Nature Communications (Apr 2024)

Reciprocal antagonism of PIN1-APC/CCDH1 governs mitotic protein stability and cell cycle entry

  • Shizhong Ke,
  • Fabin Dang,
  • Lin Wang,
  • Jia-Yun Chen,
  • Mandar T. Naik,
  • Wenxue Li,
  • Abhishek Thavamani,
  • Nami Kim,
  • Nandita M. Naik,
  • Huaxiu Sui,
  • Wei Tang,
  • Chenxi Qiu,
  • Kazuhiro Koikawa,
  • Felipe Batalini,
  • Emily Stern Gatof,
  • Daniela Arango Isaza,
  • Jaymin M. Patel,
  • Xiaodong Wang,
  • John G. Clohessy,
  • Yujing J. Heng,
  • Galit Lahav,
  • Yansheng Liu,
  • Nathanael S. Gray,
  • Xiao Zhen Zhou,
  • Wenyi Wei,
  • Gerburg M. Wulf,
  • Kun Ping Lu

DOI
https://doi.org/10.1038/s41467-024-47427-w
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 21

Abstract

Read online

Abstract Induced oncoproteins degradation provides an attractive anti-cancer modality. Activation of anaphase-promoting complex (APC/CCDH1) prevents cell-cycle entry by targeting crucial mitotic proteins for degradation. Phosphorylation of its co-activator CDH1 modulates the E3 ligase activity, but little is known about its regulation after phosphorylation and how to effectively harness APC/CCDH1 activity to treat cancer. Peptidyl-prolyl cis-trans isomerase NIMA-interacting 1 (PIN1)-catalyzed phosphorylation-dependent cis-trans prolyl isomerization drives tumor malignancy. However, the mechanisms controlling its protein turnover remain elusive. Through proteomic screens and structural characterizations, we identify a reciprocal antagonism of PIN1-APC/CCDH1 mediated by domain-oriented phosphorylation-dependent dual interactions as a fundamental mechanism governing mitotic protein stability and cell-cycle entry. Remarkably, combined PIN1 and cyclin-dependent protein kinases (CDKs) inhibition creates a positive feedback loop of PIN1 inhibition and APC/CCDH1 activation to irreversibly degrade PIN1 and other crucial mitotic proteins, which force permanent cell-cycle exit and trigger anti-tumor immunity, translating into synergistic efficacy against triple-negative breast cancer.