Forschung am Menschen und ihre kulturellen Folgen : eine Betrachtung aus ethischer Sicht

(Résumé de l'ouvrage) Dürfen Forscherinnen und Forscher Embryonen und Föten für den medizinischen Fortschritt verwenden? Wie soll die Verwendung von medizinischen Daten geregelt werden, welche für andere Zwecke erfasst wurden (z. B. Blutproben)? Worin bestehen die Hoffnungen und Grenzen der klinischen Tests? Wie verhält sich die Politik bzw. die Gesellschaft angesichts dieser brisanten wissenschaftspolitischen Fragen? Das Bundesgesetz über die Forschung am Menschen wird Bereiche regeln, die bisher kaum oder überhaupt nicht gesetzlich erfasst sind. Wegen der Fortschritte in der biomedizinischen Forschung wächst der gesetzliche Regelungsbedarf für Bereiche wie die klinischen Tests, die biomedizinische Forschung an Embryonen und Föten sowie den Umgang mit entnommenem biologischem Material (u. a. Plazenta, Nabelschnurblut, Gewebeproben). Der zweite Band der Reihe «SCIENCE & SOCIETY» enthält Positionen von Wissenschaftlerinnen und Wissenschaftlern aus Natur- und Sozialwissenschaften sowie von Mitgliedern der Eidgenössischen Räte. Francis Fukuyama (Bioethikrat des US-amerikanischen Präsidenten), Jan von Overbeck (Swiss Re), Heidi Diggelmann (Nationaler Forschungsrat, Schweizerischer Nationalfonds), Christoph Rehmann-Sutter (Nationale Ethikkommission im Bereich Humanmedizin) und Thomas Zeltner (Bundesamt für Gesundheit) sowie Expertinnen und Experten aus dem In- und Ausland diskutieren das Thema «Forschung am Menschen» aus der gesellschaftspolitischen, juristischen, naturwissenschaftlichen und ethi- schen Perspektive. Reports der Diskussionen vermitteln zusätzliche interessante Aufschlüsse.

Assessing the associations between mental disorders, cardiovascular risk factors, and cardiovascular disease : the CoLaus/PsyCoLaus study

Background: Cardio-vascular diseases (CVD), their well established risk factors (CVRF) and mental disorders are common and co-occur more frequently than would be expected by chance. However, the pathogenic mechanisms and course determinants of both CVD and mental disorders have only been partially identified.Methods/Design: Comprehensive follow-up of CVRF and CVD with a psychiatric exam in all subjects who participated in the baseline cross-sectional CoLaus study (2003-2006) (n=6'738) which also included a comprehensive genetic assessment. The somatic investigation will include a shortened questionnaire on CVRF, CV events and new CVD since baseline and measurements of the same clinical and biological variables as at baseline. In addition, pro-inflammatory markers, persistent pain and sleep patterns and disorders will be assessed. In the case of a new CV event, detailed information will be abstracted from medical records. Similarly, data on the cause of death will be collected from the Swiss National Death Registry. The comprehensive psychiatric investigation of the CoLaus/PsyCoLaus study will use contemporary epidemiological methods including semi-structured diagnostic interviews, experienced clinical interviewers, standardized diagnostic criteria including threshold according to DSM-IV and sub-threshold syndromes and supplementary information on risk and protective factors for disorders. In addition, screening for objective cognitive impairment will be performed in participants older than 65 years.Discussion: The combined CoLaus/PsyCoLaus sample provides a unique opportunity to obtain prospective data on the interplay between CVRF/CVD and mental disorders, overcoming limitations of previous research by bringing together a comprehensive investigation of both CVRF and mental disorders as well as a large number of biological variables and a genome-wide genetic assessment in participants recruited from the general population.

Toxoplasma gondii and the Immunity-Related GTPase (IRG) resistance system in mice: a review

The Immunity Related GTPases (IRG proteins) constitute a large family of interferon-inducible proteins that mediate early resistance to Toxoplasma gondii infection in mice. At least six members of this family are required for resistance of mice to virulent T. gondii strains. Recent results have shown that the complexity of the resistance arises from complex regulatory interactions between different family members. The mode of action against T. gondii depends on the ability of IRG proteins to accumulate on the parasitophorous vacuole of invading tachyzoites and to induce local damage to the vacuole resulting in disruption of the vacuolar membrane. Virulent strains of T. gondiiovercome the IRG resistance system, probably by interfering with the loading of IRG proteins onto the parasitophorous vacuole membrane. It may be assumed that T. gondii strains highly virulent for mice will be disadvantaged in the wild due to the rapid extinction of the infected host, while it is self-evident that susceptibility to virulent strains is disadvantageous to the mouse host. We consider the possibility that this double disadvantage is compensated in wild populations by segregating alleles with different resistance and susceptibility properties in the IRG system.

