Resolution of HLA-B*44:02:01G, -DRB1*14:01:01G and -DQB1*03:01:01G reveals a high allelic variability among 12 European populations.

B Vidan-Jeras; S Buhler; V Dubois; Z Grubic; M Ivanova; T Jaatinen; D Ligeiro; M-L Lokki; C Papasteriades; F Poli; M Spyropoulou-Vlachou; A Tordai; M K Viken; S Wenda; J M Nunes; A Sanchez-Mazas; J-M Tiercy

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Resolution of HLA-B44:02:01G, -DRB114:01:01G and -DQB1*03:01:01G reveals a high allelic variability among 12 European populations.

机译：HLA-B * 44：02：01G，-DRB1 * 14：01：01G和-DQB1 * 03：01：01G的分辨率揭示了12个欧洲人群之间的高等位基因变异性。

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Within the framework of the EU-funded HLA-NET action, an analysis of three G-group alleles, HLA-B*44:02:01G, DRB1*14:01:01G and DQB1*03:01:01G, was undertaken in 12 European populations. Ambiguities were resolved by polymerase chain reaction-sequence-specific amplification (PCR-SSP) or PCR-sequence-based typing (PCR-SBT) in a total of 5095 individuals. The results of the DRB1*14:01/14:54 ambiguity showed high relative ratios (24-53%) of DRB1*14:01 in Bulgarians, Croatians, Greeks, Italians and Slovenians, contrasting with low ratios (6-13%) in Austrians, Finnish, French, Hungarians, Norwegians and Swiss. Resolution of the B*44:02/44:27 ambiguity showed that B*44:27 had a high relative ratio in Slovenians (25.5%) and Bulgarians (37%) and low in French and Swiss (0.02-1%), and was not observed in Greeks and Italians. The highest relative ratio of DQB1*03:19 was found in Portuguese (11%), by contrast with low ratios (0-3%) in the other five populations. Analysis of the A, B, DRB1 phenotypes and family-derived haplotypes in 1719 and 403 individuals positive for either HLA-B*44:02G or DRB1*14:01G ambiguities, respectively, showed some preferential associations, such as A*26～DRB1*14:01, B*35～DRB1*14:01, B*38～DRB1*14:01 and B*44:27～DRB1*16. Because these ambiguities are located outside the peptide-binding site, they may not be recognized by alloreactive T-cells. However, because of strong linkage disequilibrium (LD), the DRB1*14:01 vs DRB1*14:54 and the B*44:02 vs B*44:27 mismatches are associated to DRB3-, and C-mismatches, respectively. These results are informative for algorithms searching unrelated hematopoietic stem cell donors. For B*44:27-positive patients, searches are expected to be more successful when requesting donors from Southeastern-European ancestry. Furthermore, the introduction of human leukocyte antigen (HLA)-typing strategies that allow resolving exon 4 (for class I) and exon 3 (for class II) polymorphisms can be expected to contribute significantly to population genetics studies.

机译：在欧盟资助的HLA-NET行动框架内，对三个G组等位基因HLA-B * 44：02：01G，DRB1 * 14：01：01G和DQB1 * 03：01：01G进行了分析在12个欧洲人口中。通过聚合酶链反应-序列特异性扩增（PCR-SSP）或基于PCR序列的分型（PCR-SBT）解决了总共5095人的歧义。 DRB1 * 14：01/14：54歧义的结果表明，保加利亚人，克罗地亚人，希腊人，意大利人和斯洛文尼亚人中DRB1 * 14：01的相对比率较高（24-53％），而比率较低（6-13％））在奥地利，芬兰，法国，匈牙利，挪威和瑞士。 B * 44：02/44：27歧义度的解析表明，B * 44：27在斯洛文尼亚人（25.5％）和保加利亚人（37％）中具有较高的相对比率，而在法国和瑞士人中则相对较低（0.02-1％），并且在希腊人和意大利人中没有观察到。在葡萄牙，DQB1 * 03：19的相对比例最高（11％），而其他五个人群的相对比例较低（0-3％）。分别对HLA-B * 44：02G或DRB1 * 14：01G歧义呈阳性的1719和403个人的A，B，DRB1表型和家族衍生的单倍型进行分析，显示出一些优先关联，例如A * 26〜 DRB1 * 14：01，B * 35〜DRB1 * 14：01，B * 38〜DRB1 * 14：01和B * 44：27〜DRB1 * 16。由于这些歧义性位于肽结合位点之外，因此它们可能不会被同种异体反应性T细胞识别。但是，由于强烈的连锁不平衡（LD），DRB1 * 14：01与DRB1 * 14：54以及B * 44：02与B * 44：27的错配分别与DRB3和C错配相关。这些结果为搜索无关造血干细胞供体的算法提供了有益的信息。对于B * 44：27阳性的患者，当请求东南欧血统的捐赠者时，搜索会更成功。此外，引入人类白细胞抗原（HLA）分型策略可以解决外显子4（对于I类）和外显子3（对于II类）多态性，有望为人口遗传学研究做出重要贡献。

