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Literature DB >> 7624797

Rescue of the En-1 mutant phenotype by replacement of En-1 with En-2.

M Hanks¹, W Wurst, L Anson-Cartwright, A B Auerbach, A L Joyner.

Abstract

The related mouse Engrailed genes En-1 and En-2 are expressed from the one- and approximately five-somite stages, respectively, in a similar presumptive mid-hindbrain domain. However, mutations in En-1 and En-2 produce different phenotypes. En-1 mutant mice die at birth with a large mid-hindbrain deletion, whereas En-2 mutants are viable, with cerebellar defects. To determine whether these contrasting phenotypes reflect differences in temporal expression or biochemical activity of the En proteins, En-1 coding sequences were replaced with En-2 sequences by gene targeting. This rescued all En-1 mutant defects, demonstrating that the difference between En-1 and En-2 stems from their divergent expression patterns.

Entities: Disease Gene Species

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Year: 1995 PMID： 7624797 DOI： 10.1126/science.7624797

Source DB: PubMed Journal: Science ISSN： 0036-8075 Impact factor: 47.728

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Cited

106 in total

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10. The exon 8-containing prosaposin gene splice variant is dispensable for mouse development, lysosomal function, and secretion.

Authors: Tsadok Cohen; Wojtek Auerbach; Liat Ravid; Jacques Bodennec; Amos Fein; Anthony H Futerman; Alexandra L Joyner; Mia Horowitz
Journal: Mol Cell Biol Date: 2005-03 Impact factor: 4.272

Rescue of the En-1 mutant phenotype by replacement of En-1 with En-2.

1. The role of population size, pleiotropy and fitness effects of mutations in the evolution of overlapping gene functions.

Review 2. Molecular regulation of cytokine gene expression during the immune response.

3. Divergent functions of the proneural genes Mash1 and Ngn2 in the specification of neuronal subtype identity.

4. Neuron-restricted expression of the rat gonadotropin-releasing hormone gene is conferred by a cell-specific protein complex that binds repeated CAATT elements.

5. Two lineage boundaries coordinate vertebrate apical ectodermal ridge formation.

6. N-myc can functionally replace c-myc in murine development, cellular growth, and differentiation.

7. Increased atherosclerosis in hyperlipidemic mice deficient in alpha -tocopherol transfer protein and vitamin E.

8. Duplicate genes and robustness to transient gene knock-downs in Caenorhabditis elegans.

9. Functional Equivalence of the SOX2 and SOX3 Transcription Factors in the Developing Mouse Brain and Testes.

10. The exon 8-containing prosaposin gene splice variant is dispensable for mouse development, lysosomal function, and secretion.