Host Response Changes and Their Association with Mortality in COVID-19 Patients with Lymphopenia

Erik H A Michels; Brent Appelman; Justin de Brabander; Rombout B E van Amstel; Christine C A van Linge; Osoul Chouchane; Tom D Y Reijnders; Alex R Schuurman; Titia A L Sulzer; Augustijn M Klarenbeek; Renée A Douma; Lieuwe D J Bos; W Joost Wiersinga; Hessel Peters-Sengers; Tom van der Poll; Amsterdam UMC COVID-19 Biobank Study Group

doi:10.1164/rccm.202305-0890OC

Host Response Changes and Their Association with Mortality in COVID-19 Patients with Lymphopenia

Am J Respir Crit Care Med. 2024 Feb 15;209(4):402-416. doi: 10.1164/rccm.202305-0890OC.

Authors

Erik H A Michels¹, Brent Appelman¹, Justin de Brabander¹, Rombout B E van Amstel², Christine C A van Linge¹, Osoul Chouchane¹, Tom D Y Reijnders¹, Alex R Schuurman¹, Titia A L Sulzer¹, Augustijn M Klarenbeek¹, Renée A Douma³, Lieuwe D J Bos², W Joost Wiersinga^{1

4}, Hessel Peters-Sengers^{1

5}, Tom van der Poll^{1

4}; Amsterdam UMC COVID-19 Biobank Study Group

Collaborators

Amsterdam UMC COVID-19 Biobank Study Group:
Michiel van Agtmael, Anne Geke Algera, Brent Appelman, Floor van Baarle, Martijn Beudel, Harm Jan Bogaard, Marije Bomers Peter Bonta, Lieuwe Bos, Michela Botta, Justin de Brabander, Godelieve de Bree, Sanne de Bruin, Marianna Bugiani, Esther Bulle, David T P Buis, Osoul Chouchane Alex Cloherty, Mirjam Dijkstra, Dave A Dongelmans, Romein W G Dujardin, Paul Elbers, Lucas Fleuren, Suzanne Geerlings Theo Geijtenbeek, Armand Girbes, Bram Goorhuis, Martin P Grobusch, Laura Hagens, Jorg Hamann, Vanessa Harris, Robert Hemke, Sabine M Hermans Leo Heunks, Markus Hollmann, Janneke Horn, Joppe W Hovius, Hanna K de Jong, Menno D de Jong, Rutger Koning, Bregje Lemkes, Endry H T Lim, Niels van Mourik, Jeaninne Nellen, Esther J Nossent, Sabine Olie, Frederique Paulus, Edgar Peters, Dan A I Pina-Fuentes, Tom van der Poll, Bennedikt Preckel, Jorinde Raasveld, Tom Reijnders, Maurits C F J de Rotte, Michiel Schinkel, Marcus J Schultz, Femke A P Schrauwen, Alex Schuurman, Jaap Schuurmans, Kim Sigaloff, Marleen A Slim, Patrick Smeele, Marry Smit, Cornelis S Stijnis, Willemke Stilma, Charlotte Teunissen, Patrick Thoral, Anissa M Tsonas, Pieter R Tuinman, Marc van der Valk, Denise P Veelo, Carolien Volleman, Heder de Vries, Lonneke A Vught, Michèle van Vugt, Dorien Wouters, A H Koos Zwinderman, Matthijs C Brouwer, W Joost Wiersinga, Alexander P J Vlaar, Diederik van de Beek

Affiliations

¹ Center for Experimental and Molecular Medicine.
² Department of Intensive Care Medicine, and.
³ Department of Internal Medicine, Flevo Hospital, Almere, the Netherlands; and.
⁴ Division of Infectious Diseases, Amsterdam UMC location University of Amsterdam, Amsterdam, the Netherlands.
⁵ Department of Epidemiology and Data Science, Amsterdam UMC location Vrije Universiteit Amsterdam, Amsterdam, the Netherlands.

Abstract

Rationale: Lymphopenia in coronavirus disease (COVID-19) is associated with increased mortality. Objectives: To explore the association between lymphopenia, host response aberrations, and mortality in patients with lymphopenic COVID-19. Methods: We determined 43 plasma biomarkers reflective of four pathophysiological domains: endothelial cell and coagulation activation, inflammation and organ damage, cytokine release, and chemokine release. We explored if decreased concentrations of lymphocyte-derived proteins in patients with lymphopenia were associated with an increase in mortality. We sought to identify host response phenotypes in patients with lymphopenia by cluster analysis of plasma biomarkers. Measurements and Main Results: A total of 439 general ward patients with COVID-19 were stratified by baseline lymphocyte counts: normal (>1.0 × 10⁹/L; n = 167), mild lymphopenia (>0.5 to ⩽1.0 × 10⁹/L; n = 194), and severe lymphopenia (⩽0.5 × 10⁹/L; n = 78). Lymphopenia was associated with alterations in each host response domain. Lymphopenia was associated with increased mortality. Moreover, in patients with lymphopenia (n = 272), decreased concentrations of several lymphocyte-derived proteins (e.g., CCL5, IL-4, IL-13, IL-17A) were associated with an increase in mortality (at P < 0.01 or stronger significance levels). A cluster analysis revealed three host response phenotypes in patients with lymphopenia: "hyporesponsive" (23.2%), "hypercytokinemic" (36.4%), and "inflammatory-injurious" (40.4%), with substantially differing mortality rates of 9.5%, 5.1%, and 26.4%, respectively. A 10-biomarker model accurately predicted these host response phenotypes in an external cohort with similar mortality distribution. The inflammatory-injurious phenotype showed a remarkable combination of relatively high inflammation and organ damage markers with high antiinflammatory cytokine levels yet low proinflammatory cytokine levels. Conclusions: Lymphopenia in COVID-19 signifies a heterogenous group of patients with distinct host response features. Specific host responses contribute to lymphopenia-associated mortality in COVID-19, including reduced CCL5 levels.

Keywords: biomarkers; cytokines; lymphocytes; phenotype; pneumonia.

MeSH terms

Anemia* / complications
Biomarkers
COVID-19* / complications
Cytokines
Humans
Inflammation / complications
Lymphopenia* / complications
SARS-CoV-2

Substances

Cytokines
Biomarkers

Grants and funding

10430142110001/ZONMW_/ZonMw/Netherlands