Genomewide Association Study of Severe Covid-19 with Respiratory Failure

Ellinghaus, David; Degenhardt, Frauke; Bujanda, Luís; Buti, María; Albillos, Agustı́n; Invernizzi, Pietro; Fernández, Javier; Prati, Daniele; Baselli, Guido; Asselta, Rosanna; Grimsrud, Marit M.; Milani, Chiara; Aziz, Fátima; Kässens, Jan Christian; May, Sandra; Wendorff, Mareike; Wienbrandt, Lars; Uellendahl-Werth, Florian; Zheng, Tenghao; Yi, Xiaoli; Pablo, Raúl de; Chercoles, Adolfo Garrido; Palom, Adriana; García-Fernández, Alba Estela; Rodríguez‐Frías, Francisco; Zanella, Alberto; Bandera, Alessandra; Protti, Alessandro; Aghemo, Alessio; Lleo, Ana; Biondi, Andrea; Caballero-Garralda, Andrea; Gori, Andrea; Tanck, Anja; Carreras, Anna; Latiano, Anna; Fracanzani, Anna Ludovica; Peschuck, Anna; Juliá, Antonio; Pesenti, Antonio; Voza, Antonio; Jiménez, David; Mateos, Beatriz; Jimenez, Beatriz Nafria; Quereda, Carmen; Paccapelo, Cinzia; Gassner, Christoph; Angelini, Claudio; Cea, Cristina; Solier, Aurora; Pestaña, David; Muñiz‐Díaz, Eduardo; Sandoval, Elena; Paraboschi, Elvezia Maria; Navas, Enrique; Sanchez, Felix; Ceriotti, Ferruccio; Boneschi, Filippo Martinelli; Peyvandi, Flora; Blasi, Francesco; Téllez, Luís; Blanco‐Grau, Albert; Hemmrich-Stanisak, Georg; Costantino, Giorgio; Cardamone, Giulia; Foti, Giuseppe; Aneli, Serena; Kurihara, Hayato; ElAbd, Hesham; My, Ilaria; Galván-Femenía, Iván; Martı́n, Javier; Erdmann, Jeanette; Ferrusquía‐Acosta, José; García-Etxebarria, Koldo; Izquierdo-Sánchez, Laura; Bettini, Laura Rachele; Sumoy, Lauro; Terranova, Leonardo; Moreira, Letícia; Santoro, Luigi; Scudeller, Luigia; Mesonero, Francisco; Roade, Luisa; Rühlemann, Malte; Schaefer, Marco; Carrabba, Maria; Riveiro‐Barciela, Mar; Basso, Maria Eloina Figuera; Valsecchi, Maria Grazia; Hernández-Tejero, María; Acosta‐Herrera, Marialbert; D’Angiò, Mariella; Baldini, Marina; Cazzaniga, Marina Elena; Schulzky, Martin; Cecconi, Maurizio; Wittig, Michael; Ciccarelli, Michele; Rodríguez-Gandía, Miguel Ángel; Bocciolone, Monica; Miozzo, Monica; Montano, Nicola; Braun, Nicole; Sacchi, Nicoletta; Martínez, N. M. de Oca; Özer, Onur; Palmieri, Orazio; Faverio, Paola; Preatoni, Paoletta; Bonfanti, Paolo; Omodei, Paolo; Tentorio, Paolo; Castro, Pedro; Rodrigues, Pedro M.; Ortíz, Aaron Blandino; Cid, Rafael de; Ferrer, Ricard; Gualtierotti, Roberta; Nieto, Rosa; Goerg, Siegfried; Badalamenti, Salvatore; Marsal, Sara; Matullo, Giuseppe; Pelusi, Serena; Juzėnas, Simonas; Aliberti, Stefano; Monzani, Valter; Moreno, Vı́ctor; Wesse, Tanja; Lenz, Tobias; Pumarola, Tomás; Rimoldi, Valeria; Bòsari, Silvano; Albrecht, Wolfgang; Peter, Wolfgang; Romero‐Gómez, Manuel; D’Amato, Mauro; Duga, Stefano; Bañales, Jesús M.; Hov, Johannes R.; Folseraas, Trine; Valenti, Luca; Franke, André; Karlsen, Tom H.

doi:10.1056/nejmoa2020283

Cited by 1,603 publications

(1,497 citation statements)

