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Malignant melanoma accounts for most of the increasing mortality from skin cancer. Melanoma cells were found to express Fas (also called Apo-1 or CD95) ligand (FasL). In metastatic lesions, Fas-expressing T cell infiltrates were proximal to FasL+ tumor cells. In vitro, apoptosis of Fas-sensitive target cells occurred upon incubation with melanoma tumor cells; and in vivo, injection of FasL+ mouse melanoma cells in mice led to rapid tumor formation. In contrast, tumorigenesis was delayed in Fas-deficient lpr mutant mice in which immune effector cells cannot be killed by FasL. Thus, FasL may contribute to the immune privilege of tumors.
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Hahne et al. (Fri,) studied this question.
synapsesocial.com/papers/6a11cbd4ed9c06332dfd39ce — DOI: https://doi.org/10.1126/science.274.5291.1363
Michael Hahne
Centre National de la Recherche Scientifique
Donata Rimoldi
University of Geneva
Michael Schröter
University Hospital Cologne
Science
University of Geneva
University of Lausanne
University Hospital of Zurich
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