PLoS ONE (Jan 2013)

B cells promote tumor progression via STAT3 regulated-angiogenesis.

  • Chunmei Yang,
  • Heehyoung Lee,
  • Sumanta Pal,
  • Veronica Jove,
  • Jiehui Deng,
  • Wang Zhang,
  • Dave S B Hoon,
  • Mark Wakabayashi,
  • Stephen Forman,
  • Hua Yu

DOI
https://doi.org/10.1371/journal.pone.0064159
Journal volume & issue
Vol. 8, no. 5
p. e64159

Abstract

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The role of B cells in cancer and the underlying mechanisms remain to be further explored. Here, we show that tumor-associated B cells with activated STAT3 contribute to tumor development by promoting tumor angiogenesis. B cells with or without Stat3 have opposite effects on tumor growth and tumor angiogenesis in both B16 melanoma and Lewis Lung Cancer mouse models. Ex vivo angiogenesis assays show that B cell-mediated tumor angiogenesis is mainly dependent on the induction of pro-angiogenic gene expression, which requires Stat3 signaling in B cells. Furthermore, B cells with activated STAT3 are mainly found in or near tumor vasculature and correlate significantly with overall STAT3 activity in human tumors. Moreover, the density of B cells in human tumor tissues correlates significantly with expression levels of several STAT3-downstream pro-angiogenic genes, as well as the degree of tumor angiogenesis. Together, these findings define a novel role of B cells in promoting tumor progression through angiogenesis and identify STAT3 in B cells as potential therapeutic target for anti-angiogenesis therapy.