Rare host variants in ciliary expressed genes contribute to COVID-19 severity in Bulgarian patients
Author:
Kamenarova Kunka1, Kachakova-Yordanova Darina1, Baymakova Magdalena2, Georgiev Martin1, Mihova Kalina1, Petkova Veronika1, Beltcheva Olga1, Argirova Radka3, Atanasov Petar4, Kunchev Metodi2, Andonova Radina2, Zasheva Anelia2, Drenska Rumiana4, Ivanov Ivaylo4, Pantileeva Diana4, Koleva Veselina3, Penev Anton3, Lekova-Nikova Diana3, Georgiev Delyan1, Pencheva Daniela1, Bozhilova Radosveta1, Ivanova Nevyana1, Dimova Ivanka1, Plochev Kamen2, Popov Georgi2, Popivanov Ivan2, Gabrovsky Nikolay4, Leseva Magdalena4, Mitev Vanio1, Kaneva Radka1
Affiliation:
1. Medical University 2. Military Medical Academy 3. Acibadem City Clinic, Multidisciplinary Hospital for Active Treatment "Tokuda” 4. University Multidisciplinary Hospital for Active Treatment and Emergency Medicine “N.I. Pirogov”
Abstract
Abstract
Severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) causes coronavirus disease 2019 (COVID-19), a pneumonia with extremely heterogeneous clinical presentation, ranging from asymptomatic to severely ill patients. Previous studies have reported links between the presence of host genetic variants and the outcome of the COVID-19 infection. In our study, we used whole exome sequencing in a cohort of 444 SARS-CoV-2 patients, admitted to hospital in the period October-2020-April-2022, to search for associations between rare pathogenic/potentially pathogenic variants and COVID-19 progression. We used gene prioritization-based analysis in genes that have been reported by host genetic studies. Although we did not identify correlation between the presence of rare pathogenic variants and COVID-19 outcome, in critically ill patients we detected known mutations in a number of genes associated with severe disease related to cardiovascular disease, primary ciliary dyskinesia, cystic fibrosis, DNA damage repair response, coagulation, primary immune disorder, hemoglobin subunit β, and others. Additionally, we report 93 novel pathogenic variants found in severely infected patients who required intubation or died. A network analysis showed main component, consisting of 13 highly interconnected genes related to epithelial cilium. In conclusion, we have detected rare pathogenic host variants that may have influenced the COVID-19 outcome in Bulgarian patients.
Publisher
Springer Science and Business Media LLC
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