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The Activation of Prosurvival Pathways in during Torpor.

出版信息

Physiol Biochem Zool. 2021 May-Jun;94(3):180-187. doi: 10.1086/714219.

Abstract

AbstractHibernation is a strategy used by some mammals to survive harsh winter conditions. Many small mammals, such as the little brown bat, , enter a long-term state of hibernation characterized by a period of deep torpor that can range from days to weeks. Torpid bats undergo metabolic rate depression that not only results in physiological changes but also promotes biochemical changes that favor survival. The present study utilizes multiplex technology to assess key early apoptosis markers and a select group of antioxidant enzymes in muscle, heart, and liver in euthermic controls and torpid bats. Muscle showed a significant decrease in the proapoptotic c-Jun N-terminal kinase and p53 and the antioxidant enzyme catalase but a significant increase in peroxiredoxin 2 levels. The heart responded similarly, with most proapoptotic proteins (caspase 8/9 and p53) remaining at low levels, while the antiapoptotic Bcl-2 protein significantly increased during torpor. There was no significant change in the antioxidant enzymes measured during torpor in the heart compared with the controls. The liver showed increases in catalase and Mn superoxide dismutase 2 enzymes during torpor, which correlated with activation of select antiapoptotic proteins and suppression of levels of proapoptotic ones. Overall, our data demonstrate that antiapoptotic and antioxidant defense responses have organ-specific regulation during torpor in bats. The induction of key antioxidant enzymes and antiapoptotic proteins may function as protective mechanisms that are necessary for surviving torpor.

摘要

摘要 冬眠是一些哺乳动物用来应对严酷冬季条件的一种策略。许多小型哺乳动物,如小褐蝙蝠,会进入一种长期的冬眠状态,其特征是一段可以持续数天到数周的深度休眠期。休眠中的蝙蝠会经历代谢率降低,这不仅导致生理变化,还促进了有利于生存的生化变化。本研究利用多重技术评估了正常状态下和休眠状态下的肌肉、心脏和肝脏中的关键早期凋亡标志物和一组抗氧化酶。肌肉中的促凋亡 c-Jun N-末端激酶和 p53 以及抗氧化酶过氧化氢酶显著减少,而过氧化物还原酶 2 水平显著增加。心脏的反应类似,大多数促凋亡蛋白(半胱天冬酶 8/9 和 p53)保持在低水平,而抗凋亡蛋白 Bcl-2 则在休眠期间显著增加。与对照组相比,心脏在休眠期间测量的抗氧化酶没有显著变化。肝脏在休眠期间过氧化氢酶和 Mn 超氧化物歧化酶 2 酶的增加,与选择的抗凋亡蛋白的激活和促凋亡蛋白水平的抑制相关。总的来说,我们的数据表明,在蝙蝠的冬眠过程中,抗凋亡和抗氧化防御反应具有器官特异性调节。关键抗氧化酶和抗凋亡蛋白的诱导可能是在休眠中存活所必需的保护机制。

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