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研究结核分枝杆菌中吡嗪酰胺药物代谢动力学。

Studying the dynamics of the drug processing of pyrazinamide in Mycobacterium tuberculosis.

机构信息

Laboratory of Bioinformatics and Molecular Biology, Laboratorios de Investigación y Desarrollo, Facultad de Ciencias e Ingeniería, Universidad Peruana Cayetano Heredia, Lima, San Martín de Porres, Peru.

Bioinformatics Group in Multi-Omics and Immunology, New York, NY, United States of America.

出版信息

PLoS One. 2024 Aug 29;19(8):e0309352. doi: 10.1371/journal.pone.0309352. eCollection 2024.

Abstract

Pyrazinamide (PZA) is a key drug in the treatment of Mycobacterium tuberculosis. Although not completely understood yet, the bactericidal mechanism of PZA starts with its diffusion into the cell and subsequent conversion into pyrazinoic acid (POA) after the hydrolysis of ammonia group. This leads to the acidification cycle, which involves: (1) POA extrusion into the extracellular environment, (2) reentry of protonated POA, and (3) release of a proton into the cytoplasm, resulting in acidification of the cytoplasm and accumulation of intracellular POA. To better understand this process, we developed a system of coupled non-linear differential equations, which successfully recapitulates the kinetics of PZA/POA observed in M. tuberculosis. The parametric space was explored, assessing the impact of different PZA and pH concentrations and variations in the kinetic parameters, finding scenarios of PZA susceptibility and resistance. Furthermore, our predictions show that the acidification cycle alone is not enough to result in significant intracellular accumulation of POA in experimental time scales when compared to other neutral pH scenarios. Thus, revealing the need of novel hypotheses and experimental evidence to determine the missing mechanisms that may explain the pH-dependent intracellular accumulation of POA and their subsequent effects.

摘要

吡嗪酰胺(PZA)是治疗结核分枝杆菌的关键药物。尽管其杀菌机制尚未完全阐明,但 PZA 的杀菌机制始于其扩散到细胞内,随后在氨基团水解后转化为吡嗪酸(POA)。这导致酸化循环,涉及:(1)POA 被挤出细胞外环境,(2)质子化的 POA 重新进入,以及(3)质子被释放到细胞质中,导致细胞质酸化和细胞内 POA 的积累。为了更好地理解这一过程,我们开发了一个耦合非线性微分方程系统,成功地再现了结核分枝杆菌中观察到的 PZA/POA 的动力学。我们还探索了参数空间,评估了不同 PZA 和 pH 浓度以及动力学参数变化的影响,发现了 PZA 敏感性和耐药性的情况。此外,我们的预测表明,与其他中性 pH 情况相比,酸化循环本身在实验时间范围内不足以导致 POA 在细胞内的显著积累。因此,需要新的假说和实验证据来确定可能解释 pH 依赖性 POA 细胞内积累及其后续影响的缺失机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6561/11361689/6ae177dc3d70/pone.0309352.g001.jpg

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