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携带吉田腹水肉瘤的大鼠红细胞表面的改变是由α2-巨球蛋白的一种肿瘤变体引起的。

Modification of the erythrocyte surface in rats bearing Yoshida ascites sarcoma is brought about by a tumour variant of alpha2-macroglobulin.

作者信息

Sanjay A, Kalraiya R D, Mehta N G

机构信息

Biological Chemistry Division, Cancer Research Institute, Tata Memorial Centre, Parel, Mumbai, India.

出版信息

Biochem J. 1997 Mar 1;322 ( Pt 2)(Pt 2):379-84. doi: 10.1042/bj3220379.

Abstract

Erythrocytes from the circulation of rats bearing Yoshida ascites sarcoma exhibit higher concanavalin A (ConA)-mediated agglutinability than those from normal animals. A tetrameric glycoprotein of subunit molecular mass 170 kDa, purified from the cell-free ascites fluid, was found to confer higher ConA-mediated agglutinability on erythrocytes in vitro. An antiserum to this tumour-derived protein failed to detect any cross-reactive component in normal rat plasma or in any of the normal tissues examined. An immunoreactive protein was, however, detected in blood plasma when the acute-phase reaction was stimulated by injection of turpentine. The cross-reactive acute-phase protein was purified by ConA-affinity, gel-filtration and ion-exchange chromatography, and identified as alpha2-macroglobulin. The acute-phase protein and the protein obtained from the ascites fluid have identical or very similar native and subunit molecular masses, subunit arrangement and pI. They both are able to inhibit trypsin and, as a consequence, acquire greater mobility in native PAGE. In addition, the two proteins bind to rat erythrocytes non-specifically, and in similar amounts. However, despite these similarities, the acute-phase protein is unable to enhance the agglutinability of erythrocytes. The two proteins differ in their carbohydrate content, but this differential glycosylation is not the cause of the difference in their surface modification activity. The chemically deglycosylated proteins show a small but consistent difference in the size of their polypeptides. Their tryptic peptide maps, although largely similar, show some differences, as do their amino acid compositions. It is probable that the proteins are independent members of the same (alpha-macroglobulin) family. The rat embryo is also found to express a soluble protein consisting of a 170 kDa polypeptide that cross-reacts with the antibody to the tumour-derived protein. The purified embryo protein is able to alter the ConA-mediated agglutinability of erythrocytes in vitro, and also yields a tryptic peptide map that is identical to that of the tumour-derived protein. The modification of the host cell surface in the tumour-bearing rats is thus caused by what appears to be a tumour (oncofetal?) variant of alpha2-macroglobulin.

摘要

携带吉田腹水肉瘤的大鼠循环系统中的红细胞,其伴刀豆球蛋白A(ConA)介导的凝集性高于正常动物的红细胞。从无细胞腹水液中纯化出一种亚基分子量为170 kDa的四聚体糖蛋白,发现它能在体外赋予红细胞更高的ConA介导的凝集性。针对这种肿瘤衍生蛋白的抗血清在正常大鼠血浆或所检测的任何正常组织中均未检测到任何交叉反应成分。然而,当通过注射松节油刺激急性期反应时,在血浆中检测到了一种免疫反应性蛋白。通过ConA亲和、凝胶过滤和离子交换色谱法纯化了交叉反应性急性期蛋白,并鉴定为α2-巨球蛋白。急性期蛋白和从腹水液中获得的蛋白具有相同或非常相似的天然和亚基分子量、亚基排列和pI。它们都能够抑制胰蛋白酶,因此在天然聚丙烯酰胺凝胶电泳中迁移率更高。此外,这两种蛋白都能非特异性地结合大鼠红细胞,且结合量相似。然而,尽管有这些相似之处,急性期蛋白却无法增强红细胞的凝集性。这两种蛋白的碳水化合物含量不同,但这种糖基化差异并不是它们表面修饰活性差异的原因。化学去糖基化的蛋白在多肽大小上显示出微小但一致的差异。它们的胰蛋白酶肽图虽然大体相似,但也存在一些差异,氨基酸组成也是如此。这些蛋白很可能是同一(α-巨球蛋白)家族的独立成员。还发现大鼠胚胎表达一种由170 kDa多肽组成的可溶性蛋白,它与针对肿瘤衍生蛋白的抗体发生交叉反应。纯化的胚胎蛋白能够在体外改变ConA介导的红细胞凝集性,其胰蛋白酶肽图也与肿瘤衍生蛋白的相同。因此,荷瘤大鼠宿主细胞表面的修饰似乎是由α2-巨球蛋白的一种肿瘤(癌胚?)变体引起的。

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本文引用的文献

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Structural comparison of rat alpha 1- and alpha 2-macroglobulins.大鼠α1-和α2-巨球蛋白的结构比较。
Biochem Biophys Res Commun. 1982 Sep 16;108(1):1-7. doi: 10.1016/0006-291x(82)91823-x.

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