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天然存在的人类抗带3自身抗体加速豚鼠红细胞的清除。

Naturally occurring human anti-band 3 autoantibodies accelerate clearance of erythrocytes in guinea pigs.

作者信息

Giger U, Sticher B, Naef R, Burger R, Lutz H U

机构信息

Laboratory for Biochemistry, Swiss Federal Institute of Technology, ETH-Zentrum, Zürich.

出版信息

Blood. 1995 Apr 1;85(7):1920-8.

PMID:7703495
Abstract

A variety of naturally occurring autoantibodies (NOAs) have been found in sera of animals and humans. Although their specific homeostatic role in the clearance of altered or senescent cells has been proposed and in vitro studies support such functions, in vivo evidence has been lacking. We studied the effect of affinity-purified human anti-band 3 NOA on the survival of untreated and diamide-treated erythrocytes in normal and complement C3-deficient guinea pigs. In vitro exposure to diamide, an oxidative agent, severely reduced the erythrocyte deformability and increased the amount of high-molecular-weight forms of band 3 protein and band 3-hemoglobin adducts in erythrocyte membranes, thereby markedly shortening the survival of these cells in vivo. Human anti-band 3 NOA bound in a dose-dependent manner to erythrocytes, and binding increased with exposure to diamide. In normal guinea pigs anti-band 3 NOA significantly accelerated the clearance of erythrocytes that were mildly damaged by iodine surface labeling and of those that were further oxidized by diamide. However, the anti-band 3 effect was transient and small. In contrast, anti-band 3 NOA did not significantly alter erythrocyte survival in functionally C3-deficient guinea pigs, thereby supporting the C3b requirement for anti-band 3 NOA activity. On the other hand, a pretreatment of animals with purified human band 3 protein slowed down the clearance of erythrocytes incubated with IgG depleted of anti-band 3 NOA. These results provide the first in vivo evidence of a role for anti-band 3 NOA in the clearance of erythrocytes.

摘要

在动物和人类血清中发现了多种天然存在的自身抗体(NOA)。尽管有人提出它们在清除改变或衰老细胞方面具有特定的稳态作用,并且体外研究也支持这些功能,但一直缺乏体内证据。我们研究了亲和纯化的人抗带3 NOA对正常和补体C3缺陷豚鼠中未处理和经二酰胺处理的红细胞存活的影响。体外暴露于氧化剂二酰胺会严重降低红细胞的变形能力,并增加红细胞膜中带3蛋白的高分子量形式和带3-血红蛋白加合物的量,从而显著缩短这些细胞在体内的存活时间。人抗带3 NOA以剂量依赖性方式与红细胞结合,并且随着暴露于二酰胺,结合增加。在正常豚鼠中,抗带3 NOA显著加速了因碘表面标记而轻度受损的红细胞以及因二酰胺进一步氧化的红细胞的清除。然而,抗带3的作用是短暂且微小的。相比之下,抗带3 NOA在功能上缺乏C3的豚鼠中并未显著改变红细胞的存活,从而支持了抗带3 NOA活性对C3b的需求。另一方面,用纯化的人带3蛋白对动物进行预处理会减慢与去除了抗带3 NOA的IgG一起孵育的红细胞的清除速度。这些结果首次提供了抗带3 NOA在红细胞清除中起作用的体内证据。

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