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Low prevalence of selective IgA deficiency in infected children born to HIV-seropositive mothers: An in vivo model for speculation on selective IgA deficiency pathogenesis

机译:HIV阳性母亲所生的感染儿童中选择性IgA缺乏症的患病率低:推测选择性IgA缺乏症发病机理的体内模型

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Anecdotal reports of restored immunoglobulin production in individuals with common variable immunodeficiency after acquiring HIV infection suggest that perturbation of the immune system occurring during HIV infection may force some underlying functional defects. These findings raise intriguing questions about the pathogenesis of common variable immunodeficiency. No study has investigated the possible influence of HIV infection on the development of selective IgA deficiency, a primary immunologic defect genetically related to common variable immunodeficiency. IgA serum levels were evaluated in a large cohort of children born to HIV-infected mothers from 1985 to 2006. To avoid differences possibly due to different follow-up durations we considered only infected and non-infected children aged over 4 years at last-follow-up. The study included 1,157 non-infected children and 964 infected children, aged ≥ 4 years at last-follow-up and with availability of two or more serum IgA determinations over six months of age. No child displayed immunoglobulin values compatible with diagnosis of common variable immunodeficiency. However, 0/964 infected children vs. 5/1157 non-infected children had selective IgA deficiency (P=0.048). It may be speculated that several immunological alterations, occurring simultaneously in perinatal HIV infection, surpass the functional defect exhibited in some children with selective IgA deficiency. Our data may shed light on the pathogenesis of selective IgA deficiency.
机译:关于在感染HIV感染后具有常见可变免疫缺陷的个体中恢复的免疫球蛋白生产的轶事报道表明,在HIV感染期间发生的免疫系统紊乱可能导致某些潜在的功能缺陷。这些发现提出了有关常见可变免疫缺陷病发病机制的有趣问题。尚无研究调查HIV感染对选择性IgA缺乏症发展的可能影响,选择性IgA缺乏症是与常见可变免疫缺陷症遗传相关的主要免疫缺陷。从1985年至2006年,对一大批感染HIV的母亲所生孩子的IgA血清水平进行了评估。为避免可能由于随访时间长短而引起的差异,我们仅在最后随访时考虑了4岁以上的感染和未感染孩子-向上。该研究纳入了1157名未感染儿童和964名感染儿童,他们在上次随访时的年龄≥4岁,并且在六个月以上时可进行两次或更多次血清IgA测定。没有儿童显示出与常见可变免疫缺陷病诊断兼容的免疫球蛋白值。然而,0/964感染儿童与5/1157未感染儿童的儿童有选择性的IgA缺乏症(P = 0.048)。可以推测,围产期HIV感染中同时发生的几种免疫学改变超过了某些选择性IgA缺乏儿童表现出的功能缺陷。我们的数据可能会阐明选择性IgA缺乏症的发病机理。

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