监测地塞米松治疗的重症 COVID-19 患者的单核细胞 HLA-DR 表达和 CD4 + T 淋巴细胞计数。

IF 5.7 1区 医学 Q1 CRITICAL CARE MEDICINE
Guillaume Monneret, Nicolas Voirin, Jean-Christophe Richard, Martin Cour, Thomas Rimmelé, Lorna Garnier, Hodane Yonis, Remy Coudereau, Morgane Gossez, Christophe Malcus, Florent Wallet, Marie-Charlotte Delignette, Frederic Dailler, Marielle Buisson, Laurent Argaud, Anne-Claire Lukaszewicz, Fabienne Venet
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引用次数: 0

摘要

背景:为期 10 天的地塞米松疗法已成为国际上采用的治疗严重 COVID-19 患者的标准疗法。然而,SARS-CoV-2 感染引发的免疫反应仍然是一个复杂和动态的现象,会导致不同的免疫特征和轨迹。重症 COVID-19 患者在接受完全地塞米松治疗后的免疫状况仍有待深入研究:为了分析COVID-19重症患者在地塞米松治疗后的单核细胞HLA-DR表达(mHLA-DR)和CD4 + T淋巴细胞计数(CD4),并评估它们与28天ICU死亡率的关系,研究人员纳入了ICU住院时间至少为10天且接受地塞米松治疗的COVID-19成年患者(n = 176)。评估了入住重症监护室后第 10 天测量的每个生物标志物值(或组合)与重症监护室 28 天死亡率之间的关系。在第 10 天,大多数患者的两个参数值都有所下降。低 mHLA-DR 与 28 天死亡率之间存在明显关联。在包括年龄、合并症或原有免疫抑制的多变量分析中,这种关联性仍很明显(调整后危险比 (aHR) = 2.86 [1.30-6.32], p = 0.009)。CD4 + T 细胞计数减少也有类似的结果(aHR = 2.10 [1.09-4.04],p = 0.027)。将这些生物标志物结合起来,mHLA-DR下降和CD4低下的患者28天死亡风险显著升高(即60%,aHR = 4.83 (1.72-13.57),p = 0.001):通过使用临床实践中可用的标准化免疫监测工具,有可能在为期 10 天的地塞米松治疗结束时识别出高风险死亡患者亚群。这强调了将免疫监测纳入重症监护患者监测的重要性,以便为进一步的免疫调节方法提供指导。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Monitoring monocyte HLA-DR expression and CD4 + T lymphocyte count in dexamethasone-treated severe COVID-19 patients.

Monitoring monocyte HLA-DR expression and CD4 + T lymphocyte count in dexamethasone-treated severe COVID-19 patients.

Background: A 10-day dexamethasone regimen has emerged as the internationally adopted standard-of-care for severe COVID-19 patients. However, the immune response triggered by SARS-CoV-2 infection remains a complex and dynamic phenomenon, leading to various immune profiles and trajectories. The immune status of severe COVID-19 patients following complete dexamethasone treatment has yet to be thoroughly documented.

Results: To analyze monocyte HLA-DR expression (mHLA-DR) and CD4 + T lymphocyte count (CD4) in critically ill COVID-19 patients after a dexamethasone course and evaluate their association with 28-day ICU mortality, adult COVID-19 patients (n = 176) with an ICU length of stay of at least 10 days and under dexamethasone treatment were included. Associations between each biomarker value (or in combination) measured at day 10 after ICU admission and 28-day mortality in ICU were evaluated. At day 10, the majority of patients presented decreased values of both parameters. A significant association between low mHLA-DR and 28-day mortality was observed. This association remained significant in a multivariate analysis including age, comorbidities or pre-existing immunosuppression (adjusted Hazard ratio (aHR) = 2.86 [1.30-6.32], p = 0.009). Similar results were obtained with decreased CD4 + T cell count (aHR = 2.10 [1.09-4.04], p = 0.027). When combining these biomarkers, patients with both decreased mHLA-DR and low CD4 presented with an independent and significant elevated risk of 28-day mortality (i.e., 60%, aHR = 4.83 (1.72-13.57), p = 0.001).

Conclusions: By using standardized immunomonitoring tools available in clinical practice, it is possible to identify a subgroup of patients at high risk of mortality at the end of a 10-day dexamethasone treatment. This emphasizes the significance of integrating immune monitoring into the surveillance of intensive care patients in order to guide further immumodulation approaches.

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来源期刊
Annals of Intensive Care
Annals of Intensive Care CRITICAL CARE MEDICINE-
CiteScore
14.20
自引率
3.70%
发文量
107
审稿时长
13 weeks
期刊介绍: Annals of Intensive Care is an online peer-reviewed journal that publishes high-quality review articles and original research papers in the field of intensive care medicine. It targets critical care providers including attending physicians, fellows, residents, nurses, and physiotherapists, who aim to enhance their knowledge and provide optimal care for their patients. The journal's articles are included in various prestigious databases such as CAS, Current contents, DOAJ, Embase, Journal Citation Reports/Science Edition, OCLC, PubMed, PubMed Central, Science Citation Index Expanded, SCOPUS, and Summon by Serial Solutions.
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