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叙利亚仓鼠心脏的蛰伏-觉醒周期与蛋白质质量控制系统的短暂激活有关。

Torpor-arousal cycles in Syrian hamster heart are associated with transient activation of the protein quality control system.

作者信息

Wiersma Marit, Beuren Thais M A, de Vrij Edwin L, Reitsema Vera A, Bruintjes Jantje J, Bouma Hjalmar R, Brundel Bianca J J M, Henning Robert H

机构信息

Department of Physiology, Amsterdam Cardiovascular Sciences, VU University Medical Center, Amsterdam, The Netherlands; Department of Clinical Pharmacy and Pharmacology, University of Groningen, University Medical Center Groningen, The Netherlands.

Department of Physiology, Amsterdam Cardiovascular Sciences, VU University Medical Center, Amsterdam, The Netherlands; Department of Clinical Pharmacy and Pharmacology, University of Groningen, University Medical Center Groningen, The Netherlands.

出版信息

Comp Biochem Physiol B Biochem Mol Biol. 2018 Sep;223:23-28. doi: 10.1016/j.cbpb.2018.06.001. Epub 2018 Jun 9.

Abstract

Hibernation consists of torpor, with marked suppression of metabolism and physiological functions, alternated with arousal periods featuring their full restoration. The heart is particularly challenged, exemplified by its rate reduction from 400 to 5-10 beats per minute during torpor in Syrian hamsters. In addition, during arousals, the heart needs to accommodate the very rapid return to normal function, which lead to our hypothesis that cardiac function during hibernation is supported by maintenance of protein homeostasis through adaptations in the protein quality control (PQC) system. Hereto, we examined autophagy, the endoplasmic reticulum (ER) unfolded protein (UPR) response and the heat shock response (HSR) in Syrian hamster hearts during torpor and arousal. Transition from torpor to arousal (1.5 h) was associated with stimulation of the PQC system during early arousal, demonstrated by induction of autophagosomes, as shown by an increase in LC3B-II protein abundance, likely related to the activation of the UPR during late torpor in response to proteotoxic stress. The HSR was not activated during torpor or arousal. Our results demonstrate activation of the cardiac PQC system - particularly autophagosomal degradation - in early arousal in response to cardiac stress, to clear excess aberrant or damaged proteins, being gradually formed during the torpor bout and/or the rapid increase in heart rate during the transition from torpor to arousal. This mechanism may enable the large gain in cardiac function during the transition from torpor to arousal, which may hold promise to further understand 'hibernation' of cardiomyocytes in human heart disease.

摘要

冬眠由蛰伏期和觉醒期交替组成,蛰伏期新陈代谢和生理功能显著抑制,觉醒期则完全恢复。心脏面临着特别的挑战,例如叙利亚仓鼠在蛰伏期心率从每分钟400次降至5 - 10次。此外,在觉醒过程中,心脏需要适应迅速恢复到正常功能,这使我们提出一个假设:冬眠期间心脏功能通过蛋白质质量控制(PQC)系统的适应性变化维持蛋白质稳态来得到支持。为此,我们研究了叙利亚仓鼠心脏在蛰伏期和觉醒期的自噬、内质网(ER)未折叠蛋白反应(UPR)和热休克反应(HSR)。从蛰伏期到觉醒期的转变(1.5小时)与觉醒早期PQC系统的激活有关,这通过自噬体的诱导得以证明,如LC3B-II蛋白丰度增加所示,这可能与蛰伏期末期因蛋白毒性应激而激活的UPR有关。蛰伏期或觉醒期HSR均未被激活。我们的结果表明,心脏PQC系统——特别是自噬体降解——在觉醒早期因心脏应激而被激活,以清除在蛰伏期逐渐形成的以及从蛰伏期到觉醒期心率快速增加过程中产生的过量异常或受损蛋白质。这种机制可能使从蛰伏期到觉醒期心脏功能大幅提升,这可能为进一步理解人类心脏病中心肌细胞的“冬眠”带来希望。

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