Molecular Oncology (Mar 2018)

MAD2L2 inhibits colorectal cancer growth by promoting NCOA3 ubiquitination and degradation

  • Yixin Li,
  • Liren Li,
  • Miao Chen,
  • Xinfa Yu,
  • Zhuoyu Gu,
  • Huijuan Qiu,
  • Ge Qin,
  • Qian Long,
  • Xiaoyan Fu,
  • Tianze Liu,
  • Wenbin Li,
  • Wenlin Huang,
  • Dingbo Shi,
  • Tiebang Kang,
  • Meihua Luo,
  • Xiaojun Wu,
  • Wuguo Deng

DOI
https://doi.org/10.1002/1878-0261.12173
Journal volume & issue
Vol. 12, no. 3
pp. 391 – 405

Abstract

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Nuclear receptor coactivator 3 (NCOA3) is a transcriptional coactivator that has elevated expression in multiple tumor types, including colorectal cancer (CRC). However, the molecular mechanisms that regulate the tumorigenic functions of NCOA3 in CRC remain largely unknown. In this study, we aimed to discover and identify the novel regulatory proteins of NCOA3 and explore their mechanisms of action. Immunoprecipitation (IP) coupled with mass spectrometry (IP‐MS) analysis was used to detect, identify, and verify the proteins that interacted with NCOA3 in CRC cells. The biological functions of the candidate proteins and the underlying molecular mechanism were investigated in CRC cells and mouse model in vitro and in vivo. The clinical significance of NCOA3 and its interaction partner protein in CRC patients was also studied. We identified mitotic arrest deficient 2‐like protein 2 (MAD2L2, also known as MAD2B or REV7), with two signal peptide sequences of LIPLK and EVYPVGIFQK, to be an interaction partner of NCOA3. Overexpression of MAD2L2 suppressed the proliferation, migration, and clonogenicity of CRC cells by inducing the degradation of NCOA3. The mechanism study showed that increased MAD2L2 expression in CRC cells activated p38, which was required for the phosphorylation of NCOA3 that led to its ubiquitination and degradation by the proteasome. Moreover, we found that MAD2L2 predicted favorable prognosis in CRC patients. We have discovered a novel role of MAD2L2 in the regulation of NCOA3 degradation and proposed that MAD2L2 serves as a tumor suppressor in CRC.

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