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首页> 外文期刊>Sociedade Brasileira de Medicina Tropical. Revista >Evaluation of the transcriptional immune biomarkers in peripheral blood from Warao indigenous associate with the infection by Mycobacterium tuberculosis
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Evaluation of the transcriptional immune biomarkers in peripheral blood from Warao indigenous associate with the infection by Mycobacterium tuberculosis

机译:从北非分枝杆菌的感染的原始土着助理的外周血转录免疫生物标志物评价

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INTRODUCTION: Biomarkers are critical tools for finding new approaches for controlling the spread of tuberculosis (TB), including for predicting the development of TB therapeutics, vaccines, and diagnostic tools. METHODS: Expression of immune biomarkers was analyzed in peripheral blood cells stimulated and non-stimulated with M. tuberculosis antigens ESAT-6, CFP10 and TB7.7. in Warao indigenous individuals. These biomarkers may be able to differentiate TB states, such as active tuberculosis (ATB) cases and latent tuberculosis infection (LTBI) from non-infected controls (NIC). A real-time reverse transcription polymerase chain reaction (RT-qPCR) assay was performed on 100 blood samples under non-stimulation or direct ex vivo conditions (NS=50) and stimulation conditions (S=50). RESULTS: The findings are shown as the median and interquartile range (IQR) of relative gene expression levels of IFN-γ, CD14, MMP9, CCR5, CCL11, CXCL9/MIG, and uPAR/PLAUR immune biomarkers. MMP9 levels were significantly higher in the LTBI-NS and LTBI-S groups compared with the NIC-NS and NIC-S groups. However, CCR5 levels were significantly lower in the LTBI-S group compared with both NIC-NS and NIC-S groups. CCL11 levels were significantly lower in the LTBI-S group compared with the NIC-NS group. CONCLUSIONS: Preliminary findings showed that MMP9 immune biomarkers separated LTBI indigenous individuals from NIC indigenous individuals, while CCR5, CCL11, CD14, and IFN-γ did not differentiate TB states from NIC. MMP9 may be useful as a potential biomarker for LTBI and new infected case detection among Warao indigenous individuals at high risk of developing the disease. It may also be used to halt the epidemic, which will require further validation in larger studies.
机译:介绍:生物标志物是寻找用于控制结核病(TB)扩散的新方法的关键工具,包括预测TB治疗,疫苗和诊断工具的发育。方法:在刺激和非刺激的外周血细胞中分析免疫生物标志物的表达,用M.结核抗原ESAT-6,CFP10和TB7.7刺激和非刺激。在北部土着个人。这些生物标志物可以能够将Tb状态分化,例如来自未感染的对照(NIC)的活性结核病(ATB)病例和潜在结核病感染(LTBI)。在非刺激或直接离体条件下(NS = 50)和刺激条件(S = 50),对100滴血样品进行实时逆转录聚合酶链反应(RT-QPCR)测定法。结果:该研究结果显示为IFN-γ,CD14,MMP9,CCR5,CCL11,CXCL9 / MIG和UPAR /贪污免疫生物标志物的相对基因表达水平的中值和侧链范围(IQR)。与NIC-NS和NIC-S组相比,LTBI-NS和LTBI-S群中MMP9水平显着较高。然而,与NIC-NS和NIC-S组相比,LTBI-S组中CCR5水平显着降低。与NIC-NS组相比,LTBI-S组中CCL11水平显着降低。结论:初步发现表明,MMP9免疫生物标志物从NIC土着个体分离LTBI土着个体,而CCR5,CCl11,CD14和IFN-γ没有区分NIC的态。 MMP9可用作LTBI的潜在生物标志物和在发育疾病的高风险中的北非土着人群中的新感染病例检测。它也可用于停止疫情,这将需要进一步验证较大的研究。

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