4.8 Article

Alternatively spliced vascular endothelial growth factor receptor-2 is an essential endogenous inhibitor of lymphatic vessel growth

Journal

NATURE MEDICINE
Volume 15, Issue 9, Pages 1023-U74

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/nm.2018

Keywords

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Funding

  1. US National Institutes of Health
  2. National Eye Institute [EY015422, EY018350, EY018836, EY017182, EY017950]
  3. Research to Prevent Blindness
  4. University of Kentucky University Research Professorship
  5. Fight for Sight
  6. Japan Society for the Promotion of Science for Young Scientists
  7. US Department of Defense
  8. Doris Duke Distinguished Clinical Scientist
  9. Burroughs Wellcome Fund

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Disruption of the precise balance of positive and negative molecular regulators of blood and lymphatic vessel growth can lead to myriad diseases. Although dozens of natural inhibitors of hemangiogenesis have been identified, an endogenous selective inhibitor of lymphatic vessel growth has not to our knowledge been previously described. We report the existence of a splice variant of the gene encoding vascular endothelial growth factor receptor-2 (Vegfr-2) that encodes a secreted form of the protein, designated soluble Vegfr-2 (sVegfr-2), that inhibits developmental and reparative lymphangiogenesis by blocking Vegf-c function. Tissue-specific loss of sVegfr-2 in mice induced, at birth, spontaneous lymphatic invasion of the normally alymphatic cornea and hyperplasia of skin lymphatics without affecting blood vasculature. Administration of sVegfr-2 inhibited lymphangiogenesis but not hemangiogenesis induced by corneal suture injury or transplantation, enhanced corneal allograft survival and suppressed lymphangioma cellular proliferation. Naturally occurring sVegfr-2 thus acts as a molecular uncoupler of blood and lymphatic vessels; modulation of sVegfr-2 might have therapeutic effects in treating lymphatic vascular malformations, transplantation rejection and, potentially, tumor lymphangiogenesis and lymphedema.

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