Molecular tracking of antigen-specific T cell clones in neurological immune-mediated disorders

doi:10.1093/brain/awg021

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Brain, Vol. 126, No. 1, 20-31, January 2002
© 2002 Guarantors of Brain
doi: 10.1093/brain/awg021

Molecular tracking of antigen-specific T cell clones in neurological immune-mediated disorders

Paolo A. Muraro^*^,1, Klaus-Peter Wandinger^*^,1, Bibiana Bielekova¹, Bruno Gran¹, Adriana Marques³, Ursula Utz², Henry F. McFarland¹, Steve Jacobson¹ and Roland Martin¹

¹ Neuroimmunology Branch, ² Neuroscience Center, National Institute of Neurological Disorders and Stroke, ³ Laboratory of Clinical Investigation, National Institute of Allergy Infectious Diseases, National Institutes of Health, MD, USA

Correspondence to: Dr Paolo A. Muraro, Neuroimmunology Branch, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Building 10, Room 5B-16, 10 Center Drive MSC 1400, Bethesda, MD 20892-1400, USA E-mail: murarop{at}ninds.nih.gov *These authors contributed equally to this paper

T cells recognizing self or microbial antigens may trigger orreactivate immune-mediated diseases. Monitoring the frequencyof specific T cell clonotypes to assess a possible link withthe course of disease has been a difficult task with currentlyavailable technology. Our goal was to track individual candidatepathogenic T cell clones, selected on the basis of previousextensive studies from patients with immune-mediated disordersof the CNS, including multiple sclerosis, HTLV-I associatedmyelopathy/tropical spastic paraparesis (HAM/TSP) and chronicLyme neuroborreliosis. We developed and applied a highly specificand sensitive technique to track single CD4⁺ and CD8⁺ T cellclones through the detection and quantification of T cell receptor(TCR) ${alpha}$ or ß chain complementarity-determining region3 transcripts by real-time reverse transcriptase (RT)–PCR.We examined the frequency of the candidate pathogenic T cellclones in the peripheral blood and CSF during the course ofneurological disease. Using this approach, we detected variationsof clonal frequencies that appeared to be related to clinicalcourse, significant enrichment in the CSF, or both. By integratingclonotype tracking with direct visualization of antigen-specificstaining, we showed that a single T cell clone contributed substantiallyto the overall recognition of the viral peptide/MHC complexin a patient with HAM/TSP. T cell clonotype tracking is a powerfulnew technology enabling further elucidation of the dynamicsof expansion of autoreactive or pathogen-specific T cells thatmediate pathological or protective immune responses in neurologicaldisorders.

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