Author:
Castaneda Diana Cadena,Jangra Sonia,Yurieva Marina,Martinek Jan,Callender Megan,Coxe Matthew,Choi Angela,Diego Juan García-Bernalt,Lin Jianan,Wu Te-Chia,Marches Florentina,Chaussabel Damien,Yu Peter,Salner Andrew,Aucello Gabrielle,Koff Jonathan,Hudson Briana,Church Sarah E.,Gorman Kara,Anguiano Esperanza,García-Sastre Adolfo,Williams Adam,Schotsaert Michael,Palucka Karolina
Abstract
AbstractThe COVID-19 pandemic continues to be a health crisis with major unmet medical needs. The early responses from airway epithelial cells, the first target of the virus regulating the progression towards severe disease, are not fully understood. Primary human air-liquid interface cultures representing the broncho-alveolar epithelia were used to study the kinetics and dynamics of SARS-CoV-2 variants infection. The infection measured by nucleoprotein expression, was a late event appearing between day 4-6 post infection for Wuhan-like virus. Other variants demonstrated increasingly accelerated timelines of infection. All variants triggered similar transcriptional signatures, an “early” inflammatory/immune signature preceding a “late” type I/III IFN, but differences in the quality and kinetics were found, consistent with the timing of nucleoprotein expression. Response to virus was spatially organized: CSF3 expression in basal cells and CCL20 in apical cells. Thus, SARS-CoV-2 virus triggers specific responses modulated over time to engage different arms of immune response.
Publisher
Cold Spring Harbor Laboratory