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控制横纹肌蛋白质合成的营养信号成分。

Nutrient signaling components controlling protein synthesis in striated muscle.

作者信息

Vary Thomas C, Lynch Christopher J

机构信息

Department of Cellular and Molecular Physiology, Pennsylvania State University College of Medicine, Hershey, PA 17033, USA.

出版信息

J Nutr. 2007 Aug;137(8):1835-43. doi: 10.1093/jn/137.8.1835.

Abstract

Accretion of muscle mass is dependent upon faster rates of protein synthesis than degradation. When an animal is deprived of dietary protein, loss of body weight and negative nitrogen balance ensue. Likewise, refeeding accelerates protein synthesis and results in resumption of positive nitrogen balance. Amino acids and anabolic hormones both interact to maximally enhance rates of protein synthesis acutely during refeeding through an acceleration of the messenger RNA (mRNA) translation initiation. The review will illuminate the molecular mechanisms responsible for increasing mRNA translation initiation in striated muscle. The hastening of mRNA translation initiation most likely results from a stimulation of mammalian target of rapamycin (mTOR) acting through its downstream effector proteins eukaryotic initiation factors (eIF)4E binding protein1 and possibly eIF4G to enhance assembly of eIF4G with eIF4E and 70-kDa ribosomal S6 kinase1. Amino acids and leucine in particular are as effective as a complete meal in stimulating mRNA translation initiation by targeting these specific signal transduction systems. The physiologic importance lies in the potential ability of amino acids as specific nutrients designed to counteract the accelerated host protein wasting associated with a number of disease entities, including cancer, HIV infection, sepsis, and diabetes, and to improve nutrition to maintain muscle mass in aging populations and ensure muscle growth in neonatal populations.

摘要

肌肉质量的增加取决于蛋白质合成速率快于降解速率。当动物被剥夺膳食蛋白质时,体重减轻和负氮平衡随之而来。同样,重新喂食会加速蛋白质合成并导致正氮平衡的恢复。氨基酸和合成代谢激素在重新喂食期间通过加速信使核糖核酸(mRNA)翻译起始,相互作用以最大程度地急性提高蛋白质合成速率。本综述将阐明负责增加横纹肌中mRNA翻译起始的分子机制。mRNA翻译起始的加速很可能是由于雷帕霉素哺乳动物靶标(mTOR)通过其下游效应蛋白真核起始因子(eIF)4E结合蛋白1以及可能的eIF4G起作用,从而增强eIF4G与eIF4E和70 kDa核糖体S6激酶1的组装。氨基酸尤其是亮氨酸通过靶向这些特定的信号转导系统,在刺激mRNA翻译起始方面与一顿完整的膳食一样有效。生理重要性在于氨基酸作为特定营养素的潜在能力,旨在对抗与多种疾病实体(包括癌症、HIV感染、败血症和糖尿病)相关的加速的宿主蛋白质消耗,并改善营养状况以维持老年人群的肌肉质量并确保新生儿人群的肌肉生长。

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