首页> 外文期刊>European journal of immunogenetics: official journal of the British Society for Histocompatibility and Immunogenetics >Human platelet alloantigens (HPAs): PCR-SSP genotyping of a UK population for 15 HPA alleles.
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Human platelet alloantigens (HPAs): PCR-SSP genotyping of a UK population for 15 HPA alleles.

机译:人血小板同种异体抗原(HPA):英国人群中15个HPA等位基因的PCR-SSP基因分型。

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Alloimmunization to human platelet alloantigens (HPAs) is responsible for neonatal alloimmune thrombocytopenia (NAIT), post-transfusional purpura (PTP) and platelet transfusion refractoriness. HPAs may also have a role as histocompatibility antigens in transplantation as well as associations with cardiac disease. We have developed a polymerase chain reaction-sequence-specific primer (PCR-SSP) assay capable of detecting 15 HPA allelic variants. As part of the validation of the assay, 134 UK renal donors were genotyped to determine HPA allele frequencies in the UK population. The HPA allele frequencies obtained are consistent with those of the other European studies: GP1A*1 (HPA-5a) and GP1A*2 (HPA-5b), 0.914 and 0.086, respectively; GP1BA*1 (HPA-2a) and GP1BA*2 (HPA-2b), 0.925 and 0.075; GP2B*1 (HPA-3a) and GP2B*2 (HPA-3b), 0.627 and 0.373; GP3A*1 (HPA-1a) and GP3A*2 (HPA-1b), 0.840 and 0.161. The rare alleles GP2B*3 (HPA-9bw) and GP3A*3 to *8 (HPA-4b, -6b, -7bw, -8bw, -10bw and -11bw, respectively) were all absent. This comprehensive HPA genotyping assay allows rapid, accurate and reproducible results at low cost.
机译:对人血小板同种异体抗原(HPA)的同种免疫负责新生儿同种免疫血小板减少症(NAIT),输血后紫癜(PTP)和血小板输注的难治性。 HPA在移植以及与心脏病的关联中也可能具有组织相容性抗原的作用。我们已经开发出一种聚合酶链反应序列特异性引物(PCR-SSP)分析法,能够检测15个HPA等位基因变体。作为检验验证的一部分,对134个英国肾脏供体进行了基因分型,以确定英国人群中HPA等位基因的频率。获得的HPA等位基因频率与其他欧洲研究的频率一致:GP1A * 1(HPA-5a)和GP1A * 2(HPA-5b),分别为0.914和0.086; GP1BA * 1(HPA-2a)和GP1BA * 2(HPA-2b),0.925和0.075; GP2B * 1(HPA-3a)和GP2B * 2(HPA-3b),0.627和0.373; GP3A * 1(HPA-1a)和GP3A * 2(HPA-1b),0.840和0.161。罕见等位基因GP2B * 3(HPA-9bw)和GP3A * 3至* 8(分别为HPA-4b,-6b,-7bw,-8bw,-10bw和-11bw)均不存在。这项全面的HPA基因分型测定法可实现低成本,快速,准确和可重复的结果。

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