Antigen identification and high-throughput interaction mapping by reprogramming viral entry

Author:

Dobson Connor S.,Reich Anna N.,Gaglione Stephanie,Smith Blake E.,Kim Ellen J.,Dong Jiayi,Ronsard Larance,Okonkwo Vintus,Lingwood Daniel,Dougan Michael,Dougan Stephanie K.,Birnbaum Michael E.ORCID

Abstract

AbstractDeciphering immune recognition is critical for understanding a broad range of diseases and for the development of effective vaccines and immunotherapies. Efforts to do so are limited by a lack of technologies capable of simultaneously capturing the complexity of adaptive immune receptor repertoires and the landscape of potential antigens. To address this, we present RAPTR (Receptor-Antigen Pairing by Targeted Retroviruses). RAPTR combines viral pseudotyping and molecular engineering approaches to enable one-pot library on library interaction screens by displaying antigens on the surface of lentiviruses and encoding their identity in the viral genome. Antigen-specific viral infection of cells allows readout of both antigen and receptor identities via single-cell sequencing. The resulting system is modular, scalable, and compatible with any cell type, making it easily implemented. These techniques provide a suite of new tools for targeted viral entry, molecular engineering, and interaction screens with broad potential applications.

Publisher

Cold Spring Harbor Laboratory

Cited by 2 articles. 订阅此论文施引文献 订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献

1. Mapping the T cell repertoire to a complex gut bacterial community;2022-05-04

2. OUP accepted manuscript;Protein Engineering, Design, and Selection;2022

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