Towards an understanding of the epigenetics of schistosomes: a comparative epigenomic study

As in perhaps all eukaryotes, schistosomes use a supplementary information transmitting system, the epigenetic inheritance system, to shape genetic information and to produce different phenotypes. In contrast to other important parasites, the study of epigenetic phenomena in schistosomes is still in its infancy. Nevertheless, we are beginning to grasp what goes on behind the epigenetic scene in this parasite. We have developed techniques of native chromatin immunoprecipitation (N-ChIP) and associated the necessary bioinformatics tools that allow us to run genome-wide comparative chromatin studies on Schistosoma mansoni at different stages of its life cycle, on different strains and on different sexes. We present here an application of such an approach to study the genetic and epigenetic basis for a phenotypic trait, the compatibility of S. mansoni with its invertebrate host Biomphalaria glabrata. We have applied the ChIP procedure to two strains that are either compatible or incompatible with their intermediate host. The precipitated DNA was sequenced and aligned to a reference genome and this information was used to determine regions in which both strands differ in their genomic sequence and/or chromatin structure. This procedure allowed us to identify candidate genes that display either genetic or epigenetic difference between the two strains.

Coloritto ([Edition augmentée de l'appendice et des 4 pl. (2 versions supplémentaires du visage de femme, accompagnées des deux palettes de couleurs correspondantes) ]) / ; or the harmony of colouring in painting : reduced to mechanical practice, under easy precepts, and infallible rules ; together with some colour'd figures, in order to render the said precepts and rules intelligible, not only to painters, but even to all lovers of painting. By J. C. Le Blon.

Ancien possesseur : Ledoux-Lebard, Guy (1912-2003)

Specific processing of tenascin-C by the metalloprotease meprin beta neutralizes its inhibition of cell spreading

The metalloprotease meprin has been implicated in tissue remodelling due to its capability to degrade extracellular matrix components. Here, we investigated the susceptibility of tenascin-C to cleavage by meprin beta and the functional properties of its proteolytic fragments. A set of monoclonal antibodies against chicken and human tenascin-C allowed the mapping of proteolytic fragments generated by meprin beta. In chicken tenascin-C, meprin beta processed all three major splicing variants by removal of 10 kDa N-terminal and 38 kDa C-terminal peptides, leaving a large central part of subunits intact. IN similar cleavage pattern was found for large human tenascin-C variant where two N-terminal peptides (10 or 15 kDa) and two C-terminal fragments (40 and 55 kDa) were removed from the intact subunit. N-terminal sequencing revealed the exact amino acid positions of cleavage sites. In both chicken and human tenascin-C N-terminal cleavages occurred just before and/or after the heptad repeats involved in subunit oligomerization. In the human protein, an additional cleavage site was identified in the alternative fibronectin type III repeat D. Whereas all these sites are known to be attacked by several other proteases, a unique cleavage by meprin beta was located to the 7th constant fibronectin type III repeat in both chicken and human tenascin-C, thereby removing the C-terminal domain involved in its anti-adhesive activity. In cell adhesion assays meprin beta-digested human tenascin-C was not able to interfere with fibronectin-mediated cell spreading, confirming cleavage in the anti-adhesive domain. Whereas the expression of meprin beta and tenascin-C does not overlap in normal colon tissue, inflamed lesions of the mucosa from patients with Crohn's disease exhibited many meprin beta-positive leukocytes in regions where tenascin-C was strongly induced. Our data indicate that, at least under pathological conditions, meprin beta might attack specific functional sites in tenascin-C that are important for its oligomerization and anti-adhesive activity. (C) 2009 Elsevier B.V. All rights reserved.

Le contact Gondwana - péri-Gondwana dans le Zanskar oriental (Ladakh-Himalaya)

