CIITA启动子多态性损害脓毒症休克患者单核细胞HLA-DR表达。

CIITA promoter polymorphism impairs monocytes HLA-DR expression in patients with septic shock.

作者信息

Miatello Jordi, Lukaszewicz Anne-Claire, Carter Michael J, Faivre Valérie, Hua Stéphane, Martinet Kim Z, Bourgeois Christine, Quintana-Murci Lluis, Payen Didier, Boniotto Michele, Tissières Pierre

机构信息

Institute of Integrative Biology of the Cell, CNRS, CEA, Paris-Saclay University, Gif-sur-Yvette, France.

Paediatric Intensive Care and Neonatal Medicine, AP-HP, Paris-Saclay University, Bicêtre Hospital, Le Kremlin-Bicêtre, France.

出版信息

iScience. 2022 Oct 6;25(11):105291. doi: 10.1016/j.isci.2022.105291. eCollection 2022 Nov 18.

DOI:10.1016/j.isci.2022.105291

PMID:36304101

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9593818/

Abstract

Low monocyte (m)HLA-DR expression is associated with mortality in sepsis. G-286A∗rs3087456 polymorphism in promoter III of HLA class II transactivator (), the master regulator of HLA, has been associated with autoimmune diseases but its role in sepsis has never been demonstrated. In 203 patients in septic shock, GG genotype was associated with 28-day mortality and mHLA-DR remained low whereas it increased in patients with AA or AG genotype. In cells, mHLA-DR failed to augment in GG in comparison with AG or AA genotype on exposure to IFN-γ. Promoter III transcript levels were similar in control monocytes regardless of genotype and exposure to IFN-γ. Promoter III activity was decreased in GG genotype in monocyte cell line but restored after stimulation with IFN-γ. Hereby, we demonstrated that G-286A∗rs3087456 significantly impact mHLA-DR expression in patients with septic shock in part through promoter III activity, that can be rescued using IFN-γ.

摘要

单核细胞（m）HLA - DR低表达与脓毒症死亡率相关。HLA II类反式激活因子（HLA转录的主要调节因子）启动子III中的G - 286A∗rs3087456多态性与自身免疫性疾病相关，但其在脓毒症中的作用尚未得到证实。在203例感染性休克患者中，GG基因型与28天死亡率相关，mHLA - DR仍较低，而AA或AG基因型患者的mHLA - DR升高。在细胞中，与AG或AA基因型相比，暴露于IFN - γ时，GG基因型的mHLA - DR未能增加。无论基因型和是否暴露于IFN - γ，对照单核细胞中的启动子III转录水平相似。单核细胞系中GG基因型的启动子III活性降低，但经IFN - γ刺激后恢复。因此，我们证明G - 286A∗rs3087456部分通过启动子III活性显著影响感染性休克患者的mHLA - DR表达，而使用IFN - γ可使其恢复。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4cfd/9593818/e6be23fa6052/fx1.jpg

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CIITA启动子多态性损害脓毒症休克患者单核细胞HLA-DR表达。

CIITA promoter polymorphism impairs monocytes HLA-DR expression in patients with septic shock.

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