Literature DB >> 9778510

Drosophila engrailed can substitute for mouse Engrailed1 function in mid-hindbrain, but not limb development.

M C Hanks1, C A Loomis, E Harris, C X Tong, L Anson-Cartwright, A Auerbach, A Joyner.   

Abstract

The Engrailed-1 gene, En1, a murine homologue of the Drosophila homeobox gene engrailed (en), is required for midbrain and cerebellum development and dorsal/ventral patterning of the limbs. In Drosophila, en is involved in regulating a number of key patterning processes including segmentation of the epidermis. An important question is whether, during evolution, the biochemical properties of En proteins have been conserved, revealing a common underlying molecular mechanism to their diverse developmental activities. To address this question, we have replaced the coding sequences of En1 with Drosophila en. Mice expressing Drosophila en in place of En1 have a near complete rescue of the lethal En1 mutant brain defect and most skeletal abnormalities. In contrast, expression of Drosophila en in the embryonic limbs of En1 mutants does not lead to repression of Wnt7a in the embryonic ventral ectoderm or full rescue of the embryonic dorsal/ventral patterning defects. Furthermore, neither En2 nor en rescue the postnatal limb abnormalities that develop in rare En1 null mutants that survive. These studies demonstrate that the biochemical activity utilized in mouse to mediate brain development has been retained by Engrailed proteins across the phyla, and indicate that during evolution vertebrate En proteins have acquired two unique functions during embryonic and postnatal limb development and that only En1 can function postnatally.

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Year:  1998        PMID: 9778510     DOI: 10.1242/dev.125.22.4521

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  23 in total

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5.  Regulation of cranial morphogenesis and cell fate at the neural crest-mesoderm boundary by engrailed 1.

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10.  Spatial analysis of expression patterns predicts genetic interactions at the mid-hindbrain boundary.

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