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在 K 依赖性 Na-Ca 交换器(NCKX2)中,对 K 离子转运重要的残基。

Residues important for K ion transport in the K-dependent Na-Ca exchanger (NCKX2).

机构信息

Department of Physiology and Pharmacology, Hotchkiss Brain Institute, Cumming School of Medicine, University of Calgary, Calgary, AB, Canada.

Department of Physiology and Pharmacology, Hotchkiss Brain Institute, Cumming School of Medicine, University of Calgary, Calgary, AB, Canada.

出版信息

Cell Calcium. 2018 Sep;74:61-72. doi: 10.1016/j.ceca.2018.06.005. Epub 2018 Jun 25.

Abstract

K-dependent Na-Ca exchangers (NCKXs) play an important role in Ca homeostasis in many tissues. NCKX proteins are bi-directional plasma membrane Ca-transporters which utilize the inward Na and outward K gradients to move Ca ions into and out of the cytosol (4Na:1Ca + 1 K). In this study, we carried out scanning mutagenesis of all the residues of the highly conserved α-1 and α-2 repeats of NCKX2 to identify residues important for K transport. These structural elements are thought to be critical for cation transport. Using fluorescent intracellular Ca-indicating dyes, we measured the K dependence of transport carried out by wildtype or mutant NCKX2 proteins expressed in HEK293 cells and analyzed shifts in the apparent binding affinity (K) of mutant proteins in comparison with the wildtype exchanger. Of the 93 residue substitutions tested, 34 were found to show a significant shift in the external K ion dependence of which 16 showed an increased affinity to K ions and 18 showed a decreased affinity and hence are believed to be important for K ion binding and transport. We also identified 8 residue substitutions that resulted in a partial loss of K dependence. Our biochemical data provide strong support for the cation binding sites identified in a homology model of NCKX2 based on crystal structures reported for distantly related archaeal Na-Ca exchanger NCX_Mj. In addition, we compare our results here with our previous studies that report on residues important for Ca and Na binding. Supported by CIHR MOP-81327.

摘要

依赖 K 的 Na-Ca 交换器(NCKXs)在许多组织的 Ca 稳态中发挥着重要作用。NCKX 蛋白是双向的质膜 Ca 转运体,利用内向的 Na 和外向的 K 梯度将 Ca 离子移入和移出细胞质(4Na:1Ca+1K)。在这项研究中,我们对 NCKX2 的高度保守的α-1 和 α-2 重复序列中的所有残基进行了扫描诱变,以鉴定对 K 转运重要的残基。这些结构元件被认为对阳离子转运至关重要。使用荧光细胞内 Ca 指示剂染料,我们测量了在 HEK293 细胞中表达的野生型或突变 NCKX2 蛋白进行的 K 转运的依赖性,并分析了与野生型交换器相比,突变蛋白的表观结合亲和力(K)的变化。在测试的 93 个残基取代中,发现 34 个明显改变了外 K 离子依赖性,其中 16 个对 K 离子的亲和力增加,18 个亲和力降低,因此被认为对 K 离子结合和转运很重要。我们还鉴定了 8 个导致部分丧失 K 依赖性的残基取代。我们的生化数据为基于晶体结构报告的远亲古细菌 Na-Ca 交换器 NCX_Mj 的 NCKX2 同源模型中鉴定的阳离子结合位点提供了强有力的支持。此外,我们将这里的结果与我们之前报告的对 Ca 和 Na 结合重要的残基的研究进行了比较。由加拿大卫生研究院 MOP-81327 资助。

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