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基于序列的HLA-A、-B和-Cw分型的重新分析:当今的序列特异性寡核苷酸分型在未来会有多大的歧义性。

Reanalysis of sequence-based HLA-A, -B and -Cw typings: how ambiguous is today's SBT typing tomorrow.

作者信息

Voorter C E M, Mulkers E, Liebelt P, Sleyster E, van den Berg-Loonen E M

机构信息

Tissue Typing Laboratory, University Hospital Maastricht, Maastricht, The Netherlands.

出版信息

Tissue Antigens. 2007 Nov;70(5):383-9. doi: 10.1111/j.1399-0039.2007.00921.x. Epub 2007 Sep 16.

DOI:10.1111/j.1399-0039.2007.00921.x
PMID:17868258
Abstract

The permanently increasing number of human leukocyte antigen (HLA)-alleles and the growing list of ambiguities require continuous updating of high-resolution HLA typing results. Two different kinds of ambiguities exist: the first, when two or more allele combinations have identical heterozygous sequences, and the second, when differences are located outside the analyzed region. The number of HLA-A, B and C alleles recognized in 1999 was almost tripled in 2006. Two hundred individuals, sequence-based typing (SBT) typed in the period from 1999 to 2002, were reanalyzed using the 2006 database. A final allele typing result of at least four digits was obtained for HLA-A, -B and -C by heterozygous sequencing of exons 2 and 3 and, if necessary, additional exons and/or allele-specific sequencing. Storage of the individual sequences in a specially developed database enabled reanalysis with all present and future HLA releases. In the 5-year period HLA-A, -B and -C typing results became ambiguous in 37%, 46% and 41% of the cases. Most were because of differences outside the analyzed region; ambiguities because of different allele combinations with identical heterozygous sequences were present in 7%, 8% and 13% of the HLA-A, -B and -C typings. These results indicate that within 5 years, approximately half of the HLA SBT typings become ambiguous.

摘要

人类白细胞抗原(HLA)等位基因数量持续增加,模糊性情况也越来越多,这就需要不断更新高分辨率HLA分型结果。存在两种不同类型的模糊性情况:第一种是两个或更多等位基因组合具有相同的杂合序列;第二种是差异位于分析区域之外。1999年识别出的HLA - A、B和C等位基因数量在2006年几乎增加了两倍。对1999年至2002年期间采用序列分型法(SBT)分型的200名个体,使用2006年的数据库重新进行分析。通过对第2和第3外显子进行杂合测序,并在必要时对其他外显子和/或等位基因特异性测序,获得了至少四位数字的HLA - A、- B和- C最终等位基因分型结果。将个体序列存储在专门开发的数据库中,能够利用所有当前和未来的HLA版本进行重新分析。在这5年期间,HLA - A、- B和- C分型结果在37%、46%和41%的病例中变得模糊不清。大多数情况是由于分析区域之外的差异;因具有相同杂合序列的不同等位基因组合导致的模糊性在HLA - A、- B和- C分型中分别占7%、8%和13%。这些结果表明,在5年内,大约一半的HLA SBT分型会变得模糊不清。

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