Abstract
Accurate phosphorylation of tyrosine residues in proteins plays a central role in regulation of cellular function. Although connections between aberrant tyrosine kinase activity and malignancy are well-established, significantly less is known about the roles of protein tyrosine phosphatases (PTPases) in tumorigenesis. We have previously shown that the transmembranal form of PTPase Epsilon (PTPε) is upregulated in mouse mammary tumors initiated specifically by ras or neu, suggesting that PTPε may play a role in transformation by these two oncogenes. In order to test this notion in vivo, we created transgenic mice that express elevated levels of PTPε in their mammary epithelium by use of the MMTV promoter/enhancer. Following several cycles of pregnancy female MMTV-PTPε mice uniformly developed pronounced and persistent mammary hyperplasia which was accompanied by residual milk production. Solitary mammary tumors were often detected secondary to mammary hyperplasia. The sporadic nature of the tumors, the long latency period prior to their development, and low levels of transgene expression in the tumors indicate that PTPε provides a necessary, but insufficient, signal for oncogenesis. The results provide genetic evidence that PTPε plays an accessory role in production of mammary tumors in a manner consistent with its upregulation in mammary tumors induced by ras or neu.
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Acknowledgements
Significant portions of this work were performed while the author was associated with the laboratory of Dr Philip Leder, Department of Genetics and Howard Hughes Medical Institute, Harvard Medical School; the author is deeply thankful to Dr Leder for his support and interest throughout this project. The author also thanks Anne Harrington and Fen Zhou, of the Department of Genetics, Harvard Medical School, for their help in preparation of MMTV-PTPε transgenic mice and in situ RNA analysis, respectively; Dr Robert Cardiff and his staff of the Transgenic Mouse Pathology Laboratory, University of California at Davis, School of Medicine, for preparation and interpretation of the histologic sections; and Drs Moshe Shani (Institute of Animal Research, Volcani Center, Bet-Dagan, Israel) and Lothar Hennighausen (National Institutes of Health) for their kind gift of the mouse β-casein cDNA probe. A Elson is an Alon Fellow and incumbent of the Adolfo and Evelyn Blum Career Development Chair in Cancer Research at The Weizmann Institute.
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Elson, A. Protein tyrosine phosphatase ε increases the risk of mammary hyperplasia and mammary tumors in transgenic mice. Oncogene 18, 7535–7542 (1999). https://doi.org/10.1038/sj.onc.1203098
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DOI: https://doi.org/10.1038/sj.onc.1203098
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