| Literature DB >> 25663289 |
Jin Peng1, Yumiko Yoshioka1, Masaki Mandai1,2, Noriomi Matsumura1, Tsukasa Baba1, Ken Yamaguchi1, Junzo Hamanishi1, Budiman Kharma1, Ryusuke Murakami1, Kaoru Abiko1, Susan K Murphy3, Ikuo Konishi1.
Abstract
Members of the transforming growth factor-β (TGF-β) superfamily transduce signals via SMAD proteins. SMAD2 and SMAD3 mediate TGF-β signaling, whereas SMAD1, SMAD5, and SMAD8/9 transduce bone morphogenetic protein (BMP) signals. We would like to identify the function of BMP/SMAD5 signaling in serous ovarian cancer. The protein levels of total SMAD5 and phosphorylated SMAD5 (pSMAD5) were examined by immunohistochemical analysis using clinical serous ovarian cancer samples. Following treatment with either recombinant BMP2 (rBMP2) or Dorsomorphin (DM), western blotting was performed to observe pSMAD5 protein in the cytoplasm and the nucleus, separately. Cell proliferation was detected in SMAD5 knockdown serous ovarian cancer cell lines cultured with DM or rBMP2. The impact of DM or rBMP2 on tumor growth was observed in a mouse model of serous ovarian cancer. An inverse correlation was observed between pSMAD5 levels in the nucleus and the prognosis of patients with serous ovarian cancer. The treatment of SK-OV-3 with rBMP2 stimulated pSMAD5 translocation from the cytoplasm to the nucleus, and the addition of DM inhibited this effect. The proliferation of ovarian cancer cell lines was enhanced by BMP2 and suppressed by DM via SMAD5 in vitro. In vitro and in vivo experiments clearly demonstrated BMP2-stimulated proliferation of serous ovarian cancer and inhibition of this effect by DM. Our data suggests that BMP/SMAD5 signaling plays an important role and, therefore, becomes a potential therapeutic target in serous ovarian cancer.Entities:
Keywords: BMP: bone morphogenetic protein; SMAD; serous ovarian cancer
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Year: 2015 PMID: 25663289 DOI: 10.1002/mc.22283
Source DB: PubMed Journal: Mol Carcinog ISSN: 0899-1987 Impact factor: 4.784