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免疫病理学对吡嗪酰胺抗结核活性的影响。

Impact of immunopathology on the antituberculous activity of pyrazinamide.

机构信息

Public Health Research Institute, New Jersey Medical School, Rutgers, The State University of New Jersey, Newark, NJ.

Department of Biochemistry and Biophysics, Texas A&M University, College Station, TX.

出版信息

J Exp Med. 2018 Aug 6;215(8):1975-1986. doi: 10.1084/jem.20180518. Epub 2018 Jul 17.

Abstract

In the 1970s, inclusion of pyrazinamide (PZA) in the drug regimen of tuberculosis (TB) patients for the first 2 mo achieved a drastic reduction of therapy duration. Until now, however, the mechanisms underlying PZA's unique contribution to efficacy have remained controversial, and animal efficacy data vary across species. To understand how PZA kills bacterial populations present in critical lung lesion compartments, we first characterized a rabbit model of active TB, showing striking similarities in lesion types and fates to nonhuman primate models deemed the most appropriate surrogates of human TB. We next employed this model with lesion-centric molecular and bacteriology readouts to demonstrate that PZA exhibits potent activity against residing in difficult-to-sterilize necrotic lesions. Our data also indicate that PZA is slow acting, suggesting that PZA administration beyond the first 2 mo may accelerate the cure. In conclusion, we provide a pharmacodynamic explanation for PZA's treatment-shortening effect and deliver new tools to dissect the contribution of immune response versus drug at the lesion level.

摘要

在 20 世纪 70 年代,将吡嗪酰胺 (PZA) 纳入结核病 (TB) 患者的药物治疗方案前 2 个月,实现了治疗时间的大幅缩短。然而,到目前为止,PZA 对疗效的独特贡献的机制仍存在争议,并且动物疗效数据在不同物种之间存在差异。为了了解 PZA 如何杀死存在于关键肺部病变部位的细菌种群,我们首先对活跃性结核病的兔模型进行了特征描述,该模型在病变类型和非人类灵长类动物模型的命运方面表现出惊人的相似性,而非人类灵长类动物模型被认为是人类结核病的最佳替代模型。接下来,我们利用该模型进行了以病变为中心的分子和细菌学检测,证明 PZA 对位于难以消毒的坏死病变中的细菌具有强大的活性。我们的数据还表明 PZA 作用缓慢,这表明在最初的 2 个月后给予 PZA 可能会加速治愈。总之,我们为 PZA 的缩短治疗效果提供了药效学解释,并提供了新的工具来剖析免疫反应与药物在病变水平上的贡献。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c2da/6080910/5b237d06eeb2/JEM_20180518_Fig1.jpg

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