MHC class II-independent and -dependent T cell expansion and B cell hyperactivity in vivo in mice deficient in CD152 (CTLA-4)

doi:10.1093/intimm/dxh091

International Immunology Advance Access originally published online on May 10, 2004
International Immunology 2004 16(7):895-904; doi:10.1093/intimm/dxh091

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International Immunology, Vol. 16, No. 7, pp. 895-904, July 2004
© 2004 Japanese Society for Immunology

MHC class II-independent and -dependent T cell expansion and B cell hyperactivity in vivo in mice deficient in CD152 (CTLA-4)

William Stohl, Dong Xu, Kyoung Soo Kim, Chella S. David¹ and James P. Allison²

Division of Rheumatology, Department of Medicine, University of Southern California Keck School of Medicine, Los Angeles, CA 90033, ¹ Department of Immunology, Mayo Clinic, Rochester, MN 55905 and ² Cancer Research Laboratory, Howard Hughes Medical Institute, University of California, Berkeley, CA 94720, USA

Correspondence to: W. Stohl; E-mail: stohl{at}usc.edu
Transmitting editor: T. Tedder

One of the key downregulators of T cell activation is CD152(CTLA-4). Mice genetically deficient in CD152 (cd152^–/–mice) develop massive expansion of both CD4⁺ and CD8⁺ T cellsas well as increased numbers of splenic Ig-secreting cells andserum Ig levels. To determine the dependence of the lymphoproliferationand B cell hyperactivity on MHC class II (MHCII), MHCII-deficient(mhcii^–/–) cd152^–/– mice were generated.Compared to that in their mhcii^+/+ counterparts, expansion ofCD4⁺ cells in mhcii^–/–cd152^–/– micewas markedly attenuated. Nonetheless, expansion of CD8⁺ cellswas identical in both sets of mice, demonstrating that the effectsof CD152 deficiency on CD4⁺ cells can quantitatively be dissociatedfrom those on CD8⁺ cells, and pointing to a critical downregulatoryrole for CD152 in MHCII-independent CD8⁺ cell activation invivo. B cell hyperactivity also developed in mhcii^–/–cd152^–/–mice, albeit in a manner less rapid and less intense than thatin their mhcii^+/+ counterparts, demonstrating an underlyingMHCII-independent diathesis to B cell dysregulation and pointingto a critical downregulatory role for CD152 in MHCII-independentB cell activation in vivo. When human DQ8 was introduced asa transgene into mhcii^–/–cd152^–/– mice,B cell hyperactivity was restored to levels observed in mhcii^+/+cd152^–/–mice, pointing to a critical downregulatory role for CD152 inMHCII-dependent B cell activation in vivo superimposed uponits downregulatory role on MHCII-independent B cell activation.

Keywords: CD4⁺ cells; CD8⁺ cells; IgG; IgM; Ig-secreting cells

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