Viral RNA load in plasma is associated with critical illness and a dysregulated host response in COVID-19

Jesús F Bermejo‐Martin ,Belén Fernández Caso,Luz María Ruiz,Jesús Blanco,Iria Miguéns,Raúl Méndez,Pablo García Olivares,Elena Bustamante,Luis Jorge Valdivia,José Antonio Fernández-Ratero,Milagros González-Rivera,César Aldecoa,Gregoria Megías,Pedro Enríquez,Montserrat González-Estecha,Ferrán Barbé,María Ángeles Mantecón,Rubén Herrán,Silvia Martín,Isabel Fernández Natal,Félix Del Campo,Paula González-Jiménez,Felipe Pérez-García,Ioana Muñoz,Julia Gómez Barquero,Antonio Orduña,Alyson A Kelvin,Tomás Ruíz Albi ,Antoni Torres,Jésica Abadía ,Raquel Almansa,Laia Fernández-Barat ,Ana P Tedim,José María Eirós ,Cristina Doncel,Ruth Oneizat,Sara Pelegrin,Ricard Ferrer,Anna Motos,Luís Tamayo ,José Manuel Naranjo Gómez ,Noelia Jorge,José Ángel Berezo ,Gloria Renedo,Jamil Cedeño ,Raúl López-Izquierdo ,Ramón Cicuéndez ,Dariela Micheloud,Alicia Ortega,Juan Bustamante‐Munguira ,Jesús Rico-Feijoó ,Amanda De La Fuente,Carolina Puertas,Marta Martín-Fernández ,Nuria Mamolar,Natalia Blanca‐López ,Salvador Resino,Demetrio Carriedo,Guillermo Ruíz ,Esther Gargallo,Pablo Ryan ,Marta Domínguez‐Gil ,Wysali Trapiello,Ali Toloue Ostadgavahi,Rosário Menéndez ,David J Kelvin

doi:10.1186/s13054-020-03398-0

Abstract

BackgroundCOVID-19 can course with respiratory and extrapulmonary disease. SARS-CoV-2 RNA is detected in respiratory samples but also in blood, stool and urine. Severe COVID-19 is characterized by a dysregulated host response to this virus. We studied whether viral RNAemia or viral RNA load in plasma is associated with severe COVID-19 and also to this dysregulated response.MethodsA total of 250 patients with COVID-19 were recruited (50 outpatients, 100 hospitalized ward patients and 100 critically ill). Viral RNA detection and quantification in plasma was performed using droplet digital PCR, targeting the N1 and N2 regions of the SARS-CoV-2 nucleoprotein gene. The association between SARS-CoV-2 RNAemia and viral RNA load in plasma with severity was evaluated by multivariate logistic regression. Correlations between viral RNA load and biomarkers evidencing dysregulation of host response were evaluated by calculating the Spearman correlation coefficients.ResultsThe frequency of viral RNAemia was higher in the critically ill patients (78%) compared to ward patients (27%) and outpatients (2%) (p < 0.001). Critical patients had higher viral RNA loads in plasma than non-critically ill patients, with non-survivors showing the highest values. When outpatients and ward patients were compared, viral RNAemia did not show significant associations in the multivariate analysis. In contrast, when ward patients were compared with ICU patients, both viral RNAemia and viral RNA load in plasma were associated with critical illness (OR [CI 95%], p): RNAemia (3.92 [1.183–12.968], 0.025), viral RNA load (N1) (1.962 [1.244–3.096], 0.004); viral RNA load (N2) (2.229 [1.382–3.595], 0.001). Viral RNA load in plasma correlated with higher levels of chemokines (CXCL10, CCL2), biomarkers indicative of a systemic inflammatory response (IL-6, CRP, ferritin), activation of NK cells (IL-15), endothelial dysfunction (VCAM-1, angiopoietin-2, ICAM-1), coagulation activation (D-Dimer and INR), tissue damage (LDH, GPT), neutrophil response (neutrophils counts, myeloperoxidase, GM-CSF) and immunodepression (PD-L1, IL-10, lymphopenia and monocytopenia).ConclusionsSARS-CoV-2 RNAemia and viral RNA load in plasma are associated with critical illness in COVID-19. Viral RNA load in plasma correlates with key signatures of dysregulated host responses, suggesting a major role of uncontrolled viral replication in the pathogenesis of this disease.

Highlights

COVID-19 can course with respiratory and extrapulmonary disease
When ward patients were compared with intensive care unit (ICU) patients, both viral RNAemia and viral RNA load in plasma were associated with critical illness (OR [CI 95%], p): RNAemia (3.92 [1.183–12.968], 0.025), viral RNA load (N1) (1.962 [1.244–3.096], 0.004); viral RNA load (N2) (2.229 [1.382–3.595], 0.001)
SARS-CoV-2 RNAemia and viral RNA load in plasma are associated with critical illness in COVID-19

Summary

Introduction

COVID-19 can course with respiratory and extrapulmonary disease. SARS-CoV-2 RNA is detected in res‐ piratory samples and in blood, stool and urine. SARS-CoV-2 RNA is commonly detected in nasopharyngeal swabs; viral RNA can be found in sputum, lung samples, peripheral blood, serum, stool samples and to a limited extent urine [3,4,5,6]. Patients with severe COVID-19 show signatures of dysregulated response to infection, with immunological alterations involving moderate elevation of some cytokines and chemokines such as IL-6, IL-10 or CXCL10, deep lymphopenia with neutrophilia, systemic inflammation (elevation of C-reactive protein, ferritin), endothelial dysfunction, coagulation hyper-activation (D-dimers) and tissue damage (LDH) [9,10,11,12,13,14]. Our hypothesis is that systemic distribution of the virus or viral components could be associated with the severity of COVID-19, and in turn to a number of parameters indicating the presence of a dysregulated response to the infection

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Results

Conclusion