HETEROGENEOUS EXPANSION OF POLYMORPHONUCLEAR MYELOID-DERIVED SUPPRESSOR CELLS DISTINGUISHES HIGH-RISK SEPSIS IMMUNOPHENOTYPES IN UGANDA.

IF 2.7 3区医学 Q2 CRITICAL CARE MEDICINE

SHOCK Pub Date : 2024-09-01 Epub Date: 2024-05-30 DOI:10.1097/SHK.0000000000002403

Matthew J Cummings, Vincent Guichard, Nicholas Owor, Thomas Ochar, Moses Kiwubeyi, Rittah Nankwanga, Richard Kibisi, Charles Kassaja, Jesse E Ross, Thomas S Postler, John Kayiwa, Steven J Reynolds, Martina Cathy Nakibuuka, Joweria Nakaseegu, Julius J Lutwama, W Ian Lipkin, Sankar Ghosh, Barnabas Bakamutumaho, Max R O'Donnell

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引用次数: 0

Abstract

Abstract: Background: Understanding of immune cell phenotypes associated with inflammatory and immunosuppressive host responses in sepsis is imprecise, particularly in low- and middle-income countries, where the global sepsis burden is concentrated. In these settings, elucidation of clinically relevant immunophenotypes is necessary to determine the relevance of emerging therapeutics and refine mechanistic investigations of sepsis immunopathology. Methods: In a prospective cohort of adults hospitalized with suspected sepsis in Uganda (N = 43; median age 46 years [IQR 36-59], 24 [55.8%] living with HIV, 16 [37.2%] deceased at 60 days), we combined high-dimensional flow cytometry with unsupervised machine learning and manual gating to define peripheral immunophenotypes associated with increased risk of 60-day mortality. Results: Patients who died showed heterogeneous expansion of polymorphonuclear myeloid-derived suppressor cells, with increased and decreased abundance of CD16 - PD-L1 dim and CD16 bright PD-L1 bright subsets, respectively, significantly associated with mortality. While differences between CD16 - PD-L1 dim cell abundance and mortality risk appeared consistent throughout the course of illness, those for the CD16 bright PD-L1 bright subset were more pronounced early after illness onset. Independent of HIV co-infection, depletion of CD4 + T cells, dendritic cells, and CD56 - CD16 bright NK cells were significantly associated with mortality risk, as was expansion of immature, CD56 + CD16 - CD11c + NK cells. Abundance of T cells expressing inhibitory checkpoint proteins (PD-1, CTLA-4, LAG-3) was similar between patients who died versus those who survived. Conclusions: This is the first study to define high-risk immunophenotypes among adults with sepsis in sub-Saharan Africa, an immunologically distinct region where biologically informed treatment strategies are needed. More broadly, our findings highlight the clinical importance and complexity of myeloid derived suppressor cell expansion during sepsis and support emerging data that suggest a host-protective role for PD-L1 myeloid checkpoints in acute critical illness.

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乌干达多形核骨髓源性抑制细胞的异质性扩增可区分高风险败血症免疫分型。

背景：对脓毒症中与炎症和免疫抑制宿主反应相关的免疫细胞表型的了解并不精确，尤其是在中低收入国家，因为全球脓毒症负担主要集中在这些国家。在这些地区，有必要阐明对预后具有重要意义的免疫表型，以确定新兴疗法的相关性，并完善脓毒症免疫病理学的机理研究：方法：我们在乌干达对疑似败血症住院成人（N = 43；中位年龄 46 岁 [IQR 36-59]，24 [55.8%] 感染 HIV，16 [37.2%] 在 60 天内死亡）进行了前瞻性队列研究，将高维流式细胞术与无监督机器学习和手动选通相结合，确定了与 60 天内死亡风险增加相关的外周免疫表型：结果：死亡患者的多形核髓源性抑制细胞（PMN-MDSCs）呈现异质性扩张，CD16negPD-L1dim亚群和CD16brightPD-L1bright亚群的丰度增加和减少分别与死亡率显著相关。在整个病程中，CD16negPD-L1dim细胞丰度与死亡风险之间的差异似乎是一致的，而CD16brightPD-L1bright亚群的差异在发病初期更为明显。与艾滋病毒合并感染无关，CD4+ T细胞、树突状细胞和CD56-CD16bright NK细胞的耗竭与死亡风险显著相关，未成熟的CD56+CD16-CD11c+ NK细胞的扩增也与死亡风险显著相关。死亡患者与存活患者中表达抑制性检查点蛋白（PD-1、CTLA-4、LAG3）的T细胞数量相似：这是首次界定撒哈拉以南非洲成人败血症患者高风险免疫表型的研究。更广泛地说，我们的研究结果凸显了脓毒症期间MDSC扩增的临床重要性和复杂性，并支持了新出现的数据，这些数据表明PD-L1髓系检查点在急性危重症中具有宿主保护作用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

SHOCK 医学-外科

CiteScore

6.20

自引率

3.20%

发文量

199

审稿时长

1 months

期刊介绍： SHOCK®: Injury, Inflammation, and Sepsis: Laboratory and Clinical Approaches includes studies of novel therapeutic approaches, such as immunomodulation, gene therapy, nutrition, and others. The mission of the Journal is to foster and promote multidisciplinary studies, both experimental and clinical in nature, that critically examine the etiology, mechanisms and novel therapeutics of shock-related pathophysiological conditions. Its purpose is to excel as a vehicle for timely publication in the areas of basic and clinical studies of shock, trauma, sepsis, inflammation, ischemia, and related pathobiological states, with particular emphasis on the biologic mechanisms that determine the response to such injury. Making such information available will ultimately facilitate improved care of the traumatized or septic individual.