Author: Solanich, Xavier; Vargas-Parra, Gardenia; van der Made, Caspar I.; Simons, Annet; Schuurs-Hoeijmakers, Janneke; AntolÃ, Arnau; del Valle, Jesús; Rocamora-Blanch, Gemma; Setién, Fernando; Esteller, Manel; van Reijmersdal, Simon V.; Riera-Mestre, Antoni; Sabater-Riera, Joan; Capellá, Gabriel; van de Veerdonk, Frank L.; van der Hoven, Ben; Corbella, Xavier; Hoischen, Alexander; Lázaro, Conxi
Title: Genetic Screening for TLR7 Variants in Young and Previously Healthy Men With Severe COVID-19 Cord-id: v1qj47sa Document date: 2021_7_23
ID: v1qj47sa
Snippet: INTRODUCTION: Loss-of-function TLR7 variants have been recently reported in a small number of males to underlie strong predisposition to severe COVID-19. We aimed to determine the presence of these rare variants in young men with severe COVID-19. METHODS: We prospectively studied males between 18 and 50 years-old without predisposing comorbidities that required at least high-flow nasal oxygen to treat COVID-19. The coding region of TLR7 was sequenced to assess the presence of potentially deleter
Document: INTRODUCTION: Loss-of-function TLR7 variants have been recently reported in a small number of males to underlie strong predisposition to severe COVID-19. We aimed to determine the presence of these rare variants in young men with severe COVID-19. METHODS: We prospectively studied males between 18 and 50 years-old without predisposing comorbidities that required at least high-flow nasal oxygen to treat COVID-19. The coding region of TLR7 was sequenced to assess the presence of potentially deleterious variants. RESULTS: TLR7 missense variants were identified in two out of 14 patients (14.3%). Overall, the median age was 38 (IQR 30-45) years. Both variants were not previously reported in population control databases and were predicted to be damaging by in silico predictors. In a 30-year-old patient a maternally inherited variant [c.644A>G; p.(Asn215Ser)] was identified, co-segregating in his 27-year-old brother who also contracted severe COVID-19. A second variant [c.2797T>C; p.(Trp933Arg)] was found in a 28-year-old patient, co-segregating in his 24-year-old brother who developed mild COVID-19. Functional testing of this variant revealed decreased type I and II interferon responses in peripheral mononuclear blood cells upon stimulation with the TLR7 agonist imiquimod, confirming a loss-of-function effect. CONCLUSIONS: This study supports a rationale for the genetic screening for TLR7 variants in young men with severe COVID-19 in the absence of other relevant risk factors. A diagnosis of TLR7 deficiency could not only inform on treatment options for the patient, but also enables pre-symptomatic testing of at-risk male relatives with the possibility of instituting early preventive and therapeutic interventions.
Search related documents:
Co phrase search for related documents- abo blood group and lung injury: 1
- acute ards respiratory distress syndrome and low effect: 1, 2
- acute ards respiratory distress syndrome and lung injury: 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25
- adapter protein and lung injury: 1
- low effect and lung injury: 1, 2
Co phrase search for related documents, hyperlinks ordered by date