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Redefining Chronic Inflammation in Aging and Age-Related Diseases: Proposal of the Senoinflammation Concept

机译:重新定义衰老和与年龄有关的疾病中的慢性炎症:Senoinflammation概念的建议

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Age-associated chronic inflammation is characterized by unresolved and uncontrolled inflammation with multivariable low-grade, chronic and systemic responses that exacerbate the aging process and age-related chronic diseases. Currently, there are two major hypotheses related to the involvement of chronic inflammation in the aging process: molecular inflammation of aging and inflammaging. However, neither of these hypotheses satisfactorily addresses age-related chronic inflammation, considering the recent advances that have been made in inflammation research. A more comprehensive view of age-related inflammation, that has a scope beyond the conventional view, is therefore required. In this review, we discuss newly emerging data on multi-phase inflammatory networks and proinflammatory pathways as they relate to aging. We describe the age-related upregulation of nuclear factor (NF)-κB signaling, cytokines/chemokines, endoplasmic reticulum (ER) stress, inflammasome, and lipid accumulation. The later sections of this review present our expanded view of age-related senescent inflammation, a process we term “senoinflammation”, that we propose here as a novel concept. As described in the discussion, senoinflammation provides a schema highlighting the important and ever-increasing roles of proinflammatory senescence-associated secretome, inflammasome, ER stress, TLRs, and microRNAs, which support the senoinflammation concept. It is hoped that this new concept of senoinflammation opens wider and deeper avenues for basic inflammation research and provides new insights into the anti-inflammatory therapeutic strategies targeting the multiple proinflammatory pathways and mediators and mediators that underlie the pathophysiological aging process.
机译:与年龄相关的慢性炎症的特征是无法解决且不受控制的炎症,以及多变量的低度,慢性和全身性反应,加剧了衰老过程和与年龄相关的慢性疾病。当前,有两个主要的假设与衰老过程中的慢性炎症有关:衰老和发炎的分子炎症。然而,考虑到炎症研究方面的最新进展,这些假设都不能令人满意地解决与年龄有关的慢性炎症。因此,需要一种与年龄有关的炎症的更全面的观点,其范围超出了常规观点。在这篇综述中,我们讨论了与衰老相关的多相炎症网络和促炎途径的新兴数据。我们描述了与年龄相关的核因子(NF)-κB信号,细胞因子/趋化因子,内质网(ER)应激,炎症小体和脂质蓄积的上调。本文的后续部分介绍了我们对与年龄相关的衰老性炎症的扩展观点,该过程被我们称为“感觉炎症”,在此我们将其作为一个新概念提出。如讨论中所述,senoinflammation提供了一个方案,突出了促炎性衰老相关的分泌蛋白,炎症小体,ER压力,TLR和microRNA的重要且不断增加的作用,这些都支持senoinflammation概念。希望这种新的自然炎症的概念为基础炎症研究开辟更广泛和更深层次的途径,并为靶向多种促炎途径和病理生理老化过程基础的介体和介体的抗炎治疗策略提供新见解。

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