Differential Homing Commitments of Antigen-specific T Cells After Oral or Parenteral Immunization in Humans

Overview

Journal J Immunol

Specialty Allergy & Immunology

Date 1999 May 5

PMID 10227989

Citations 50

Authors

A Kantele

J Zivny

M Hakkinen

C O Elson

J Mestecky

Affiliations

Soon will be listed here.

Abstract

Animal experiments show that lymphocytes activated in the intestine circulate through mesenteric lymph nodes, lymphatics, and blood, returning to the gut. Homing into intestinal lamina propria is mediated by lymphocyte surface homing receptors, mainly the alpha4beta7-integrin. We studied in humans whether intestinal T cells entering the blood upon antigenic activation would exhibit homing commitments to the gut. Volunteers were immunized with keyhole limpet hemocyanin (KLH) first orally and then parenterally or only parenterally, and the expression of alpha4beta7 on T cells specific for KLH or tetanus toxoid was studied. Circulating T cells were depleted of alpha4beta7+ cells by immunomagnetic selection. This depletion removed a significant proportion of the KLH-specific cells (mean decrease in proliferative response of 71%) in the orally immunized volunteers. No difference in the KLH-induced proliferation was found between the total and the alpha4beta7-depleted populations in volunteers parenterally immunized with KLH, regardless of whether a preceding mucosal priming had taken place or not. In both immunization groups, the depletion of alpha4beta7+ cells had no influence on the proliferative response to tetanus toxoid. We conclude that, in contrast to T cells activated by parenteral immunization, gut-derived T cells have preferential homing commitments to the gut. This commitment was no longer observed after a subsequent parenteral Ag administration. Besides showing that the site of Ag encounter determines the expression of homing receptors, the present study is the first to provide evidence for a circulation of newly activated Ag-specific intestinal T cells back to the gut in humans.

Citing Articles

IRF4 is required for migration of CD4 T cells to the intestine but not for Th2 and Th17 cell maintenance.

Schmidt C, Harberts A, Reimers D, Bertram T, Voss L, Schmid J Front Immunol. 2023; 14:1182502.

PMID: 37469513 PMC: 10352983. DOI: 10.3389/fimmu.2023.1182502.

SARS-CoV-2-specific T cells in unexposed adults display broad trafficking potential and cross-react with commensal antigens.

Bartolo L, Afroz S, Pan Y, Xu R, Williams L, Lin C Sci Immunol. 2022; 7(76):eabn3127.

PMID: 35857619 PMC: 9348748. DOI: 10.1126/sciimmunol.abn3127.

SARS-CoV-2-specific T cells in unexposed adults display broad trafficking potential and cross-react with commensal antigens.

Bartolo L, Afroz S, Pan Y, Xu R, Williams L, Lin C bioRxiv. 2021; .

PMID: 34873598 PMC: 8647649. DOI: 10.1101/2021.11.29.470421.

Site-Specific DC Surface Signatures Influence CD4 T Cell Co-stimulation and Lung-Homing.

Pejoski D, Ballester M, Auderset F, Vono M, Christensen D, Andersen P Front Immunol. 2019; 10:1650.

PMID: 31396211 PMC: 6668556. DOI: 10.3389/fimmu.2019.01650.

The Dynamics of the Skin's Immune System.

Nguyen A, Soulika A Int J Mol Sci. 2019; 20(8).

PMID: 31013709 PMC: 6515324. DOI: 10.3390/ijms20081811.