The Effects of Malignant Transformation on Susceptibility of Human Urothelial Cells to CD40-Mediated Apoptosis

doi:10.1093/jnci/94.18.1381

JNCI Journal of the National Cancer Institute 2002 94(18):1381-1395; doi:10.1093/jnci/94.18.1381
© 2002 by Oxford University Press

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Journal of the National Cancer Institute, Vol. 94, No. 18, 1381-1395, September 18, 2002
© 2002 Oxford University Press

ARTICLE

The Effects of Malignant Transformation on Susceptibility of Human Urothelial Cells to CD40-Mediated Apoptosis

Urszula Bugajska, Nikolaos T. Georgopoulos, Jennifer Southgate, Peter W. M. Johnson, Pierre Graber, John Gordon, Peter J. Selby, Ludwik K. Trejdosiewicz

Affiliations of authors: U. Bugajska, N. T. Georgopoulos, P. W. M. Johnson, P. J. Selby, L. K. Trejdosiewicz, Cancer Research U.K. Clinical Centre, St. James's University Hospital, Leeds, U.K.; J. Southgate, Jack Birch Unit of Molecular Carcinogenesis, Department of Biology, University of York, York, U.K., P. Graber, Ares-Serono Pharmaceutical Research Institute, Geneva, Switzerland; J. Gordon, Medical Research Council Centre for Immune Recognition, University of Birmingham Medical School, Birmingham, U.K.

Correspondence to: Ludwik Trejdosiewicz, Ph.D., Lymphoepithelial Interactions Laboratory, Cancer Research U.K. Clinical Centre, St. James's University Hospital, Leeds LS9 7TF, U.K. (e-mail: l.k.trejdosiewicz{at}leeds.ac.uk).

Background: The tumor necrosis factor (TNF) superfamily of ligandsand receptors mediates immune cell survival. Some members possessa death domain, a protein motif that functions to transmit apoptoticsignals, whereas others, such as CD40, do not. CD40 is expressedby both normal and malignant epithelial cells. To investigatethe functional significance of this expression, we studied theeffects of ligation of CD40, Fas, and TNF receptors (TNFRs)on the proliferation and survival of normal and malignant humanurothelial cells and urothelial cells with disabled p53 function.Methods: Normal and malignant human urothelial cells were culturedwith soluble TNF family agonists (CD40 ligand [CD40L], TNF- ${alpha}$ ,anti-Fas antibody, or cocultured with mouse fibroblasts stablytransfected with plasmids that caused the cells to constitutivelyexpress CD40L or CD32; cell proliferation was estimated by an[³H]thymidine incorporation assay, and apoptosis was determinedby Annexin V staining and by a DNA fragmentation assay. MessengerRNA levels for CD40 and potential downstream effector moleculeswere quantified by polymerase chain reaction-based and ribonucleaseprotection assays, respectively, and nuclear factor (NF) ${kappa}$ B nucleartranslocation was detected by immunofluorescence. All statisticaltests were two-sided. Results: Soluble trimeric CD40L inhibitedthe growth of normal and malignant urothelial cells but didnot induce apoptosis. Cell surface-presented CD40L induced massiveapoptosis in CD40-positive transitional cell carcinoma cellsbut not in normal urothelial cells. Normal cells underwent CD40L-mediatedapoptosis only in the presence of other TNFR agonists. An agonisticanti-CD40 antibody presented on the surface of CD32-transfectedfibroblasts also induced apoptosis in transitional cell carcinomacells and in normal urothelial cells. Apoptotic responses oftumor (but not normal) cells to soluble agonists were enhancedby blocking protein synthesis. Karyotypically normal urothelialcells with disabled p53 function underwent apoptosis duringcoculture with CD40L-expressing fibroblasts alone but were notadditionally sensitive to additional TNFR agonists. Conclusions:Susceptibility to CD40 ligation-induced apoptosis may be a novelmechanism for eliminating neoplastically transformed urothelialcells. Loss of CD40 expression may be an important adaptivemechanism for transitional cell carcinoma development and progression.

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