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HIV 患者中有无卡氏肺孢子菌肺炎的血清学对肺孢子菌蛋白的反应。

Serologic responses to pneumocystis proteins in HIV patients with and without Pneumocystis jirovecii pneumonia.

机构信息

Department of Medicine, University of Pittsburgh School of Medicine, Pittsburgh, PA, USA.

出版信息

J Acquir Immune Defic Syndr. 2011 Jul 1;57(3):190-6. doi: 10.1097/QAI.0b013e3182167516.

Abstract

BACKGROUND

Immune responses to Pneumocystis jirovecii are not well understood in HIV infection, but antibody responses to proteins may be useful as a marker of Pneumocystis risk or presence of Pneumocystis pneumonia (PcP).

DESIGN

Retrospective analysis of a prospective cohort.

METHODS

Enzyme-linked immunosorbent assays of antibodies to recombinant Pneumocystis proteins of major surface glycoprotein fragments (MsgC1, C3, C8, and C9) and of antibody titers to recombinant kexin protein (KEX1) were performed on 3 sequential serum samples up to 18 months before and 3 samples after first AIDS-defining illness from Multicenter AIDS Cohort Study participants and compared between those who had PcP or a non-PcP AIDS-defining illness.

RESULTS

Fifty-four participants had PcP and 47 had a non-PcP AIDS-defining illness. IgG levels to MsgC fragments were similar between groups before first AIDS-defining illness, but the PcP group had higher levels of IgG to MsgC9 (median units/mL 50.2 vs. 22.2, P = 0.047) post-illness. Participants with PcP were more likely to have an increase in MsgC3 [odds ratio (OR): 3.9, P = 0.02], MsgC8 (OR: 5.5, P = 0.001), and MsgC9 (OR: 4.0, P = 0.007). The PcP group was more likely to have low KEX1 IgG before development of PcP (OR: 3.6, P = 0.048) independent of CD4 cell count and to have an increase in high IgG titers to KEX1 after PcP.

CONCLUSIONS

HIV-infected individuals develop immune responses to both Msg and kexin proteins after PcP. Low KEX1 IgG titers may be a novel marker of future PcP risk before CD4 cell count has declined below 200 cells per microliter.

摘要

背景

在 HIV 感染中,人们对卡氏肺孢子虫的免疫反应了解甚少,但针对蛋白的抗体反应可能作为卡氏肺孢子虫风险或卡氏肺孢子虫肺炎(PcP)存在的标志物。

设计

前瞻性队列的回顾性分析。

方法

对多中心艾滋病队列研究参与者的 3 个连续血清样本进行酶联免疫吸附试验,检测针对主要表面糖蛋白片段(MsgC1、C3、C8 和 C9)的重组卡氏肺孢子虫蛋白的抗体和针对重组克赛因蛋白(KEX1)的抗体滴度,然后将这些抗体与那些患有 PcP 或非 PcP 艾滋病定义性疾病的患者进行比较。

结果

54 名参与者患有 PcP,47 名参与者患有非 PcP 艾滋病定义性疾病。在首次艾滋病定义性疾病之前,两组间 MsgC 片段的 IgG 水平相似,但 PcP 组在发病后 MsgC9 的 IgG 水平较高(中位数单位/ml 50.2 与 22.2,P = 0.047)。患有 PcP 的参与者更有可能增加 MsgC3 [比值比(OR):3.9,P = 0.02]、MsgC8(OR:5.5,P = 0.001)和 MsgC9(OR:4.0,P = 0.007)。在发生 PcP 之前,PcP 组更有可能出现低水平的 KEX1 IgG(OR:3.6,P = 0.048),独立于 CD4 细胞计数,在发生 PcP 后,高水平的 KEX1 IgG 会增加。

结论

HIV 感染者在发生 PcP 后会对 Msg 和 kexin 蛋白产生免疫反应。在 CD4 细胞计数降至每微升 200 个细胞以下之前,低水平的 KEX1 IgG 可能是未来发生 PcP 风险的新标志物。

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