Title of article :
Expression of Costimulatory Molecules CD80 and/or CD86 by a Kaposiʹs Sarcoma Tumor Cell Line Induces Differential T-Cell Activation and Proliferation
Author/Authors :
Foreman، نويسنده , , Kimberly E. and Wrone-Smith، نويسنده , , Tamara and Krueger، نويسنده , , Ann E. and Nickoloff، نويسنده , , Brian J.، نويسنده ,
Issue Information :
روزنامه با شماره پیاپی سال 1999
Pages :
9
From page :
345
To page :
353
Abstract :
During physiological stimulation of resting T-cells, at least two activation signals by antigen presenting cells are required. Besides the first antigen-specific signal, the second costimulatory signal involves CD80 and CD86 expressed by the antigen presenting cell. These costimulatory molecules have been suggested to be of clinical relevance in many different autoimmune and malignant disease processes. We previously observed that tumor cells in Kaposiʹs sarcoma (a common AIDS-related cutaneous neoplasm) completely lack both CD80 and CD86, and these tumor cells fail to stimulate T-cell proliferation. In this study, using a Kaposiʹs sarcoma tumor cell line designated SLK, various stable transfected cell lines were produced. Tumor cells that were either singly positive for either CD80 or CD86, as well as a double-positive cell line, were examined for their ability to induce T-cell activation, T-cell proliferation, and cytokine production profiles. Compared to the parental double-negative tumor cell line, the CD80-positive cells, but not the CD86-positive tumor cells, induced significant T-cell activation and proliferation. Tumor cells expressing both CD80 and CD86 also induced T-cell activation. After stimulation by the transfected tumor cells, T-cells produced a Th-1 type cytokine production profile with increased IL-2 and IFN-γ levels. These results demonstrate that Kaposiʹs sarcoma tumor cells lacking costimulatory molecules cannot induce T-cell activation; however, if they express CD80, they can induce peripheral blood T-cell proliferation, and there is a differential response as expression of CD86 did not have the same immunostimulatory effect.
Keywords :
costimulatory molecules , T-lymphocytes , Kaposiיs Sarcoma
Journal title :
Clinical Immunology
Serial Year :
1999
Journal title :
Clinical Immunology
Record number :
1848084
Link To Document :
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