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横纹肌细胞的能量代谢设计。

Energy metabolism design of the striated muscle cell.

机构信息

Muscle Energetics Laboratory, National Heart, Lung, and Blood Insititute and National Institute of Arthritis and Musculoskeletal and Skin Disease, Bethesda, Maryland.

Laboratory of Cardiac Energetics, National Heart, Lung, and Blood Insititute, Bethesda, Maryland.

出版信息

Physiol Rev. 2021 Oct 1;101(4):1561-1607. doi: 10.1152/physrev.00040.2020. Epub 2021 Mar 18.

Abstract

The design of the energy metabolism system in striated muscle remains a major area of investigation. Here, we review our current understanding and emerging hypotheses regarding the metabolic support of muscle contraction. Maintenance of ATP free energy, so called energy homeostasis, via mitochondrial oxidative phosphorylation is critical to sustained contractile activity, and this major design criterion is the focus of this review. Cell volume invested in mitochondria reduces the space available for generating contractile force, and this spatial balance between mitochondria acontractile elements to meet the varying sustained power demands across muscle types is another important design criterion. This is accomplished with remarkably similar mass-specific mitochondrial protein composition across muscle types, implying that it is the organization of mitochondria within the muscle cell that is critical to supporting sustained muscle function. Beyond the production of ATP, ubiquitous distribution of ATPases throughout the muscle requires rapid distribution of potential energy across these large cells. Distribution of potential energy has long been thought to occur primarily through facilitated metabolite diffusion, but recent analysis has questioned the importance of this process under normal physiological conditions. Recent structural and functional studies have supported the hypothesis that the mitochondrial reticulum provides a rapid energy distribution system via the conduction of the mitochondrial membrane potential to maintain metabolic homeostasis during contractile activity. We extensively review this aspect of the energy metabolism design contrasting it with metabolite diffusion models and how mitochondrial structure can play a role in the delivery of energy in the striated muscle.

摘要

横纹肌能量代谢系统的设计仍是一个主要的研究领域。在这里,我们回顾了我们目前对肌肉收缩代谢支持的理解和新兴假说。通过线粒体氧化磷酸化维持 ATP 自由能,即所谓的能量平衡,对持续的收缩活动至关重要,这是本综述的主要设计标准。细胞中线粒体的投入体积减少了产生收缩力的可用空间,因此,在线粒体和无收缩元素之间存在另一个重要的设计标准,即保持空间平衡以满足不同肌肉类型的持续功率需求。这是通过在不同肌肉类型中具有非常相似的线粒体蛋白组成来实现的,这意味着线粒体在肌肉细胞内的组织对于支持持续的肌肉功能至关重要。除了产生 ATP 之外,ATP 酶在肌肉中的广泛分布要求在这些大细胞中快速分配潜在能量。长期以来,人们一直认为潜在能量的分布主要通过易化代谢物扩散来实现,但最近的分析对这种过程在正常生理条件下的重要性提出了质疑。最近的结构和功能研究支持了这样一种假说,即线粒体网通过传导线粒体膜电位为肌肉收缩活动期间的代谢平衡提供了一种快速的能量分配系统。我们广泛地回顾了这个能量代谢设计的方面,将其与代谢物扩散模型进行了对比,并讨论了线粒体结构如何在横纹肌的能量传递中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2d91/8576364/13542575a0b4/prv-00040-2020r01.jpg

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