A l'Est du fleuve Zanskar (Ladakh), la zone de suture de l'Indus sépare les nappes de la bordure nord-indienne du Gondwana (Haut-Himalaya, nappes du Zanskar, cristallin de Tso Morari) des éléments péri·gondwaniens du Trans-himalaya. Des recherches géologiques entreprises entre l'Indus el la Tsarap ont montré que: - la molasse autochlone du Ladakh est surmontée par un édifice de flysch et molasses tertiaires, rétrocharrié vers le NordEst et coiffé par les conglomérats post· éocène moyen du Stok Kangri et une formation eontinentale de molasse rouge; - - la zone de suture comprend deux unités. principales : a) au Nord et au Nord-Ouest, l'unité volcano-sédimentaire de Dras-Nindam avec des conglomérats et flysch crétacés, des brèches massives à radiolarHes et roches vertes; cette unité est accompagnée d'un mélange coloré à roches ultra-basiques, blocs exoti(Iues divers et une méga lentille de brèche carbonatée polygénique à grands Foraminifères (Nummulites ?) ; b) au Sud, l'unité de la Markha, un flysch à lentilles de calcaires plus ou moins marmoréens datée de la base du Jurassique moyen et que nons corrélons avec le Oysch de Lamayuru ; - l'unité complexe de Nimaling représente la terminaison occidentale du crist allin de Rupshn (Tso MOI'ari) ; il comprend un socle gneissique, des roches vert.es et une couverture de schistes quartzitiques, quartzites el dolomies. Cet ensemble est intrudé pal' un granite porphyrique et il est surmonté, en contact tectonique, par une épaisse série métamorphique de calcschistes, shales et grès de faciès schistes lustrés, d'âge inconnu; dans ce tte série, on note au moins trois phases de fortes déformaljons superposées (linéations replissées) ; le long de la vallée de la Markha, le style st.ructural évoque, avec des plis isoclinaux de 2" phase à axes verticaux, une « zone de racine" et pourrait également témoigner de mouvements horizontaux importants; - l'édifice des napp es du Zanskar a été subdivisé en trois unités; il surmonte vers le Nord-Est les schistes lustrés du groupe de Langtang et vient buter vers le Sud-Ouest, le long d'un aceident chevauchant, contre la nappe de Zangla (Haut Himalaya). Les séries sédimentaires (Trias - Crétacé supérieur) sont d'affinité téthysienne. De nouvelles datations sont apportées et nous mettons en évidence, directement à l'Est du fleuve Zanskar, la présence de Crétacé sous faciès calcaires multicolores à microfaune planctique ; transgressif sur les grès de Giumal, ce faciès calcaire déhut.e déjà dans l'Alhien supérieur, c'est-à-dire nellement plus tôt que dans les régions plus orientales de l 'Himalaya; - les nappes du Haut Himalaya comprennent du Nord-Est vers le Sud-Ouest la nappe de Zangla qui chevauche par l'intermédiaire d'une semelle de « Panjal Traps » des témoins écaillés de Paléozoïque inférieur, puis la nappe de cristallin. La nappe de Zangla correspond à l'unité qui, à l 'Ouest du Zanskar supporte la klippe ophiolitique de Spongtang.

Anti-CD154 mAb and rapamycin induce T regulatory cell mediated tolerance in rat-to-mouse islet transplantation.

BACKGROUND: Anti-CD154 (MR1) monoclonal antibody (mAb) and rapamycin (RAPA) treatment both improve survival of rat-to-mouse islet xenograft. The present study investigated the effect of combined RAPA/MR1 treatment on rat-to-mouse islet xenograft survival and analyzed the role of CD4(+)CD25(+)Foxp3(+) T regulatory cells (Treg) in the induction and maintenance of the ensuing tolerance. METHODOLOGY/PRINCIPAL FINDINGS: C57BL/6 mice were treated with MR1/RAPA and received additional monoclonal anti-IL2 mAb or anti CD25 mAb either early (0-28 d) or late (100-128 d) post-transplantation. Treg were characterised in the blood, spleen, draining lymph nodes and within the graft of tolerant and rejecting mice by flow cytometry and immunohistochemistry. Fourteen days of RAPA/MR1 combination therapy allowed indefinite islet graft survival in >80% of the mice. Additional administration of anti-IL-2 mAb or depleting anti-CD25 mAb at the time of transplantation resulted in rejection (100% and 89% respectively), whereas administration at 100 days post transplantation lead to lower rejection rates (25% and 40% respectively). Tolerant mice showed an increase of Treg within the graft and in draining lymph nodes early post transplantation, whereas 100 days post transplantation no significant increase of Treg was observed. Rejecting mice showed a transient increase of Treg in the xenograft and secondary lymphoid organs, which disappeared within 7 days after rejection. CONCLUSIONS/SIGNIFICANCES: These results suggest a critical role for Treg in the induction phase of tolerance early after islet xenotransplantation. These encouraging data support the need of developing further Treg therapy for overcoming the species barrier in xenotransplantation.

Impairment of mossy fiber long-term potentiation and associative learning in pituitary adenylate cyclase activating polypeptide type I receptor-deficient Mice

The pituitary adenylate cyclase activating polypeptide (PACAP) type I receptor (PAC1) is a G-protein-coupled receptor binding the strongly conserved neuropeptide PACAP with 1000-fold higher affinity than the related peptide vasoactive intestinal peptide. PAC1-mediated signaling has been implicated in neuronal differentiation and synaptic plasticity. To gain further insight into the biological significance of PAC1-mediated signaling in vivo, we generated two different mutant mouse strains, harboring either a complete or a forebrain-specific inactivation of PAC1. Mutants from both strains show a deficit in contextual fear conditioning, a hippocampus-dependent associative learning paradigm. In sharp contrast, amygdala-dependent cued fear conditioning remains intact. Interestingly, no deficits in other hippocampus-dependent tasks modeling declarative learning such as the Morris water maze or the social transmission of food preference are observed. At the cellular level, the deficit in hippocampus-dependent associative learning is accompanied by an impairment of mossy fiber long-term potentiation (LTP). Because the hippocampal expression of PAC1 is restricted to mossy fiber terminals, we conclude that presynaptic PAC1-mediated signaling at the mossy fiber synapse is involved in both LTP and hippocampus-dependent associative learning.