Dcir Deficiency Causes Development of Autoimmune Diseases in Mice Due to Excess Expansion of Dendritic Cells

Overview

Journal Nat Med

Specialties General Medicine
Molecular Biology

Date 2008 Jan 22

PMID 18204462

Citations 89

Authors

Noriyuki Fujikado

Shinobu Saijo

Tomo Yonezawa

Kazusuke Shimamori

Akina Ishii

Sho Sugai

Hayato Kotaki

Katsuko Sudo

Masato Nose

Yoichiro Iwakura

Affiliations

Soon will be listed here.

Abstract

The dendritic cell immunoreceptor (official gene symbol Clec4a2, called Dcir here) is a C-type lectin receptor expressed mainly in dendritic cells (DCs) that has a carbohydrate recognition domain in its extracellular portion and an immunoreceptor tyrosine-based inhibitory motif, which transduces negative signals into cells, in its cytoplasmic portion. We found high Dcir expression in the joints of two mouse rheumatoid arthritis models. Because the structural characteristics of Dcir suggest that it may have an immune regulatory role, and because autoimmune-related genes are mapped to the DCIR locus in humans, we generated Dcir-/- mice to learn more about the pathological roles of this molecule. We found that aged Dcir-/- mice spontaneously develop sialadenitis and enthesitis associated with elevated serum autoantibodies. Dcir-/- mice showed a markedly exacerbated response to collagen-induced arthritis. The DC population was expanded excessively in aged and type II collagen-immunized Dcir-/- mice. Upon treatment with granulocyte-macrophage colony-stimulating factor, Dcir-/- mouse-derived bone marrow cells (BMCs) differentiated into DCs more efficiently than did wild-type BMCs, owing to enhanced signal transducer and activator of transcription-5 phosphorylation. These observations indicate that Dcir is a negative regulator of DC expansion and has a crucial role in maintaining the homeostasis of the immune system.

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