Activation of P38 MAP Kinase and Stress Signalling in Fibroblasts from the Progeroid Rothmund-Thomson Syndrome

Overview

Journal Age (Dordr)

Publisher Springer

Specialty Geriatrics

Date 2012 Sep 25

PMID 23001818

Citations 7

Authors

Terence Davis

Hannah S E Tivey

Amy J C Brook

Julia W Grimstead

Michal J Rokicki

David Kipling

Affiliations

Soon will be listed here.

Abstract

Rothmund-Thomson fibroblasts had replicative lifespans and growth rates within the range for normal fibroblasts; however, they show elevated levels of the stress-associated p38 MAP kinase, suggestive of stress during growth. Treatment with the p38 MAP kinase inhibitor SB203580 increased both lifespan and growth rate, as did reduction of oxidative stress using low oxygen in some strains. At replicative senescence p53, p21(WAF1) and p16(INK4A) levels were elevated, and abrogation of p53 using shRNA knockdown allowed the cells to bypass senescence. Ectopic expression of human telomerase allowed Rothmund-Thomson fibroblasts to bypass senescence. However, activated p38 was still present, and continuous growth for some telomerised clones required either a reduction in oxidative stress or SB203580 treatment. Overall, the evidence suggests that replicative senescence in Rothmund-Thomson cells resembles normal senescence in that it is telomere driven and p53 dependent. However, the lack of RECQL4 leads to enhanced levels of stress during cell growth that may lead to moderate levels of stress-induced premature senescence. As replicative senescence is believed to underlie human ageing, a moderate level of stress-induced premature senescence and p38 activity may play a role in the relatively mild ageing phenotype seen in Rothmund-Thomson.

Citing Articles

Patient-derived iPSCs link elevated mitochondrial respiratory complex I function to osteosarcoma in Rothmund-Thomson syndrome.

Jewell B, Xu A, Zhu D, Huang M, Lu L, Liu M PLoS Genet. 2021; 17(12):e1009971.

PMID: 34965247 PMC: 8716051. DOI: 10.1371/journal.pgen.1009971.

Opposite roles for p38MAPK-driven responses and reactive oxygen species in the persistence and resolution of radiation-induced genomic instability.

Werner E, Wang H, Doetsch P PLoS One. 2014; 9(10):e108234.

PMID: 25271419 PMC: 4182705. DOI: 10.1371/journal.pone.0108234.

Nijmegen breakage syndrome fibroblasts expressing the C-terminal truncated NBN(p70) protein undergo p38/MK2-dependent premature senescence.

Davis T, Tivey H, Brook A, Kipling D Biogerontology. 2014; 16(1):43-51.

PMID: 25214013 PMC: 4305097. DOI: 10.1007/s10522-014-9530-3.

Oxidative stress and mitochondrial dysfunction across broad-ranging pathologies: toward mitochondria-targeted clinical strategies.

Pagano G, Aiello Talamanca A, Castello G, Cordero M, dIschia M, Gadaleta M Oxid Med Cell Longev. 2014; 2014:541230.

PMID: 24876913 PMC: 4024404. DOI: 10.1155/2014/541230.

Senescence induced by RECQL4 dysfunction contributes to Rothmund-Thomson syndrome features in mice.

Lu H, Fang E, Sykora P, Kulikowicz T, Zhang Y, Becker K Cell Death Dis. 2014; 5:e1226.

PMID: 24832598 PMC: 4047874. DOI: 10.1038/cddis.2014.168.

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