BMB Reports (May 2012)

FGF-2 inhibits TNF-α mediated apoptosis through upregulation of Bcl2-A1 and Bcl-xL in ATDC5 cells

  • Hey-Ryun Kim,
  • Youn-Moo Heo,
  • Kyoung-Il Jeong,
  • Yong-Min Kim,
  • Hae Lan Jang,
  • Kwang-Yeol Lee,
  • Chang-Yeol Yeo,
  • Sung Hoon Kim,
  • Hak-Kyo Lee,
  • Seung-Ryul Kim,
  • Eung-Gook Kim,
  • Joong-Kook Choi

DOI
https://doi.org/10.5483/BMBRep.2012.45.5.287
Journal volume & issue
Vol. 45, no. 5
pp. 287 – 292

Abstract

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FGF-2 is involved in cell survival, proliferation, apoptosis, andangiogenesis in a wide variety of cells. FRGRs, PI3K and MAPkinases are well known mediators of FGF signaling. Despite itsknown roles during many developmental processes, includingosteogenesis, there are few known targets of FGF-2. In thepresent study, we identified Bcl2-A1 and Bcl-xL as two prominenttargets involved in promoting cell survival. Pretreatmentof ATDC5 cells with FGF-2 increased cell survival, whilesiRNAs specific for Bcl2-A1 and Bcl-xL compromised the anti-apoptotic effect of FGF-2, sensitized the cells to apoptosistriggered by TNF-α. Chemical inhibition of FGFR, NFkB, andPI3K activity by PD173074, pyrrolidine dithiocarbamate, andLY294002 respectively abrogated the FGF-2-mediated inductionof Bcl2-A1 and Bcl-xL expression. Taken together, our datademonstrate that a subset of Bcl2 family proteins are the targetsof FGF-2 signaling that promotes the survival of ATDC5cells. [BMB reports 2012; 45(5): 287-292]

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