In vivo clonal expansion and phenotypes of hypocretin-specific CD4+ T cells in narcolepsy patients and controls

Author:

Jiang WeiORCID,Birtley James R.ORCID,Hung Shu-Chen,Wang WeiqiORCID,Chiou Shin-Heng,Macaubas Claudia,Kornum Birgitte,Tian Lu,Huang HuangORCID,Adler Lital,Weaver GrantORCID,Lu Liying,Ilstad-Minnihan Alexandra,Somasundaram SriramORCID,Ayyangar Sashi,Davis Mark M.ORCID,Stern Lawrence J.ORCID,Mellins Elizabeth D.ORCID

Abstract

AbstractIndividuals with narcolepsy suffer from abnormal sleep patterns due to loss of neurons that uniquely supply hypocretin (HCRT). Previous studies found associations of narcolepsy with the human leukocyte antigen (HLA)-DQ6 allele and T-cell receptor α (TRA) J24 gene segment and also suggested that in vitro-stimulated T cells can target HCRT. Here, we present evidence of in vivo expansion of DQ6-HCRT tetramer+/TRAJ24+/CD4+ T cells in DQ6+ individuals with and without narcolepsy. We identify related TRAJ24+ TCRαβ clonotypes encoded by identical α/β gene regions from two patients and two controls. TRAJ24-G allele+ clonotypes only expand in the two patients, whereas a TRAJ24-C allele+ clonotype expands in a control. A representative tetramer+/G-allele+ TCR shows signaling reactivity to the epitope HCRT87–97. Clonally expanded G-allele+ T cells exhibit an unconventional effector phenotype. Our analysis of in vivo expansion of HCRT-reactive TRAJ24+ cells opens an avenue for further investigation of the autoimmune contribution to narcolepsy development.

Funder

GlaoSmithKline Biologicals SA

The Child Health Research Institute, Lucile Packard Foundation for Children’s Health, as well as the Stanford CTSA

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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