Longitudinal analysis of mucosa-associated invariant T cells in sepsis reveals their early numerical decline with prognostic implications and a progressive loss of antimicrobial functions

IF 3.2 4区 医学 Q3 CELL BIOLOGY Immunology & Cell Biology Pub Date : 2023-01-05 DOI:10.1111/imcb.12619
Joshua Choi, Crystal L Schmerk, Tina S Mele, Patrick T Rudak, Christine M Wardell, Gansen Deng, Farzan R Pavri, Kyoungok Kim, Gediminas Cepinskas, Wenqing He, SM Mansour Haeryfar
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引用次数: 4

Abstract

Sepsis-elicited immunosuppression elevates the risk of secondary infections. We used a clinically relevant mouse model and serial peripheral blood samples from patients to assess the antimicrobial activities of mucosa-associated invariant T (MAIT) cells in sepsis. Hepatic and splenic MAIT cells from B6-MAITCAST mice displayed increased CD69 expression and a robust interferon-γ (IFNγ) production capacity shortly after sublethal cecal ligation and puncture, but not at a late timepoint. Peripheral blood MAIT cell frequencies were reduced in septic patients at the time of intensive care unit (ICU) admission, and more dramatically so among nonsurvivors, suggesting the predictive usefulness of early MAIT cell enumeration. In addition, at ICU admission, MAIT cells from sepsis survivors launched stronger IFNγ responses to several bacterial species compared with those from patients who subsequently died of sepsis. Of note, while low human leukocyte antigen (HLA)-DR+ monocyte frequencies, widely regarded as a surrogate indicator of sepsis-induced immunosuppression, were gradually corrected, the numerical insufficiency of MAIT cells was not resolved over time, and their CD69 expression continued to decline. MAIT cell responses to bacterial pathogens, a major histocompatibility complex–related protein 1 (MR1) ligand, and interleukin (IL)-12 and IL-18 were also progressively lost during sepsis and did not recover by the time of ICU/hospital discharge. We propose that MAIT cell dysfunctions contribute to post-sepsis immunosuppression.

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脓毒症中粘膜相关不变T细胞的纵向分析揭示了其早期数量下降与预后的影响和抗菌功能的逐渐丧失
脓毒症引起的免疫抑制会增加继发感染的风险。我们使用临床相关的小鼠模型和患者的一系列外周血样本来评估脓毒症中粘膜相关不变性T (MAIT)细胞的抗菌活性。B6-MAITCAST小鼠的肝脏和脾脏MAIT细胞在亚致死性盲肠结扎和穿刺后不久显示出CD69表达增加和干扰素γ (IFNγ)产生能力增强,但在后期时间点则没有。脓毒症患者在重症监护病房(ICU)入院时,外周血MAIT细胞频率降低,非幸存者的情况更明显,提示早期MAIT细胞计数的预测作用。此外,在ICU入院时,与随后死于败血症的患者相比,来自败血症幸存者的MAIT细胞对几种细菌产生了更强的IFNγ反应。值得注意的是,虽然被广泛认为是脓毒症诱导免疫抑制的替代指标的人类白细胞抗原(HLA)-DR+单核细胞频率较低,但随着时间的推移,MAIT细胞的数量不足并没有得到解决,它们的CD69表达继续下降。脓毒症期间,MAIT细胞对细菌病原体、主要组织相容性复合物相关蛋白1 (MR1)配体以及白细胞介素(IL)-12和IL-18的反应也逐渐丧失,直到ICU/出院时也没有恢复。我们认为MAIT细胞功能障碍有助于脓毒症后的免疫抑制。
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来源期刊
Immunology & Cell Biology
Immunology & Cell Biology 医学-免疫学
CiteScore
7.50
自引率
2.50%
发文量
98
审稿时长
4-8 weeks
期刊介绍: The Australasian Society for Immunology Incorporated (ASI) was created by the amalgamation in 1991 of the Australian Society for Immunology, formed in 1970, and the New Zealand Society for Immunology, formed in 1975. The aim of the Society is to encourage and support the discipline of immunology in the Australasian region. It is a broadly based Society, embracing clinical and experimental, cellular and molecular immunology in humans and animals. The Society provides a network for the exchange of information and for collaboration within Australia, New Zealand and overseas. ASI members have been prominent in advancing biological and medical research worldwide. We seek to encourage the study of immunology in Australia and New Zealand and are active in introducing young scientists to the discipline.
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