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首页> 外文期刊>Chest: The Journal of Circulation, Respiration and Related Systems >Defining a Research Agenda to Address the Converging Epidemics of Tuberculosis and Diabetes Part 2: Underlying Biologic mechanisms
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Defining a Research Agenda to Address the Converging Epidemics of Tuberculosis and Diabetes Part 2: Underlying Biologic mechanisms

机译:定义研究议程,以解决结核病和糖尿病的聚合流行病第2部分:基础生物机制

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摘要

There is growing interest in the re-emerging interaction between type 2 diabetes (DM) and TB, but the underlying biologic mechanisms are poorly understood despite their possible implications in clinical management. Experts in epidemiologic, public health, basic science, and clinical studies recently convened and identified research priorities for elucidating the underlying mechanisms for the co-occurrence of TB and DM. We identified gaps in current knowledge of altered immunity in patients with DM during TB, where most studies suggest an underperforming innate immunity, but exaggerated adaptive immunity to Mycobacterium tuberculosis. Various molecular mechanisms and pathways may underlie these observations in the DM host. These include signaling induced by excess advanced glycation end products and their receptor, higher levels of reactive oxidative species and oxidative stress, epigenetic changes due to chronic hyperglycemia, altered nuclear receptors, and/or differences in cell metabolism (immunometabolism). Studies in humans at different stages of DM (no DM, pre DM, and DM) or TB (latent or active TB) should be complemented with findings in animal models, which provide the unique opportunity to study early events in the host-pathogen interaction. Such studies could also help identify biomarkers that will complement clinical studies in order to tailor the prevention of TB-DM, or to avoid the adverse TB treatment outcomes that are more likely in these patients. Such studies will also inform new approaches to host-directed therapies.
机译:尽管在临床管理中可能的影响,但在2型糖尿病(DM)和TB之间的重新出现相互作用越来越感兴趣,但潜在的生物机制很差。流行病学,公共卫生,基础科学和临床研究的专家最近召开并确定了阐明了阐明了TB和DM的潜在机制的研究优先事项。我们确定了TB中DM患者患者的改变的抗扰度知识的差距,大多数研究表明表现出不佳的先天免疫力,但夸大了结核分枝杆菌的适应性抗扰度。各种分子机制和途径可能在DM宿主中提高这些观察结果。这些包括通过过量的先进糖糖末端产物及其受体,具有较高水平的反应性氧化物质和氧化应激,表观遗传变化引起的信号传导,由于慢性高血糖,改变的核受体和/或细胞代谢的差异(免疫素描)。在DM的不同阶段(NO DM,PRE DM和DM)或TB(潜在或活性TB)的人类的研究应与动物模型中的结果进行补充,这提供了学习宿主互动中早期事件的独特机会。这些研究还可以帮助鉴定将补充临床研究的生物标志物,以定制预防TB-DM,或避免这些患者中更可能的不良结核病治疗结果。此类研究还将向举办托管疗法提供新方法。

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