A Mutation in Mouse rad51 Results in an Early Embryonic Lethal That Is Suppressed by a Mutation in p53

1 December 1996

journal article
research article
Published by Taylor & Francis in Molecular and Cellular Biology

Vol. 16 (12) , 7133-7143
https://doi.org/10.1128/mcb.16.12.7133

Abstract

RecA in Escherichia coli and its homolog, ScRad51 in Saccharomyces cerevisiae, are known to be essential for recombinational repair. The homolog of RecA and ScRad51 in mice, MmRad51, was mutated to determine its function. Mutant embryos arrested early during development. A decrease in cell proliferation, followed by programmed cell death and chromosome loss, was observed. Radiation sensitivity was demonstrated in trophectoderm-derived cells. Interestingly, embryonic development progressed further in a p53 null background; however, fibroblasts derived from double-mutant embryos failed to proliferate in tissue culture.

Keywords

This publication has 89 references indexed in Scilit:

Requirement for Ku80 in growth and immunoglobulin V(D)J recombination
Nature, 1996
p53 Status and the Efficacy of Cancer Therapy in Vivo
Science, 1994
Catalysis of ATP-Dependent Homologous DNA Pairing and Strand Exchange by Yeast RAD51 Protein
Science, 1994
p53 is required for radiation-induced apoptosis in mouse thymocytes
Nature, 1993
DNA Double-strand Breaks: Their Repair and Relationship to Cell Killing in Yeast
International Journal of Radiation Biology, 1990
Cloning and expression of the mouse pgk-1 gene and the nucleotide sequence of its promoter
Gene, 1987
Differential Effects of Polyadenylation Regions on Gene Expression in Mammalian Cells
DNA, 1986
Molecular aspects of aging
Molecular Aspects of Medicine, 1985
A general method for determining the replicative age of normal animal cell cultures
Mechanisms of Ageing and Development, 1980
Repair of DNA double-strand breaks in Escherichia coli, which requires recA function and the presence of a duplicate genome
Journal of Molecular Biology, 1977