作者
Dauren Alimbetov, Terence Davis, Amy JC Brook, Lynne S Cox, Richard GA Faragher, Talgat Nurgozhin, Zhaxybay Zhumadilov, David Kipling
发表日期
2016/4/1
期刊
Biogerontology
卷号
17
期号
2
页码范围
305-315
出版商
Springer Netherlands
简介
Senescent cells show an altered secretome profile termed the senescence-associated secretory phenotype (SASP). There is an increasing body of evidence that suggests that the accumulation of SASP-positive senescent cells in humans is partially causal in the observed shift to a low-level pro-inflammatory state in aged individuals. This in turn suggests the SASP as a possible therapeutic target to ameliorate inflammatory conditions in the elderly, and thus a better understanding of the signalling pathways underlying the SASP are required. Prior studies using the early generation p38 MAPK inhibitor SB203580 indicated that p38 signalling was required for the SASP. In this study, we extend these observations using two next-generation p38 inhibitors (UR-13756 and BIRB 796) that have markedly improved selectivity and specificity compared to SB203580, to strengthen the evidence that the SASP is p38 …
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