一项基于转录组学的研究旨在探讨腹部手术后患者肺炎易感性的相关机制。
A Transcriptomic Approach to Understand Patient Susceptibility to Pneumonia After Abdominal Surgery.
机构信息
Division of Anaesthetics, Pain Medicine & Intensive Care Department of Surgery & Cancer, Faculty of Medicine, Imperial College London, London. UK.
Wellcome Centre for Human Genetics, University of Oxford, Oxford. UK.
出版信息
Ann Surg. 2024 Mar 1;279(3):510-520. doi: 10.1097/SLA.0000000000006050. Epub 2023 Jul 27.
OBJECTIVE
To describe immune pathways and gene networks altered following major abdominal surgery and to identify transcriptomic patterns associated with postoperative pneumonia.
BACKGROUND
Nosocomial infections are a major healthcare challenge, developing in over 20% of patients aged 45 or over undergoing major abdominal surgery, with postoperative pneumonia associated with an almost 5-fold increase in 30-day mortality.
METHODS
From a prospective consecutive cohort (n=150) undergoing major abdominal surgery, whole-blood RNA was collected preoperatively and at 3 time-points postoperatively (2-6, 24, and 48 h). Twelve patients diagnosed with postoperative pneumonia and 27 matched patients remaining infection-free were identified for analysis with RNA-sequencing.
RESULTS
Compared to preoperative sampling, 3639 genes were upregulated and 5043 downregulated at 2 to 6 hours. Pathway analysis demonstrated innate-immune activation with neutrophil degranulation and Toll-like-receptor signaling upregulation alongside adaptive-immune suppression. Cell-type deconvolution of preoperative RNA-sequencing revealed elevated S100A8/9-high neutrophils alongside reduced naïve CD4 T-cells in those later developing pneumonia. Preoperatively, a gene-signature characteristic of neutrophil degranulation was associated with postoperative pneumonia acquisition ( P =0.00092). A previously reported Sepsis Response Signature (SRSq) score, reflecting neutrophil dysfunction and a more dysregulated host response, at 48 hours postoperatively, differed between patients subsequently developing pneumonia and those remaining infection-free ( P =0.045). Analysis of the novel neutrophil gene-signature and SRSq scores in independent major abdominal surgery and polytrauma cohorts indicated good predictive performance in identifying patients suffering later infection.
CONCLUSIONS
Major abdominal surgery acutely upregulates innate-immune pathways while simultaneously suppressing adaptive-immune pathways. This is more prominent in patients developing postoperative pneumonia. Preoperative transcriptomic signatures characteristic of neutrophil degranulation and postoperative SRSq scores may be useful predictors of subsequent pneumonia risk.
目的
描述大腹部手术后改变的免疫途径和基因网络,并确定与术后肺炎相关的转录组模式。
背景
医院获得性感染是一个主要的医疗保健挑战,超过 45 岁接受大腹部手术的患者中有 20%以上会发生这种感染,而术后肺炎使 30 天死亡率增加近 5 倍。
方法
从一个前瞻性连续队列(n=150)中,在大腹部手术后采集术前和术后 3 个时间点(2-6、24 和 48 小时)的全血 RNA。确定了 12 例术后肺炎诊断患者和 27 例匹配的无感染患者进行 RNA 测序分析。
结果
与术前采样相比,2 至 6 小时时有 3639 个基因上调,5043 个基因下调。通路分析表明,中性粒细胞脱颗粒和 Toll 样受体信号上调的固有免疫激活,以及适应性免疫抑制。术前 RNA 测序的细胞类型去卷积显示,在以后发生肺炎的患者中,S100A8/9 高的中性粒细胞增加,而幼稚 CD4 T 细胞减少。术前,具有中性粒细胞脱颗粒特征的基因特征与术后肺炎的发生相关(P=0.00092)。在术后 48 小时,反映中性粒细胞功能障碍和更失调宿主反应的先前报道的败血症反应特征(SRSq)评分与肺炎患者和无感染患者不同(P=0.045)。在独立的大腹部手术和多发伤队列中对新型中性粒细胞基因特征和 SRSq 评分的分析表明,在识别以后感染的患者方面具有良好的预测性能。
结论
大腹部手术急性上调固有免疫途径,同时抑制适应性免疫途径。在发生术后肺炎的患者中更为明显。具有中性粒细胞脱颗粒特征的术前转录组特征和术后 SRSq 评分可能是预测后续肺炎风险的有用指标。
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