Novel lymphocyte-independent mechanisms to initiate inflammatory arthritis via bone marrow-derived cells of Ali18 mutant mice

doi:10.1093/rheumatology/kem358

Rheumatology 2008 47(3):292-300; doi:10.1093/rheumatology/kem358

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Novel lymphocyte-independent mechanisms to initiate inflammatory arthritis via bone marrow-derived cells of Ali18 mutant mice

K. Abe¹^,2, S. Wechs¹, S. Kalaydjiev³^,6, T. J. Franz³, D. H. Busch³, H. Fuchs¹, D. Soewarto¹, H. Behrendt⁴, S. Wagner¹, T. Jakob⁴^,5 and M. Hrabé de Angelis¹

¹Institute of Experimental Genetics, Helmholtz Zentrum München, German Research Center for Environmental Health, Neuherberg, Germany, ²Department of Basic Medical Science and Molecular Medicine, Tokai University Medical School, Kanagawa, Japan, ³Institute for Medical Microbiology, Immunology and Hygiene, ⁴Division of Environmental Dermatology and Allergy GSF/TUM, Technical University Munich, Munich, ⁵Allergy Research Group, Department of Dermatology, University Medical Center Freiburg, Freiburg, Germany and ⁶Faculty of Life Sciences, Michael Smith Building, University of Manchester, Manchester, UK.

Correspondence to: K. Abe, Department of Basic Medical Science and Molecular Medicine, Tokai University Medical School, Shimokasuya 143, Isehara, Kanagawa 259–1193, Japan. E-mail: abeko{at}is.icc.u-tokai.ac.jp

Abstract

Objective. In a large-scale ENU (N-ethyl-N-nitrosourea) mousemutagenesis programme, we previously have identified and characterizeda novel mutation Ali18 that causes inflammatory arthritis likelesions in peripheral joints. In this study, we analysed theimmune system of Ali18 mice to understand mechanisms underlyingthe spontaneous inflammation.

Methods. Humoral and cellular components of the immune systemwere phenotyped by ELISA and flow cytometry. The contributionof the immune system for phenotype expression was analysed indisease transfer experiments. The involvement of the adaptiveimmune system was investigated in Ali18;Rag1 double mutantsand the influence of environmental factors was analysed in Ali18mice reared under germ-free conditions.

Results. Bone marrow cells from Ali18 mice were able to transferthe disease phenotype to naïve wild-type recipients suggestingthat cellular components of the reconstituted immune systemwere sufficient to induce arthritis. Ali18 mice revealed abnormalleucocyte populations including lymphocytes and granulocytes,as well as increased plasma IL-5 and IgE levels. Ali18;Rag1double homozygous mutants, which lack mature lymphocytes, stilldeveloped arthritis, suggesting that the phenotype is independentof the adaptive immune system. In addition, the arthritis phenotypeappeared to be independent from environmental conditions asdemonstrated in mice reared under germ-free conditions.

Conclusions. The Ali18 mutation induces inflammatory arthritisthrough bone marrow-derived cells. However, non-pro-inflammatorycytokine cascades and mature lymphocyte independent-mechanismsare crucial for initiation and progression of the phenotype.Ali18 mice may thus represent a model to study mechanisms involvedin seronegative arthritis induced by cells of the innate immunesystem.

KEY WORDS: Psoriatic arthritis, Animal model, Inflammatory arthritis, ENU, Mouse mutant

Submitted 19 June 2007; revised version accepted 6 December 2007.
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