感染人类免疫缺陷病毒和未感染人类免疫缺陷病毒的乌干达人的新型隐球菌反应和总免疫球蛋白概况。

Krishanthi Subramaniam, Neil French, Liise-Anne Pirofski
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引用次数: 0

摘要

我们对参加肺炎球菌疫苗接种随机对照试验的乌干达人进行了一项回顾性病例对照研究,测定了感染人类免疫缺陷病毒 (HIV) 和未感染 HIV 的乌干达人的总抗体和新型隐球菌葡萄糖醛酸甘露聚糖 (GXM) 反应性抗体复合物。这项研究包括 192 名成年人:其中 48 人后来患上了隐球菌脑膜炎 (CM);(HIV+ CM+);2 人在 CD4+ T 细胞水平、HIV 疾病阶段和年龄方面与他们相符,但没有患上 CM(HIV+ CM-);以及 48 名未受 HIV 感染的人。使用隐球菌病发生前获得的HIV+ CM+受试者血清库中的血清,测定血清总免疫球蛋白浓度以及免疫球蛋白M (IgM)、IgG和IgA对GXM、肺炎球菌多糖和表达某些V(H)3特异型抗体的滴度。结果显示,与未感染艾滋病毒的受试者相比,感染艾滋病毒的受试者体内的 GXM IgM 水平明显较低,但总免疫球蛋白、GXM IgG 和 IgA 水平较高。有肺炎病史的艾滋病病毒感染者体内的 GXM 结合抗体水平较高,而有带状疱疹病史的艾滋病病毒感染者体内的 GXM 结合抗体水平较低。GXM抗体与肺炎球菌疫苗中的多糖之间几乎没有交叉反应。在 HIV+ CM+ 和 HIV+ CM- 受试者的抗体库中未发现明显差异,但在无肺炎病史的受试者中,HIV+ CM+ 受试者的 V(H)3 阳性抗体水平有低于 HIV+ CM- 受试者的趋势。我们的研究结果表明,既往传染病与艾滋病毒感染者总抗体和 GXM 反应性抗体库的差异之间存在关联,并表明某些微生物是否会调节随后对 GXM 的抗体反应这一问题值得进一步研究。
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Cryptococcus neoformans-reactive and total immunoglobulin profiles of human immunodeficiency virus-infected and uninfected Ugandans.

We determined total and Cryptococcus neoformans glucuronoxylomannan (GXM)-reactive antibody repertoires of human immunodeficiency virus (HIV)-infected and HIV-uninfected Ugandans in a retrospective, case-control study of participants in a randomized controlled trial of pneumococcal vaccination. The study included 192 adults: 48 who subsequently developed cryptococcal meningitis (CM); (HIV+ CM+); 2 individuals who matched them in CD4+ T-cell level, stage of HIV disease, and age but did not develop CM (HIV+ CM-); and 48 HIV-uninfected individuals. Total serum immunoglobulin concentrations and titers of immunoglobulin M (IgM), IgG, and IgA to GXM, pneumococcal polysaccharides, and antibodies expressing certain V(H)3 idiotypes were determined with banked sera obtained before the development of cryptococcosis for HIV+ CM+ subjects. The results showed that HIV-infected subjects had significantly lower levels of IgM to GXM but higher levels of total immunoglobulin and IgG and IgA to GXM than those of HIV-uninfected subjects. HIV-infected subjects with a history of pneumonia had higher levels, and those with a history of herpes zoster had lower levels of GXM-binding antibodies than subjects with no history of either disease. Minimal to no cross-reactivity was demonstrated between antibodies to GXM and polysaccharides in a pneumococcal vaccine. No significant differences between the antibody repertoires of HIV+ CM+ and HIV+ CM- subjects were identified, but among subjects without a history of pneumonia, there was a trend towards lower V(H)3-positive antibody levels among HIV+ CM+ than among HIV+ CM- subjects. Our findings demonstrate an association between previous infectious diseases and differences in the total and GXM-reactive antibody repertoires of HIV-infected subjects and suggest the question of whether certain microbes modulate subsequent antibody responses to GXM deserves further study.

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