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Human platelet antigens - 2013

机译:人类血小板抗原- 2013

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摘要

To date, 33 human platelet alloantigens (HPAs) have been identified on six functionally important platelet glycoprotein (GP) complexes and have been implicated in alloimmune platelet disorders including foetal and neonatal alloimmune thrombocytopenia (FNAIT), posttransfusion purpura (PTP) and multitransfusion platelet refractoriness (MPR). The greatest number of recognized HPA (20 of 33) resides on the GPIIb/IIIa complex, which serves as the receptor for ligands important in mediating haemostasis and inflammation. These include HPA-1a, the most commonly implicated HPA in FNAIT and PTP in Caucasian populations. Other platelet GP complexes, GPIb/V/IX, GPIa/IIa and CD109, express the remaining 13 HPAs. Of the recognized HPAs, 12 occur as six serologically and genetically defined biallelic 'systems' where the -a form designates the higher frequency allele and the -b form, the lower. Twenty-one other HPAs are low-frequency or rare antigens for which postulated higher frequency -a alleles have not yet been identified as antibody specificities. In addition to the HPA markers, platelets also express ABO and human leucocyte antigen (HLA) antigens; antibodies directed at the former are occasionally important in FNAIT, and to the latter, in MPR.
机译:到目前为止,33人血小板同种抗原(hpa)已确定6个功能重要的血小板糖蛋白(GP)复合物与同种免疫性血小板障碍包括胎儿和新生儿同种免疫性血小板减少症(FNAIT),posttransfusion紫癜(PTP)和multitransfusion血小板耐火度(MPR)。最大数量的公认HPA 33的(20)位于GPIIb / iii a复杂,服务作为配体的受体的重要调解止血和炎症。包括HPA-1a,最常涉及HPA在FNAIT和PTP在高加索人群。血小板GP复合物,GPIb / V / IX, GPIa /花絮和CD109,表达其余13 hpa。公认的hpa 12发生六个血清和基因定义biallelic‘系统’——形式指定更高的频率等位基因和- b形式,较低。其他hpa低频或罕见的抗原假设高频率——等位基因没有被确认为抗体特异性。血小板也表达ABO血型和人类白细胞抗原(HLA)抗原;前者在FNAIT偶尔重要,在MPR,后者。

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