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由于秀丽隐杆线虫钠氢交换体NHX - 2缺失导致肠道细胞胞内pH值降低,从而延长了寿命。

A reduction in intestinal cell pHi due to loss of the Caenorhabditis elegans Na+/H+ exchanger NHX-2 increases life span.

作者信息

Nehrke Keith

机构信息

Gastroenterology Unit, Department of Medicine, University of Rochester Medical Center, Rochester, New York 14642, USA.

出版信息

J Biol Chem. 2003 Nov 7;278(45):44657-66. doi: 10.1074/jbc.M307351200. Epub 2003 Aug 25.

Abstract

Na+/H+ exchangers are involved in cell volume regulation, fluid secretion and absorption, and pH homeostasis. NHX-2 is a Caenorhabditis elegans Na+/H+ exchanger expressed exclusively at the apical membrane of intestinal epithelial cells. The inactivation of various intestinal nutrient transport proteins has been shown previously to influence aging via metabolic potential and a mechanism resembling caloric restriction. We report here a functional coupling of NHX-2 activity with nutrient uptake that results in long lived worms. Gene inactivation of nhx-2 by RNAi led to a loss of fat stores in the intestine and a 40% increase in longevity. The NHX-2 protein was coincidentally expressed with OPT-2, an oligopeptide transporter that is driven by a transmembrane proton gradient and that is also known to be involved in fat accumulation. Gene inactivation of opt-2 led to a phenotype resembling that of nhx-2, although not as severe. In order to explore this potential functional interaction, we combined RNA interference with a genetically encoded, fluorescence-based reagent to measure intestinal intracellular pH (pHi) in live worms under physiological conditions. Our results suggest first that OPT-2 is the main dipeptide uptake pathway in the nematode intestine, and second that dipeptide uptake results in intestinal cell acidification, and finally that recovery following dipeptide-induced acidification is normally a function of NHX-2. The loss of NHX-2 protein results in decreased steady-state intestinal cell pHi, and we hypothesize that this change perturbs proton-coupled nutrient uptake processes such as performed by OPT-2. Our data demonstrate a functional role for a Na+/H+ exchanger in nutrient absorption in vivo and lays the groundwork for examining integrated acid-base physiology in a non-mammalian model organism.

摘要

钠氢交换体参与细胞体积调节、液体分泌与吸收以及pH稳态。NHX - 2是一种仅在秀丽隐杆线虫肠道上皮细胞顶端膜表达的钠氢交换体。先前已表明,各种肠道营养转运蛋白的失活会通过代谢潜能和一种类似于热量限制的机制影响衰老。我们在此报告NHX - 2活性与营养物质摄取之间的功能偶联,这会导致线虫寿命延长。通过RNA干扰使nhx - 2基因失活会导致肠道脂肪储存减少,寿命延长40%。NHX - 2蛋白与OPT - 2同时表达,OPT - 2是一种由跨膜质子梯度驱动的寡肽转运体,也已知其参与脂肪积累。使opt - 2基因失活会导致类似于nhx - 2的表型,尽管程度没那么严重。为了探究这种潜在的功能相互作用,我们将RNA干扰与一种基于荧光的基因编码试剂相结合,以测量生理条件下活线虫肠道内的细胞内pH(pHi)。我们的结果首先表明OPT - 2是线虫肠道中主要的二肽摄取途径,其次表明二肽摄取会导致肠道细胞酸化,最后表明二肽诱导酸化后的恢复通常是NHX - 2的功能。NHX - 2蛋白的缺失会导致肠道细胞pHi的稳态降低,我们推测这种变化会扰乱质子偶联的营养物质摄取过程,如OPT - 2所执行的过程。我们的数据证明了钠氢交换体在体内营养物质吸收中的功能作用,并为在非哺乳动物模式生物中研究酸碱综合生理学奠定了基础。

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