CD1b tetramers bind αβ T cell receptors to identify a mycobacterial glycolipid-reactive T cell repertoire in humans

AG Kasmar, I van Rhijn, TY Cheng, M Turner… - Journal of Experimental …, 2011 - rupress.org
AG Kasmar, I van Rhijn, TY Cheng, M Turner, C Seshadri, A Schiefner, RC Kalathur
Journal of Experimental Medicine, 2011rupress.org
Microbial lipids activate T cells by binding directly to CD1 and T cell receptors (TCRs) or by
indirect effects on antigen-presenting cells involving induction of lipid autoantigens, CD1
transcription, or cytokine release. To distinguish among direct and indirect mechanisms, we
developed fluorescent human CD1b tetramers and measured T cell staining. CD1b tetramer
staining of T cells requires glucose monomycolate (GMM) antigens, is specific for TCR
structure, and is blocked by a recombinant clonotypic TCR comprised of TRAV17 and …
Microbial lipids activate T cells by binding directly to CD1 and T cell receptors (TCRs) or by indirect effects on antigen-presenting cells involving induction of lipid autoantigens, CD1 transcription, or cytokine release. To distinguish among direct and indirect mechanisms, we developed fluorescent human CD1b tetramers and measured T cell staining. CD1b tetramer staining of T cells requires glucose monomycolate (GMM) antigens, is specific for TCR structure, and is blocked by a recombinant clonotypic TCR comprised of TRAV17 and TRBV4-1, proving that CD1b–glycolipid complexes bind the TCR. GMM-loaded tetramers brightly stain a small subpopulation of blood-derived cells from humans infected with Mycobacterium tuberculosis, providing direct detection of a CD1b-reactive T cell repertoire. Polyclonal T cells from patients sorted with tetramers are activated by GMM antigens presented by CD1b. Whereas prior studies emphasized CD8+ and CD4CD8 CD1b-restricted clones, CD1b tetramer-based studies show that nearly all cells express the CD4 co-receptor. These findings prove a cognate mechanism whereby CD1b–glycolipid complexes bind to TCRs. CD1b tetramers detect a natural CD1b-restricted T cell repertoire ex vivo with unexpected features, opening a new investigative path to study the human CD1 system.
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