Homeostatically proliferating CD4 super(+) T cells are involved in the pathogenesis of an Omenn syndrome murine model

• Published in: The Journal of clinical investigation Vol. 117; no. 5; pp. 1270 - 1281
• Main Authors: Khiong, Khie, Murakami, Masaaki, Kitabayashi, Chika, Ueda, Naoko, Sawa, Shin-Ichiro, Sakamoto, Akemi, Kotzin, Brian L, Rozzo, Stephen J, Ishihara, Katsuhiko, Verella-Garcia, Marileila, Kappler, John, Marrack, Philippa, Hirano, Toshio
• Format: Journal Article
• Language: English
• Published: 01.05.2007
• ISSN: 0021-9738
• DOI: 10.1172/JCI30513

Patients with Omenn syndrome (OS) have hypomorphic RAG mutations and develop varying manifestations of severe combined immunodeficiency. It is not known which symptoms are caused directly by the RAG mutations and which depend on other polymorphic genes. Our current understanding of OS is limited by the lack of an animal model. In the present study, we identified a C57BL/10 mouse with a spontaneous mutation in, and reduced activity of, RAG1. Mice bred from this animal contained high numbers of memory-phenotype T cells and experienced hepatosplenomegaly and eosinophilia, had oligoclonal T cells, and demonstrated elevated levels of IgE, major symptoms of OS. Depletion of CD4 super(+) T cells in the mice caused a reduction in their IgE levels. Hence these "memory mutant" mice are a model for human OS; many symptoms of their disease were direct results of the Rag hypomorphism and some were caused by malfunctions of their CD4 super(+) T cells.