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Comparison of antibody responses against Mycobacterium tuberculosis antigen Rv0679c in tuberculosis patients from the endemic and non-endemic regions of the Beijing genotype: a case control study

机译:北京基因型流行区和非流行区结核病患者抗结核分枝杆菌抗原Rv0679c抗体反应的比较:病例对照研究

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Background Strains of the Beijing genotype of Mycobacterium tuberculosis (MTB) are reportedly associated with the virulence of tuberculosis (TB) infection, unfavorable outcomes of anti-TB treatment, and the global TB pandemic. Rv0679c, a hypothetical membrane protein related to host cell invasion, has a Beijing genotype-specific mutation at residue 142 (Asn142Lys). Antigenicity differences between Rv0679c-Asn142 (N-type) and Rv0679c-Lys142 (K-type) have been previously observed in mice antigen-antibody responses. However, the immune response to Rv0679c in humans remains unknown. Therefore, we aimed to investigate the anti-Rv0679c immune response in TB patients from the endemic and non-endemic regions of the Beijing MTB genotype. Methods We analyzed the Rv0679c-specific antibody responses in 84 subjects from the endemic region of the Beijing genotype MTB in China, including 45 pulmonary TB patients (C-PTB) and 39 healthy controls (C-HC), and 81 subjects from the Philippines (the endemic region of the non-Beijing genotype), including 51 pulmonary TB patients (P-PTB) and 30 healthy controls (P-HC). Anti-tuberculous-glycolipid (TBGL) antigen was used as the control antibody. Results TBGL IgG titers were higher in both C-PTB and P-PTB than those in their corresponding HC (C-PTB median 4.2, P-PTB median 11.2; C-PTB vs. P-PTB, p >?0.05), suggesting immune response comparability in PTB from two different countries. C-PTB showed a higher response compared to C-HC for anti-K-type IgG (53.3%) than anti-N-type IgG (6.67%); this response was not observed in P-PTB (both N-type and K-type 9.80%). Conclusion Dimorphic antigen Rv0679c was found to be associated with distinct immune response patterns, indicating the role of Beijingon-Beijing genotype of MTB in stimulating specific responses in TB patients from the endemic region of Beijing MTB. Meanwhile, reactions to Rv0679c in patients and HC from non-endemic regions of the Beijing MTB may be caused by the response to the common epitope of Rv0679c N/K-type.
机译:背景技术北京结核分枝杆菌(MTB)基因型的菌株据报道与结核菌(TB)感染的毒力,抗结核治疗的不良结果以及全球结核病大流行有关。 Rv0679c是一种与宿主细胞入侵有关的假设性膜蛋白,在残基142(Asn142Lys)处具有北京基因型特异性突变。先前已在小鼠抗原抗体反应中观察到Rv0679c-Asn142(N型)和Rv0679c-Lys142(K型)之间的抗原性差异。但是,人类对Rv0679c的免疫反应仍然未知。因此,我们旨在研究北京MTB基因型流行区和非流行区的结核病患者的抗Rv0679c免疫反应。方法我们分析了中国北京基因型MTB流行地区的84名受试者的Rv0679c特异性抗体反应,包括45名肺结核患者(C-PTB)和39名健康对照者(C-HC),以及81名菲律宾患者(非北京基因型的流行地区),包括51例肺结核患者(P-PTB)和30例健康对照(P-HC)。抗结核糖脂(TBGL)抗原用作对照抗体。结果C-PTB和P-PTB的TBGL IgG滴度均高于相应的HC(C-PTB中位数4.2,P-PTB中位数11.2; C-PTB与P-PTB,p>?0.05),表明来自两个不同国家的PTB的免疫反应可比性。与C-HC相比,抗K型IgG(53.3%)比抗N型IgG(6.67%)的响应高。在P-PTB中未观察到这种反应(N型和K型均为9.80%)。结论发现双态抗原Rv0679c与不同的免疫反应模式有关,表明北京/非北京基因型的MTB在刺激北京MTB流行地区的结核病患者中特异性反应中的作用。同时,患者对Rv0679c的反应以及来自北京MTB非流行地区的HC可能是由对Rv0679c N / K型共同表位的反应引起的。

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