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外周血单核细胞的内源性血浆再悬浮可预防预处理相关应激,这种应激会改变富含多聚腺苷酸的RNA对后续急性应激源的反应。

Endogenous plasma resuspension of peripheral blood mononuclear cells prevents preparative-associated stress that modifies polyA-enriched RNA responses to subsequent acute stressors.

作者信息

Li Dongyang, Al-Dahleh Karina, Murphy Daniel A, Georgieva Sonya, Matthews Nik, Shovlin Claire L

机构信息

National Heart and Lung Institute, Imperial College London London, W12 ONN UK.

National Institute for Health Research (NIHR) Imperial Biomedical Research Centre London, W2 1NY UK.

出版信息

Cell Stress. 2024 Nov 28;11:112-124. doi: 10.15698/cst2024.11.301. eCollection 2024.

Abstract

Human peripheral blood mononuclear cells (PBMCs) are used to examine biological processes and disease, when basal variability in cellular activation and splicing is described and unexplained. Using isolation systems that maintained buffy coat cells (PBMCs, platelets) in their own plasma, poly-A enriched RNA-sequencing (RNASeq) detected 42,720 Ensembl gene IDs, including >95% of the top 100 Genotype Tissue Expression Project (GTEx)-expressed genes in lung, colon, heart, skeletal muscle and liver, and 10/17 clinically-actionable genes listed by the Pharmacogenomics Knowledgebase. Transcriptome changes were defined after 1h treatment with 32°C hypothermia (hsp70 family member change), 10 μmol/L ferric citrate that had no discernible effect, and 100 μg/mL cycloheximide leading to induction of primary response (immediate early) genes including IL1B and TNF. Same-donor PBMCs prepared conventionally using washes then resuspension in serum-supplemented media demonstrated basal upregulation of stress signalling pathway genes that masked and overlapped differential gene expression profiles after 100 µg/L cycloheximide. Plasma-resuspended PBMCs demonstrated minor transcriptome changes after 40 μmol/L ferric citrate, whereas consistent and greater magnitude changes were observed for washed/media-resuspended PBMCs. We conclude that endogenous plasma-maintained PBMCs provide a more robust platform to interrogate acute cellular perturbations triggering innate immunity, and that varying susceptibility of PBMCs to preparative stresses is an important component of experimental variability.

摘要

当细胞激活和剪接的基础变异性被描述但无法解释时,人类外周血单核细胞(PBMC)被用于研究生物学过程和疾病。使用能将血沉棕黄层细胞(PBMC、血小板)维持在自身血浆中的分离系统,聚腺苷酸富集RNA测序(RNASeq)检测到42,720个Ensembl基因ID,包括肺、结肠、心脏、骨骼肌和肝脏中前100个基因型组织表达项目(GTEx)表达基因的95%以上,以及药物基因组学知识库列出的17个临床可操作基因中的10个。在用32°C低温处理1小时后(hsp70家族成员变化)、10 μmol/L柠檬酸铁(无明显作用)和100 μg/mL环己酰亚胺处理后定义转录组变化,后者导致包括IL1B和TNF在内的初级反应(立即早期)基因的诱导。使用洗涤然后重悬于血清补充培养基中常规制备的同供体PBMC显示应激信号通路基因的基础上调,这掩盖并重叠了100 µg/L环己酰亚胺处理后的差异基因表达谱。血浆重悬的PBMC在40 μmol/L柠檬酸铁处理后显示出微小的转录组变化,而洗涤/培养基重悬的PBMC则观察到一致且更大程度的变化。我们得出结论,内源性血浆维持的PBMC为研究触发先天免疫的急性细胞扰动提供了一个更强大的平台,并且PBMC对制备应激的不同敏感性是实验变异性的一个重要组成部分。

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