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

Mark Hanks; Wolfgang Wurst; Lynn Anson-Cartwright; Anna B. Auerbach; Alexandra L. Joyner

doi:10.1126/science.7624797

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

Mark Hanks
, Wolfgang Wurst
, Lynn Anson-Cartwright
, Anna B. Auerbach
, Alexandra L. Joyner

Mount Sinai Hospital of University of Toronto
Procter and Gamble Pharmaceuticals
Helmholtz Zentrum München German Research Center for Environmental Health
New York University (NYU)

Research output: Contribution to journal › Article › peer-review

372 Scopus citations

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.

Original language	English
Pages (from-to)	679-682
Number of pages	4
Journal	Science
Volume	269
Issue number	5224
DOIs	https://doi.org/10.1126/science.7624797
State	Published - 1995
Externally published	Yes

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title = "Rescue of the En-1 mutant phenotype by replacement of En-1 with En-2",

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.",

author = "Mark Hanks and Wolfgang Wurst and Lynn Anson-Cartwright and Auerbach, \{Anna B.\} and Joyner, \{Alexandra L.\}",

year = "1995",

doi = "10.1126/science.7624797",

language = "English",

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T1 - Rescue of the En-1 mutant phenotype by replacement of En-1 with En-2

AU - Hanks, Mark

AU - Wurst, Wolfgang

AU - Anson-Cartwright, Lynn

AU - Auerbach, Anna B.

AU - Joyner, Alexandra L.

PY - 1995

Y1 - 1995

N2 - 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.

AB - 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.

UR - https://www.scopus.com/pages/publications/0029059790

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VL - 269

SP - 679

EP - 682

JO - Science

JF - Science

IS - 5224

ER -

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

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