Close Related Drug-Resistance Beijing Isolates of Mycobacterium tuberculosis Reveal a Different Transcriptomic Signature in a Murine Disease Progression Model

在小鼠疾病进展模型中,密切相关的耐药性北京分离株结核分枝杆菌表现出不同的转录组特征。

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作者:María Irene Cerezo-Cortés ,Juan Germán Rodríguez-Castillo ,Dulce Adriana Mata-Espinosa ,Estela Isabel Bini ,Jorge Barrios-Payan ,Zyanya Lucia Zatarain-Barrón ,Juan Manuel Anzola ,Fernanda Cornejo-Granados ,Adrian Ochoa-Leyva ,Patricia Del Portillo ,Martha Isabel Murcia ,Rogelio Hernández-Pando

Abstract

Mycobacterium tuberculosis (MTB) lineage 2/Beijing is associated with high virulence and drug resistance worldwide. In Colombia, the Beijing genotype has circulated since 1997, predominantly on the pacific coast, with the Beijing-Like SIT-190 being more prevalent. This genotype conforms to a drug-resistant cluster and shows a fatal outcome in patients. To better understand virulence determinants, we performed a transcriptomic analysis with a Beijing-Like SIT-190 isolate (BL-323), and Beijing-Classic SIT-1 isolate (BC-391) in progressive tuberculosis (TB) murine model. Bacterial RNA was extracted from mice lungs on days 3, 14, 28, and 60. On average, 0.6% of the total reads mapped against MTB genomes and of those, 90% against coding genes. The strains were independently associated as determined by hierarchical cluster and multidimensional scaling analysis. Gene ontology showed that in strain BL-323 enriched functions were related to host immune response and hypoxia, while proteolysis and protein folding were enriched in the BC-391 strain. Altogether, our results suggested a differential bacterial transcriptional program when evaluating these two closely related strains. The data presented here could potentially impact the control of this emerging, highly virulent, and drug-resistant genotype. Keywords: Mycobacterium tuberculosis; RNAseq; in vivo transcriptomics; lineage 2/Beijing; murine model; virulence.

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