González-Osuna Luis, Sierra-Cristancho Alfredo, Rojas Carolina, Cafferata Emilio A, Melgar-Rodríguez Samanta, Cárdenas Angélica M, Vernal Rolando
1Periodontal Biology Laboratory, Faculty of Dentistry, Universidad de Chile, Santiago, Chile.
2Faculty of Dentistry, Universidad Andres Bello, Santiago, Chile.
Aging Dis. 2021 Aug 1;12(5):1150-1161. doi: 10.14336/AD.2021.0110. eCollection 2021 Aug.
Cellular senescence is a biological process triggered in response to time-accumulated DNA damage, which prioritizes cell survival over cell function. Particularly, senescent T lymphocytes can be generated prematurely during chronic inflammatory diseases regardless of chronological aging. These senescent T lymphocytes are characterized by the loss of CD28 expression, a co-stimulatory receptor that mediates antigen presentation and effective T-cell activation. An increased number of premature senescent CD4CD28 T lymphocytes has been frequently observed in osteolytic diseases, including rheumatoid arthritis, juvenile idiopathic arthritis, ankylosing spondylitis, osteopenia, osteoporosis, and osteomyelitis. Indeed, CD4CD28 T lymphocytes produce higher levels of osteoclastogenic molecular mediators directly related to pathologic bone loss, such as tumor necrosis factor (TNF)-α, interleukin (IL)-17A, and receptor-activator of nuclear factor κB ligand (RANKL), as compared with regular CD4CD28 T lymphocytes. In addition, premature senescent CD8CD28 T lymphocytes have been negatively associated with bone healing and regeneration by inhibiting osteoblast differentiation and mesenchymal stromal cell survival. Therefore, accumulated evidence supports the role of senescent T lymphocytes in osteoimmunology. Moreover, premature senescence of T-cells seems to be associated with the functional imbalance between the osteolytic T-helper type-17 (Th17) and bone protective T regulatory (Treg) lymphocytes, as well as the phenotypic instability of Treg lymphocytes responsible for its trans-differentiation into RANKL-producing exFoxp3Th17 cells, a key cellular phenomenon directly related to bone loss. Herein, we present a framework for the understanding of the pathogenic characteristics of T lymphocytes with a premature senescent phenotype; and particularly, we revise and discuss their role in the osteoimmunology of osteolytic diseases.
细胞衰老乃是一种因应随时间累积的DNA损伤而触发的生物学过程,该过程将细胞存活置于细胞功能之上。特别地,衰老的T淋巴细胞可在慢性炎症性疾病期间过早产生,而与实际年龄无关。这些衰老的T淋巴细胞的特征在于CD28表达丧失,CD28是一种共刺激受体,介导抗原呈递和有效的T细胞活化。在包括类风湿性关节炎、幼年特发性关节炎、强直性脊柱炎、骨质减少、骨质疏松症和骨髓炎在内的溶骨性疾病中,经常观察到过早衰老的CD4CD28 T淋巴细胞数量增加。事实上,与正常的CD4CD28 T淋巴细胞相比,CD4CD28 T淋巴细胞产生更高水平的与病理性骨质流失直接相关的破骨细胞生成分子介质,如肿瘤坏死因子(TNF)-α、白细胞介素(IL)-17A和核因子κB受体激活剂配体(RANKL)。此外,过早衰老的CD8CD28 T淋巴细胞通过抑制成骨细胞分化和间充质基质细胞存活而与骨愈合和再生呈负相关。因此,越来越多的证据支持衰老的T淋巴细胞在骨免疫学中的作用。此外,T细胞的过早衰老似乎与溶骨性17型辅助性T细胞(Th17)和骨保护性调节性T(Treg)淋巴细胞之间的功能失衡有关,也与负责其转分化为产生RANKL的exFoxp3Th17细胞的Treg淋巴细胞的表型不稳定性有关,这是一种与骨质流失直接相关的关键细胞现象。在此,我们提出一个框架,以理解具有过早衰老表型的T淋巴细胞的致病特征;特别是,我们修订并讨论它们在溶骨性疾病骨免疫学中的作用。
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