References 42 publications

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“…With this in mind, even though the collected knowledge is still limited to few studies, some susceptibility markers other than HLA have been proposed for Covid-19. An association with ABO blood antigens has been observed in a cohort of Chinese patients, with the type A and 0 being respectively at highest and lowest risk to be infected, as previously been reported for other viral infections [36,37]. Genetic polymorphisms of key genes of the virus entry machinery (Ace2, Tmprss2, CtsB, and CtsL) or of the in ammatory/immune response (e.g.…”

Section: Discussionsupporting

confidence: 66%

Correlation of the two most frequent HLA haplotypes in the Italian population to the differential regional incidence of Covid-19

Pisanti

Deelen

Gallina

et al. 2020

Preprint

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Background: Understanding how HLA polymorphisms may affect both susceptibility, course and severity of Covid-19 infection could help both at the clinical level to identify individuals at higher risk from the disease and at the epidemiological one to explain the differences in the epidemic trend among countries or even within a specific country. Covid-19 disease in Italy showed a peculiar geographical distribution from the northern most affected regions to the southern ones only slightly touched. Methods: In this study we analysed the regional frequencies for the most common Italian haplotypes from the Italian Bone Marrow Donor Registry (HLA-A, -B, -C and -DRB1 at four-digit level). Then we performed Pearson correlation analyses among regional haplotypes estimated frequency in the population and Covid-19 incidence and mortality.Results: In this study we found that the two most frequent HLA haplotypes in the Italian population, HLA-A*:01:01g-B*08:01g-C*07:01g-DRB1*03:01g and HLA-A*02.01g-B*18.01g-C*07.01g-DRB1*11.04g, had a regional distribution overlapping that of Covid-19 and showed respectively a positive (suggestive of susceptibility) and negative (suggestive of protection) significant correlation with both Covid-19 incidence and mortality. Conclusions: Based on these results, in order to define such HLA polymorphisms as a factor effectively associated to the disease susceptibility, the creation of national networks that can collect patients’ samples from all regions for HLA typing should be highly encouraged.

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Section: Discussionsupporting

confidence: 66%

Correlation of the two most frequent HLA haplotypes in the Italian population to the differential regional incidence of Covid-19

Pisanti

Deelen

Gallina

et al. 2020

Preprint

View full text Add to dashboard Cite

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“…For rs657152, the overall frequency of the protective allele C was 0.5468 (222/406) in our data, with the lowest rate found in the critical group (AF = 0.382, 13/34, Fisher's exact test P = 0.04896). For rs11385942, the risk allele GA was not detected in any patient in our study, as this variant was rare in Chinese people 27 (Supplementary Table 4.4), consistent with previously reported global distribution 26 . Quantitative trait locus (QTL) analysis has been widely applied to infer the contribution of genetic variations to complex phenotypes 28 .…”

Section: Genomic Architecture Of Covid-19 Patientssupporting

confidence: 91%

“…Additionally, PTGIS possesses anti-in ammatory properties by modulating the expression of IL-1, IL-6, IL-10, which may be associated with the COVID-19 severity 25 . We also assessed two loci, rs657152 at locus 9q34.2 and rs11385942 at locus 3p21.31, which have been found to be associated with COVID-19 patients with severe respiratory failure in Spanish and Italian populations 26 . For rs657152, the overall frequency of the protective allele C was 0.5468 (222/406) in our data, with the lowest rate found in the critical group (AF = 0.382, 13/34, Fisher's exact test P = 0.04896).…”

Section: Genomic Architecture Of Covid-19 Patientsmentioning

confidence: 99%

The Trans-omics Landscape of COVID-19

Chen

Ding

et al. 2020

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The outbreak of coronavirus disease 2019 (COVID-19) has been causing a global health emergency. Although previous studies investigated COVID-19 at different omics levels, the molecular hallmarks of COVID-19, especially in those patients without comorbidities, have not been fully investigated. Here, we presented a trans-omics landscape for COVID-19 based on integrative analysis of genomic, transcriptomic, proteomic, metabolomic and lipidomic profiles from blood samples of 231 COVID-19 patients, ranging from asymptomatic to critically ill, importantly excluding those with any comorbidities. Notably, we found neutrophils heterogeneity existed between asymptomatic and critically ill patients. Expression discordance of inflammatory cytokines at mRNA and protein levels in asymptomatic patients could possibly be explained by post-transcriptional regulation by RNA binding proteins (RBPs) and microRNAs. Neutrophils over-activation, induced arginine depletion, and tryptophan metabolites accumulation contributed to T/NK cell dysfunction in critical patients. Anti-virus interferons were gradually suppressed along with disease severity. Overall, our study systematically revealed multi-omics characteristics of COVID-19, and the data we generated could hopefully help illuminate COVID-19 pathogenesis and provide valuable clues about potential therapeutic strategies for COVID-19.

