1. T-cell senescence accelerates angiotensin II-induced target organ damage
- Author
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Xiao-Hui Chen, Dong-Rui Chen, Cheng-Chao Ruan, Hong-Jin Chen, Pingjin Gao, Ling-Ran Kong, Fang Wu, and Xiao-Xi Pan
- Subjects
Senescence ,Male ,Adoptive cell transfer ,Time Factors ,Physiology ,Immunosenescence ,T cell ,T-Lymphocytes ,Kidney ,Recombination-activating gene ,Cell Line ,Interferon-gamma ,Superoxides ,Physiology (medical) ,Renin–angiotensin system ,medicine ,Animals ,Humans ,Aorta ,Homeodomain Proteins ,Mice, Knockout ,business.industry ,Angiotensin II ,Myocardium ,Acquired immune system ,Adoptive Transfer ,Mice, Inbred C57BL ,Disease Models, Animal ,Oxidative Stress ,medicine.anatomical_structure ,Phenotype ,Cardiovascular Diseases ,Hypertension ,Cancer research ,Kidney Diseases ,Inflammation Mediators ,Cardiology and Cardiovascular Medicine ,business - Abstract
Aims Aging is a risk factor for cardiovascular diseases and adaptive immunity has been implicated in angiotensin (Ang) II-induced target organ dysfunction. Herein, we sought to determine the role of T-cell senescence in Ang II-induced target organ impairment and to explore the underlying mechanisms. Methods and results Flow cytometric analysis revealed that T cell derived from aged mice exhibited immunosenescence. Adoptive transfer of aged T cells to immunodeficient RAG1 KO mice accelerates Ang II-induced cardiovascular and renal fibrosis compared with young T-cell transfer. Aged T cells also promote inflammatory factor expression and superoxide production in these target organs. In vivo and in vitro studies revealed that Ang II promotes interferon-gamma (IFN-γ) production in the aged T cells comparing to young T cells. Importantly, transfer of senescent T cell that IFN-γ KO mitigates the impairment. Aged T-cell-conditioned medium stimulates inflammatory factor expression and oxidative stress in Ang II-treated renal epithelial cells compared with young T cells, and these effects of aged T-cell-conditioned medium are blunted after IFN-γ-neutralizing antibody pre-treatment. Conclusion These results provide a significant insight into the contribution of senescent T cells to Ang II-induced cardiovascular dysfunction and provide an attractive possibility that targeting T cell specifically might be a potential strategy to treat elderly hypertensive patients with end-organ dysfunction.
- Published
- 2019