Lack of NLRP3 Inflammasome Activation Reduces Age-Dependent Sarcopenia and Mitochondrial Dysfunction, Favoring the Prophylactic Effect of Melatonin

肌萎缩 褪黑素 炎症体 内科学 内分泌学 基因剔除小鼠 细胞凋亡 线粒体 碎片(计算) 老化 衰老 生物 医学 炎症 细胞生物学 生物化学 受体 生态学
作者
Ramy K. A. Sayed,Marisol Fernández‐Ortiz,María Elena Díaz-Casado,Paula Aranda‐Martínez,José Fernández‐Martínez,Ana Guerra‐Librero,Germaine Escames,Luís C. López,Reem M. Alsaadawy,Darío Acuña‐Castroviejo
出处
期刊:The Journals of Gerontology [Oxford University Press]
卷期号:74 (11): 1699-1708 被引量:54
标识
DOI:10.1093/gerona/glz079
摘要

Abstract To investigate the role of NLRP3 inflammasome in muscular aging, we evaluated here the morphological and functional markers of sarcopenia in the NLRP3-knockout mice, as well as the beneficial effect of melatonin supplementation. The gastrocnemius muscles of young (3 months), early-aged (12 months), and old-aged (24 months) NLRP3-knockout female mice were examined. Moreover, locomotor activity and apoptosis were assessed. The results revealed early markers of sarcopenia at the age of 12 months, including reduction of lactate, ratio of muscle weight to body weight, muscle fibers number, and mitochondrial number. Increased interstitial tissues, apoptosis, and muscle fibers area, as well as mitochondrial damage were detected, with little muscular activity effects. In the old-aged, these alterations progressed with a reduction in locomotor activity, mitochondrial cristae destruction, nuclear fragmentation, tubular aggregates (TAs) formation, and increased frailty index. Oral melatonin supplementation preserved the normal muscular structure, muscle fibers number, and muscular activity in old age. Melatonin enhanced lactate production, recovered mitochondria, inhibited TAs formation, reduced apoptosis, and normalized frailty index. The fewer sarcopenic changes as well as the highly detectable prophylactic effects of melatonin treatment reported here in the muscle of NLRP3-knockout mice comparing with that previously detected in wild-type mice, confirming NLRP3 inflammasome implication in muscular aging and sarcopenia onset and progression.
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