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参与血小板输注无效的糖蛋白 Ibα 中氨基酸二态性的遗传和结构特征

Genetic and structural characterization of an amino acid dimorphism in glycoprotein Ib alpha involved in platelet transfusion refractoriness.

作者信息

Murata M, Furihata K, Ishida F, Russell S R, Ware J, Ruggeri Z M

机构信息

Department of Molecular and Experimental Medicine/Committee on Vascular Biology, Scripps Research Institute, La Jolla, CA 92037.

出版信息

Blood. 1992 Jun 1;79(11):3086-90.

PMID:1586750
Abstract

The platelet-specific alloantigen, Siba, located within the alpha-subunit of the glycoprotein (GP) Ib-IX membrane receptor, has been found to be involved in the pathogenesis of platelet transfusion refractoriness. We have identified the existence of a naturally occurring threonine/methionine dimorphism at position 145 of the GPIb alpha sequence, and determined that the Siba antigen corresponds to the molecule containing methionine145. The diallelic codons can be detected by restriction enzyme analysis of amplified genomic DNA fragments from the GPIb alpha gene. Evaluation of 61 healthy blood donors showed that the allele frequencies are 89% and 11% for the threonine145 and methionine145 codons, respectively. A positive correlation exists between platelet reactivity with the anti-Siba antibody and the presence of a methionine145-encoding allele. Moreover, recombinant expression of two soluble GPIb alpha fragments differing only at residue 145, provided definitive evidence that the human anti-Siba antibody reacts only with the molecule containing methionine145. These results explain the structural basis of the Siba human alloantigen system and define screening methodologies useful in transfusion medicine to match donor and recipient platelets accordingly.

摘要

血小板特异性同种抗原Siba位于糖蛋白(GP)Ib-IX膜受体的α亚基内,已发现其与血小板输注无效的发病机制有关。我们已确定在GPIbα序列的第145位存在天然存在的苏氨酸/蛋氨酸二态性,并确定Siba抗原对应于含有蛋氨酸145的分子。通过对来自GPIbα基因的扩增基因组DNA片段进行限制性酶切分析,可以检测到双等位密码子。对61名健康献血者的评估表明,苏氨酸145和蛋氨酸145密码子的等位基因频率分别为89%和11%。血小板与抗Siba抗体的反应性与编码蛋氨酸145的等位基因的存在之间存在正相关。此外,仅在第145位残基不同的两个可溶性GPIbα片段的重组表达提供了确凿证据,表明人抗Siba抗体仅与含有蛋氨酸145的分子反应。这些结果解释了Siba人类同种抗原系统的结构基础,并确定了在输血医学中用于相应匹配供体和受体血小板的筛选方法。

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