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两兄弟患多发性骨髓瘤。一项免疫化学和免疫遗传学家族研究。

Multiple myeloma in two brothers. An immunochemical and immunogenetic familial study.

作者信息

Grosbois B, Gueguen M, Fauchet R, Lebouc H, Guenot A, Lancelin F, Lauvin R, Leblay R, Genetet B

出版信息

Cancer. 1986 Dec 1;58(11):2417-21. doi: 10.1002/1097-0142(19861201)58:11<2417::aid-cncr2820581111>3.0.co;2-s.

Abstract

When multiple myeloma was diagnosed within 6 months in two brothers a family study was carried out in 34 relatives to assess the genetic factors involved. The monoclonal immunoglobulin isotype identified was identical for the two brothers (IgG kappa) as well as their genotype (a = A2B12BfSDR4 GIo2/d:A9B27BfSDR2GIol). Blood protein electrophoresis and the major histocompatibility complex markers (HLA A, B, DR, Bf, glyoxalase phenotypes) were also determined in the other family members. The immunochemical study revealed no other case of monoclonal gammapathy, but 12 cases of low gamma-globulin and three cases of polyclonal hypergammapathy were found. The immunogenetic study showed that no other family member had the a/d genotype of the two brothers, whereas nine family members were semi-identical for haplotype a and five for haplotype d. It is unlikely that a double immunochemical and immunogenetic identity in two siblings with multiple myeloma would be due only to random encounter, rather this finding suggests that, besides environmental factors, genetic factors may be involved in the pathogenesis. Systematic immunochemical and immunogenetic studies in familial multiple myeloma are proposed as a method to further elucidate an eventual genetic background in multiple myeloma.

摘要

当两兄弟在6个月内均被诊断出患有多发性骨髓瘤时,对34名亲属进行了一项家族研究,以评估其中涉及的遗传因素。两兄弟所鉴定出的单克隆免疫球蛋白同种型相同(IgG κ),其基因型也相同(a = A2B12BfSDR4 GIo2/d:A9B27BfSDR2GIol)。还对其他家庭成员进行了血液蛋白电泳和主要组织相容性复合体标记物(HLA A、B、DR、Bf、乙二醛酶表型)检测。免疫化学研究未发现其他单克隆丙种球蛋白病病例,但发现12例低γ球蛋白血症和3例多克隆高γ球蛋白血症病例。免疫遗传学研究表明,没有其他家庭成员具有两兄弟的a/d基因型,而9名家庭成员的单倍型a半相同,5名家庭成员的单倍型d半相同。两名患有多发性骨髓瘤的兄弟姐妹在免疫化学和免疫遗传学上的双重相同不太可能仅由随机巧合导致,相反,这一发现表明,除环境因素外,遗传因素可能也参与了发病机制。建议对家族性多发性骨髓瘤进行系统的免疫化学和免疫遗传学研究,作为进一步阐明多发性骨髓瘤潜在遗传背景的一种方法。

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