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      CANCER, WARTS, AND SUNSHINE IN RENAL TRANSPLANT PATIENTS

      , , , ,
      The Lancet
      Elsevier BV

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          Suppressor T lymphocytes control the development of primary skin cancers in ultraviolet-irradiated mice.

          Exposure of mice to ultraviolet radiation results in the development of suppressor T lymphocytes in lymphoid organs, followed by the appearance of primary skin cancers. The presence or absence of these suppressor lymphocytes determines whether or not primary cancers will develop in the ultraviolet-irradiated skin. This demonstrates the importance of immunological regulatory pathways in carcinogenesis and provides an example of immunological surveillance.
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            Collaborative United Kingdom-Australasian study of cancer in patients treated with immunosuppressive drugs.

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              Ultraviolet light depletes surface markers of Langerhans cells.

              This report defines the influence of ultraviolet light (UV) on Langerhans cells (LC). Human volunteers and hairless mice (Swiss ha/ha) were exposed to various single and/or cumulative doses of either UV-A, UV-B, or UV-A plus small amounts of UV-B (UV-A (+B)). 24 hr after the last irradiation, morphology of the entire epidermis was evaluated by both light and electron microscopy while LC, in addition, were tested for expression of specific histochemical (ATPase) and functional immunological markers (Ia antigens). In both men and mice, cumulative doses of either 80-120 J/cm2 UV-A (+B) or 1-2 X 100 J/cm2 UV-A resulted in a dramatic reduction of cells exhibiting ATPase and Ia-reactivity. In the UV-B spectrum, single doses of 60-80 mJ/cm2 produced a virtually complete elimination of LC membrane markers. By contrast, pemphigus antigens of keratinocytes were unaffected by these energy doses. Electron microscopy revealed cellular damage of some LC after UV-doses which produce a virtually complete abolition of LC membrane markers. At certain dose ranges (15-30 mJ/cm2 UV-B and 1 x 40 to 2 x 100 J/cm2 UV-A) LC were the only epidermal cells to display morphological damage at the ultrastructural level whereas higher doses affected all epidermal cells. The finding that LC surface markers and to a lesser extent the cells themselves are particularly susceptible to UV irradiation has important implications in view of previous findings that LC are potent stimulators of antigen-specific and allogeneic T cell activation. UV-induced alteration of LC plasma membrane integrity may represent a tool to manipulate adverse immune reactions involving the epidermis.
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                Author and article information

                Journal
                The Lancet
                The Lancet
                Elsevier BV
                01406736
                March 1984
                March 1984
                : 323
                : 8379
                : 702-705
                Article
                10.1016/S0140-6736(84)92221-9
                61b78382-d6af-4f87-990e-9b28a275b7a4
                © 1984

                http://www.elsevier.com/tdm/userlicense/1.0/

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