Elevated Calprotectin and Abnormal Myeloid Cell Subsets Discriminate Severe from Mild COVID-19

Silvin, Aymeric; Chapuis, Nicolas; Dunsmore, Garett; Goubet, Anne-Gaëlle; Dubuisson, Agathe; Derosa, Lisa; Almire, Carole; Hénon, Clémence; Kosmider, Olivier; Droin, Nathalie; Rameau, Philippe; Catelain, Cyril; Alfaro, Alexia; Dussiau, Charles; Friedrich, Chloé; Sourdeau, Élise; Marin, Nathalie; Szwebel, Tali‐Anne; Cantin, D.; Mouthon, Luc; Borderie, Didier; Deloger, Marc; Bredel, Delphine; Mouraud, Séverine; Drubay, Damien; Andrieu, Muriel; L’Honneur, Anne-Sophie; Saada, Véronique; Stoclin, Annabelle; Willekens, Christophe; Pommeret, Fanny; Griscelli, Franck; Ng, Lai Guan; Zhang, Zheng; Bost, Pierre; Amit, Ido; Barlési, Fabrice; Marabelle, Aurélien; Pène, Frédéric; Gachot, Bertrand; André, Fabrice; Zitvogel, Laurence; Ginhoux, Florent; Fontenay, Michaëla; Solary, Éric

doi:10.1016/j.cell.2020.08.002

Cited by 753 publications

(1,172 citation statements)

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“…Interestingly, we also found an upregulation of cytoplasmic S100A9 in monocyte subsets specifically amplified in COVID-19 patients irrespectively of their ARDS status. These data suggest that, in the early stage of the disease, monocytes could contribute to the burst of circulating calprotectin (S100A8/S100A9), recently proposed to contribute to the secondary cytokine release syndrome described in severe COVID-19 and attributed to neutrophils (18).…”

Section: Discussionmentioning

confidence: 61%

“…The amplification of CD169 pos circulating monocytes has already been highlighted in the context of COVID-19 (11,18,36,37), and is reminiscent of other inflammatory conditions found in viral infections, such as with Human Immunodeficiency Virus or Epstein-Barr Virus, in which the CD169 sialoadhesin is induced in an IFN-dependent manner on the surface of circulating monocytes (38,39). Consistent with the inflammatory response, we showed that the accumulation of CD169 pos monocytes in COVID-19 pos patients is positively correlated with an increase of plasmablasts and mature plasma cells, Th1-like CD8 effector T cells, cytotoxic mature NK cells, and activated CD4 effector memory T cells displaying a CTLA4 high PD1 high phenotype.…”

Section: Discussionmentioning

confidence: 86%

“…Immune response to COVID-19 infection has been recently intensively studied at transcriptomic and proteomic levels. However, most studies focused on either the lymphoid (15,17,19) or the myeloid compartments (9,16,18), and only few performed a wide analysis of the circulating immune landscape (10,12,13,20,32), thus precluding the definition of complex patterns of immune parameter alterations associated with COVID-19 severity or physiopathology. Moreover, these works were designed to identify differences in immune cell subset frequencies between COVID-19 patients and healthy donors, and eventually correlated with the severity of the disease, but did not include severe non-COVID-19 patients as controls, although critically ill patients were largely demonstrated previously to display immune reprogramming (33).…”

Section: Discussionmentioning

confidence: 99%

“…Consistent with the inflammatory response, we showed that the accumulation of CD169 pos monocytes in COVID-19 pos patients is positively correlated with an increase of plasmablasts and mature plasma cells, Th1-like CD8 effector T cells, cytotoxic mature NK cells, and activated CD4 effector memory T cells displaying a CTLA4 high PD1 high phenotype. CD169 pos activated monocytes were detected in mild disease (18), and were proposed to rise rapidly and transiently in patients with COVID-19, in association with a high expression of IFNγ and CCL8 (11). This could be due to the transient nature of this monocytic population, either losing CD169, being short-lived, or being recruited into tissues as CD169 pos macrophages, as suggested by the high expression of CCR2 on Mo243 and Mo180, the two monocyte subsets identified here in COVID-19 patients, and the local inflammation and lung tissue destruction mediated by monocytederived macrophages in severe cases of SARS-CoV2 infections (40,41).…”

Section: Discussionmentioning

confidence: 99%

“…A number of high-resolution studies have recently concentrated on the determination of circulating markers that can distinguish severe from mild forms of COVID-19, providing a tremendous amount of data describing phenotypic and functional alterations in T cell, B cell, and myeloid cell subsets (9)(10)(11)(12)(13)(14)(15)(16)(17)(18)(19)(20). In particular, CD14 pos HLA-DR low , CD14 pos CD16 pos , CD14 low CD16 pos , and immature monocytes were demonstrated as increased among peripheral blood mononuclear cells (PBMCs) from critically ill COVID-19 patients (11,16,18,(21)(22)(23). Various alterations of lymphoid cells have also been described, including a T-cell lymphopenia, predictive of patient outcome, a broad T-cell activation including Th1, Th2, and Th17, an alteration of B-cell and T-cell repertoires, and a strong increase of plasmablasts, most prominent in ARDS COVID-19 patients (12,20,(24)(25)(26).…”

Section: Introductionmentioning

confidence: 99%

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Mass cytometry and artificial intelligence define CD169 as a specific marker of SARS-CoV2-induced acute respiratory distress syndrome

