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AMP 激活的蛋白激酶下调渗透溶质转运蛋白 SMIT 和 BGT1。

Downregulation of the osmolyte transporters SMIT and BGT1 by AMP-activated protein kinase.

机构信息

Department of Physiology, Gmelinstr. 5, University of Tübingen, D72076 Tübingen, Germany.

出版信息

Biochem Biophys Res Commun. 2012 Jun 8;422(3):358-62. doi: 10.1016/j.bbrc.2012.04.092. Epub 2012 Apr 25.

Abstract

The myoinositol transporter SMIT (SLC5A3) and the betaine/γ-aminobutyric acid (GABA) transporter BGT1 (SLC6A12) accomplish cellular accumulation of organic osmolytes and thus contribute to cell volume regulation. Challenges of cell volume constancy include energy depletion, which compromises the function of the Na(+)/K(+) ATPase leading to cellular Na(+) accumulation and subsequent cell swelling. Energy depletion is sensed by AMP-activated protein kinase (AMPK). The present study explored whether AMPK influences the activity of SMIT and BGT1. To this end, cRNA encoding SMIT or BGT1 was injected into Xenopus oocytes with and without additional injection of wild type AMPK (AMPKα1+AMPKβ1+AMPKγ1), of constitutively active (γR70Q)AMPK (AMPKα1+AMPKβ1+(R70Q)AMPKγ1) or of catalytically inactive (αK45R)AMPK ((K45R)AMPKα1+AMPKβ1+AMPKγ1). Substrate-induced current in dual electrode voltage-clamp experiments was taken as measure of osmolyte transport. As a result, in SMIT-expressing, but not in water-injected Xenopus oocytes, myoinositol, added to the extracellular bath, generated a current (I(SMIT)), which was half maximal (K(M)) at ≈7.2μM myoinositol concentration. Furthermore, in BGT1-expressing, but not in water-injected Xenopus oocytes, GABA added to the bath generated a current (I(GABA)), which was half maximal (K(M)) at ≈0.5mM GABA concentration. Coexpression of AMPK and of (γR70Q)AMPK but not of (αK45R)AMPK significantly decreased I(SMIT) and I(GABA). AMPK decreased the respective maximal currents without significantly modifying the respective K(M). In conclusion, the AMP-activated kinase AMPK is a powerful regulator of the organic osmolyte transporters SMIT and BGT1 and thus interacts with cell volume regulation.

摘要

肌醇转运蛋白 SMIT(SLC5A3)和甜菜碱/γ-氨基丁酸(GABA)转运蛋白 BGT1(SLC6A12)完成细胞内有机渗透物的积累,从而有助于细胞体积调节。细胞体积恒定性的挑战包括能量耗竭,这会损害 Na(+)/K(+)ATP 酶的功能,导致细胞内 Na(+)积累和随后的细胞肿胀。能量耗竭由 AMP 激活的蛋白激酶(AMPK)感知。本研究探讨了 AMPK 是否影响 SMIT 和 BGT1 的活性。为此,将编码 SMIT 或 BGT1 的 cRNA 注入非洲爪蟾卵母细胞中,并在没有或有野生型 AMPK(AMPKα1+AMPKβ1+AMPKγ1)、组成型激活(γR70Q)AMPK(AMPKα1+AMPKβ1+(R70Q)AMPKγ1)或催化失活(αK45R)AMPK((K45R)AMPKα1+AMPKβ1+AMPKγ1)的情况下进行额外注射。双电极电压钳实验中的底物诱导电流被用作渗透物转运的测量。结果表明,在 SMIT 表达的,但不是在水注入的非洲爪蟾卵母细胞中,细胞外浴中添加肌醇会产生电流(I(SMIT)),其在约 7.2μM 肌醇浓度下达到半最大值(K(M))。此外,在 BGT1 表达的,但不是在水注入的非洲爪蟾卵母细胞中,浴中添加 GABA 会产生电流(I(GABA)),其在约 0.5mM GABA 浓度下达到半最大值(K(M))。AMPK 和(γR70Q)AMPK 的共表达,但不是(αK45R)AMPK 的共表达显著降低了 I(SMIT)和 I(GABA)。AMPK 降低了各自的最大电流,而没有显著改变各自的 K(M)。总之,AMP 激活的蛋白激酶 AMPK 是有机渗透物转运蛋白 SMIT 和 BGT1 的强大调节剂,因此与细胞体积调节相互作用。

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