Joint modeling of monocyte HLA-DR expression trajectories predicts 28-day mortality in severe SARS-CoV-2 patients

IF 3.1 3区 医学 Q2 PHARMACOLOGY & PHARMACY CPT: Pharmacometrics & Systems Pharmacology Pub Date : 2024-06-05 DOI:10.1002/psp4.13145
Gaelle Baudemont, Coralie Tardivon, Guillaume Monneret, Martin Cour, Thomas Rimmelé, Lorna Garnier, Hodane Yonis, Jean-Christophe Richard, Remy Coudereau, Morgane Gossez, Florent Wallet, Marie-Charlotte Delignette, Frederic Dailler, Marielle Buisson, Anne-Claire Lukaszewicz, Laurent Argaud, Cédric Laouenan, Julie Bertrand, Fabienne Venet, for the RICO study group
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Abstract

The recent SarsCov2 pandemic has disrupted healthcare system notably impacting intensive care units (ICU). In severe cases, the immune system is dysregulated, associating signs of hyperinflammation and immunosuppression. In the present work, we investigated, using a joint modeling approach, whether the trajectories of cellular immunological parameters were associated with survival of COVID-19 ICU patients. This study is based on the REA-IMMUNO-COVID cohort including 538 COVID-19 patients admitted to ICU between March 2020 and May 2022. Measurements of monocyte HLA-DR expression (mHLA-DR), counts of neutrophils, of total lymphocytes, and of CD4+ and CD8+ subsets were performed five times during the first month after ICU admission. Univariate joint models combining survival at day 28 (D28), hospital discharge and longitudinal analysis of those biomarkers’ kinetics with mixed-effects models were performed prior to the building of a multivariate joint model. We showed that a higher mHLA-DR value was associated with a lower risk of death. Predicted mHLA-DR nadir cutoff value that maximized the Youden index was 5414 Ab/C and led to an AUC = 0.70 confidence interval (95%CI) = [0.65; 0.75] regarding association with D28 mortality while dynamic predictions using mHLA-DR kinetics until D7, D12 and D20 showed AUCs of 0.82 [0.77; 0.87], 0.81 [0.75; 0.87] and 0.84 [0.75; 0.93]. Therefore, the final joint model provided adequate discrimination performances at D28 after collection of biomarker samples until D7, which improved as more samples were collected. After severe COVID-19, decreased mHLA-DR expression is associated with a greater risk of death at D28 independently of usual clinical confounders.

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单核细胞 HLA-DR 表达轨迹联合建模可预测严重 SARS-CoV-2 患者 28 天的死亡率。
最近的 SarsCov2 大流行扰乱了医疗系统,特别是对重症监护病房(ICU)造成了影响。在严重病例中,免疫系统失调,伴有高炎症和免疫抑制症状。在本研究中,我们采用联合建模方法研究了细胞免疫学参数的变化轨迹是否与 COVID-19 ICU 患者的存活率相关。本研究基于 REA-IMMUNO-COVID 队列,包括 2020 年 3 月至 2022 年 5 月期间入住 ICU 的 538 名 COVID-19 患者。在入住重症监护室后的第一个月内,对单核细胞 HLA-DR 表达(mHLA-DR)、中性粒细胞计数、淋巴细胞总数以及 CD4+ 和 CD8+ 亚群进行了五次测量。在建立多变量联合模型之前,我们结合第28天(D28)的存活率、出院情况和这些生物标志物动力学的纵向分析,使用混合效应模型建立了单变量联合模型。结果表明,mHLA-DR值越高,死亡风险越低。最大化尤登指数的 mHLA-DR nadir 临界值预测值为 5414 Ab/C,与 D28 死亡率相关的 AUC = 0.70,置信区间 (95%CI) = [0.65; 0.75],而使用 mHLA-DR 动力学进行动态预测,直到 D7、D12 和 D20,AUC 分别为 0.82 [0.77; 0.87]、0.81 [0.75; 0.87] 和 0.84 [0.75; 0.93]。因此,最终的联合模型在收集生物标志物样本后的第 28 天至第 7 天提供了足够的分辨性能,随着收集样本的增多,分辨性能也有所提高。在严重的 COVID-19 后,mHLA-DR 表达的降低与 D28 时更大的死亡风险相关,而与通常的临床混杂因素无关。
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来源期刊
CiteScore
5.00
自引率
11.40%
发文量
146
审稿时长
8 weeks
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