Acquired decrease of the C3b/C4b receptor (CR1, CD35) and increased C4d deposits on erythrocytes from ICU COVID-19 patients

Aymric Kisserli; Nathalie Schneider; Sandra Audonnet; Thierry Tabary; Antoine Goury; Joel Cousson; Rachid Mahmoudi; Firouze Bani-Sadr; Lukshe Kanagaratnam; Damien Jolly; Jacques Hm Cohen

doi:10.1016/j.imbio.2021.152093

Acquired decrease of the C3b/C4b receptor (CR1, CD35) and increased C4d deposits on erythrocytes from ICU COVID-19 patients

Immunobiology. 2021 May;226(3):152093. doi: 10.1016/j.imbio.2021.152093. Epub 2021 May 9.

Authors

Affiliations

¹ Oncogeriatric Coordination Unit, Rheims University Hospital, Rheims, France; Nanosciences Research Laboratory LRN EA 4682, University of Rheims Champagne-Ardenne, Rheims, France.
² Biochemistry, Pharmacology and Toxicology Unit, Rheims University Hospital, Rheims, France.
³ URCACyt, Flow Cytometry Technical Platform, University of Rheims Champagne-Ardenne, Rheims, France.
⁴ Nanosciences Research Laboratory LRN EA 4682, University of Rheims Champagne-Ardenne, Rheims, France; Immunology Laboratory, Rheims University Hospital, Rheims, France.
⁵ Medical-Surgical ICU, Rheims University Hospital, Rheims, France.
⁶ Department of Internal Medicine and Geriatrics, Rheims University Hospital, Rheims, France; Aging and Fragility Unit EA 3797, University of Rheims Champagne-Ardenne, Rheims, France.
⁷ Aging and Fragility Unit EA 3797, University of Rheims Champagne-Ardenne, Rheims, France; Research Promotion and Support Unit, Rheims University Hospital, Rheims, France.
⁸ Nanosciences Research Laboratory LRN EA 4682, University of Rheims Champagne-Ardenne, Rheims, France. Electronic address: jacques.cohen@univ-reims.fr.

Abstract

In order to study the mechanisms of COVID-19 damage following the complement activation phase occurring during the innate immune response to SARS-CoV-2, CR1 (the regulating complement activation factor, CD35, the C3b/C4b receptor), C4d deposits on Erythrocytes (E), and the products of complement activation C3b/C3bi, were assessed in 52 COVID-19 patients undergoing O₂ therapy or assisted ventilation in ICU units in Rheims France. An acquired decrease of CR1 density on E from COVID-19 patients was observed (Mean = 418, SD = 162, N = 52) versus healthy individuals (Mean = 592, SD = 287, N = 400), Student's t-test p < 10^-6, particularly among fatal cases, and in parallel with several parameters of clinical severity. Large deposits of C4d on E in patients were well above values observed in normal individuals, mostly without concomitant C3 deposits, in more than 80% of the patients. This finding is reminiscent of the increased C4d deposits on E previously observed to correlate with sub endothelial pericapillary deposits in organ transplant rejection, and with clinical SLE flares. Conversely, significant C3 deposits on E were only observed among ¼ of the patients. The decrease of CR1/E density, deposits of C4 fragments on E and previously reported detection of virus spikes or C3 on E among COVID-19 patients, suggest that the handling and clearance of immune complex or complement fragment coated cell debris may play an important role in the pathophysiology of SARS-CoV-2. Measurement of C4d deposits on E might represent a surrogate marker for assessing inflammation and complement activation occurring in organ capillaries and CR1/E decrease might represent a cumulative index of complement activation in COVID-19 patients. Taken together, these original findings highlight the participation of complement regulatory proteins and indicate that E are important in immune pathophysiology of COVID-19 patients. Besides a potential role for monitoring the course of disease, these observations suggest that novel therapies such as the use of CR1, or CR1-like molecules, in order to down regulate complement activation and inflammation, should be considered.

Keywords: C3; C4; CD35; COVID-19; CR1; Complement; Erythrocytes.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antigen-Antibody Complex / metabolism*
COVID-19 / immunology*
COVID-19 / therapy
Complement Activation
Complement C4b / metabolism*
Erythrocytes / metabolism*
Erythrocytes / pathology
France
Gene Expression Regulation
Humans
Intensive Care Units
Peptide Fragments / metabolism*
Receptors, Complement 3b / genetics
Receptors, Complement 3b / metabolism*
Receptors, Complement 3b / therapeutic use
SARS-CoV-2 / physiology*

Substances

Antigen-Antibody Complex
CR1 protein, human
Peptide Fragments
Receptors, Complement 3b
Complement C4b
complement C4d