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质膜钙泵:膜靶向、钙结合位点、组织特异性同工型表达

The calcium pump of the plasma membrane: membrane targeting, calcium binding sites, tissue-specific isoform expression.

作者信息

Guerini D, Garcia-Martin E, Zecca A, Guidi F, Carafoli E

机构信息

Institute of Biochemistry, Swiss Federal Institute of Technology (ETH), Zurich, Switzerland.

出版信息

Acta Physiol Scand Suppl. 1998 Aug;643:265-73.

PMID:9789569
Abstract

The two Ca2+ pumps of higher eucaryotes are strictly targeted to different membrane systems: the plasma membrane (PMCA) and the sarco(endo)plasmic reticulum (SERCA). Chimeric constructs of the two pumps expressed in COS-7 cells have revealed a strong signal for endoplasmic reticulum retention in the N-terminal cytosolic portion of the SERCA pump: the signal is contained in a stretch of 28 amino acids that follows the N-terminus. A second, but masked, endoplasmic reticulum retention signal is contained in a cytosolic C-terminal sequence immediately preceding the calmodulin-binding domain of the Ca2+ pump. Selective mutations on the SERCA pump have led to the conclusion that 5 conserved residue membrane domains (TM)4, 5, and 6 form the Ca2+ channel through the pump protein. A comparative sequence inspection has failed to reveal any of these residues in TM5 of the PMCA pump. Mutation of the conserved residue in TM4 and of two in TM6 abolished the ability of the pump to form the Ca(2+)-dependent phosphoenzyme. However, one of the mutations (N979, TM6) also caused retention of the PMCA pump in the reticulum, suggesting structural alterations. Of the four basic isoforms of the pump, two (1, 4) are ubiquitously expressed, two (2, 3) are essentially brain specific. Isoform 2 has the highest calmodulin affinity. Primary cultures of cerebellar granule cells from newborn rats did not express isoforms 2 and 3 at plating time. Incubation of the cells in depolarizing concentrations of KCl, which promote Ca2+ influx, promoted the expression of isoforms 2 and 3, and of a brain specific spliced variant of isoform 1. Incubation of the cells in L-type Ca2+ channel blockers abolished the upregulation of the pump genes.

摘要

高等真核生物的两种钙离子泵严格定位于不同的膜系统

质膜(质膜钙泵)和肌浆(内质)网(肌浆内质网钙泵)。在COS-7细胞中表达的两种泵的嵌合构建体显示,肌浆内质网钙泵的N端胞质部分存在内质网滞留的强信号:该信号包含在N端之后的一段28个氨基酸中。第二个但被掩盖的内质网滞留信号包含在钙离子泵钙调蛋白结合结构域之前紧邻的胞质C端序列中。对肌浆内质网钙泵的选择性突变得出结论,5个保守残基的膜结构域(跨膜结构域)4、5和6构成了穿过泵蛋白的钙离子通道。比较序列检查未能在质膜钙泵的跨膜结构域5中发现这些残基中的任何一个。跨膜结构域4中的保守残基和跨膜结构域6中的两个保守残基发生突变,消除了泵形成钙依赖磷酸酶的能力。然而,其中一个突变(N979,跨膜结构域6)也导致质膜钙泵滞留在内质网中,提示结构改变。在泵的四种基本同工型中,两种(1、4)普遍表达,两种(2、3)基本为脑特异性。同工型2具有最高的钙调蛋白亲和力。新生大鼠小脑颗粒细胞的原代培养物在接种时不表达同工型2和3。将细胞置于促进钙离子内流的去极化浓度的氯化钾中孵育,可促进同工型2和3以及同工型1的脑特异性剪接变体的表达。将细胞置于L型钙离子通道阻滞剂中孵育,可消除泵基因的上调。

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