败血症
炎症
病理生理学
串扰
免疫学
肝损伤
转录组
生物
医学
药理学
内科学
基因
基因表达
生物化学
光学
物理
作者
Qian Zhang,Jing Liu,Jing Shen,Jinhuan Ou,Yin Kwan Wong,Lulin Xie,Jingnan Huang,Chun‐Ting Zhang,Chunjin Fu,Junhui Chen,Jiayun Chen,Xueling He,Fei Shi,Piao Luo,Ping Gong,Xueyan Liu,Jigang Wang
出处
期刊:MedComm
[Wiley]
日期:2023-10-01
卷期号:4 (5)
摘要
Sepsis is a difficult-to-treat systemic condition in which liver dysfunction acts as both regulator and target. However, the dynamic response of diverse intrahepatic cells to sepsis remains poorly characterized. Capsaicin (CAP), a multifunctional chemical derived from chilli peppers, has recently been shown to potentially possess anti-inflammatory effects, which is also one of the main approaches for drug discovery against sepsis. We performed single-cell RNA transcriptome sequencing on 86,830 intrahepatic cells isolated from normal mice, cecal ligation and puncture-induced sepsis model mice and CAP-treated mice. The transcriptional atlas of these cells revealed dynamic changes in hepatocytes, macrophages, neutrophils, and endothelial cells in response to sepsis. Among the extensive crosstalk across these major subtypes, KC_Cxcl10 shared strong potential interaction with other cells when responding to sepsis. CAP mitigated the severity of inflammation by partly reversing these pathophysiologic processes. Specific cell subpopulations in the liver act collectively to escalate inflammation, ultimately causing liver dysfunction. CAP displays its health-promoting function by ameliorating liver dysfunction induced by sepsis. Our study provides valuable insights into the pathophysiology of sepsis and suggestions for future therapeutic gain.
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