In canine species, in vitro maturation (IVM) rates of oocytes collected from anoestrous ovaries are low (<20%). Several IVM media have been tested without significant improvements. A critical step in the evaluation of culture conditions is the observation of the meiotic stage reached by the oocytes. The present study was designed to investigate the chromatin patterns of in vitro matured oocytes by visualizing Germinal Vesicle (GV) and Germinal Vesicle Breakdown (GVBD) structures at 72 h of IVM. Nuclear stages of 1678 oocytes were evaluated by confocal microscopy after IVM. 1204 oocytes were non-degenerated, and 94.4% were still immature and at GV stage. Five different patterns of chromatin configuration were observed. Higher percentages of oocytes with unmodified GV and with diffuse (58%; Type A) and filamentous chromatin (19%; Type B) were observed in comparison with those with modifications in the GV such as patched chromatin (12.5%; Type C), surrounded-nucleolus (3%; Type D) and in vivo type chromatin/fully grouped chromatin (2.5%; Type E). These results indicate that GVBD (absence of nucleolus, nucleus breakdown) is rarely observed in vitro. The percentage of type C-D-E GVs and MI (meiotic resumption) and of MII (completion of meiosis) can be used to evaluate meiotic resumption after IVM. Our results indicate that although a low number of in vitro matured oocytes exhibit the chromatin configurations observed in in vivo collected oocytes, chromatin changes in the GV can be induced during IVM.
(1) (2) (communication présentée le 17 février 2005) L'ovocyte de chienne constitue un modèle de méiose très particulier parmi les mammifères. Sa maturation in vitro, étudiée depuis une dizaine d'années seulement, reste très mal maîtrisée : faible taux de métaphase II (10 à 20 % contre plus de 90 % chez les bovins) et fort taux de dégénérescence en culture (20 à 60 %) malgré les essais d'amélioration des milieux de culture. Or la maturation in vitro est une étape indispensable pour avoir accès, tant chez le chien que chez les Canidés en voie de disparition, aux biotechnologies de la reproduction (fécondation et production d'embryons in vitro notamment). Il est indispensable de mieux comprendre la biologie de l'ovocyte chez la chienne pour amé-liorer les taux de maturation. Nous nous sommes intéressées, en premier lieu, au rôle de l'AMPc dans la reprise de la méiose in vitro. Nous avons modulé la concentration intraovocytaire d'AMPc en soumettant les ovocytes à des molécules qui la diminuent (Rp-AMPc) ou l'augmentent (dbAMPc et forskoline), ou en dénudant l'ovocyte pour arrêter tout apport par les cellules du cumulus. Nous avons ainsi montré que l'AMPc jouerait un rôle dans la poursuite de la méiose dont la reprise serait éga-lement contrôlée par une autre voie, peut-être calcique. En parallèle, nous explorons l'évolution de l'ultrastructure de l'ovocyte au cours de la maturation in vivo et in vitro, pour détecter les anomalies cytoplasmiques qui peuvent apparaître au cours de la maturation.
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