Dendritic Cell Maturation Overrules H-2d–Mediated Natural Killer T (Nkt) Cell Inhibition

Author:

Ikarashi Yoshinori1,Mikami Rumiko1,Bendelac Albert2,Terme Magali1,Chaput Nathalie1,Terada Masahiro3,Tursz Thomas1,Angevin Eric1,Lemonnier François A.4,Wakasugi Hiro3,Zitvogel Laurence1

Affiliation:

1. Unité d'Immunologie, Département de Biologie Clinique, Institut Gustave Roussy, 94805 Villejuif Cedex, France

2. Princeton University, Princeton, NJ 08544

3. Pharmacology Division, National Cancer Center, Tokyo 104-0045, Japan

4. Unité d'Immunologie Cellulaire Antivirale, Institut Pasteur, Paris 75015, France

Abstract

Given the broad expression of H-2 class Ib molecules on hematopoietic cells, antigen presentation pathways among CD1d expressing cells might tightly regulate CD1d-restricted natural killer T (NKT) cells. Bone marrow–derived dendritic cells (BM-DCs) and not adherent splenocytes become capable of triggering NK1.1+/T cell receptor (TCR)int hepatic NKT cell activation when (a) immature BM-DCs lack H-2Db−/− molecules or (b) BM-DCs undergo a stress signal of activation. In such conditions, BM-DCs promote T helper type 1 predominant CD1d-restricted NKT cell stimulation. H-2 class Ia–mediated inhibition involves more the direct H-2Db presentation than the indirect Qa-1b pathway. Such inhibition can be overruled by B7/CD28 interactions and marginally by CD40/CD40L or interleukin 12. These data point to a unique regulatory role of DCs in NKT cell innate immune responses and suggest that H-2 class Ia and Ib pathways differentially control NKT cell recognition of DC antigens.

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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