IL-4 Producing CD4+ TCR Alpha Beta Int Liver Lymphocytes: Influence of Thymus, Beta 2-microglobulin and NK1.1 Expression

Overview

Journal Int Immunol

Specialty Allergy & Immunology

Date 1995 Nov 1

PMID 8580071

Citations 20

Authors

M Emoto

Y Emoto

S H Kaufmann

Affiliations

Soon will be listed here.

Abstract

The present report describes developmental, phenotypic and functional features of unconventional CD4+ TCR alpha beta lymphocytes. In C57BL/6 mice, the majority of liver lymphocytes expressing intermediate intensity of TCR alpha beta (TCR alpha beta int) are CD4+ NK1.1+ and express a highly restricted TCR V beta repertoire, dominated by V beta 8 with some contribution by V beta 7 and V beta 2. Although these cells express the CD4 co-receptor, they are present in H2-1 A beta (A beta)-/- gene disruption mutants but are markedly reduced in beta 2-microglobulin (beta 2m)-/- mutant mice and hence are beta 2m dependent. Thymocytes expressing the CD4+ NK1.1+ TCR alpha beta phenotype are also beta 2m contingent, suggesting that these two T lymphocyte populations are related. The CD4+ NK1.1+ TCR alpha beta lymphocytes in liver and thymus share several markers such as LFA-1+, CD44+, CD5+, LECAM-1- and IL-2R alpha-. The CD4+ NK1.1+ TCR alpha beta int liver lymphocytes were not detected in athymic nu/nu mice. We conclude that beta 2m expression is crucial for development of the CD4+ NK1.1+ TCR alpha beta int liver lymphocytes and that thymus plays a major role. CD4+ TCR alpha beta int liver lymphocytes were also identified in NK1.1- mouse strains, there lacking the NK1.1 marker. We assume that the NK1.1 molecule is a characteristic marker of the CD4+ TCR alpha beta int liver lymphocytes in NK1.1+ mouse strains, although its expression is not obligatory for their development. The liver lymphocytes from beta 2m+/-, but not from beta 2m-/-, mice are potent IL-4 producers in response to CD3 or TCR alpha beta engagement and the IL-4 production by liver lymphocytes was markedly reduced by treatment with anti-NK1.1 mAb. We conclude that the CD4+ NK1.1+ TCR alpha beta int liver lymphocytes are capable of producing IL-4 in response to TCR stimulation.

Citing Articles

Alpha-galactosylceramide promotes killing of Listeria monocytogenes within the macrophage phagosome through invariant NKT-cell activation.

Emoto M, Yoshida T, Fukuda T, Kawamura I, Mitsuyama M, Kita E Infect Immun. 2010; 78(6):2667-76.

PMID: 20351146 PMC: 2876567. DOI: 10.1128/IAI.01441-09.

Dissociated expression of natural killer 1.1 and T-cell receptor by invariant natural killer T cells after interleukin-12 receptor and T-cell receptor signalling.

Emoto M, Shimizu T, Koike H, Yoshizawa I, Hurwitz R, Kaufmann S Immunology. 2009; 129(1):62-74.

PMID: 20028429 PMC: 2807487. DOI: 10.1111/j.1365-2567.2009.03148.x.

Role for hedgehog pathway in regulating growth and function of invariant NKT cells.

Syn W, Witek R, Curbishley S, Jung Y, Choi S, Enrich B Eur J Immunol. 2009; 39(7):1879-92.

PMID: 19544307 PMC: 2965448. DOI: 10.1002/eji.200838890.

Intracellular bacterial infection and invariant NKT cells.

Emoto M, Emoto Y Yonsei Med J. 2009; 50(1):12-21.

PMID: 19259343 PMC: 2649871. DOI: 10.3349/ymj.2009.50.1.12.

Relative importance of T-cell subsets in monocytotropic ehrlichiosis: a novel effector mechanism involved in Ehrlichia-induced immunopathology in murine ehrlichiosis.

Ismail N, Crossley E, Stevenson H, Walker D Infect Immun. 2007; 75(9):4608-20.

PMID: 17562770 PMC: 1951155. DOI: 10.1128/IAI.00198-07.