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肌肉 Psn 基因与运动相结合,通过适应性调节 Sirt1/PGC-1α 和 arm 通路,有助于骨骼肌的健康衰老和寿命延长。

Muscle Psn gene combined with exercise contribute to healthy aging of skeletal muscle and lifespan by adaptively regulating Sirt1/PGC-1α and arm pathway.

机构信息

Ludong University, City Yantai, Shandong Province, China.

出版信息

PLoS One. 2024 May 16;19(5):e0300787. doi: 10.1371/journal.pone.0300787. eCollection 2024.

Abstract

The Presenilin (Psn) gene is closely related to aging, but it is still unclear the role of Psn genes in skeletal muscle. Here, the Psn-UAS/Mhc-GAL4 system in Drosophila was used to regulate muscle Psn overexpression(MPO) and muscle Psn knockdown(MPK). Drosophila were subjected to endurance exercise from 4 weeks to 5 weeks old. The results showed that MPO and exercise significantly increased climbing speed, climbing endurance, lifespan, muscle SOD activity, Psn expression, Sirt1 expression, PGC-1α expression, and armadillo (arm) expression in aged Drosophila, and they significantly decreased muscle malondialdehyde levels. Interestingly, when the Psn gene is knockdown by 0.78 times, the PGC-1α expression and arm expression were also down-regulated, but the exercise capacity and lifespan were increased. Furthermore, exercise combined with MPO further improved the exercise capacity and lifespan. MPK combined with exercise further improves the exercise capacity and lifespan. Thus, current results confirmed that the muscle Psn gene was a vital gene that contributed to the healthy aging of skeletal muscle since whether it was overexpressed or knocked down, the aging progress of skeletal muscle structure and function was slowed down by regulating the activity homeostasis of Sirt1/PGC-1α pathway and Psn/arm pathway. Exercise enhanced the function of the Psn gene to delay skeletal muscle aging by up regulating the activity of the Sirt1/PGC-1α pathway and Psn/arm pathway.

摘要

早老素(Psn)基因与衰老密切相关,但 Psn 基因在骨骼肌中的作用尚不清楚。本研究利用果蝇的 Presenilin-UAS/Mhc-GAL4 系统来调控肌肉中 Psn 的过表达(MPO)和敲低(MPK)。从 4 周到 5 周龄,对果蝇进行耐力运动。结果显示,MPO 和运动显著提高了老年果蝇的攀爬速度、攀爬耐力、寿命、肌肉 SOD 活性、Psn 表达、Sirt1 表达、PGC-1α 表达和 Arm 表达,同时显著降低了肌肉丙二醛水平。有趣的是,当 Psn 基因被敲低 0.78 倍时,PGC-1α 表达和 Arm 表达也下调,但运动能力和寿命增加。此外,运动与 MPO 联合进一步提高了运动能力和寿命。MPK 结合运动进一步提高了运动能力和寿命。因此,目前的结果证实,肌肉 Psn 基因是一个重要的基因,它有助于骨骼肌的健康衰老,因为无论过表达还是敲低,通过调节 Sirt1/PGC-1α 通路和 Psn/Arm 通路的活性平衡,都能减缓骨骼肌结构和功能的衰老进程。运动通过上调 Sirt1/PGC-1α 通路和 Psn/Arm 通路的活性,增强了 Psn 基因的功能,从而延缓了骨骼肌的衰老。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b1ec/11098322/fbef6190f864/pone.0300787.g001.jpg

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