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首页> 外文期刊>Vox Sanguinis: International Journal of Blood Transfusion and Immunohaematology >Establishment of reference panel for human platelet antigen genotyping
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Establishment of reference panel for human platelet antigen genotyping

机译:建立参考面板为人类血小板抗原基因分型

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Background and Objectives: Human platelet antigens (HPAs) are platelet-specific alloantigens associated with polymorphisms of platelet surface glycoproteins (GPs), and they can induce alloantibodies when individuals lacking a particular polymorphism are exposed to them via pregnancy or transfusion. Immune responses to HPAs are involved in the pathogenesis of several clinical syndromes. HPA genotyping is therefore important for clinical diagnosis and laboratory research. This study aims to establish a reference panel for HPA genotyping. Materials and Methods: Genomic DNA extracted from human blood was used as the template for amplifying HPA (1a-5a and 15a) gene fragments using specific primers. The amplified products were cloned into pGM-T vectors, which were transformed into competent TOP10 cells. After clone screening and amplification, the plasmids were extracted and sequenced. Next, the gene fragments HPA-1b-5b and 15b were obtained by site-directed mutagenesis using the corresponding HPA-1a-5a and 15a plasmids as template DNA. Results: We successfully constructed reference plasmids for HPA genotyping with HPA-1a-5a, 15a, HPA-1b-5b and 15b. The DNA sequences were consistent with those published in GenBank. Conclusion: Obtaining reference DNA for low-frequency HPAs is very difficult, and the successful construction of reference plasmids for the six HPA systems may solve this problem. Establishment of this panel has laid the foundation for future research on HPA genotyping.
机译:背景和目的:人类血小板抗原(hpa) platelet-specific同种抗原与血小板表面的多态性有关糖蛋白(GPs),他们可以诱导当个人缺乏同种抗体特定的多态性是通过暴露怀孕或输血。hpa参与几个的发病机理临床症状。重要的临床诊断和实验室研究。参考面板HPA基因分型。方法:从人血中提取的DNA是用作放大HPA模板(一)a-5a 15使用特定基因片段引物。pGM-T向量,变成了主管全球细胞。放大,提取质粒测序。15 b被定点诱变获得使用相应的HPA-1a-5a和15质粒DNA作为模板。成功地构造参考质粒与HPA-1a-5a HPA基因分型,15一个,HPA-1b-5b和15 b。发表在基因库。参考DNA低频hpa非常困难,成功的建设参考6 HPA系统可能的质粒解决这个问题。为未来的研究奠定了基础HPA基因分型。

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