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《Tissue antigens.》 |2014年第5期|共6页
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B Vidan-Jeras; S Buhler; V Dubois; Z Grubic; M Ivanova; T Jaatinen; D Ligeiro; M-L Lokki; C Papasteriades; F Poli; M Spyropoulou-Vlachou; A Tordai; M K Viken; S Wenda; J M Nunes; A Sanchez-Mazas; J-M Tiercy;
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中图分类人体形态学;
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1. Resolution of HLA-B*44:02:01G, -DRB1*14:01:01G and -DQB1*03:01:01G reveals a high allelic variability among 12 European populations. [J] . B Vidan-Jeras, S Buhler, V Dubois, Tissue antigens. . 2014,第5期

机译：HLA-B * 44：02：01G，-DRB1 * 14：01：01G和-DQB1 * 03：01：01G的分辨率揭示了12个欧洲人群之间的高等位基因变异性。
2. DISTRIBUTION ANALYSIS OF DPB1*104:01 UNEXPECTED RESULTS FOR A MEMBER OF THE DPB1*03:01:01G AMBIGUOUS ALLELE GROUP [J] . Antovich Zachary, Singh Komal M., Russnak Roland, HLA. . 2016,第4期

机译：DPB1 * 03：01：01G歧义等位基因群成员的DPB1 * 104：01异常结果分析
3. DISTRIBUTION ANALYSIS OF DPB1*104:01-UNEXPECTED RESULTS FOR A MEMBER OF THE DPB1*03:01:01G AMBIGUOUS ALLELE GROUP [J] . Antovich Zachary, Singh Komal, Russnak Roland, Human Immunology: Official Journal of the American Society for Histocompatibility and Immunogenetics . 2016,第Suppla1期

机译：DPB1 * 03：01：01G成员等位基因DPB1 * 104：01的异常结果分析
4. Human Leukocyte Antigen and Systemic Sclerosis in Japanese: The Sign of the Four Independent Protective Alleles DRB1*13:02 DRB1*14:06 DQB1*03:01 and DPB1*02:01 [O] . Hiroshi Furukawa, Shomi Oka, Aya Kawasaki, -1

机译：日语中的人类白细胞抗原和全身性硬化症：四个独立保护性等位基因的标志DRB1 * 13：02DRB1 * 14：06DQB1 * 03：01和DPB1 * 02：01
5. Identification of the new HLA-B*44:02:45, DQB1*02:85, DQB1*06:210, DRB1*01:01:30 alleles by monoallelic Sanger sequencing [O] . Elena V. Kuzmich, Alexander L. Alyanskiy, Svetlana S. Tyapushkina, 2018

机译：识别新的HLA-B * 44：02：45，DQB1 * 02：85，DQB1 * 06：210，DRB1 * 01：01：30通过单一的Sanger测序等位基因

Resolution of HLA-B*44:02:01G, -DRB1*14:01:01G and -DQB1*03:01:01G reveals a high allelic variability among 12 European populations.

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Resolution of HLA-B44:02:01G, -DRB114:01:01G and -DQB1*03:01:01G reveals a high allelic variability among 12 European populations.