Effects of Immunotherapy on the Distribution and Clonality of TCR Vγ and Vδ Subfamily T Cells in Allergic Rhinitis Patients

Qintai Yang,Yangqiu Li,Gehua Zhang,Xuekun Huang,Xiuli Wu,Peng Li,Yulian Chen

doi:10.2478/v10011-011-0046-y

Abstract

Effects of Immunotherapy on the Distribution and Clonality of TCR Vγ and Vδ Subfamily T Cells in Allergic Rhinitis PatientsThe aim of this study was to investigate the changes in the peripheral specific IgE level, distribution of TCR Vg and Vd subfamily T cells and mRNA expressions of TCR Vg I-III following specific immunotherapy (SIT) with house-dust-mite extract in allergic rhinitis (AR) patients. Ten AR patients undergoing SIT with house-dust-mite extract for 1 year were recruited. Quantitative analysis of immunofluorescence was performed to detect the serum specific IgE (sIgE) level before and after SIT; RT-PCR-genescan analysis was employed to detect the mRNA expressions of TCR Vg (I-III) and Vd (1-8) in the peripheral mononuclear cells followed by analysis of T cell clonality. Real-time quantitative PCR was applied to detect the expressions of TCR Vg I-III genes. Ten healthy volunteers served as controls. For AR patients, SIT treatment could improve the symptoms, but the serum sIgE level was not markedly decreased. Before SIT, the expressions of TCR Vg I-III gene were similar between AR patients and controls (P>0.05) but markedly decreased after SIT in AR patients (P<0.05 in TCR VgI and VgII). The expressions of TCR Vd (1-8) before and after SIT were 5.3±0.82 and 4.9±0.57, respectively, and that in healthy controls was 5.2±1.40. Vd1, 2, 3 and 6 were the most common genes found in these patients. Significant difference in the TCR Vd6 subfamily T cells was found between the two groups. Polyclonal or biclonal proliferation was found in the T cells of patients before SIT and in healthy controls, but oligoclonal proliferation in only 1 subject before SIT. After SIT, the proportion of patients with oligoclonal proliferation of T cells (6/10) was markedly increased (P<0.05). SIT for 1 year could alter the expressions of TCR Vg I-III genes, the distribution of TCR Vg and Vd T cells and the ways in which T cells proliferate. The early improvement of symptoms following immunotherapy might not be related to the serum sIgE content in AR patients, but associated with the TCR gd T cells, especially the TCR V d6 T cells.

Highlights

Based on the types of T cell receptors (TCR), T cells can be classified into TCR ab T cells and TCR gd T cells
The knowledge on TCR gd T cells is still insufficient as compared to TCR ab T cells, and few studies report the role of TCR gd T cells in allergic rhinitis (AR) and specific immunotherapy (SIT)
The present study aimed to investigate the changes in the peripheral specific IgE level, distribution of TCR Vg and Vd T cells and expressions of TCRVg I–III following SIT for 1 year

Summary

Introduction

Based on the types of T cell receptors (TCR), T cells can be classified into TCR ab T cells and TCR gd T cells. The TCR gd T cells are the predominant type and can recognize antigens. TCR gd T cells account for only 1–10% of T cells in the peripheral blood but for as high as 20–50% in the intestinal and respiratory mucosa and they can directly recognize antigens [1]. Studies reveal TCR gd T cells can be classified into Th1 cells and Th2 cells. The knowledge on TCR gd T cells is still insufficient as compared to TCR ab T cells, and few studies report the role of TCR gd T cells in allergic rhinitis (AR) and SIT. The present study aimed to investigate the changes in the peripheral specific IgE level, distribution of TCR Vg and Vd T cells and expressions of TCRVg I–III following SIT for 1 year

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