RACK1 regulates centriole duplication through promoting the activation of polo-like kinase 1 by Aurora A

Yuki Yoshino, Akihiro Kobayashi, Huicheng Qi, Shino Endo, Zhenzhou Fang, Kazuha Shindo, Ryo Kanazawa, Natsuko Chiba

Research output: Contribution to journalArticlepeer-review

1 Citation (Scopus)

Abstract

Breast cancer gene 1 (BRCA1) contributes to the regulation of centrosome number. We previously identified receptor for activated C kinase 1 (RACK1) as a BRCA1-interacting partner. RACK1, a scaffold protein that interacts with multiple proteins through its seven WD40 domains, directly binds to BRCA1 and localizes to centrosomes. RACK1 knockdown suppresses centriole duplication, whereas RACK1 overexpression causes centriole overduplication in a subset of mammary gland-derived cells. In this study, we showed that RACK1 binds directly to polo-like kinase 1 (PLK1) and Aurora A, and promotes the Aurora A–PLK1 interaction. RACK1 knockdown decreased phosphorylated PLK1 (p-PLK1) levels and the centrosomal localization of Aurora A and p-PLK1 in S phase, whereas RACK1 overexpression increased p-PLK1 level and the centrosomal localization of Aurora A and p-PLK1 in interphase, resulting in an increase of cells with abnormal centriole disengagement. Overexpression of cancer-derived RACK1 variants failed to enhance the Aurora A–PLK1 interaction, PLK1 phosphorylation and the centrosomal localization of p-PLK1. These results suggest that RACK1 functions as a scaffold protein that promotes the activation of PLK1 by Aurora A in order to promote centriole duplication.

Original languageEnglish
Article numberjcs238931
JournalJournal of cell science
Volume133
Issue number17
DOIs
Publication statusPublished - 2020 Sep

Keywords

  • Aurora A
  • Cancer
  • Centriole duplication
  • Centrosome
  • PLK1

ASJC Scopus subject areas

  • Cell Biology

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