Histone deficiency and hypoacetylation in the aging retinal pigment epithelium

被引:3
作者
Dubey, Sushil K. [1 ]
Dubey, Rashmi [1 ]
Prajapati, Subhash C. [2 ]
Jung, Kyungsik [1 ]
Mohan, Kabhilan [1 ]
Liu, Xinan [3 ]
Roney, Jacob [4 ]
Tian, Wenjian [1 ]
Abney, Jennifer [4 ]
Giarmarco, Michelle M. [5 ]
Hernandez, Alvaro G. [6 ]
Liu, Jinze [7 ]
Kleinman, Mark E. [1 ,8 ]
机构
[1] East Tennessee State Univ, Dept Surg, Johnson City, TN 37614 USA
[2] Univ Virginia, Dept Biochem & Mol Genet, Charlottesville, VA USA
[3] Univ Kentucky, Dept Comp Sci, Lexington, KY USA
[4] Univ Kentucky, Dept Ophthalmol & Visual Sci, Lexington, KY USA
[5] Univ Washington, Dept Ophthalmol, Seattle, WA USA
[6] Univ Illinois, Roy J Carver Biotechnol Ctr, Urbana, IL USA
[7] Virginia Commonwealth Univ, Dept Biostat, Richmond, VA USA
[8] East Tennessee State Univ, James H Quillen Coll Med, Dept Surg, Johnson City, TN 37614 USA
关键词
aging; epigenetics; HINFP; histone acetylation; histones; replicative senescence; retinal pigment epithelium; CELL-CYCLE; GENE-EXPRESSION; SENESCENCE DRIVEN; HINF-P; AGE; REPLICATION; TRANSCRIPTION; INACTIVATION; ACCUMULATION; ACETYLATION;
D O I
10.1111/acel.14108
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Histones serve as a major carrier of epigenetic information in the form of post-translational modifications which are vital for controlling gene expression, maintaining cell identity, and ensuring proper cellular function. Loss of histones in the aging genome can drastically impact the epigenetic landscape of the cell leading to altered chromatin structure and changes in gene expression profiles. In this study, we investigated the impact of age-related changes on histone levels and histone acetylation in the retinal pigment epithelium (RPE) and retina of mice. We observed a global reduction of histones H1, H2A, H2B, H3, and H4 in aged RPE/choroid but not in the neural retina. Transcriptomic analyses revealed significant downregulation of histones in aged RPE/choroid including crucial elements of the histone locus body (HLB) complex involved in histone pre-mRNA processing. Knockdown of HINFP, a key HLB component, in human RPE cells induced histone loss, senescence, and the upregulation of senescence-associated secretory phenotype (SASP) markers. Replicative senescence and chronological aging in human RPE cells similarly resulted in progressive histone loss and acquisition of the SASP. Immunostaining of human retina sections revealed histone loss in RPE with age. Acetyl-histone profiling in aged mouse RPE/choroid revealed a specific molecular signature with loss of global acetyl-histone levels, including H3K14ac, H3K56ac, and H4K16ac marks. These findings strongly demonstrate histone loss as a unique feature of RPE aging and provide critical insights into the potential mechanisms linking histone dynamics, cellular senescence, and aging. In this study, we demonstrated an age-related loss of core and linker histones in aged mouse and human donor RPE with correlating results in vitro. Depleting histones in vitro reduced cell proliferation and upregulated SASP markers. Furthermore, a notable reduction in histone acetylation, a classical histone PTM, was observed in aged mice RPE. Thus, the altered histone expression and acetylation status with age may be a critical epigenetic component of RPE cell aging and senescence.image
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页数:17
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