complete compilation of the expression pattern of all 23 human MMPs in astrocytic tumors. This study will support a better understanding of the specific expression patterns and interaction of proteolytic enzymes in malignant human glioma and may provide additional starting points for targeted patient therapy.
As recently reviewed, 1026 neuroprotective drug candidates in stroke research have all failed on their road towards validation and clinical translation, reasons being quality issues in preclinical research and publication bias. Quality control guidelines for preclinical stroke studies have now been established. However, sufficient understanding of the underlying mechanisms of neuronal death after stroke that could be possibly translated into new therapies is lacking. One exception is the hypothesis that cellular death is mediated by oxidative stress. Oxidative stress is defined as an excess of reactive oxygen species (ROS) derived from different possible enzymatic sources. Among these, NADPH oxidases (NOX1-5) stand out as they represent the only known enzyme family that has no other function than to produce ROS. Based on data from different NOX knockout mouse models in ischemic stroke, the most relevant isoform appears to be NOX4. Here we discuss the state-of-the-art of this target with respect to stroke and open questions that need to be addressed on the path towards clinical translation.
The two bradykinin receptors B1R and B2R are central components of the kallikrein–kinin system with different expression kinetics and binding characteristics. Activation of these receptors by kinins triggers inflammatory responses in the target organ and in most situations enhances tissue damage. We could recently show that blocking of B1R, but not B2R, protects from cortical cryolesion by reducing inflammation and edema formation. In the present study, we investigated the role of B1R and B2R in a closed head model of focal traumatic brain injury (TBI; weight drop). Increased expression of B1R in the injured hemispheres of wild-type mice was restricted to the later stages after brain trauma, i.e. day 7 (P<0.05), whereas no significant induction could be observed for the B2R (P>0.05). Mice lacking the B1R, but not the B2R, showed less functional deficits on day 3 (P<0.001) and day 7 (P<0.001) compared with controls. Pharmacological blocking of B1R in wild-type mice had similar effects. Reduced axonal injury and astroglia activation could be identified as underlying mechanisms, while inhibition of B1R had only little influence on the local inflammatory response in this model. Inhibition of B1R may become a novel strategy to counteract trauma-induced neurodegeneration.
Inflammation following ischaemic stroke attracts high priority in current research, particularly using human-like models and long-term observation periods considering translational aspects. The present study aimed on the spatio-temporal course of macrophage-like cell accumulation after experimental thromboembolic stroke and addressed microglial and astroglial reactions in the ischaemic border zone. Further, effects of tissue plasminogen activator (tPA) as currently best treatment for stroke and the potentially neuroprotective co-administration of hyperbaric oxygen (HBO) were investigated. Rats underwent middle cerebral artery occlusion and were assigned to control, tPA or tPA+HBO. Twenty-four hours, 7, 14 and 28 days were determined as observation time points. The accumulation of macrophage-like cells was semiquantitatively assessed by CD68 staining in the ischaemic area and ischaemic border zone, and linked to the clinical course. CD11b, ionized calcium binding adaptor molecule 1 (Iba), glial fibrillary acidic protein (GFAP) and Neuronal Nuclei (NeuN) were applied to reveal delayed glial and neuronal alterations. In all groups, the accumulation of macrophage-like cells increased distinctly from 24 hours to 7 days post ischaemia. tPA+HBO tended to decrease macrophage-like cell accumulation at day 14 and 28. Overall, a trend towards an association of increased accumulation and pronounced reduction of the neurological deficit was found. Concerning delayed inflammatory reactions, an activation of microglia and astrocytes with co-occurring neuronal loss was observed on day 28. Thereby, astrogliosis was found circularly in contrast to microglial activation directly in the ischaemic area. This study supports previous data on long-lasting inflammatory processes following experimental stroke, and additionally provides region-specific details on glial reactions. The tendency towards a decreasing macrophage-like cell accumulation after tPA+HBO needs to be discussed critically since neuroprotective properties were recently ascribed to long-term inflammatory processes.
Parent of origin imprints on the genome have been implicated in the regulation of neural cell type differentiation. The ability of human parthenogenetic (PG) embryonic stem cells (hpESCs) to undergo neural lineage and cell type-specific differentiation is undefined. We determined the potential of hpESCs to differentiate into various neural subtypes. Concurrently, we examined DNA methylation and expression status of imprinted genes. Under culture conditions promoting neural differentiation, hpESC-derived neural stem cells (hpNSCs) gave rise to glia and neuron-like cells that expressed subtype-specific markers and generated action potentials. Analysis of imprinting in hpESCs and in hpNSCs revealed that maternal-specific gene expression patterns and imprinting marks were generally maintained in PG cells upon differentiation. Our results demonstrate that despite the lack of a paternal genome, hpESCs generate proliferating NSCs that are capable of differentiation into physiologically functional neuron-like cells and maintain allele-specific expression of imprinted genes. Thus, hpESCs can serve as a model to study the role of maternal and paternal genomes in neural development and to better understand imprinting-associated brain diseases.
Hintergrund: Obwohl als Standardverfahren bei der intraoperativen Überwachung bei der Akustikusneurinom (AN)-Chirurgie etabliert, handelt es sich bei der Ableitung akustisch evozierter Potentiale (AEP) um eine „Far-Field“-Technik mit einigen Einschränkungen. Diese Arbeit soll die Elektrocochleographie (ECoG) als Zusatzverfahren für den Hörerhalt überprüfen. Material und Methoden: 84 Patienten mit einseitigem intra-/extrameatalem AN (extrameataler Durchmesser 5-55mm) mit noch vorhandener Hörfunktion wurden unter Verwendung eines kombinierten neuro-/otochirurgischen suboccipitalen Zugangs operiert. Nach Einbringung einer Nadelelektrode auf das Promontorium unter otoskopischer Kontrolle wurden ECoG und AEP simultan abgeleitet. Ergebnisse: Bei 43 von 84 Patienten wurde ein Hörerhalt erzielt, wobei davon 40 sowohl AEP als auch ECoG aufwiesen. Alle 24 Patienten mit Verlust beider Modalitäten wurden taub. Hörerhalt wurde bei 4 von 12 Patienten mit erhaltenem ECoG, aber Verlust des AEP (Wellen III-V) nachgewiesen, im umgekehrten Fall kam es zu postoperativer Taubheit in zwei Fällen. Trotz signifikanter Korrelation der AEP- und ECoG-Amplituden mit prä- und postoperativem Hören, erwiesen sich die Latenzen von Summations- und Aktionspotential als verläßlichere Indikatoren für Hörerhalt als beim AEP. Der Vorhersagewert erloschener AEP-Amplituden übertraf den der ECoG-Parameter. Nur bei Tumoren über 2cm war die Größe signifikant für den Hörerhalt. Außer postoperativer Otoliquorrhoe (3 Patienten) und einer lokalen Blutung im äußeren Gehörgang (1 Patient) wurden keine Nebenwirkungen beobachtet. Schlußfolgerung: Die ECoG-Ableitung erweist sich in Kombination mit AEPs als nützliches Zusatzverfahren zum Hörerhalt in der AN-Chirurgie. Besonders hilfreich ist es bei Verwendung der Bipolar-Pinzette sowie beim Bohren, da keine Mittelung notwendig ist. Spezielle Anwendungsmöglichkeiten sind kleine Tumoren mit funktioneller Hörfunktion und/oder einem großen intrameatalen Anteil sowie Fälle mit verlorenem oder gefährdetem kontralateralen Hören (z. B. bilaterale AN), wenn sogar der Erhalt von nicht-funktionellem Hören wünschenswert ist.