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Cdkn1a transcript variant 2 is a marker of aging and cellular senescence
Aging (Albany NY). 2021 May 25;13. doi: 10.18632/aging.203110.
José Alberto López-Domínguez 1, Sandra Rodríguez-López 2, Ulises Ahumada-Castro 3 4, Pierre-Yves Desprez 1, Maria Konovalenko 1, Remi-Martin Laberge 5, César Cárdenas 1 3 4 6, José Manuel Villalba 2, Judith Campisi 1 7
Abstract:
...In mice, the p21Cip1/Waf1 encoding locus, Cdkn1a, is known to generate two transcripts that produce identical proteins, but one of these transcript variants is poorly characterized. We show that the Cdkn1a transcript variant 2, but not the better-studied variant 1, is selectively elevated during natural aging across multiple mouse tissues. Importantly, mouse cells induced to senescence in culture by genotoxic stress (ionizing radiation or doxorubicin) upregulated both transcripts, but with different temporal dynamics: variant 1 responded nearly immediately to genotoxic stress, whereas variant 2 increased much more slowly as cells acquired senescent characteristics. Upon treating mice systemically with doxorubicin, which induces widespread cellular senescence in vivo, variant 2 increased to a larger extent than variant 1. Variant 2 levels were also more sensitive to the senolytic drug ABT-263 in naturally aged mice. Thus, variant 2 is a novel and more sensitive marker than variant 1 or total p21Cip1/Waf1 protein for assessing the senescent cell burden and clearance in mice.
PMID: 34035185
Tags: biomarkers, Cdkn1a, cellular senescence, mice, p21, p21Cip1, Waf1