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Título : Pulmonary Inflammatory Response in Lethal COVID-19 Reveals Potential Therapeutic Targets and Drugs in Phases III/IV Clinical Trials
Autor : López Cortés, Andrés
Guerrero, Santiago
Ortiz Prado, Esteban
Yumiceba, Verónica
Vera Guapi, Antonella
León Cáceres, Ángela
Simbaña Rivera, Katherine
Gómez Jaramillo, Ana María
Echeverría Garcés, Gabriela
García Cárdenas, Jennyfer M.
Puig San Andrés, Lourdes
Guevara Ramírez, Patricia
Cabrera Andrade, Alejandro
Bautista, Jhommara
Pérez Villa, Andy
Ramos Medin, María José
Pérez Meza, Álvaro Alexander
Nieto Jaramillo, Karol
Jácome, Andrea V.
Morillo, Andrea
Palabras clave : ulmonary inflammatory response
Clinical trials, drugs
Lethal COVID-19
Single nucleus RNA sequencing
Fecha de publicación : 2022
Editorial : Scopus
Citación : López-Cortés, A., Guerrero, S., Ortiz-Prado, E., Yumiceba, V., Vera-Guapi, A., León Cáceres, Á., Simbaña-Rivera, K., Gómez-Jaramillo, A. M., Echeverría-Garcés, G., García-Cárdenas, J. M., Guevara-Ramírez, P., Cabrera-Andrade, A., Puig San Andrés, L., Cevallos-Robalino, D., Bautista, J., Armendáriz-Castillo, I., Pérez-Villa, A., Abad-Sojos, A., Ramos-Medina, M. J., … Kyriakidis, N. C. (2022). Pulmonary Inflammatory Response in Lethal COVID-19 Reveals Potential Therapeutic Targets and Drugs in Phases III/IV Clinical Trials. Frontiers in Pharmacology, 13(March). https://doi.org/10.3389/fphar.2022.833174
Citación : PRODUCCIÓN CIENTÍFICA- ARTÍCULOS CIENTÍFICOS;A-IKIAM-000373
Resumen : The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), etiological agent of the coronavirus disease 2019 (COVID-19), has led to more than 425 million cases and more than 5.9 million deaths globally (WHO, 2021). Since the World Health Organization (WHO) declared the outbreak of COVID-19 as a pandemic, the novel coronavirus has been acquiring several mutations that not only increase its transmissibility rate but also mediates evasion of the host immune response and vaccination surveillance. Positive selection maintains amino-acid variants that increase virus fitness, whereas negative selection generally removes changes that reduce virus fitness (Lo Presti et al., 2020). For instance, some of the most predominant variants are capable of escaping monoclonal antibodies, partially eluding the polyclonal immune responses induced by previous infection or even allowing re-infections. It should be noted that recent improvements in immune escape are linked to mutations that alter the N-terminal domain (NTD) rather than the receptor-binding domain (RBD) of the spike (S) protein, where early and functionally important alterations predominated (Burioni and Topol, 2021).
URI : http://repositorio.ikiam.edu.ec/jspui/handle/RD_IKIAM/529
ISSN : https://doi.org/10.3389/fphar.2022.833174
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