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Generation and application of DNA aptamers against HspX for accurate diagnosis of tuberculous meningitis

机译:DNA适体对Hspx进行高温诊断治疗结核性脑膜炎的生成和应用

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Tuberculous meningitis (TBM) is the most severe manifestation of tuberculosis and its diagnosis remains a challenge even today due to the lack of an adequate test. HspX antigen of Mycobacterium tuberculosis was previously established as a reliable diagnostic biomarker for TBM in an ELISA test format using anti-HspX polyclonal antibodies. Towards overcoming the limitations of batch-to-batch variation and challenges of scalability in antibody generation, we utilized Systematic Evolution of Ligands by EXponential enrichment (SELEX) to develop high affinity DNA aptamers against HspX as an alternative diagnostic reagent. Post-SELEX optimization of the best-performing aptamer candidate, H63, established its derivative H63 SL-2 M6 to be superior to its parent. Aptamer H63 SL-2 M6 displayed a specific and high affinity interaction with HspX (K-d similar to 9.0x10(-8) M). In an Aptamer Linked Immobilized Sorbent Assay (ALISA), H63 SL-2 M6 significantly differentiated between cerebrospinal fluid specimens from TBM and non-TBM subjects (n = 87, *** p 0.0001) with similar to 100% sensitivity and similar to 91% specificity. Notably, ALISA exhibited comparable performance with previously reported antibody-based ELISA and qPCR. Altogether, our findings establish the utility of HspX aptamer for the reliable diagnosis of TBM and pave the way for developing an aptamer-based point-of-care test for TBM.
机译:结核性脑膜炎(TBM)是结核病最严重的表现,由于缺乏足够的测试,即使今天也仍然是挑战。使用抗HSPX多克隆抗体,以先前建立了结核分枝杆菌的HSPX抗原作为ELISA测试形式的TBM可靠的诊断生物标志物。为了克服批量生产的批量变异和抗体性挑战的局部,我们利用指数富集(SELEX)来利用配体的系统演化,以将高亲和力DNA适体作为替代诊断试剂。 SELEX优化最佳性能的适体候选H63,建立了其衍生H63 SL-2 M6,以优于其父母。适体H63 SL-2 M6显示与Hspx的特定和高亲和力相互作用(K-D类似于9.0×10(-8)m)。在适体连接的固定的吸附剂测定(ALISA)中,H63 SL-2M6显着分化为来自TBM的脑脊液样本和非TBM受试者(n = 87,*** P <0.0001),其具有类似于100%的灵敏度和相似91%的特异性。值得注意的是,Alisa表现出与先前报道的基于抗体的ELISA和QPCR相当的性能。我们的研究结果完全建立了HSPX适体的效用,以获得TBM的可靠诊断,并为开发基于适体的TBM的护理点测试提供铺平道路。

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