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人类白细胞抗原(HLA)与免疫球蛋白G亚型(Gm)在自身免疫性慢性活动性肝炎中的相互作用

Interaction of HLA and Gm in autoimmune chronic active hepatitis.

作者信息

Whittingham S, Mathews J D, Schanfield M S, Tait B D, Mackay I R

出版信息

Clin Exp Immunol. 1981 Jan;43(1):80-6.

Abstract

An immunogenetic study of autoimmune chronic active hepatitis (CAH) showed the relative risk (RR) for this disease was 11.6 for patients who were HLA-B8, 11.7 for patients who were DR3 and 2.3 for patients who were Gma+x+. Moreover, the Gm haplotype Gma+x+ was present in 18 of 40 (45%) patients with HLA-B8, but in none of 10 patients negative for HLA-B8, whereas in 180 healthy controls Gma+x+ was evenly distributed among those positive (24%) and negative (18%) for HLA-B8. The RR was lowest in patients lacking HLA-B8 but positive for Gma+x+. Relative to this low-risk group, the risk was increased 39 times in subjects with both HLA-B8 and Gma+x+, 15 times in subjects with HLA-B8 who were not Gma+x+ and twice in subjects who were neither HLA-B8 nor Gma+x+. Statistical analysis indicated that the three-factor effect (disease risk affected by non-additive effects of HLA-B8 and Gma+x+) was significant (P less than 0.01), as were the main effects of HLA-B8 (P less than 0.001) and Gma+x+ (P less than 0.02). Thus in the presence of HLA-B8, genes linked to Gma+x+, an immunoglobulin CH allotype, may contribute to the development of autoimmune chronic active hepatitis; in the absence of HLA-B8 these same genes appear to be inactive. This may indicate interactions between MHC gene products and VH gene products in the presentation and recognition of autoantigen(s) in autoimmune hepatitis.

摘要

一项关于自身免疫性慢性活动性肝炎(CAH)的免疫遗传学研究表明,对于携带HLA - B8的患者,该疾病的相对风险(RR)为11.6;对于携带DR3的患者,RR为11.7;对于携带Gma+x+的患者,RR为2.3。此外,在40例(45%)携带HLA - B8的患者中有18例存在Gm单倍型Gma+x+,而在10例HLA - B8阴性的患者中均未出现。在180名健康对照者中,Gma+x+在HLA - B8阳性者(24%)和阴性者(18%)中分布均匀。RR在缺乏HLA - B8但Gma+x+阳性的患者中最低。相对于这个低风险组,同时携带HLA - B8和Gma+x+的受试者风险增加39倍,携带HLA - B8但不携带Gma+x+的受试者风险增加15倍,既不携带HLA - B8也不携带Gma+x+的受试者风险增加两倍。统计分析表明,三因素效应(疾病风险受HLA - B8和Gma+x+的非加性效应影响)显著(P小于0.01),HLA - B8的主效应(P小于0.001)和Gma+x+的主效应(P小于0.02)也显著。因此,在存在HLA - B8的情况下,与免疫球蛋白CH同种异型Gma+x+相关的基因可能有助于自身免疫性慢性活动性肝炎的发展;在缺乏HLA - B8时,这些相同的基因似乎不活跃。这可能表明在自身免疫性肝炎中,主要组织相容性复合体(MHC)基因产物与可变区(VH)基因产物在自身抗原的呈递和识别过程中存在相互作用。

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