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Publication : Deficiency of heat shock factor 4 promotes lens epithelial cell senescence through upregulating p21<sup>cip1</sup> expression.

First Author  Cui X Year  2021
Journal  Biochim Biophys Acta Mol Basis Dis Volume  1867
Issue  11 Pages  166233
PubMed ID  34339841 Mgi Jnum  J:312483
Mgi Id  MGI:6788936 Doi  10.1016/j.bbadis.2021.166233
Citation  Cui X, et al. (2021) Deficiency of heat shock factor 4 promotes lens epithelial cell senescence through upregulating p21(cip1) expression. Biochim Biophys Acta Mol Basis Dis 1867(11):166233
abstractText  Genetic mutations in heat shock factor 4 (Hsf4) is associated with both congenital and age-related cataracts. Hsf4 regulates lens development through its ability to both activate and inhibit transcription. Previous studies suggested Hsf4 is involved in modulating cellular senescence depending on p21(cip1) and p27 (kip1) expression in MEF cells. Here, we found that Hsf4 acts as a suppressor of p21(cip1) expression and plays an anti-senescence role during lens development. Knocking out Hsf4 facilitated UVB-induced cellular senescence in mouse lens epithelial cells (mLECs). p21(cip1) was upregulated at both the mRNA and protein levels in HSF4(-/-) mLECs under control and UVB-treated conditions, and knockdown of p21(cip1) by siRNA alleviated UVB-induced cellular senescence. HSF4 directly bound to the p21(cip1) promoter and increased H3K27m3 levels at the p21(cip1) proximal promoter region by recruiting the methyltransferase EZH2. In animal models, p21(cip1) was gradually upregulated in wild-type mouse lenses with increasing age, while Hsf4 levels decreased. We generated a Hsf4 mutant mice line (Hsf4(del-42)) which displayed obvious congenital cataract phenotype. The expression of p21(cip1) and senescence-associated cytokines were induced in the cataractous lenses of Hsf4(del-42) mice. H3K27m3 and EZH2 levels decreased in p21(cip1) promoters in the lenses of Hsf4(del-42) mice. The SA-beta-Gal activities were positive in lens epithelia of aged Hsf4(null) zebrafish compared to wild-type lenses. p21(cip1) and senescence-associated cytokines levels were also upregulated in lenses of Hsf4(null) zebrafish. Accordingly, we propose that HSF4 plays a protective role in lens epithelial cells against cellular senescence during lens development and aging, partly by fine-tuning p21(cip1) expression.
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