内皮细胞老化与自噬失调

Basheer Abdullah Marzoog
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摘要

熵是一个影响所有活细胞的自然过程,包括衰老,衰老是一个不可逆转的生理过程,会损害细胞的平衡。年龄是疾病发生的一个重要因素,而内皮细胞衰老的发病机制是多因素的。自噬功能障碍会加速内皮细胞衰老和细胞死亡,而自噬则通过细胞内平衡和基因表达调控来保持内皮细胞的年轻状态。Sirt、mTORC1 和 AMPK 是青春基因,它们通过抑制 mTOR 和上调 FIP200/Atg13/ULK1 来诱导自噬。衰老的内皮细胞中 Lamin B1、γH2AX、Ki67、BrdU、PCNA 和 SA β-Gal 的水平下降。 保持健康年轻的内皮细胞可以预防大多数心血管疾病。以自噬为靶点是未来改变内皮细胞年龄、延缓或逆转衰老过程的潜在治疗策略。本文介绍了有关自噬在内皮细胞衰老中作用的最新研究。假设自噬失调与早期内皮细胞功能障碍和进一步的临床后遗症(包括动脉粥样硬化的形成)有关,从而导致各种心血管疾病。
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Endothelial Cell Aging and Autophagy Dysregulation.

Entropy is a natural process that affects all living cells, including senescence, an irreversible physiological process that impairs cell homeostasis. Age is a significant factor in disease development, and the pathogenesis of endothelial cell aging is multifactorial. Autophagy dysfunction accelerates endothelial cell aging and cell death, while autophagy preserves endothelial cell youthfulness through intracellular homeostasis and gene expression regulation. Sirt, mTORC1, and AMPK are youthfulness genes that induce autophagy by inhibiting mTOR and upregulating FIP200/Atg13/ULK1. Aged endothelial cells have decreased levels of Lamin B1, γH2AX, Ki67, BrdU, PCNA, and SA β-Gal. Maintaining healthy young endothelial cells can prevent most cardiovascular diseases. Autophagy targeting is a potential future therapeutic strategy to modify endothelial cell age and potentially slow or reverse the aging process. This article provides state-of-the-art research on the role of autophagy in endothelial cell aging. Hypothesizing that autophagy dysregulation is associated with early endothelial cell dysfunction and further clinical sequelae, including atherosclerosis formation, leading to various cardiovascular diseases.

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