Journal article

Early establishment of diverse T cell receptor profiles for influenza-specific CD8 CD62Lhi memory T cells

K Kedzierska, V Venturi, K Field, MP Davenport, SJ Turner, PC Doherty

Proceedings of the National Academy of Sciences of the United States of America | Published : 2006

DOI: 10.1073/pnas.0603289103

Abstract

Single-cell analysis of endogenous, primary CD8+ T cell responses to the influenza DbNP366 and D bPA224 epitopes indicates that prominent clonotypes bearing "public" or "shared" T cell receptors (TCRs) subset early into CD62Lhi and CD62Llo populations. The CD62L lo effectors divide more and are rapidly eliminated during the contraction phase, whereas stable CD62Lhi memory populations persist in the long-term. Reflecting the high frequency of small CD62Lhi clones expressing "private" TCRs, the TCR diversity range per mouse is generally two times higher within the CD62LhiCD8+D bNP366+ set (1.6 times higher for CD62L hiCD8+DbPA224+) from 8 to >180 days after antigen challenge. Memory CD8+CD62Lh..

View full abstract

University of Melbourne Researchers

Grants

Awarded by National Institute of Allergy and Infectious Diseases

Citation metrics

87Scopus
78Web of Science
83Dimensions

Keywords

Generation
32 Biomedical and Clinical Sciences
Selective Expression
Pneumonia & Influenza
Emerging Infectious Diseases
Subsets
Differentiation
Persistence
3204 Immunology
Infectious Diseases
Inflammatory and Immune System
Science & Technology
Immunity
Infection
Science & Technology - Other Topics
Responses
Influenza
T Cell Receptor Repertoire
Effector
Biodefense
In-Vivo
3207 Medical Microbiology
Multidisciplinary Sciences