Jean Mayer USDA Human Nutrition Research Center on Aging at Tufts University, Boston, Massachusetts, USA.
Aging Cell. 2024 Jan;23(1):e13988. doi: 10.1111/acel.13988. Epub 2023 Sep 20.
Originally identified as an outcome of continuous culture of primary cells, cellular senescence has moved beyond the culture dish and is now a bona fide driver of aging and disease in animal models, and growing links to human disease. This cellular stress response consists of a stable proliferative arrest coupled to multiple phenotypic changes. Perhaps the most important of these is the senescence-associated secretory phenotype, or senescence-associated secretory phenotype -a complex and variable collection of secreted molecules release by senescent cells with a number of potent biological activities. Senescent cells appear in multiple age-associated conditions in humans and mice, and interventions that eliminate these cells can prevent or even reverse multiple diseases in mouse models. Here, we review salient aspects of senescent cells in the context of human disease and homeostasis. Senescent cells increase in abundance during several diseases that associated with premature aging. Conversely, senescent cells have a key role in beneficial processes such as development and wound healing, and thus can help maintain tissue homeostasis. Finally, we speculate on mechanisms by which deleterious aspects of senescent cells might be targeted while retaining homeostatic aspects in order to improve age-related outcomes.
最初被认为是原代细胞连续培养的结果,细胞衰老已经超越了培养皿,现在是动物模型中衰老和疾病的真正驱动因素,并与人类疾病有越来越多的联系。这种细胞应激反应包括稳定的增殖停滞,加上多种表型变化。其中最重要的可能是衰老相关分泌表型或衰老相关分泌表型 - 衰老细胞分泌的多种具有强大生物学活性的分泌分子的复杂和可变集合。衰老细胞出现在人类和小鼠的多种与年龄相关的疾病中,消除这些细胞的干预措施可以预防甚至逆转小鼠模型中的多种疾病。在这里,我们将在人类疾病和体内平衡的背景下回顾衰老细胞的显著方面。衰老细胞在与早衰相关的几种疾病中大量增加。相反,衰老细胞在发育和伤口愈合等有益过程中起着关键作用,因此可以帮助维持组织内稳态。最后,我们推测靶向衰老细胞有害方面的机制,同时保留体内平衡方面,以改善与年龄相关的结果。
