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同一基因座对两种鞘脂激活蛋白(SAP - 1和SAP - 2)进行编码。

Coding of two sphingolipid activator proteins (SAP-1 and SAP-2) by same genetic locus.

作者信息

O'Brien J S, Kretz K A, Dewji N, Wenger D A, Esch F, Fluharty A L

机构信息

Department of Neurosciences, University of California, San Diego, La Jolla 92093.

出版信息

Science. 1988 Aug 26;241(4869):1098-101. doi: 10.1126/science.2842863.

Abstract

Several complementary DNAs (cDNAs) coding for sphingolipid activator protein-2 (SAP-2) were isolated from a lambda gt-11 human hepatoma library by means of polyclonal antibodies. The nucleotide sequence of the largest cDNA was colinear with the derived amino acid sequence of SAP-2 and with the nucleotide sequence of the cDNA coding for the 70-kilodalton precursor of SAP-1 (SAP precursor cDNA). The coding sequence for mature SAP-2 was located 3' to that coding for SAP-1 in the SAP precursor cDNA. Both SAP-1 and SAP-2 appeared to be derived by proteolytic processing from a common precursor that is coded by a genetic locus on human chromosome 10. Two other domains similar to SAP-1 and SAP-2 were also identified in SAP precursor protein. Each of the four domains was approximately 80 amino acid residues long, had nearly identical placement of cysteine residues, potential glycosylation sites, and proline residues. Each domain also contained internal amino acid sequences capable of forming amphipathic helices separated by helix breakers to give a cylindrical hydrophobic domain that is probably stabilized by disulfide bridges. Protein immunoblotting experiments indicated that SAP precursor protein (70 kilodaltons) as well as immunoreactive SAP-like proteins of intermediate sizes (65, 50, and 31 kilodaltons) are present in most human tissues.

摘要

利用多克隆抗体从λgt - 11人肝癌文库中分离出了几个编码鞘脂激活蛋白-2(SAP - 2)的互补DNA(cDNA)。最大的cDNA的核苷酸序列与推导的SAP - 2氨基酸序列以及编码SAP - 1的70千道尔顿前体的cDNA(SAP前体cDNA)的核苷酸序列共线。成熟SAP - 2的编码序列位于SAP前体cDNA中SAP - 1编码序列的3'端。SAP - 1和SAP - 2似乎都是由人类10号染色体上一个基因座编码的共同前体经蛋白水解加工而来。在SAP前体蛋白中还鉴定出另外两个与SAP - 1和SAP - 2相似的结构域。四个结构域中的每一个大约有80个氨基酸残基长,半胱氨酸残基、潜在糖基化位点和脯氨酸残基的位置几乎相同。每个结构域还包含能够形成两亲性螺旋的内部氨基酸序列,这些螺旋由螺旋破坏者隔开,形成一个可能由二硫键稳定的圆柱形疏水结构域。蛋白质免疫印迹实验表明,大多数人类组织中都存在SAP前体蛋白(70千道尔顿)以及中等大小的免疫反应性SAP样蛋白(65、50和31千道尔顿)。

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