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抗结核治疗期间的代谢变化 。 你提供的原文似乎不完整,“Metabolic Changes of ”后面缺少具体内容。

Metabolic Changes of during the Anti-Tuberculosis Therapy.

作者信息

Bespyatykh Julia, Shitikov Egor, Bespiatykh Dmitry, Guliaev Andrei, Klimina Ksenia, Veselovsky Vladimir, Arapidi Georgij, Dogonadze Marine, Zhuravlev Viacheslav, Ilina Elena, Govorun Vadim

机构信息

Federal Research and Clinical Centre of Physical-Chemical Medicine, 119435 Moscow, Russia.

Moscow Institute of Physics and Technology (State University), 141701 Dolgoprudny, Russia.

出版信息

Pathogens. 2020 Feb 18;9(2):131. doi: 10.3390/pathogens9020131.

Abstract

Tuberculosis, caused by complex bacteria, remains one of the most pressing health problems. Despite the general trend towards reduction of the disease incidence rate, the situation remains extremely tense due to the distribution of the resistant forms. Most often, these strains emerge through the intra-host microevolution of the pathogen during treatment failure. In the present study, the focus was on three serial clinical isolates of Beijing B0/W148 cluster from one patient with pulmonary tuberculosis, to evaluate their changes in metabolism during anti-tuberculosis therapy. Using whole genome sequencing (WGS), 9 polymorphisms were determined, which occurred in a stepwise or transient manner during treatment and were linked to the resistance (GyrA D94A; t-8a) or virulence. The effect of the t-8a mutation was confirmed on both proteomic and transcriptomic levels. Additionally, the amount of RpsL protein, which is a target of anti-tuberculosis drugs, was reduced. At the systemic level, profound changes in metabolism, linked to the evolution of the pathogen in the host and the effects of therapy, were documented. An overabundance of the FAS-II system proteins (HtdX, HtdY) and expression changes in the virulence factors have been observed at the RNA and protein levels.

摘要

由复合菌引起的结核病仍然是最紧迫的健康问题之一。尽管疾病发病率总体呈下降趋势,但由于耐药形式的传播,形势仍然极其严峻。这些菌株最常通过治疗失败期间病原体在宿主体内的微进化产生。在本研究中,重点关注来自一名肺结核患者的三株北京B0/W148簇的连续临床分离株,以评估它们在抗结核治疗期间的代谢变化。通过全基因组测序(WGS),确定了9个多态性,这些多态性在治疗期间以逐步或短暂的方式出现,并与耐药性(GyrA D94A;t-8a)或毒力相关。t-8a突变的影响在蛋白质组学和转录组学水平上均得到证实。此外,作为抗结核药物靶点的RpsL蛋白的量减少。在系统水平上,记录了与病原体在宿主体内的进化和治疗效果相关的代谢的深刻变化。在RNA和蛋白质水平上均观察到FAS-II系统蛋白(HtdX、HtdY)的过量表达以及毒力因子的表达变化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6bb8/7168336/341acfd3bf95/pathogens-09-00131-g001.jpg

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