Sarcopenia and cognitive impairment: a multidimensional study of clinical associations, shared genetics, and causal links

肌少症与认知障碍:临床关联、共同遗传因素和因果关系的多维度研究

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Abstract

OBJECTIVE: To comprehensively investigate the relationship between sarcopenia and cognitive impairment by examining their clinical associations, shared genetic architecture, and potential causal links, using a multidimensional approach. METHODS: To assess the sarcopenia and cognitive impairment risk, multivariable-adjusted logistic regression was conducted on Wuhan Junshan Community data. Utilizing large-scale GWAS summary statistics, we identified potential genetic overlaps between sarcopenia and cognitive impairment. Cross-trait pleiotropic analyses were conducted to uncover shared genetic loci and pleiotropic genes between these conditions. Comprehensive functional annotation and tissue-specific expression analyses were then performed to characterize the biological roles of these shared genetic factors. Finally, we employed Mendelian randomization (MR) approaches to examine potential causal relationships between sarcopenia and cognitive impairment. RESULTS: In this study, we recruited 575 participants for this observational study. Multivariable-adjusted logistic regression revealed a significant positive association between sarcopenia and cognitive impairment risk (OR = 3.26, 95% CI: 1.65 to 6.42). Genomic analysis revealed that there was a significant genetic correlation between sarcopenia and cognitive impairment, and 19 pairs of significantly correlated trait combinations were identified. Pleiotropic analysis revealed 79 risk loci and 428 pleiotropic genes such as FoxO3 and SLC39A8, which were enriched in neurodegenerative pathway and FoxO signaling pathway. MR analysis showed that appendicular lean mass and usual walking pace had potential causal protective effects on cognitive function, while low hand grip strength had the opposite effect. CONCLUSION: This study provides evidence for both clinical and genetic links between sarcopenia and cognitive impairment, uncovering their potential biological mechanisms.

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