A broad-spectrum human lung fibroblast-derived mitogen is a variant of hepatocyte growth factor

  1. J S Rubin,
  2. A M Chan,
  3. D P Bottaro,
  4. W H Burgess,
  5. W G Taylor,
  6. A C Cech,
  7. D W Hirschfield,
  8. J Wong,
  9. T Miki, and
  10. P W Finch
  1. Laboratory of Cellular and Molecular Biology, National Cancer Institute, Bethesda, MD 20892.

Abstract

A heparin-binding mitogen was isolated from conditioned medium of human embryonic lung fibroblasts. It exhibited broad target-cell specificity whose pattern was distinct from that of any known growth factor. It rapidly stimulated tyrosine phosphorylation of a 145-kDa protein in responsive cells, suggesting that its signaling pathways involved activation of a tyrosine kinase. Purification identified a major polypeptide with an apparent molecular mass of 87 kDa under reducing conditions. Partial amino acid sequence analysis and cDNA cloning revealed that it was a variant of hepatocyte growth factor, a mitogen thought to be specific for hepatic cells and structurally related to plasminogen. Recombinant expression of the cDNA in COS-1 cells established that it encoded the purified growth factor. Its site of synthesis and spectrum of targets imply that this growth factor may play an important role as a paracrine mediator of the proliferation of melanocytes and endothelial cells, as well as cells of epithelial origin.

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  1. PNAS January 15, 1991 vol. 88 no. 2 415-419
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