4.6 Article

Impact of Fibroblast Growth Factor-Binding Protein-1 Expression on Angiogenesis and Wound Healing

Journal

AMERICAN JOURNAL OF PATHOLOGY
Volume 179, Issue 5, Pages 2220-2232

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.ajpath.2011.07.043

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Funding

  1. NIH [RO1 CA71508, PO1 HL068686]
  2. Lombardi Cancer Center Shared Resources [P30 CA51008]

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Fibroblast growth factors (FGFs) participate in embryonic development, in maintenance of tissue homeostasis in the adult, and in various diseases. FGF-binding proteins (FGFBP) are secreted proteins that chaperone FGFs stored in the extracellular matrix to their receptor, and can thus modulate FGF signaling. FGFBP1 (alias BP1, FGF-BP1, or HBp17) expression is required for embryonic survival, can modulate FGF-dependent vascular permeability in embryos, and is an angiogenic switch in human cancers. To determine the function of BP1 in vivo, we generated tetracycline-regulated conditional BP1 transgenic mice. BP1-expressing adult mice are viable, fertile, and phenotypically indistinguishable from their littermates. Induction of BP1 expression increased mouse primary fibroblast motility in vitro, increased angiogenic sprouting into subcutaneous matrigel plugs in animals and accelerated the healing of excisional skin wounds. FGF-receptor kinase inhibitors blocked these effects. Healing skin wounds showed increased macrophage invasion as well as cell proliferation after BP1 expression. Also, BP1 expression increased angiogenesis during the healing of skin wounds as well as after ischemic injury to hindlimb skeletal muscles. We conclude that BP1 can enhance FGF effects that are required for the healing and repair of injured tissues in adult animals. (Am J Pathol 2011, 179:2220-2232; DOI: 10.1016/j.ajpath.2011.07.043)

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