Regulation of Cutaneous Malignancy by γδ T Cells

Michael Girardi; David Oppenheim; Carrie R. Steele; Julia M. Lewis; Earl J. Glusac; Renata B. Filler; Paul Hobby; Brian J. Sutton; Robert E. Tigelaar; Adrian Hayday

doi:10.1126/science.1063916

Regulation of Cutaneous Malignancy by γδ T Cells

Michael Girardi(Skin Research Center), David Oppenheim(The King's College), Carrie R. Steele(The King's College), Julia M. Lewis(Skin Research Center), Earl J. Glusac(Skin Research Center), Renata B. Filler(Skin Research Center), Paul Hobby(Guy's Hospital), Brian J. Sutton(Guy's Hospital), Robert E. Tigelaar(Skin Research Center), Adrian Hayday(The King's College)

Science

October 19, 2001

10.1126/science.1063916

Cited by 972Open Access

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Abstract

The localization of gammadelta T cells within epithelia suggests that these cells may contribute to the down-regulation of epithelial malignancies. We report that mice lacking gammadelta cells are highly susceptible to multiple regimens of cutaneous carcinogenesis. After exposure to carcinogens, skin cells expressed Rae-1 and H60, major histocompatibility complex-related molecules structurally resembling human MICA. Each of these is a ligand for NKG2d, a receptor expressed by cytolytic T cells and natural killer (NK) cells. In vitro, skin-associated NKG2d+ gammadelta cells killed skin carcinoma cells by a mechanism that was sensitive to blocking NKG2d engagement. Thus, local T cells may use evolutionarily conserved proteins to negatively regulate malignancy.

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