Alpha 2.0
Login Register
» Articles » PMID: 20214619

Mechanisms of Drug-induced Mitotic Catastrophe in Cancer Cells

Overview
Journal Curr Pharm Des
Publisher Bentham Science Publishers
Date 2010 Mar 11
PMID 20214619
Citations 59
Authors
Jose Portugal
Sylvia Mansilla
Marc Bataller
Affiliations
Soon will be listed here.
Abstract

Mitotic catastrophe is a mechanism of cell death characterized by the occurrence of aberrant mitosis with the formation of large cells that contain multiple nuclei, which are morphologically distinguishable from apoptotic cells. Sometimes, mitotic catastrophe is used restrictively to indicate a type of cell death that occurs during or after a faulty mitosis leading to cell death, which takes place via necrosis or apoptosis, rather than a cell death itself. Several antitumor drugs and ionizing radiation are known to induce mitotic catastrophe, but precisely how the ensuring lethality is regulated or what signals are involved is barely characterized. The type of cell death resulting from antitumor therapy can be determined by the mechanism of action of the antitumor agent, dosing regimen of the therapy, and the genetic background in the cells being treated. Wild-type p53 promotes apoptosis or senescence, while mitotic catastrophe is independent of p53. Mitotic catastrophe can be regarded as a delayed response of p53-mutant tumors that are resistant to some damage. In this context, the elucidation of the mechanisms of treatment-induced mitotic catastrophe should contribute to an improvement of the antitumor therapy, because most of the solid tumors bear an inactive p53 protein.

Citing Articles

Carbon ion irradiation conquers the radioresistance by inducing complex DNA damage and apoptosis in U251 human glioblastomas cells.

Guo Y, Li P, Zhang J, Hao S, Zhou X, Di C Med Oncol. 2025; 42(3):64.

PMID: 39903402 DOI: 10.1007/s12032-025-02616-5.

DRG2 levels in prostate cancer cell lines predict response to PARP inhibitor during docetaxel treatment.

Lee J, Lee W, Cho S, Park J, Kwon H, Kim J Investig Clin Urol. 2025; 66(1):56-66.

PMID: 39791585 PMC: 11729229. DOI: 10.4111/icu.20240263.

Transcriptome analysis reveals the anticancer effects of fenbendazole on ovarian cancer: an in vitro and in vivo study.

Wang X, Tian W, Wang N, Yang X, Liu Z, Li L BMC Cancer. 2024; 24(1):1593.

PMID: 39736624 PMC: 11686899. DOI: 10.1186/s12885-024-13361-9.

Combined inhibition of RAD51 and CHK1 causes synergistic toxicity in cisplatin resistant cancer cells by triggering replication fork collapse.

Mann J, Niedermayer K, Krautstrunk J, Abbey L, Wiesmuller L, Piekorz R Int J Cancer. 2024; 156(2):389-402.

PMID: 39239809 PMC: 11578078. DOI: 10.1002/ijc.35164.

The Mechanisms of Regulated Cell Death: Structural and Functional Proteomic Pathways Induced or Inhibited by a Specific Protein-A Narrative Review.

Fernandez-Lazaro D, Sanz B, Seco-Calvo J Proteomes. 2024; 12(1).

PMID: 38250814 PMC: 10801515. DOI: 10.3390/proteomes12010003.