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“…rs11385942 may act trough the regulation of the memory lymphoid cell migration Expression pro les generated by scRNA-seq can be overlaid with genome-wide association studies (GWASs) to pinpoint speci c cell types and identify potential cellular and molecular mechanisms explaining the described genetic associations [28]. In addition to the ABO group locus, a recent study found that another genomic locus is associated with the development of severe forms of COVID-19 [23].…”

Section: Covid-19 Affects Blood and Lung Lymphocyte Compartments In Amentioning

confidence: 99%

“…Unfortunately, none of the past studies analyzed the immune regulatory properties of myeloid cells at functional level. A speci c genetic locus including immune related genes (such as C-X-C motif chemokine receptor 6 -CXCR6), was found to be associated with worse prognosis in COVID-19 patients [23]. Other studies exclusively performed on broncho-alveolar lavage uids (BAL), elucidated the sustained interplay between macrophages releasing in ammatory cytokines and lung epithelial cells in more severe COVID-19 disease stages [21], whereas pointed out highly clonally expanded CD8 + T cells in moderate patients [22].…”

Section: Introductionmentioning

confidence: 99%

Deciphering the state of immune silence in fatal COVID-19 patients

Amit

Bost

Sanctis

et al. 2020

Preprint

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Since the beginning of the SARS-CoV-2 pandemic, COVID-19 has appeared as a unique disease with unconventional tissue and systemic immune features. While COVID-19 severe forms share clinical and laboratory aspects with various pathologies such as hemophagocytic lymphohistiocyto-sis, sepsis or cytokine release syndrome, their exact nature remains unknown. This is severely imped-ing the ability to treat patients facing severe stages of the disease. To this aim, we performed an in-depth, single-cell RNA-seq analysis of more than 150.000 immune cells isolated from matched blood samples and broncho-alveolar lavage fluids of COVID-19 patients and healthy controls, and integrated it with clinical, immunological and functional ex vivo data. We unveiled an immune sig-nature of disease severity that correlated with the accumulation of naïve lymphoid cells in the lung and an expansion and activation of myeloid cells in the periphery. Moreover, we demonstrated that myeloid-driven immune suppression is a hallmark of COVID-19 evolution and arginase 1 expression is significantly associated with monocyte immune regulatory features. Noteworthy, we found mon-ocyte and neutrophil immune suppression loss associated with fatal clinical outcome in severe pa-tients. Additionally, our analysis discovered that the strongest association of the patients clinical outcome and immune phenotype is the lung T cell response. We found that patients with a robust CXCR6+ effector memory T cell response have better outcomes. This result is line with the rs11385942 COVID-19 risk allel, which is in proximity to the CXCR6 gene and suggest effector memory T cell are a primary feature in COVID-19 patients. By systemically quantifying the viral landscape in the lung of severe patients, we indeed identified Herpes-Simplex-Virus 1 (HSV-1) as a potential opportunistic virus in COVID-19 patients. Lastly, we observed an unexpectedly high SARS-CoV-2 viral load in an immuno-compromised patient, allowing us to study the SARS-CoV-2 in-vivo life cycle. The development of myeloid dysfunctions and the impairment of lymphoid arm establish a condition of immune paralysis that supports secondary bacteria and virus infection and can progress to “immune silence” in patients facing death.

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Genomewide Association Study of Severe Covid-19 with Respiratory Failure

Cited by 1,603 publications

References 42 publications

Correlation of the two most frequent HLA haplotypes in the Italian population to the differential regional incidence of Covid-19

Correlation of the two most frequent HLA haplotypes in the Italian population to the differential regional incidence of Covid-19

The Trans-omics Landscape of COVID-19

Deciphering the state of immune silence in fatal COVID-19 patients

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