H beta 58, an insertional mutation affecting early postimplantation development of the mouse embryo

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H beta 58, an insertional mutation affecting early postimplantation development of the mouse embryo

G Radice, JJ Lee and F Costantini
Department of Genetics and Development, College of Physicians and Surgeons, Columbia University, New York, NY 10032.

The generation and analysis of insertional mutations affecting mouse embryogenesis provides a powerful method to identify new genes that function in early development. In this paper, we describe an insertional mutation that interferes with postimplantation mouse development beginning at the time of gastrulation. Embryos homozygous for the H beta 58 transgenic insertion developed normally through the early postimplantation, egg cylinder stage (day 6.5 of development). At the primitive streak stage (day 7.5), however, they began to display characteristic abnormalities, including a retardation in the growth of the embryonic ectoderm (the earliest identifiable defect), and in some cases abnormalities of the amnion and chorion. Homozygotes continued to develop for 2-3 more days, reaching the size of a normal 8.5 day embryo, and formed tissues representative of all three germ layers, including several differentiated cell types. The site of insertion was mapped, by a combination of cytogenetic and genetic methods, to chromosome 10, and it appeared to define a new genetic locus. The inserted transgene provided a probe to clone and characterize the mutant locus, as well as the corresponding wild-type locus. In addition to an insertion of 10-20 copies of the transgene, the mutant locus contained a deletion of 2-3 kb of DNA found at the wild-type locus, and possibly an insertion of mouse repetitive DNA. However, genomic sequences on both sides of the insertion site remained co-linear in the wild-type and mutant genomes, and no chromosomal abnormalities could be detected. Five single copy DNA probes spanning the insertion site were tested for their ability to hybridize to RNA from 8.5 day embryos; one of the probes (located within the region deleted from the mutant chromosome) hybridized to a 2.7 kb mRNA encoded at the H beta 58 locus, thus identifying a gene whose disruption appears to be responsible for the mutant phenotype.

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				S. Strope, R. Rivi, T. Metzger, K. Manova, and E. Lacy Mouse amnionless, which is required for primitive streak assembly, mediates cell-surface localization and endocytic function of cubilin on visceral endoderm and kidney proximal tubules Development, October 1, 2004; 131(19): 4787 - 4795. [Abstract] [Full Text] [PDF]

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				W S Chen, K Manova, D C Weinstein, S A Duncan, A S Plump, V R Prezioso, R F Bachvarova, and J E Darnell Disruption of the HNF-4 gene, expressed in visceral endoderm, leads to cell death in embryonic ectoderm and impaired gastrulation of mouse embryos. Genes & Dev., October 15, 1994; 8(20): 2466 - 2477. [Abstract] [PDF]

				A K Bachhawat, J Suhan, and E W Jones The yeast homolog of H < beta > 58, a mouse gene essential for embryogenesis, performs a role in the delivery of proteins to the vacuole. Genes & Dev., June 15, 1994; 8(12): 1379 - 1387. [Abstract] [PDF]

				A D Reith and A Bernstein Molecular basis of mouse developmental mutants. Genes & Dev., July 1, 1991; 5(7): 1115 - 1123. [PDF]