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The murine dilute suppressor gene encodes a cell autonomous suppressor.
Author(s) -
K J Moore,
Deborah A. Swing,
Neal G. Copeland,
N.A. Jenkins
Publication year - 1994
Publication title -
genetics.
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.792
H-Index - 246
ISSN - 3049-7094
DOI - 10.1093/genetics/138.2.491
Subject(s) - biology , suppressor , gene , positional cloning , melanocyte , phenotype , genetics , myosin , cloning (programming) , cell , mutation , microbiology and biotechnology , tumor suppressor gene , carcinogenesis , melanoma , computer science , programming language
The murine dilute suppressor gene (dsu) suppresses the coat-color phenotype of three pigment mutations, dilute (d), ashen (ash) and leaden (ln), that each produce adendritic melanocytes. Suppression is due to the ability of dsu to partially restore (ash and ln), or almost completely restore (d), normal melanocyte morphology. While the ash and ln gene products have yet to be identified, the d gene encodes a novel myosin heavy chain (myosin 12), which is speculated to be necessary for the elaboration, maintenance, and/or function of melanocyte cell processes. To begin to discriminate between different models of dsu action, we have produced aggregation chimeras between mice homozygous for dsu and mice homozygous for d to determine if dsu acts cell autonomously or cell nonautonomously. In addition, we have further refined the map location of dsu in order to examine a number of possible dsu candidate genes mapping in the region and to provide a genetic basis for the positional cloning of dsu.

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