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一种针对人血小板细胞内膜的单克隆抗体(PL/IM 430),它能抑制钙离子的摄取而不影响钙离子 + 镁离子 - ATP酶。

A monoclonal antibody (PL/IM 430) to human platelet intracellular membranes which inhibits the uptake of Ca2+ without affecting the Ca2+ +Mg2+-ATPase.

作者信息

Hack N, Wilkinson J M, Crawford N

机构信息

Department of Biochemistry, Hunterian Institute, Royal College of Surgeons of England, London, U.K.

出版信息

Biochem J. 1988 Mar 1;250(2):355-61. doi: 10.1042/bj2500355.

Abstract

To probe the structure-function relationships of proteins present in the endoplasmic reticulum-like intracellular membranes of human blood platelets a panel of monoclonal antibodies have been raised, using as immunogen highly purified platelet intracellular membrane vesicles isolated by continuous flow electrophoresis [Menashi, Weintroub & Crawford (1981) J. Biol. Chem. 256, 4095-4101]. Four of these antibodies recognize a single 100 kDa polypeptide in the platelet membrane by immunoblotting. One antibody PL/IM 430 (of IgG1 subclass) inhibited (approximately 70%) the energy-dependent uptake of Ca2+ into the vesicles without affecting the Ca2+ +Mg2+-ATPase activity or the protein phosphorylation previously shown to proceed concomitantly with Ca2+ sequestration [Hack, Croset & Crawford (1986) Biochem. J. 233, 661-668]. The inhibition is independent of ATP concentration over a range 0-2 mM-ATP but shows dose-dependency for external [Ca2+] with maximum inhibition of Ca2+ translocation at concentrations of Ca2+ greater than 500 nM. This capacity of the antibody PL/IM 430 functionally to dislocate components of the intracellular membrane Ca2+ pump complex may have value in structural studies.

摘要

为了探究人血小板内质网样细胞内膜中蛋白质的结构 - 功能关系,我们制备了一组单克隆抗体,所用的免疫原是通过连续流电泳分离得到的高度纯化的血小板细胞内膜囊泡[梅纳西、温特劳布和克劳福德(1981年)《生物化学杂志》256卷,4095 - 4101页]。通过免疫印迹法,其中四种抗体识别血小板膜中的一种单一的100 kDa多肽。一种抗体PL/IM 430(IgG1亚类)抑制(约70%)Ca²⁺向囊泡中的能量依赖性摄取,而不影响Ca²⁺ + Mg²⁺ - ATP酶活性或先前显示与Ca²⁺螯合同时发生的蛋白质磷酸化[哈克、克罗塞和克劳福德(1986年)《生物化学杂志》233卷,661 - 668页]。在0 - 2 mM - ATP范围内,这种抑制作用与ATP浓度无关,但对细胞外[Ca²⁺]表现出剂量依赖性,在Ca²⁺浓度大于500 nM时,Ca²⁺转运的抑制作用最大。抗体PL/IM 430在功能上使细胞内膜Ca²⁺泵复合物的成分错位的这种能力,可能在结构研究中有价值。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3f85/1148863/4566890c3e9c/biochemj00236-0050-a.jpg

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