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人类红细胞膜阴离子转运蛋白带3的免疫学研究。

An immunological study of band 3, the anion transport protein of the human red blood cell membrane.

作者信息

England B J, Gunn R B, Steck T L

出版信息

Biochim Biophys Acta. 1980 May 29;623(1):171-82. doi: 10.1016/0005-2795(80)90019-7.

Abstract

Band 3, the predominant membrane-spanning polypeptide and purported anion transport protein of human red cells, was isolated by a new procedure which utilized selective solubilization and anion exchange chromatography on Affi-Gel 102 in 0.5% and Triton X-100/0.03% sodium dodecyl sulfate. Rabbit anti-serum prepared against the purified protein reacted with human and monkey band 3 but gave no immunoprecipitate with membrane proteins from several non-primate species. The antiserum was directed solely towards a portion of the cytoplasmic pole of the band 3 polypeptide contained within a 23,000 dalton amino-terminal fragment, as shown by agglutination, absorption, double diffusion and immunoprecipitation techniques. Saturation of both surfaces of resealed erythrocyte ghosts with the anti-band 3 antiserum had no significant effect on chloride transport. Our data define the topographically-limited immunogenicity of human band 3 in rabbits, demonstrate a lack of immunological cross-reactivity of band 3 between primates and non-primates, and support the hypothesis that the cytoplasmic domain of band 3 is not intimately involved in anion transport.

摘要

带3是人类红细胞中主要的跨膜多肽和所谓的阴离子转运蛋白,它是通过一种新方法分离出来的。该方法利用选择性溶解和在含有0.5% Triton X - 100/0.03%十二烷基硫酸钠的Affi - Gel 102上进行阴离子交换色谱法。用针对纯化蛋白制备的兔抗血清与人及猴的带3发生反应,但与几种非灵长类动物的膜蛋白没有产生免疫沉淀。通过凝集、吸收、双向扩散和免疫沉淀技术表明,该抗血清仅针对带3多肽细胞质端内一个23,000道尔顿氨基末端片段中的一部分。用抗带3抗血清使重封红细胞血影的两个表面饱和,对氯化物转运没有显著影响。我们的数据确定了人带3在兔体内的拓扑学上有限的免疫原性,证明了带3在灵长类和非灵长类之间缺乏免疫交叉反应性,并支持带3的细胞质结构域与阴离子转运没有密切关系这一假说。

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