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蛋白质-碳水化合物摄入改变Vps34在人骨骼肌中的细胞定位,且与激酶活性变化无关。

Protein-carbohydrate ingestion alters Vps34 cellular localization independent of changes in kinase activity in human skeletal muscle.

作者信息

Hodson Nathan, Dent Jessica R, Song Zhe, O'Leary Mary F, Nicholson Thomas, Jones Simon W, Murray James T, Jeromson Stewart, Hamilton D Lee, Breen Leigh, Philp Andrew

机构信息

School of Sport, Exercise and Rehabilitation Sciences, University of Birmingham, Birmingham, UK.

Institute of Inflammation and Ageing, University of Birmingham, Birmingham, UK.

出版信息

Exp Physiol. 2020 Dec;105(12):2178-2189. doi: 10.1113/EP088805. Epub 2020 Oct 17.

Abstract

NEW FINDINGS

What is the central question of the study? Is Vps34 a nutrient-sensitive activator of mTORC1 in human skeletal muscle? What is the main finding and its importance? We show that altering nutrient availability, via protein-carbohydrate feeding, does not increase Vps34 kinase activity in human skeletal muscle. Instead, feeding increased Vps34-mTORC1 co-localization in parallel to increased mTORC1 activity. These findings may have important implications in the understanding nutrient-induced mTORC1 activation in skeletal muscle via interaction with Vps34.

ABSTRACT

The Class III PI3Kinase, Vps34, has recently been proposed as a nutrient sensor, essential for activation of the mechanistic target of rapamycin (mTOR) complex 1 (mTORC1). We therefore investigated the effects of increasing nutrient availability through protein-carbohydrate (PRO-CHO) feeding on Vps34 kinase activity and cellular localization in human skeletal muscle. Eight young, healthy males (21 ± 0.5 yrs, 77.7 ± 9.9 kg, 25.9 ± 2.7 kg/m , mean ± SD) ingested a PRO-CHO beverage containing 20/44/1 g PRO/CHO/FAT respectively, with skeletal muscle biopsies obtained at baseline and 1 h and 3 h post-feeding. PRO-CHO feeding did not alter Vps34 kinase activity, but did stimulate Vps34 translocation toward the cell periphery (PRE (mean ± SD) - 0.273 ± 0.040, 1 h - 0.348 ± 0.061, Pearson's Coefficient (r)) where it co-localized with mTOR (PRE - 0.312 ± 0.040, 1 h - 0.348 ± 0.069, Pearson's Coefficient (r)). These alterations occurred in parallel to an increase in S6K1 kinase activity (941 ± 466% of PRE at 1 h post-feeding). Subsequent in vitro experiments in C2C12 and human primary myotubes displayed no effect of the Vps34-specific inhibitor SAR405 on mTORC1 signalling responses to elevated nutrient availability. Therefore, in summary, PRO-CHO ingestion does not increase Vps34 activity in human skeletal muscle, whilst pharmacological inhibition of Vps34 does not prevent nutrient stimulation of mTORC1 in vitro. However, PRO-CHO ingestion promotes Vps34 translocation to the cell periphery, enabling Vps34 to associate with mTOR. Therefore, our data suggests that interaction between Vps34 and mTOR, rather than changes in Vps34 activity per se may be involved in PRO-CHO activation of mTORC1 in human skeletal muscle.

摘要

新发现

该研究的核心问题是什么?Vps34是否是人类骨骼肌中对营养敏感的mTORC1激活剂?主要发现及其重要性是什么?我们发现,通过蛋白质-碳水化合物喂养改变营养供应情况,并不会增加人类骨骼肌中Vps34激酶的活性。相反,喂养会使Vps34与mTORC1的共定位增加,同时mTORC1的活性也会增加。这些发现对于理解通过与Vps34相互作用实现营养诱导的骨骼肌中mTORC1激活可能具有重要意义。

摘要

III类磷脂酰肌醇3激酶Vps34最近被认为是一种营养传感器,对雷帕霉素机制靶点(mTOR)复合物1(mTORC1)的激活至关重要。因此,我们研究了通过蛋白质-碳水化合物(PRO-CHO)喂养增加营养供应对人类骨骼肌中Vps34激酶活性和细胞定位的影响。八名年轻健康男性(21±0.5岁,77.7±9.9千克,25.9±2.7千克/米²,平均值±标准差)摄入了分别含有20/44/1克蛋白质/碳水化合物/脂肪的PRO-CHO饮料,并在基线、喂养后1小时和3小时获取骨骼肌活检样本。PRO-CHO喂养并未改变Vps34激酶活性,但确实刺激了Vps34向细胞周边易位(PRE(平均值±标准差)-0.273±0.040,1小时-0.348±0.061,皮尔逊相关系数(r)),在细胞周边它与mTOR共定位(PRE-0.312±0.040,1小时-0.348±0.069,皮尔逊相关系数(r))。这些变化与S6K1激酶活性增加(喂养后1小时为PRE的941±466%)同时发生。随后在C2C12和人类原代肌管中进行的体外实验显示,Vps34特异性抑制剂SAR405对mTORC1对营养供应增加的信号反应没有影响。因此,综上所述,摄入PRO-CHO不会增加人类骨骼肌中Vps34的活性,而在体外对Vps34进行药理抑制并不能阻止营养对mTORC1的刺激。然而,摄入PRO-CHO会促进Vps34向细胞周边易位,使Vps34能够与mTOR结合。因此,我们的数据表明,Vps34与mTOR之间的相互作用,而非Vps34活性本身的变化,可能参与了PRO-CHO对人类骨骼肌中mTORC1的激活。

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