Author: Andonegui-Elguera, Sergio; Taniguchi-Ponciano, Keiko; Gonzales-Bonilla, Cesar Raul; Torres, Javier; Mayani, Hector; Herrera, Luis Alonso; Peña-MartÃnez, Eduardo; Silva-Román, Gloria; Vela-Patiño, Sandra; Ferreira-Hermosillo, Aldo; Ramirez-Renteria, Claudia; Carvente-Garcia, Roberto; Mata-Lozano, Carlos; Marrero-RodrÃguez, Daniel; Mercado, Moises
Title: Molecular Alterations Prompted by SARS-CoV-2 Infection: Induction of Hyaluronan, Glycosaminoglycan and Mucopolysaccharide Metabolism Cord-id: nz36i2oa Document date: 2020_6_18
ID: nz36i2oa
Snippet: Abstract Background The SARS-CoV-2 is the etiological agent causing COVID-19 which has infected more than 2 million people with more than 200000 deaths since its emergence in December 2019. In the majority of cases patients are either asymptomatic or show mild to moderate symptoms and signs of a common cold. A subset of patients, however, develop a severe atypical pneumonia, with the characteristic ground-glass appearance on chest x-ray and computerized tomography, which evolves into an acute re
Document: Abstract Background The SARS-CoV-2 is the etiological agent causing COVID-19 which has infected more than 2 million people with more than 200000 deaths since its emergence in December 2019. In the majority of cases patients are either asymptomatic or show mild to moderate symptoms and signs of a common cold. A subset of patients, however, develop a severe atypical pneumonia, with the characteristic ground-glass appearance on chest x-ray and computerized tomography, which evolves into an acute respiratory distress syndrome, that requires mechanical ventilation and eventually results in multiple organ failure and death. The Molecular pathogenesis of COVID-19 is still unknown. Aim of the study In the present work we performed a stringent metanalysis from the publicly available RNAseq data from bronchoalveolar cells and peripheral blood mononuclear cells to elucidate molecular alterations and cellular deconvolution to identify immune cell profiles. Results Alterations in genes involved in hyaluronan, glycosaminoglycan and mucopolysaccharides metabolism were over-represented in bronchoalveolar cells infected by SARS-CoV-2, as well as potential lung infiltration with neutrophils, NK cells, T CD4+ cell and macrophages. The blood mononuclear cells presented a proliferative state. Dramatic reduction of neutrophils, NK and T lymphocytes, whereas an exacerbated increase in monocytes. Conclusions In summary our results revealed molecular pathogenesis of the SARS-CoV-2 infection to bronchoalveolar cells inducing the hyaluronan and glycosaminoglycan metabolism that could shape partially the components of the ground-glass opacities observed in CT. And the potential immune response profile in COVID-19.
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