Efficient encoding of large antigenic spaces by epitope prioritization with Dolphyn

Author:

Liebhoff Anna-MariaORCID,Venkataraman ThiagarajanORCID,Morgenlander William RORCID,Na Miso,Kula TomaszORCID,Waugh Kathleen,Morrison CharlesORCID,Rewers MarianORCID,Longman RandyORCID,Round JuneORCID,Elledge StephenORCID,Ruczinski IngoORCID,Langmead BenORCID,Larman H BenjaminORCID

Abstract

AbstractWe investigated a relatively underexplored component of the gut-immune axis by profiling the antibody response to gut phages using Phage Immunoprecipitation Sequencing (PhIP-Seq). To enhance this approach, we developed Dolphyn, a novel method that uses machine learning to select peptides from protein sets and compresses the proteome through epitope-stitching. Dolphyn improves the fraction of gut phage library peptides bound by antibodies from 10% to 31% in healthy individuals, while also reducing the number of synthesized peptides by 78%. In our study on gut phages, we discovered that the immune system develops antibodies to bacteria-infecting viruses in the human gut, particularlyE.coli-infectingMyoviridae. Cost-effective PhIP-Seq libraries designed with Dolphyn enable the assessment of a wider range of proteins in a single experiment, thus facilitating the study of the gut-immune axis.

Publisher

Cold Spring Harbor Laboratory

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