CP-31398 restores mutant p53 tumor suppressor function and inhibits UVB-induced skin carcinogenesis in mice
Xiuwei Tang, … , David R. Bickers, Mohammad Athar
Xiuwei Tang, … , David R. Bickers, Mohammad Athar
Published December 3, 2007
Citation Information: J Clin Invest. 2007;117(12):3753-3764. https://doi.org/10.1172/JCI32481.
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Research Article

CP-31398 restores mutant p53 tumor suppressor function and inhibits UVB-induced skin carcinogenesis in mice

Abstract

Mutations in the tumor suppressor p53 are detectable in over 50% of all human malignancies. Mutant p53 protein is incapable of transactivating its downstream target genes that are required for DNA repair and apoptosis. Chronic exposure to UVB induces p53 mutations and is carcinogenic in both murine and human skin. CP-31398, a styrylquinazoline compound, restores the tumor suppressor functions of mutant forms of p53 in tumor cells. However, its effectiveness in vivo remains unclear. Here, we demonstrate that CP-31398 blocked UVB-induced skin carcinogenesis and was associated with increases in p53, p21, and BclXs. CP-31398 downregulated Bcl2, proliferating nuclear cell antigen, and cyclin D1. Activation of caspase-3 and cleavage of poly (ADP-ribose) polymerase also occurred in both tumor and perilesional skin following treatment. CP-31398 induced the expression of p53-dependent target proteins, and this was followed by apoptosis in UVB-irradiated wild-type mice but not in their p53-deficient littermates. Similar effects were observed in human skin carcinoma A431 cells expressing mutant p53. In addition, CP-31398 induced mitochondrial translocation of p53, leading to changes in mitochondrial membrane permeability pore transition (MPT) and consequent cytochrome c release in these cells. Blocking MPT diminished p53 translocation and apoptosis. These studies indicate that reconstituting p53 tumor suppressor functions in vivo by small molecular weight compounds may block the pathogenesis and progression of skin cancer.

Authors

Xiuwei Tang, Yucui Zhu, Lydia Han, Arianna L. Kim, Levy Kopelovich, David R. Bickers, Mohammad Athar

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Figure 2

Effects of CP-31398 treatment on the growth of UVB-induced skin tumors in SKH-1 mice.

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Effects of CP-31398 treatment on the growth of UVB-induced skin tumors i...
(A) Drawing showing experimental protocol design. CP-31398 administered i.p. reduces growth of UVB-induced skin tumors in SKH-1 mice in terms of tumor number (lower left panel) and tumor volume (lower right panel). (B) Effect of CP-31398 on the expression of p53 and its downstream target genes PUMA-α and mdm-2 in perilesional skin and tumors. (C) Effect of CP-31398 on the expression of cyclins A, B1, D1, and E in perilesional skin and tumors. (D) PARP cleavage and expression of antiapoptotic Bcl2 in perilesional skin and tumors following CP-31398 treatment. (E) Immunohistochemical analyses showing expression of Bcl2 and Bax in UVB-irradiated skin and UVB-induced SCC following CP-31398 treatment. Arrows indicate Bax- or BCL2-expressing cells. Treatment protocol and other experimental details are provided in Methods. P values represent significance when compared with vehicle-treated control at corresponding time point.