Escape from Therapy-induced Accelerated Cellular Senescence in P53-null Lung Cancer Cells and in Human Lung Cancers

Overview

Journal Cancer Res

Specialty Oncology

Date 2005 Apr 5

PMID 15805280

Citations 188

Authors

Rachel S Roberson

Steven J Kussick

Eric Vallieres

Szu-Yu J Chen

Daniel Y Wu

Affiliations

Soon will be listed here.

Abstract

Accelerated cellular senescence (ACS) has been described for tumor cells treated with chemotherapy and radiation. Following exposure to genotoxins, tumor cells undergo terminal growth arrest and adopt morphologic and marker features suggestive of cellular senescence. ACS is elicited by a variety of chemotherapeutic agents in the p53-null, p16-deficient human non-small cell H1299 carcinoma cells. After 10 to 21 days, infrequent ACS cells (1 in 10(6)) can bypass replicative arrest and reenter cell cycle. These cells express senescence markers and resemble the parental cells in their transcription profile. We show that these escaped H1299 cells overexpress the cyclin-dependent kinase Cdc2/Cdk1. The escape from ACS can be disrupted by Cdc2/Cdk1 kinase inhibitors or by knockdown of Cdc2/Cdk1 with small interfering RNA and can be promoted by expression of exogenous Cdc2/Cdk1. We also present evidence that ACS occurs in vivo in human lung cancer following induction chemotherapy. Viable tumors following chemotherapy also overexpress Cdc2/Cdk1. We propose that ACS is a mechanism of in vivo tumor response and that mechanisms aberrantly up-regulate Cdc2/Cdk1 promotes escape from the senescence pathway may be involved in a subset of tumors and likely accounts for tumor recurrence/progression.

Citing Articles

Current Methodologies to Assess Cellular Senescence in Cancer.

Laouris P, Munoz-Espin D Methods Mol Biol. 2025; 2906:21-44.

PMID: 40082348 DOI: 10.1007/978-1-0716-4426-3_2.

Unraveling AURKB as a potential therapeutic target in pulmonary hypertension using integrated transcriptomic analysis and pre-clinical studies.

Lemay S, Mougin M, Sauvaget M, El Kabbout R, Valasarajan C, Yamamoto K Cell Rep Med. 2025; 6(2):101964.

PMID: 39933527 PMC: 11866512. DOI: 10.1016/j.xcrm.2025.101964.

PP2C phosphatases-terminators of suicidal thoughts.

Lagorgette L, Bogdanova D, Belotserkovskaya E, Garrido C, Demidov O Cell Death Dis. 2024; 15(12):919.

PMID: 39702569 PMC: 11659304. DOI: 10.1038/s41419-024-07269-2.

Resistance to spindle inhibitors in glioblastoma depends on STAT3 and therapy induced senescence.

Zarco N, Dovas A, de Araujo Farias V, Nagaiah N, Haddock A, Sims P iScience. 2024; 27(12):111311.

PMID: 39640583 PMC: 11617384. DOI: 10.1016/j.isci.2024.111311.

Senolytics: charting a new course or enhancing existing anti-tumor therapies?.

Czajkowski K, Herbet M, Murias M, Piatkowska-Chmiel I Cell Oncol (Dordr). 2024; .

PMID: 39633108 DOI: 10.1007/s13402-024-01018-5.