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Use of triple tissue blastocyst reconstitution to study the development of diploid parthenogenetic primitive ectoderm in combination with fertilization-derived trophectoderm and primitive endoderm

Published online by Cambridge University Press:  14 April 2009

R. L. Gardner ,
S. C. Barton  and
M. A. H. Surani
R. L. Gardner*
Affiliation:
Imperial Cancer Research Fund, Developmental Biology Unit, Department of Zoology, South Parks Road, Oxford, OX1 3PS
S. C. Barton
Affiliation:
Department of Molecular Embryology, AFRC Institute of Animal Physiology and Genetics Research, Cambridge Research Station, Babraham Hall, Cambridge, CB2 4AT
M. A. H. Surani
Affiliation:
Department of Molecular Embryology, AFRC Institute of Animal Physiology and Genetics Research, Cambridge Research Station, Babraham Hall, Cambridge, CB2 4AT
*
Corresponding author.
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Diploid mouse conceptuses lacking a paternal genome can form morphologically normal but small fetuses of up to 25 somites, but they invariably fail to develop beyond mid-gestation. Such conceptuses differ from normal most notably in the poor development of extra-embryonic tissues which are largely of trophectodermal and primitive endodermal origin. However, it is not clear whether the demise of diploid parthenogenetic (P) or gynogenetic (G) conceptuses is attributable entirely to the defective development of these two tissues or whether differentiation of the primitive ectoderm, the precursor of the foetus, extra-embryonic mesoderm and amnion, is also impaired by the absence of a paternal genome. Therefore, a new blastocyst reconstitution technique was used which enabled primitive ectoderm from P blastocysts to be combined with primitive endoderm and trophectoderm from fertilization-derived (F) blastocysts. One third of the ‘triple tissue’ reconstituted blastocysts that implanted yielded foetuses. However, all foetuses recovered on the llth or 12th day of gestation were small and, with one exception, either obviously retarded or arrested in development. The exception was a living 44 somite specimen which is the most advanced P foetus yet recorded. Foetuses were invariably degenerating in conceptuses recovered on the 13th day. In contrast, at least 16% of control reconstituted blastocysts with primitive ectoderm as well as primitive endoderm and trophectoderm of F origin developed normally on the 13th day of gestation or to term. Hence, the presence of a paternal genome seems to be essential for normal differentiation of all 3 primary tissues of the mouse blastocyst.

The P foetuses that developed from reconstituted blastocysts were so closely invested by their membranes that they often showed abnormal flexure of the posterior region of the body. Several also showed a deficiency of allantoic tissue. Therefore, the possibility that the defect in development of P primitive ectoderms resided in their extra-embryonic tissues was investigated by analysing a series of chimaeras produced by injecting them into intact F blastocysts. The foregoing anomalies were not discernible even when P cells made a large contribution to the extra-embryonic mesoderm or amnion plus umbilical cord. Furthermore, selection against P cells was no greater in extra-embryonic derivatives of the primitive ectoderm than in the foetus itself.

Type
Research Article
Information
Genetics Research , Volume 56 , Issue 2-3 , October 1990 , pp. 209 - 222
Copyright
Copyright © Cambridge University Press 1990

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