A Novel Strategy to Block Mitotic Progression for Targeted Therapy

Overview

Journal EBioMedicine

Specialty Biomedical Engineering

Date 2019 Nov 1

PMID 31669221

Citations 28

Authors

Junlong Jack Chi

Hongchun Li

Zhuan Zhou

Javier Izquierdo-Ferrer

Yifan Xue

Cindy M Wavelet

Gary E Schiltz

Bin Zhang

Massimo Cristofanilli

Xinghua Lu

Ivet Bahar

Yong Wan

Affiliations

Soon will be listed here.

Abstract

Background: Blockade of mitotic progression is an ideal approach to induce mitotic catastrophe that suppresses cancer cell expansion. Cdc20 is a critical mitotic factor governing anaphase initiation and the exit from mitosis through recruiting substrates to APC/C for degradation. Results from recent TCGA (The Cancer Genome Atlas) and pathological studies have demonstrated a pivotal oncogenic role for Cdc20-APC/C in tumor progression as well as drug resistance. Thus, deprivation of the mitotic role for Cdc20-APC/C by either inhibition of Cdc20-APC/C activity or elimination of Cdc20 protein via induced protein degradation emerges as an effective therapeutic strategy to control cancer.

Methods: We designed a proteolysis targeting chimera, called CP5V, which comprises a Cdc20 ligand and VHL binding moiety bridged by a PEG5 linker that induces Cdc20 degradation. We characterized the effect of CP5V in destroying Cdc20, arresting mitosis, and inhibiting tumor progression by measuring protein degradation, 3D structure dynamics, cell cycle control, tumor cell killing and tumor inhibition using human breast cancer xenograft mouse model.

Findings: Results from our study demonstrate that CP5V can specifically degrade Cdc20 by linking Cdc20 to the VHL/VBC complex for ubiquitination followed by proteasomal degradation. Induced degradation of Cdc20 by CP5V leads to significant inhibition of breast cancer cell proliferation and resensitization of Taxol-resistant cell lines. Results based on a human breast cancer xenograft mouse model show a significant role for CP5V in suppressing breast tumor progression.

Interpretation: CP5V-mediated degradation of Cdc20 could be an effective therapeutic strategy for anti-mitotic therapy.

Citing Articles

Targeting APC/C Ubiquitin E3-Ligase Activation with Pyrimidinethylcarbamate Apcin Analogues for the Treatment of Breast Cancer.

Kapanidou M, Curtis N, Diaz-Minguez S, Agudo-Alvarez S, Rus Sanchez A, Mayah A Biomolecules. 2024; 14(11).

PMID: 39595615 PMC: 11591962. DOI: 10.3390/biom14111439.

Negative regulation of APC/C activation by MAPK-mediated attenuation of Cdc20 under stress.

Sun L, Chen X, Song C, Shi W, Liu L, Bai S Elife. 2024; 13.

PMID: 39412391 PMC: 11483130. DOI: 10.7554/eLife.97896.

Suppressing Anaphase-Promoting Complex/Cyclosome-Cell Division Cycle 20 Activity to Enhance the Effectiveness of Anti-Cancer Drugs That Induce Multipolar Mitotic Spindles.

Schuyler S, Chen H, Chang K Int J Mol Sci. 2024; 25(12).

PMID: 38928036 PMC: 11203710. DOI: 10.3390/ijms25126329.

MAPK-dependent control of mitotic progression in S. pombe.

Iglesias-Romero A, Soto T, Flor-Parra I, Salas-Pino S, Ruiz-Romero G, Gould K BMC Biol. 2024; 22(1):71.

PMID: 38523261 PMC: 10962199. DOI: 10.1186/s12915-024-01865-6.

Upregulated expression of is associated with progression of pancreatic cancer.

He Y, Du Z, Peng H, Reddy A, Cao P J Gastrointest Oncol. 2024; 15(1):435-457.

PMID: 38482253 PMC: 10932678. DOI: 10.21037/jgo-23-979.

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