HYPOTAURINE REQUIREMENT FOR INVITRO DEVELOPMENT OF GOLDEN-HAMSTER ONE-CELL EMBRYOS INTO MORULAE AND BLASTOCYSTS, AND PRODUCTION OF TERM OFFSPRING FROM INVITRO-FERTILIZED OVA

被引:108
作者
BARNETT, DK
BAVISTER, BD
机构
[1] Animal Health/Biomedical Sci. Dept., University of Wisconsin, Madison, WI 53706
关键词
D O I
10.1095/biolreprod47.2.297
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
Almost 30 years after the first successful in vitro fertilization (IVF) in golden hamsters (Mesocricetus auratus), we report that IVF hamster embryos can develop in a chemically defined, protein-free culture medium into morulae and blastocysts, and produce normal offspring after transfer to recipients. When examined 96 h post-insemination, 82% (160/200) of IVF ova had cleaved to at least 2 cells, 55% (97/200) had developed beyond the 4-cell stage, and 22% (38/200) had developed into morulae/blastocysts. In vitro development of IVF embryos to greater-than-or-equal-to 8 cells was absolutely dependent on hypotaurine. Twenty living offspring were produced from transfer of IVF embryos to recipients, with an overall success rate of 5% and 17% for oviductal (2-cell) and uterine (8-cell/morulae) transfers, respectively. In vivo-fertilized pronucleate embryos collected 3 h after egg activation were less able to develop in vitro than embryos collected only 6 h later, revealing a critical influence of the oviduct within the first hours of embryo development. Hypotaurine partly compensated for the decreased oviductal exposure of early 1-cell embryos. Establishment of a key role for hypotaurine in hamster embryo development, support of IVF embryos to morula/blastocyst stages in vitro, and production of living offspring after IVF embryo transfer are significant steps towards the goal of obtaining comparative data on preimplantation embryogenesis.
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页码:297 / 304
页数:8
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