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通过对灵长类动物坏死性肌炎的多维分析鉴定出新的发病机制和转化治疗靶点。

New Pathogenesis Mechanisms and Translational Leads Identified by Multidimensional Analysis of Necrotizing Myositis in Primates.

机构信息

Center for Molecular and Translational Human Infectious Diseases Research, Department of Pathology and Genomic Medicine, Houston Methodist Research Institute and Houston Methodist Hospital, Houston, Texas, USA.

Department of Pathology and Laboratory Medicine, Weill Cornell Medical College, New York, New York, USA.

出版信息

mBio. 2020 Feb 18;11(1):e03363-19. doi: 10.1128/mBio.03363-19.

Abstract

A fundamental goal of contemporary biomedical research is to understand the molecular basis of disease pathogenesis and exploit this information to develop targeted and more-effective therapies. Necrotizing myositis caused by the bacterial pathogen is a devastating human infection with a high mortality rate and few successful therapeutic options. We used dual transcriptome sequencing (RNA-seq) to analyze the transcriptomes of and host skeletal muscle recovered contemporaneously from infected nonhuman primates. The bacterial transcriptome was strikingly remodeled compared to organisms grown , with significant upregulation of genes contributing to virulence and altered regulation of metabolic genes. The transcriptome of muscle tissue from infected nonhuman primates (NHPs) differed significantly from that of mock-infected animals, due in part to substantial changes in genes contributing to inflammation and host defense processes. We discovered significant positive correlations between group A streptococcus (GAS) virulence factor transcripts and genes involved in the host immune response and inflammation. We also discovered significant correlations between the magnitude of bacterial virulence gene expression and pathogen fitness, as assessed by previously conducted genome-wide transposon-directed insertion site sequencing (TraDIS). By integrating the bacterial RNA-seq data with the fitness data generated by TraDIS, we discovered five new pathogen genes, namely, 0281 ( []), , , , and , that contribute to necrotizing myositis and confirmed these findings using isogenic deletion-mutant strains. Taken together, our study results provide rich new information about the molecular events occurring in severe invasive infection of primate skeletal muscle that has extensive translational research implications. Necrotizing myositis caused by has high morbidity and mortality rates and relatively few successful therapeutic options. In addition, there is no licensed human vaccine. To gain enhanced understanding of the molecular basis of this infection, we employed a multidimensional analysis strategy that included dual RNA-seq and other data derived from experimental infection of nonhuman primates. The data were used to target five streptococcal genes for pathogenesis research, resulting in the unambiguous demonstration that these genes contribute to pathogen-host molecular interactions in necrotizing infections. We exploited fitness data derived from a recently conducted genome-wide transposon mutagenesis study to discover significant correlation between the magnitude of bacterial virulence gene expression and pathogen fitness. Collectively, our findings have significant implications for translational research, potentially including vaccine efforts.

摘要

当代生物医学研究的一个基本目标是了解疾病发病机制的分子基础,并利用这些信息开发针对疾病的、更有效的治疗方法。由细菌病原体 引起的坏死性肌炎是一种具有高死亡率和治疗方法选择有限的毁灭性人类感染。我们使用双转录组测序(RNA-seq)分析了同时从感染的非人灵长类动物中回收的 和宿主骨骼肌的转录组。与在 中生长的生物体相比, 细菌转录组发生了惊人的重塑,毒力相关基因显著上调,代谢基因的调控发生改变。感染的非人灵长类动物(NHP)肌肉组织的转录组与模拟感染动物的转录组有显著差异,部分原因是参与炎症和宿主防御过程的基因发生了实质性变化。我们发现链球菌 A(GAS)毒力因子转录物与参与宿主免疫反应和炎症的基因之间存在显著的正相关。我们还发现细菌毒力基因表达的幅度与病原体适应性之间存在显著相关性,这是通过之前进行的全基因组转座子定向插入位点测序(TraDIS)评估的。通过将细菌 RNA-seq 数据与 TraDIS 生成的适应性数据进行整合,我们发现了五个新的病原体基因,即 0281([])、、、、和 ,它们有助于坏死性肌炎,并使用同源缺失突变株验证了这些发现。总之,我们的研究结果为严重侵袭性感染灵长类骨骼肌中发生的分子事件提供了丰富的新信息,具有广泛的转化研究意义。 引起的坏死性肌炎发病率和死亡率高,治疗方法相对较少。此外,还没有许可的人类 疫苗。为了更深入地了解这种感染的分子基础,我们采用了多维分析策略,包括双 RNA-seq 和其他源自非人类灵长类动物实验感染的数据。这些数据用于针对五个链球菌基因进行发病机制研究,明确证明这些基因在坏死性感染中有助于病原体-宿主分子相互作用。我们利用最近进行的全基因组转座子诱变研究获得的适应性数据,发现细菌毒力基因表达幅度与病原体适应性之间存在显著相关性。总的来说,我们的研究结果对转化研究具有重要意义,可能包括疫苗研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ff8c/7029145/91d8361b503f/mBio.03363-19-f0001.jpg

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