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有证据表明,CD31、CD49b和CD62L是HLA相同的同胞骨髓移植中免疫显性的次要组织相容性抗原。

Evidence that CD31, CD49b, and CD62L are immunodominant minor histocompatibility antigens in HLA identical sibling bone marrow transplants.

作者信息

Maruya E, Saji H, Seki S, Fujii Y, Kato K, Kai S, Hiraoka A, Kawa K, Hoshi Y, Ito K, Yokoyama S, Juji T

机构信息

Department of Research, Kyoto Red Cross Blood Center, Kyoto, Japan; the Department of Internal Medicine, Saku Central Hospital, Nagano, the Department of Transfusion Medicine, Yamaguchi University Hospital, Japan.

出版信息

Blood. 1998 Sep 15;92(6):2169-76.

PMID:9731077
Abstract

Despite complete matching of siblings for the HLA loci, after bone marrow transplantation (BMT), approximately 20% develop graft-versus-host disease (GVHD). This is presumably due to incompatibility of minor histocompatibility antigens (mHa). We investigated the polymorphisms of 14 adhesion molecules (CD2, CD28, CD31, CD34, CD36, CD42, CD44, CD48, CD49b, CD54, CD62L, CD86, CD102, and CD106) in Japanese subjects and their association with the occurrence of GVHD after allogeneic HLA identical BMT. Six molecules (CD2, CD31, CD42, CD49b, CD54, and CD62L), which were found to be polymorphic, were then examined in 118 HLA identical sibling donors and recipients who had undergone BMT. Association of the incompatibility of the polymorphic molecules with the presence or absence of GVHD was examined. In these six, we observed a significant correlation between acute GVHD and the compatibility of CD31 (codons 563/670) (Pcorrected = .018), and CD31 (codons 563/670) + CD62L (Pcorrected = .018) in patients with the HLA-B44-like superfamily. In patients with the HLA-A3-like superfamily, the compatibility of CD62L (Pcorrected = .03) and CD62L + CD49b (P = . 004, Pcorrected = .078) was associated with acute GVHD. Therefore, CD31, CD49b, and CD62L might be candidates for immunodominant mHa.

摘要

尽管同胞之间的人类白细胞抗原(HLA)位点完全匹配,但在骨髓移植(BMT)后,仍有大约20%的患者会发生移植物抗宿主病(GVHD)。这可能是由于次要组织相容性抗原(mHa)不相容所致。我们研究了日本受试者中14种黏附分子(CD2、CD28、CD31、CD34、CD36、CD42、CD44、CD48、CD49b、CD54、CD62L、CD86、CD102和CD106)的多态性及其与异基因HLA相同的BMT后GVHD发生的相关性。然后,在118名接受BMT的HLA相同的同胞供体和受者中检测了6种具有多态性的分子(CD2、CD31、CD42、CD49b、CD54和CD62L)。研究了多态性分子的不相容性与GVHD存在与否之间的关联。在这6种分子中,我们观察到HLA - B44样超家族患者的急性GVHD与CD31(密码子563/670)的相容性(校正P值 = 0.018)以及CD31(密码子563/670) + CD62L(校正P值 = 0.018)之间存在显著相关性。在HLA - A3样超家族患者中,CD62L的相容性(校正P值 = 0.03)以及CD62L + CD49b(P = 0.004,校正P值 = 0.078)与急性GVHD相关。因此,CD31、CD49b和CD62L可能是免疫显性mHa的候选分子。

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