Neonatal and Adult Recent Thymic Emigrants Produce IL-8 and Express Complement Receptors CR1 and CR2

Overview

Journal JCI Insight

Specialties Biomedical Engineering
General Medicine

Date 2017 Aug 18

PMID 28814669

Citations 31

Authors

Marcin L Pekalski

Arcadio Rubio Garcia

Ricardo C Ferreira

Daniel B Rainbow

Deborah J Smyth

Meghavi Mashar

Jane Brady

Natalia Savinykh

Xaquin Castro Dopico

Sumiyya Mahmood

Simon Duley

Helen E Stevens

Neil M Walker

Antony J Cutler

Frank Waldron-Lynch

David B Dunger

Claire Shannon-Lowe

Alasdair J Coles

Joanne L Jones

Chris Wallace

John A Todd

Linda S Wicker

Affiliations

Soon will be listed here.

Abstract

The maintenance of peripheral naive T lymphocytes in humans is dependent on their homeostatic division, not continuing emigration from the thymus, which undergoes involution with age. However, postthymic maintenance of naive T cells is still poorly understood. Previously we reported that recent thymic emigrants (RTEs) are contained in CD31+CD25- naive T cells as defined by their levels of signal joint T cell receptor rearrangement excision circles (sjTRECs). Here, by differential gene expression analysis followed by protein expression and functional studies, we define that the naive T cells having divided the least since thymic emigration express complement receptors (CR1 and CR2) known to bind complement C3b- and C3d-decorated microbial products and, following activation, produce IL-8 (CXCL8), a major chemoattractant for neutrophils in bacterial defense. We also observed an IL-8-producing memory T cell subpopulation coexpressing CR1 and CR2 and with a gene expression signature resembling that of RTEs. The functions of CR1 and CR2 on T cells remain to be determined, but we note that CR2 is the receptor for Epstein-Barr virus, which is a cause of T cell lymphomas and a candidate environmental factor in autoimmune disease.

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