Steel-Dickie mutation encodes a c-kit ligand lacking transmembrane and cytoplasmic domains

  1. C I Brannan,
  2. S D Lyman,
  3. D E Williams,
  4. J Eisenman,
  5. D M Anderson,
  6. D Cosman,
  7. M A Bedell,
  8. N A Jenkins, and
  9. N G Copeland
  1. Mammalian Genetics Laboratory, National Cancer Institute-Frederick Cancer Research and Development Center, MD 21702-1201.

Abstract

Mice homozygous for the viable Sl allele steel-Dickie (Sld) are sterile, severely anemic, and black-eyed white. The nature of the Sld mutation was investigated at the molecular level and was found to be due to a 4.0-kilobase intragenic deletion in mast cell growth factor (MGF) genomic sequences, providing conclusive evidence that Sl encodes MGF. As a consequence of this deletion, Sld is only capable of encoding a soluble truncated growth factor that lacks both transmembrane and cytoplasmic domains. Northern analysis indicates that Sld mRNA is expressed at approximately wild-type levels in adult tissues, and yeast expression studies suggest that the Sld protein is as biologically active as wild-type soluble MGF. These studies provide a molecular basis for explaining the Sld phenotype, a description of a germ-line mutation in the transmembrane and cytoplasmic domains of a membrane-bound growth factor, and in vivo evidence for the importance of membrane-bound forms of growth factors in mammalian development.

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  1. PNAS June 1, 1991 vol. 88 no. 11 4671-4674
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