Roussel

Ferrant

Reizine

et al. 2020

Preprint

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Acute respiratory distress syndrome (ARDS) is the main complication of COVID-19, requiring admission to Intensive Care Unit (ICU). Despite recent immune profiling of COVID-19 patients, to what extent COVID-19-associated ARDS specifically differs from other causes of ARDS remains unknown, To address this question, we built 3 cohorts of patients categorized in COVID-19negARDSpos, COVID-19posARDSpos, and COVID-19posARDSneg, and compared their immune landscape analyzed by high-dimensional mass cytometry on peripheral blood followed by artificial intelligence analysis. A cell signature associating S100A9/calprotectin-producing CD169pos monocytes, plasmablasts, and Th1 cells was specifically found in COVID-19posARDSpos, unlike COVID-19negARDSpos patients. Moreover, this signature was shared by COVID-19posARDSneg patients, suggesting severe COVID-19 patients, whatever they experienced or not ARDS, displayed similar immune dysfunctions. We also showed an increase in CD14posHLA-DRlow and CD14lowCD16pos monocytes correlated to the occurrence of adverse events during ICU stay. Our study demonstrates that COVID-19-associated ARDS display a specific immune profile, and might benefit from personalized therapy in addition to standard ARDS management.

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Section: Discussionmentioning

confidence: 61%

Section: Discussionmentioning

confidence: 86%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Mass cytometry and artificial intelligence define CD169 as a specific marker of SARS-CoV2-induced acute respiratory distress syndrome

Roussel

Ferrant

Reizine

et al. 2020

Preprint

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Neurological pathophysiology of SARS‐CoV‐2 and pandemic potential RNA viruses: a comparative analysis

et al. 2021

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SARS‐CoV‐2 has infected hundreds of millions of people with over four million dead, resulting in one of the worst global pandemics in recent history. Neurological symptoms associated with COVID‐19 include anosmia, ageusia, headaches, confusion, delirium, and strokes. These may manifest due to viral entry into the central nervous system (CNS) through the blood–brain barrier (BBB) by means of ill‐defined mechanisms. Here, we summarize the abilities of SARS‐CoV‐2 and other neurotropic RNA viruses, including Zika virus and Nipah virus, to cross the BBB into the CNS, highlighting the role of magnetic resonance imaging (MRI) in assessing presence and severity of brain structural changes in COVID‐19 patients. We present new insight into key mutations in SARS‐CoV‐2 variants B.1.1.7 (P681H) and B.1.617.2 (P681R), which may impact on neuropilin 1 (NRP1) binding and CNS invasion. We postulate that SARS‐CoV‐2 may infect both peripheral cells capable of crossing the BBB and brain endothelial cells to traverse the BBB and spread into the brain. COVID‐19 patients can be followed up with MRI modalities to better understand the long‐term effects of COVID‐19 on the brain.

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Single Cell RNA Sequencing Identifies a Unique Inflammatory Macrophage Subset as a Druggable Target for Alleviating Acute Kidney Injury

Yao

Chen

et al. 2022

Advanced Science

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Acute kidney injury (AKI) is a complex clinical disorder associated with poor outcomes. Targeted regulation of the degree of inflammation has been a potential strategy for AKI management. Macrophages are the main effector cells of kidney inflammation. However, macrophage heterogeneity in ischemia reperfusion injury induced AKI (IRI‐AKI) remains unclear. Using single‐cell RNA sequencing of the mononuclear phagocytic system in the murine IRI model, the authors demonstrate the complementary roles of kidney resident macrophages (KRMs) and monocyte‐derived infiltrated macrophages (IMs) in modulating tissue inflammation and promoting tissue repair. A unique population of S100a9 hi Ly6c hi IMs is identified as an early responder to AKI, mediating the initiation and amplification of kidney inflammation. Kidney infiltration of S100A8/A9 + macrophages and the relevance of renal S100A8/A9 to tissue injury is confirmed in human AKI. Targeting the S100a8/a9 signaling with small‐molecule inhibitors exhibits renal protective effects represented by improved renal function and reduced mortality in bilateral IRI model, and decreased inflammatory response, ameliorated kidney injury, and improved long‐term outcome with decreased renal fibrosis in the unilateral IRI model. The findings support S100A8/A9 blockade as a feasible and clinically relevant therapy potentially waiting for translation in human AKI.

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Elevated Calprotectin and Abnormal Myeloid Cell Subsets Discriminate Severe from Mild COVID-19

Abstract: Highlights d Patients with severe COVID-19 accumulate HLA-DR Low monocytes and immature neutrophils in blood/lungs d Calprotectin level positively correlates with neutrophil count and disease severity d Loss of non-classical monocytes could identify high risk of severe COVID-19

Cited by 753 publications

References 71 publications

Mass cytometry and artificial intelligence define CD169 as a specific marker of SARS-CoV2-induced acute respiratory distress syndrome

Mass cytometry and artificial intelligence define CD169 as a specific marker of SARS-CoV2-induced acute respiratory distress syndrome

Neurological pathophysiology of SARS‐CoV‐2 and pandemic potential RNA viruses: a comparative analysis

Single Cell RNA Sequencing Identifies a Unique Inflammatory Macrophage Subset as a Druggable Target for Alleviating Acute Kidney Injury

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