Longitudinal proteomic analysis of severe COVID-19 reveals survival-associated signatures, tissue-specific cell death, and cell-cell interactions

免疫系统 生物 蛋白质组 细胞 疾病 电池类型 程序性细胞死亡 炎症 蛋白酵素 免疫学 医学 生物信息学 病理 细胞凋亡 遗传学 生物化学
作者
Michael R. Filbin,Arnav Mehta,Alexis M. Schneider,Kyle R. Kays,Jamey Guess,Matteo Gentili,Bánk G. Fenyves,Nicole C. Charland,Anna L.K. Gonye,Irena Gushterova,Hargun K. Khanna,Thomas J. LaSalle,Kendall M. Lavin-Parsons,Brendan M. Lilley,Carl L. Lodenstein,Kasidet Manakongtreecheep,Justin Margolin,Brenna McKaig,Maricarmen Rojas-López,Brian C. Russo,Nihaarika Sharma,Jessica Tantivit,Molly Thomas,Robert E. Gerszten,Graham Heimberg,Paul Hoover,David Lieb,Brian Lin,Debby Ngo,Karin Pelka,Miguel Reyes,Christopher S. Smillie,Avinash Waghray,Thomas E. Wood,Amanda S. Zajac,Lori L. Jennings,Ida Grundberg,Roby P. Bhattacharyya,Blair A. Parry,Alexandra‐Chloé Villani,Moshe Sade-Feldman,Nir Hacohen,Marcia B. Goldberg
出处
期刊:Cell reports medicine [Elsevier]
卷期号:2 (5): 100287-100287 被引量:231
标识
DOI:10.1016/j.xcrm.2021.100287
摘要

Mechanisms underlying severe coronavirus disease 2019 (COVID-19) disease remain poorly understood. We analyze several thousand plasma proteins longitudinally in 306 COVID-19 patients and 78 symptomatic controls, uncovering immune and non-immune proteins linked to COVID-19. Deconvolution of our plasma proteome data using published scRNA-seq datasets reveals contributions from circulating immune and tissue cells. Sixteen percent of patients display reduced inflammation yet comparably poor outcomes. Comparison of patients who died to severely ill survivors identifies dynamic immune-cell-derived and tissue-associated proteins associated with survival, including exocrine pancreatic proteases. Using derived tissue-specific and cell-type-specific intracellular death signatures, cellular angiotensin-converting enzyme 2 (ACE2) expression, and our data, we infer whether organ damage resulted from direct or indirect effects of infection. We propose a model in which interactions among myeloid, epithelial, and T cells drive tissue damage. These datasets provide important insights and a rich resource for analysis of mechanisms of severe COVID-19 disease.

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