Actionable Cytopathogenic Host Responses of Human Alveolar Type 2 Cells to SARS-CoV-2

人类 II 型肺泡细胞对 SARS-CoV-2 的可操作细胞病变宿主反应

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作者:Ryan M Hekman ,Adam J Hume ,Raghuveera Kumar Goel ,Kristine M Abo ,Jessie Huang ,Benjamin C Blum ,Rhiannon B Werder ,Ellen L Suder ,Indranil Paul ,Sadhna Phanse ,Ahmed Youssef ,Konstantinos D Alysandratos ,Dzmitry Padhorny ,Sandeep Ojha ,Alexandra Mora-Martin ,Dmitry Kretov ,Peter E A Ash ,Mamta Verma ,Jian Zhao ,J J Patten ,Carlos Villacorta-Martin ,Dante Bolzan ,Carlos Perea-Resa ,Esther Bullitt ,Anne Hinds ,Andrew Tilston-Lunel ,Xaralabos Varelas ,Shaghayegh Farhangmehr ,Ulrich Braunschweig ,Julian H Kwan ,Mark McComb ,Avik Basu ,Mohsan Saeed ,Valentina Perissi ,Eric J Burks ,Matthew D Layne ,John H Connor ,Robert Davey ,Ji-Xin Cheng ,Benjamin L Wolozin ,Benjamin J Blencowe ,Stefan Wuchty ,Shawn M Lyons ,Dima Kozakov ,Daniel Cifuentes ,Michael Blower ,Darrell N Kotton ,Andrew A Wilson ,Elke Mühlberger ,Andrew Emili

Abstract

Human transmission of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), causative pathogen of the COVID-19 pandemic, exerts a massive health and socioeconomic crisis. The virus infects alveolar epithelial type 2 cells (AT2s), leading to lung injury and impaired gas exchange, but the mechanisms driving infection and pathology are unclear. We performed a quantitative phosphoproteomic survey of induced pluripotent stem cell-derived AT2s (iAT2s) infected with SARS-CoV-2 at air-liquid interface (ALI). Time course analysis revealed rapid remodeling of diverse host systems, including signaling, RNA processing, translation, metabolism, nuclear integrity, protein trafficking, and cytoskeletal-microtubule organization, leading to cell cycle arrest, genotoxic stress, and innate immunity. Comparison to analogous data from transformed cell lines revealed respiratory-specific processes hijacked by SARS-CoV-2, highlighting potential novel therapeutic avenues that were validated by a high hit rate in a targeted small molecule screen in our iAT2 ALI system. Keywords: COVID-19; SARS-CoV-2; antivirals; infection; mass spectrometry; pathogenesis; pathways; phosphoproteomics; pneumocytes; time course.

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