Tumor Biology (Jun 2017)

Proteasome beta-4 subunit contributes to the development of melanoma and is regulated by miR-148b

  • Xiaodong Zhang,
  • Di Lin,
  • Yueqin Lin,
  • Hongqing Chen,
  • Minghua Zou,
  • Shan Zhong,
  • Xuefeng Yi,
  • Siqi Han

DOI
https://doi.org/10.1177/1010428317705767
Journal volume & issue
Vol. 39

Abstract

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The proteasome beta-4 subunit is required for the assembly of 20S proteasome complex, forming a pivotal component for the ubiquitin–proteasome system. Emerging evidence indicates that proteasome beta-4 subunit may be involved in underlying progression and mechanisms of malignancies. However, the role of proteasome beta-4 subunit in melanoma is currently unknown. Here, we reported that proteasome beta-4 subunit was markedly upregulated in human melanoma tissues and cells, compared with normal skin samples. High proteasome beta-4 subunit levels were significantly associated with poor overall survival in patients with melanoma. Proteasome beta-4 subunit knockdown strongly decreased melanoma cell growth in vitro and in vivo. We further identified miR-148b as a negative regulator of proteasome beta-4 subunit. Enforced expression of miR-148b resulted in vitro growth inhibition of melanoma cells, whereas this inhibition was further abolished by enforced expression of proteasome beta-4 subunit. Our findings, for the first time, indicated that the miR-148b/proteasome beta-4 subunit axis contributed to the development of melanoma, revealing novel therapeutic targets for the treatment of melanoma.