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酒精性肝炎中外周血和肝脏单核细胞的功能多样的炎症反应。

Functionally Diverse Inflammatory Responses in Peripheral and Liver Monocytes in Alcohol-Associated Hepatitis.

作者信息

Kim Adam, Bellar Annette, McMullen Megan R, Li Xiaoxia, Nagy Laura E

机构信息

Northern Ohio Alcohol Center Center for Liver Disease Research Department of Inflammation and Immunity Lerner Research Institute Cleveland Clinic Cleveland OH.

出版信息

Hepatol Commun. 2020 Aug 4;4(10):1459-1476. doi: 10.1002/hep4.1563. eCollection 2020 Oct.

Abstract

Alcohol-associated hepatitis (AH) is an acute inflammatory disease in which gut-microbial byproducts enter circulation and peripheral immune cells infiltrate the liver, leading to nonresolving inflammation and injury. Single-cell RNA sequencing of peripheral blood mononuclear cells isolated from patients with AH and healthy controls paired with lipopolysaccharide (LPS) challenge revealed how diverse monocyte responses are divided among individual cells and change in disease. After LPS challenge, one monocyte subtype expressed pro-inflammatory genes in both disease and healthy controls, while another monocyte subtype was anti-inflammatory in healthy controls but switched to pro-inflammatory in AH. Numerous immune genes are clustered within genomic cassettes, including chemokines and C-type lectin receptors (CTRs). CTRs sense byproducts of diverse microbial and host origin. Single-cell data revealed correlated expression of genes within cassettes, thus further diversifying different monocyte responses to individual cells. Monocyte up-regulation of CTRs in response to LPS caused hypersensitivity to diverse microbial and host-derived byproducts, indicating a secondary immune surveillance pathway up-regulated in a subset of cells by a closely associated genomic cassette. Finally, expression of CTR genes was higher in livers of patients with severe AH, but not other chronic liver diseases, implicating secondary immune surveillance in nonresolving inflammation in severe AH.

摘要

酒精性肝炎(AH)是一种急性炎症性疾病,肠道微生物副产物进入血液循环,外周免疫细胞浸润肝脏,导致炎症和损伤持续不愈。对从AH患者和健康对照中分离的外周血单核细胞进行单细胞RNA测序,并结合脂多糖(LPS)刺激,揭示了不同单核细胞反应如何在单个细胞之间划分以及在疾病中如何变化。LPS刺激后,一种单核细胞亚型在疾病组和健康对照组中均表达促炎基因,而另一种单核细胞亚型在健康对照组中具有抗炎作用,但在AH中转变为促炎作用。许多免疫基因聚集在基因组盒中,包括趋化因子和C型凝集素受体(CTR)。CTR可感知来自不同微生物和宿主来源的副产物。单细胞数据揭示了盒内基因的相关表达,从而进一步使不同单核细胞对单个细胞的反应多样化。单核细胞对LPS反应时CTR的上调导致对多种微生物和宿主来源副产物的超敏反应,表明在一部分细胞中由紧密相关的基因组盒上调了一种二级免疫监视途径。最后,CTR基因在重度AH患者肝脏中的表达较高,但在其他慢性肝病中则不然,这表明二级免疫监视与重度AH中炎症持续不愈有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/613f/7527760/52ed42abf081/HEP4-4-1459-g001.jpg

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