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小鼠中耐药性的转录适应性

Transcriptional adaptation of drug-tolerant in mice.

作者信息

Wynn Elizabeth A, Dide-Agossou Christian, Reichlen Matthew, Rossmassler Karen, Al Mubarak Reem, Reid Justin J, Tabor Samuel T, Born Sarah E M, Ransom Monica R, Davidson Rebecca M, Walton Kendra N, Benoit Jeanne B, Hoppers Amanda, Bauman Allison A, Massoudi Lisa M, Dolganov Gregory, Nahid Payam, Voskuil Martin I, Robertson Gregory T, Moore Camille M, Walter Nicholas D

机构信息

Rocky Mountain Regional VA Medical Center, Aurora, CO, USA.

Department of Biostatistics and Informatics, University of Colorado, Anschutz Medical Campus, Aurora, CO, USA.

出版信息

bioRxiv. 2023 Mar 8:2023.03.06.531356. doi: 10.1101/2023.03.06.531356.

Abstract

Transcriptome evaluation of in the lungs of laboratory animals during long-term treatment has been limited by extremely low abundance of bacterial mRNA relative to eukaryotic RNA. Here we report a targeted amplification RNA sequencing method called SEARCH-TB. After confirming that SEARCH-TB recapitulates conventional RNA-seq , we applied SEARCH-TB to -infected BALB/c mice treated for up to 28 days with the global standard isoniazid, rifampin, pyrazinamide, and ethambutol regimen. We compared results in mice with 8-day exposure to the same regimen . After treatment of mice for 28 days, SEARCH-TB suggested broad suppression of genes associated with bacterial growth, transcription, translation, synthesis of rRNA proteins and immunogenic secretory peptides. Adaptation of drug-stressed appeared to include a metabolic transition from ATP-maximizing respiration towards lower-efficiency pathways, modification and recycling of cell wall components, large-scale regulatory reprogramming, and reconfiguration of efflux pumps expression. Despite markedly different expression at pre-treatment baseline, murine and samples had broadly similar transcriptional change during treatment. The differences observed likely indicate the importance of immunity and pharmacokinetics in the mouse. By elucidating the long-term effect of tuberculosis treatment on bacterial cellular processes , SEARCH-TB represents a highly granular pharmacodynamic monitoring tool with potential to enhance evaluation of new regimens and thereby accelerate progress towards a new generation of more effective tuberculosis treatment.

摘要

长期治疗期间实验动物肺部细菌的转录组评估一直受到细菌mRNA相对于真核RNA极低丰度的限制。在此,我们报告一种名为SEARCH-TB的靶向扩增RNA测序方法。在确认SEARCH-TB能够重现传统RNA测序结果后,我们将SEARCH-TB应用于用全球标准的异烟肼、利福平、吡嗪酰胺和乙胺丁醇方案治疗长达28天的结核分枝杆菌感染的BALB/c小鼠。我们比较了暴露于相同方案8天的小鼠的结果。在对小鼠进行28天治疗后,SEARCH-TB表明与细菌生长、转录、翻译、rRNA蛋白合成和免疫原性分泌肽相关的基因受到广泛抑制。药物应激结核分枝杆菌的适应性似乎包括从最大化ATP呼吸向效率较低途径的代谢转变、细胞壁成分的修饰和再循环、大规模调节重编程以及外排泵表达的重新配置。尽管治疗前基线表达明显不同,但小鼠和结核分枝杆菌样本在治疗期间的转录变化大致相似。观察到的差异可能表明免疫和药代动力学在小鼠中的重要性。通过阐明结核病治疗对细菌细胞过程的长期影响,SEARCH-TB代表了一种高度精细的药效学监测工具,具有增强新方案评估的潜力,从而加速新一代更有效结核病治疗的进展。

相似文献

1
Transcriptional adaptation of drug-tolerant in mice.小鼠中耐药性的转录适应性
bioRxiv. 2023 Mar 8:2023.03.06.531356. doi: 10.1101/2023.03.06.531356.
2
Emergence of antibiotic-specific phenotypes during prolonged treatment of mice.小鼠长期治疗期间抗生素特异性表型的出现。
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