CD36 family members are TCR-independent ligands for CD1 antigen-presenting molecules

Author:

Gherardin Nicholas A.ORCID,Redmond Samuel J.,McWilliam Hamish E.G.,Almeida Catarina F.,Gourley Katherine H.A.,Seneviratna Rebecca,Li Shihan,De Rose Robert,Nguyen-Robertson Catriona V.,Su Shian,Ritchie Matthew E.,Villadangos Jose A.,Moody D. Branch,Pellicci Daniel G.,Uldrich Adam P.,Godfrey Dale I.

Abstract

AbstractCD1c presents lipid-based antigens to CD1c-restricted T cells which are thought to be a major component of the human T cell pool. The study of CD1c-restricted T cells, however, is hampered by the presence of an abundantly expressed CD1c-binding partner on blood cells distinct to the T cell receptor (TCR), confounding analysis of TCR-mediated CD1c tetramer staining. Here, we identify the CD36 family (CD36, CD36-L1 and CD36-L2) as novel ligands for CD1c, CD1b and CD1d proteins, and show that CD36 is the receptor responsible for non-TCR-mediated CD1c tetramer staining of blood cells. Moreover, CD36-blockade enables tetramer-based identification of CD1c-restricted T cells and clarifies identification of CD1b- and CD1d-restricted T cells. We use this technique to characterise CD1c-restricted T cells ex vivo and show diverse phenotypic features, TCR repertoire and antigen-specific subsets. Accordingly, this work will enable further studies into the biology of CD1 and human CD1-restricted T cells.One Sentence SummaryCD1 molecules bind CD36 family members and blockade of this interaction facilitates the study of CD1-restricted T cells.

Publisher

Cold Spring Harbor Laboratory

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