A general platform for targeting MHC-II antigens via a single loop

Author:

Du Haotian,Liu Jingjia,Jude Kevin M.,Yang Xinbo,Li Ying,Bell Braxton,Yang Hongli,Kassardjian Audrey,Mobedi Ali,Parekh Udit,Sperberg R. Andres Parra,Julien Jean-Philippe,Mellins Elizabeth D.ORCID,Garcia K. ChristopherORCID,Huang Po-SsuORCID

Abstract

AbstractClass-II major histocompatibility complexes (MHC-IIs) are central to the communications between CD4+ T cells and antigen presenting cells (APCs), but intrinsic structural features associated with MHC-II make it difficult to develop a general targeting system with high affinity and antigen specificity. Here, we introduce a protein platform, Targeted Recognition of Antigen-MHC Complex Reporter for MHC-II (TRACeR-II), to enable the rapid development of peptide-specific MHC-II binders.TRACeR-IIhas a small helical bundle scaffold and uses an unconventional mechanism to recognize antigens via a single loop. This unique antigen-recognition mechanism renders this platform highly versatile and amenable to direct structural modeling of the interactions with the antigen. We demonstrate thatTRACeR-IIbinders can be rapidly evolved across multiple alleles, while computational protein design can produce specific binding sequences for a SARS-CoV-2 peptide of unknown complex structure.TRACeR-IIsheds light on a simple and straightforward approach to address the MHC peptide targeting challenge, without relying on combinatorial selection on complementarity determining region (CDR) loops. It presents a promising basis for further exploration in immune response modulation as well as a broad range of theragnostic applications.

Publisher

Cold Spring Harbor Laboratory

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