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Sonic Hedgehog Promotes Cell Cycle Progression in Activated Peripheral CD4⁺ T Lymphocytes¹

Jacqueline A. Lowrey^2,*,, Gareth A. Stewart^*,, Susannah Lindey^*,, Gerard F. Hoyne^*,, Margaret J. Dallman, Sarah E. M. Howie^*, and Jonathan R. Lamb^*,

^* Immunobiology Group, Medical Research Council Center for Inflammation Research, Respiratory Medicine Unit, and Department of Pathology, University of Edinburgh Medical School, Edinburgh, United Kingdom; and Department of Biological Sciences, Imperial College of Science, Technology and Medicine, London, United Kingdom

Sonic hedgehog (Shh) signaling is important in the growth and differentiation of many cell types and recently has been reported to play a role in T cell development in the thymus. This prompted us to investigate whether or not Shh contributes to the clonal expansion of peripheral CD4⁺ T cells. In this study, we demonstrate that Shh and other components of the signaling pathway patched, smoothened, and Gli1 (glioma-associated oncogene) are expressed in peripheral CD4⁺ T cells. The addition of the biologically active amino-terminal Shh peptide had no effect on resting CD4⁺ T cells, but significantly enhanced proliferation of anti-CD3/28 Ab-activated CD4⁺ T cells. This was not due to antiapoptotic effects, but by promoting entry of T cells into the S-G₂ proliferative phase of the cell cycle. Neutralizing anti-Shh Ab reduced T cell proliferation by inhibiting cell transition into the S-G₂ phase, suggesting that endogenously produced Shh plays a physiological role in the clonal expansion of T cells. Furthermore, we have observed a significant up-regulation of Shh and Gli1 (glioma-associated oncogene) mRNA in activated CD4⁺ T cells with or without addition of exogenous Shh, which corresponds with maximal CD4⁺ T cell proliferation, whereas bcl-2 was only up-regulated in activated cells in the presence of Shh. Our findings suggest that endogenously produced Shh may play a role in sustaining normal CD4⁺ T cell proliferation and exogenously added Shh enhances this response.

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