High diversity, turnover, and structural constraints characterize TCR α and β repertoire selection

Author:

Kamga Larisa,Gil Anna,Song Inyoung,Chirravuri Ramakanth,Aslan Nuray,Ghersi Dario,Stern Lawrence J.,Selin Liisa K.,Luzuriaga Katherine

Abstract

AbstractRecognition modes of individual T-cell receptors (TCR) are well studied, but how TCR repertoires are selected during acute through persistent human virus infections is less clear. Here, we show that persistent EBV-specific clonotypes account for only 9% of unique clonotypes but are highly expanded in acute infectious mononucleosis, and have distinct antigen-specific public features that drive selection into convalescence. The other 91% of highly diverse unique clonotypes disappear and are replaced in convalescence by equally diverse “de-novo” clonotypes. These broad fluctuating repertoires lend plasticity to antigen recognition and potentially protect against T-cell clonal loss and viral escape.

Publisher

Cold Spring Harbor Laboratory

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