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呼吸道感染后免疫记忆的揭示:通过用灭活肺炎球菌全细胞刺激小鼠脾细胞:转录组分析证据表明早期回忆反应。

Immune Memory After Respiratory Infection With Is Revealed by Stimulation of Murine Splenocytes With Inactivated Pneumococcal Whole Cells: Evidence of Early Recall Responses by Transcriptomic Analysis.

机构信息

Microbiotec srl, Siena, Italy.

Laboratory of Molecular Microbiology and Biotechnology (LAMMB), Department of Medical Biotechnologies, University of Siena, Siena, Italy.

出版信息

Front Cell Infect Microbiol. 2022 Jun 20;12:869763. doi: 10.3389/fcimb.2022.869763. eCollection 2022.

Abstract

The stimulation of immune system cells with live or killed bacteria is essential for understanding the host response to pathogens. In the present study, we propose a model combining transcriptomic and cytokine assays on murine splenocytes to describe the immune recall in the days following pneumococcal lung infection. Mice were sacrificed at days 1, 2, 4, and 7 after (TIGR4 serotype 4) intranasal infection and splenocytes were cultured in the presence or absence of the same inactivated bacterial strain to access the transcriptomic and cytokine profiles. The stimulation of splenocytes from infected mice led to a higher number of differentially expressed genes than the infection or stimulation alone, resulting in the enrichment of 40 unique blood transcription modules, including many pathways related to adaptive immunity and cytokines. Together with transcriptomic data, cytokines levels suggested the presence of a recall immune response promoting both innate and adaptive immunity, stronger from the fourth day after infection. Dimensionality reduction and feature selection identified key variables of this recall response and the genes associated with the increase in cytokine concentrations. This model could study the immune responses involved in pneumococcal infection and possibly monitor vaccine immune response and experimental therapies efficacy in future studies.

摘要

用活细菌或死细菌刺激免疫系统细胞对于理解宿主对病原体的反应至关重要。在本研究中,我们提出了一个结合了鼠脾细胞的转录组学和细胞因子分析的模型,以描述肺炎球菌肺部感染后几天的免疫回忆。在(TIGR4 血清型 4)鼻内感染后第 1、2、4 和 7 天处死小鼠,并在存在或不存在相同灭活细菌株的情况下培养脾细胞,以获取转录组和细胞因子图谱。感染小鼠的脾细胞刺激导致差异表达基因的数量高于感染或单独刺激,导致 40 个独特的血液转录模块富集,包括许多与适应性免疫和细胞因子相关的途径。结合转录组数据,细胞因子水平表明存在促进先天和适应性免疫的回忆免疫反应,从感染后第四天开始增强。降维和特征选择确定了这种回忆反应的关键变量以及与细胞因子浓度增加相关的基因。该模型可用于研究肺炎球菌感染涉及的免疫反应,并可能在未来的研究中监测疫苗免疫反应和实验治疗的疗效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/acf3/9251119/fc2fc50a8260/fcimb-12-869763-g001.jpg

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