| Literature DB >> 33688651 |
Joel J Credle, Jonathan Gunn, Puwanat Sangkhapreecha, Daniel R Monaco, Xuwen Alice Zheng, Hung-Ji Tsai, Azaan Wilbon, William R Morgenlander, Yi Dong, Sahana Jayaraman, Lorenzo Tosi, Biju Parekkadan, Alan N Baer, Mario Roederer, Evan M Bloch, Aaron A R Tobian, Israel Zyskind, Jonathan I Silverberg, Avi Z Rosenberg, Andrea L Cox, Tom Lloyd, Andrew L Mammen, H Benjamin Larman.
Abstract
Unbiased antibody profiling can identify the targets of an immune reaction. A number of likely pathogenic autoreactive antibodies have been associated with life-threatening SARS-CoV-2 infection; yet, many additional autoantibodies likely remain unknown. Here we present Molecular Indexing of Proteins by Self Assembly (MIPSA), a technique that produces ORFeome-scale libraries of proteins covalently coupled to uniquely identifying DNA barcodes for analysis by sequencing. We used MIPSA to profile circulating autoantibodies from 55 patients with severe COVID-19 against 11,076 DNA-barcoded proteins of the human ORFeome library. MIPSA identified previously known autoreactivities, and also detected undescribed neutralizing interferon lambda 3 (IFN-λ3) autoantibodies. At-risk individuals with anti-IFN-λ3 antibodies may benefit from interferon supplementation therapies, such as those currently undergoing clinical evaluation. ONE-SENTENCEEntities:
Year: 2021 PMID: 33688651 PMCID: PMC7941622 DOI: 10.1101/2021.03.02.432977
Source DB: PubMed Journal: bioRxiv