作为疾病候选生物标志物的沙眼衣原体表面蛋白血清抗体:巴尔的摩青少年/青年衣原体生殖管理(CHARM)队列的研究结果。

FEMS microbes Pub Date : 2022-02-28 eCollection Date: 2022-01-01 DOI:10.1093/femsmc/xtac004
Patricia X Marques, Handan Wand, Melissa Nandy, Chun Tan, Huizhong Shou, Mishka Terplan, Katrina Mark, Rebecca M Brotman, David P Wilson, Jacques Ravel, Ru-Ching Hsia, Patrik M Bavoil
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引用次数: 0

摘要

我们以前曾观察到,沙眼衣原体的九元自体转运多态膜蛋白(Pmps)家族在细胞培养中的表达各不相同。此外,沙眼衣原体感染患者血清中的 Pmp 特异性抗体谱也不尽相同,这间接表明独特 Pmp 谱的表达是感染期间对宿主特异性刺激的一种适应性反应。在此,我们提出,宿主对 Pmp 和其他外表面蛋白的反应可能与疾病的严重程度相关。本研究使用一种酶联免疫吸附试验(ELISA)对沙眼衣原体青少年/青年生殖管理(CHARM)队列中的 265 名参与者的血清 IgG 抗体进行了检测,该抗体可特异性检测九种沙眼衣原体 Pmp 亚型和四种免疫优势抗原(MOMP、OmcB、Hsp60、ClpP)。感染沙眼衣原体的女性比男性(35.9%-40.7% 的女性比 24.2%-30.0% 的男性)显示出更高的 Pmp 特异性抗体水平(临界指数),其中 PmpC、F 和 H 具有统计学意义(P < 0.05)。在临床诊断为盆腔炎(PID)的沙眼衣原体感染女性与未诊断为盆腔炎的女性之间,未观察到 Pmp 特异性抗体谱的差异。不过,高水平的 OmcB 特异性抗体与 PID 诊断之间存在统计学意义(P< 0.05)。利用抗体水平作为抗原表达的间接衡量标准,我们的研究结果表明,性别和/或特定部位(女性宫颈与男性尿道)的刺激可能会控制感染患者的 pmp 表达。这些结果还支持可能存在与疾病相关的衣原体感染免疫生物标志物,并强调了在人体血清中进行高分辨率筛查的必要性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Serum antibodies to surface proteins of Chlamydia trachomatis as candidate biomarkers of disease: results from the Baltimore Chlamydia Adolescent/Young Adult Reproductive Management (CHARM) cohort.

We previously observed that the nine-member family of autotransported polymorphic membrane proteins (Pmps) of Chlamydia trachomatis is variably expressed in cell culture. Additionally, C. trachomatis-infected patients display variable Pmp-specific serum antibody profiles indirectly suggesting expression of unique Pmp profiles is an adaptive response to host-specific stimuli during infection. Here, we propose that the host response to Pmps and other outer surface proteins may correlate with disease severity. This study tests this hypothesis using an ELISA that measures serum IgG antibodies specific for the nine C. trachomatis Pmp subtypes and four immunodominant antigens (MOMP, OmcB, Hsp60, ClpP) in 265 participants of the Chlamydia Adolescent/Young Adult Reproductive Management (CHARM) cohort. More C. trachomatis-infected females displayed high Pmp-specific antibody levels (cut-off Indexes) than males (35.9%-40.7% of females vs. 24.2%-30.0% of males), with statistical significance for PmpC, F and H (P < 0.05). Differences in Pmp-specific antibody profiles were not observed between C. trachomatis-infected females with a clinical diagnosis of pelvic inflammatory disease (PID) and those without. However, a statistically significant association between high levels of OmcB-specific antibody and a PID diagnosis (P< 0.05) was observed. Using antibody levels as an indirect measure of antigen expression, our results suggest that gender- and/or site-specific (cervix in females vs. urethra in males) stimuli may control pmp expression in infected patients. They also support the possible existence of immune biomarkers of chlamydial infection associated with disease and underline the need for high resolution screening in human serum.

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