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成骨细胞感染 后转录组结构揭示强烈的炎症反应以及代谢和表观遗传失调的特征。

Transcriptome Architecture of Osteoblastic Cells Infected With Reveals Strong Inflammatory Responses and Signatures of Metabolic and Epigenetic Dysregulation.

机构信息

Institut National de Recherche pour l'agriculture, l'alimentation et l'environnement (INRAE), Institut Agro, Science et Technologie du Lait et de l'OEuf (STLO), Rennes, France.

Cytometry and Biomarkers Centre de Ressources et Recherches Technologiques (C2RT), Institut Pasteur, Paris, France.

出版信息

Front Cell Infect Microbiol. 2022 Apr 7;12:854242. doi: 10.3389/fcimb.2022.854242. eCollection 2022.

Abstract

is an opportunistic pathogen that causes a range of devastating diseases including chronic osteomyelitis, which partially relies on the internalization and persistence of  in osteoblasts. The identification of the mechanisms of the osteoblast response to intracellular  is thus crucial to improve the knowledge of this infectious pathology. Since the signal from specifically infected bacteria-bearing cells is diluted and the results are confounded by bystander effects of uninfected cells, we developed a novel model of long-term infection. Using a flow cytometric approach we isolated only -bearing cells from mixed populations that allows to identify signals specific to intracellular infection. Here we present an in-depth analysis of the effect of long-term  infection on the transcriptional program of human osteoblast-like cells. After RNA-seq and KEGG and Reactome pathway enrichment analysis, the remodeled transcriptomic profile of infected cells revealed exacerbated immune and inflammatory responses, as well as metabolic dysregulations that likely influence the intracellular life of bacteria. Numerous genes encoding epigenetic regulators were downregulated. The later included genes coding for components of chromatin-repressive complexes (, NuRD, BAHD1 and PRC1) and epifactors involved in DNA methylation. Sets of genes encoding proteins of cell adhesion or neurotransmission were also deregulated. Our results suggest that intracellular infection has a long-term impact on the genome and epigenome of host cells, which may exert patho-physiological dysfunctions additionally to the defense response during the infection process. Overall, these results not only improve our conceptual understanding of biological processes involved in the long-term infections of osteoblast-like cells, but also provide an atlas of deregulated host genes and biological pathways and identify novel markers and potential candidates for prophylactic and therapeutic approaches.

摘要

是一种机会性病原体,可引起多种破坏性疾病,包括慢性骨髓炎,这部分依赖于 在成骨细胞中的内化和持续存在。因此,确定成骨细胞对细胞内 的反应机制对于提高对这种感染性病理的认识至关重要。由于来自特定感染细菌的带菌细胞的信号被稀释,并且未感染细胞的旁观者效应使结果复杂化,因此我们开发了一种新的长期感染模型。我们使用流式细胞术从混合群体中仅分离出带有 的细胞,这使得可以识别特定于细胞内感染的信号。在这里,我们对长期 感染对人成骨样细胞转录程序的影响进行了深入分析。在 RNA-seq 和 KEGG 和 Reactome 途径富集分析后,受感染细胞的重构转录组谱揭示了加剧的免疫和炎症反应,以及代谢失调,这可能影响细菌的细胞内生活。许多编码表观遗传调节剂的基因下调。后者包括编码染色质抑制复合物(,, NuRD, BAHD1 和 PRC1)和涉及 DNA 甲基化的外因子的基因。编码细胞粘附或神经递质的蛋白质的基因集也被下调。我们的结果表明,细胞内 感染对宿主细胞的基因组和表观基因组具有长期影响,这可能在感染过程中的防御反应之外对病理生理功能产生影响。总体而言,这些结果不仅提高了我们对涉及成骨样细胞中长期 感染的生物学过程的概念理解,而且还提供了宿主基因和生物学途径失调的图谱,并确定了新的标记物和潜在的预防和治疗方法的候选物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a348/9067450/3888286db656/fcimb-12-854242-g001.jpg

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