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Emerging strategies of blood group genotyping for patients with hemoglobinopathies

机译:血吸虫病患者血型基因分型的新兴策略

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摘要

Red cell alloimmunization is a serious problem in chronically transfused patients. A number of high throughput DNA assays have been developed to extend or replace traditional serologic antigen typing. DNA-based typing methods may be easily automated and multiplexed, and provide reliable information on a patient. Molecular genotyping promises to become cheaper, being not dependent on serologic immunoglobulin reagents. Patients with hemoglobinopathies could benefit from receiving extended genomic typing. This could limit post transfusional complications depending on subtle antigenic differences between donors and patients. Patient/donor compatibility extended beyond the phenotype Rh/Kell may allows improved survival of transfused units of red blood cells (RBC) and lead to reduced need for blood transfusion and leading to less iron overload and reduced risk of alloimmunization. Here we discuss the advantages and limitations of current techniques, that detect only predefined genetic variants. In contrast, target enrichment next-generation sequencing (NGS) has been used to detect both known and de novo genetic polymorphisms, including single-nucleotide polymorphisms, indels (insertions/deletions), and structural variations. NGS approaches can be used to develop an extended blood group genotyping assay system. (C) 2016 Elsevier Ltd. All rights reserved.
机译:红细胞同种异体症是长期转发患者的严重问题。已经开发了许多高通量DNA测定以延伸或替代传统的血清抗原打字。基于DNA的键入方法可以容易地自动化和多路复用,并提供对患者的可靠信息。分子基因分型承诺变得更便宜,不依赖于血清素免疫球蛋白试剂。血吸虫病的患者可以免受接受延长的基因组打字。这可能会根据捐献者和患者之间的细微抗原差异限制输血后并发症。患者/供体兼容性延伸超出表型RH / Kell可以允许改善红细胞(RBC)的输血单位的存活率,并导致需求降低输血并导致较少的铁过载和降低同种免疫的风险降低。在这里,我们讨论了当前技术的优点和局限性,其仅检测预定义的遗传变形。相反,靶富集的下一代测序(NGS)已被用于检测已知和de Novo遗传多态性,包括单核苷酸多态性,诱导(插入/缺失)和结构变异。 NGS方法可用于开发扩展的血型基因分型测定系统。 (c)2016 Elsevier Ltd.保留所有权利。

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