Unrelated donor HLA re-typing effort to verify prevalence of newer alleles: HLA-A*24:23, A*30:10, DRB1*08:11, DRB1*15:03, and DRB1*15:06.

J Kempenich; J Dehn; G Flickinger; M Setterholm

首页> 外文期刊>Tissue antigens. >Unrelated donor HLA re-typing effort to verify prevalence of newer alleles: HLA-A*24:23, A*30:10, DRB1*08:11, DRB1*15:03, and DRB1*15:06.

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Unrelated donor HLA re-typing effort to verify prevalence of newer alleles: HLA-A24:23, A30:10, DRB108:11, DRB115:03, and DRB1*15:06.

机译：不相关的供体HLA重新键入工作以验证较新的等位基因的流行：HLA-A * 24：23，A * 30：10，DRB1 * 08：11，DRB1 * 15：03和DRB1 * 15：06。

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The National Marrow Donor Program (NMDP) is committed to maintaining accurate human leukocyte antigen (HLA) data for each of the 11.5 million volunteer donors on the Be The Match Registry(?) . Qualitative data analysis identified five population specific alleles suspect of being incorrectly characterized. Alleles evaluated were HLA-A*24:03 for the presence of A*24:23 in Native Americans, A*30:02 for the presence of A*30:10 when B*41 and DRB1*04:05 were in the haplotype, DRB1*08:02 for the presence of DRB1*08:11 in Native Americans, and DRB1*15:01 for the presence of DRB1*15:03 in African Americans or DRB1*15:06 in Asian donors. Discrepancy rate was 55%, 86%, 31%, 75%, and 13%, respectively. Utilizing the HLA typing date, race, and date an allele in question was described may provide a selection strategy leading to the consideration of additional unrelated donors for searching patients.

机译：国家骨髓捐献者计划（NMDP）致力于为Be The Match Registry（？）上的1150万自愿捐献者中的每一个维护准确的人类白细胞抗原（HLA）数据。定性数据分析确定了五个特定人群的等位基因，其特征可能不正确。当B * 41和DRB1 * 04：05在美洲原住民中时，评估的等位基因为HLA-A * 24：03是否存在A * 24：23，A * 30：02是否存在A * 30：10。单倍型，在美洲原住民中存在DRB1 * 08：11表示为DRB1 * 08：02，在非裔美国人中存在DRB1 * 15：03表示为DRB1 * 15：01或在亚洲捐赠者中存在DRB1 * 15：06。差异率分别为55％，86％，31％，75％和13％。利用HLA分型日期，种族和描述等位基因的日期可以提供选择策略，从而导致考虑使用其他无关的供体来搜索患者。

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《Tissue antigens.》 |2014年第5期|共3页
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J Kempenich; J Dehn; G Flickinger; M Setterholm;
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1. Unrelated donor HLA re-typing effort to verify prevalence of newer alleles: HLA-A*24:23, A*30:10, DRB1*08:11, DRB1*15:03, and DRB1*15:06. [J] . J Kempenich, J Dehn, G Flickinger, Tissue antigens. . 2014,第5期

机译：不相关的供体HLA重新键入工作以验证较新的等位基因的流行：HLA-A * 24：23，A * 30：10，DRB1 * 08：11，DRB1 * 15：03和DRB1 * 15：06。
2. Characterization of a novel HLA‐DRB1*03 HLA‐DRB1*03 HLA‐DRB1*03 allele, DRB1*03:171 DRB1*03:171 DRB1*03:171 [J] . HLA. . 2020,第1期

机译：Castierzt f一个nofal hala-derb 1 * 03 Hala-Dart 1 * 03 Hala-Dart 1 * 03 Elly，Drab 1 * 03：171 DRB1 * 03：171 DRB1 * 03：171
3. HLA‐DRB1*15:03 and HLA‐DRB1*11: useful predictive alleles for alloantibody production in thalassemia patients [J] . Darvishi P., Sharifi Z., Azarkeivan A., Transfusion medicine . 2019,第3期

机译：HLA-DRB1 * 15：03和HLA-DRB1 * 11：中西血症患者的异丙化体生产有用的预测等位基因
4. Comparison of Outcomes of Hematopoietic Cell Transplants from T-Replete Haploidentical Donors Using Post-Transplantation Cyclophosphamide with 10 of 10 HLA-A, -B, -C, -DRB1, and -DQB1 Allele-Matched Unrelated Donors and HLA-Identical Sibling Donors: A Multivariable Analysis Including Disease Risk Index [O] . Bashey Asad, Zhang Xu, Jackson Katelin, 2016

机译：使用移植后的环磷酰胺与10个HLA-A，-B，-C，-DRB1和-DQB1等位基因匹配的无关供体和与HLA相同的同胞供体中的10个进行比较，从T型单倍体供体的造血细胞移植结果比较：包括疾病风险指数在内的多变量分析

Unrelated donor HLA re-typing effort to verify prevalence of newer alleles: HLA-A*24:23, A*30:10, DRB1*08:11, DRB1*15:03, and DRB1*15:06.

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Unrelated donor HLA re-typing effort to verify prevalence of newer alleles: HLA-A24:23, A30:10, DRB108:11, DRB115:03, and DRB1*15:06.