Arachidonate 15-Lipoxygenase 2 as an Endogenous Inhibitor of Prostate Cancer Development

Abstract

Our recent work has demonstrated that: 1) 15-lipoxygenase 2 (15-LOX2), which metabolizes AA to generate 15(S)-HETE, is the major LOX expressed in adult prostate epithelial cells but down-regulated or lost in PCa in vitro as well as in vivo; 2) 15-LOX2 expression is inversely correlated with the pathological grade and Gleason scores of PCapatients; 3) 15-LOX2 is a negative cell-cycle regulator in normal human prostate (NHP) epithelial cells; 4) 15(S)-HETE inhibits PCa cell migration and invasion and re-expression of 15-LOX2, or its splice variant 15-LOX2sv-b,inhibits PCa cell proliferation in vitro and tumor development in vivo; 5) 15-LOX2 expression in NHP cells is positively regulated by the transcription factor Sp1 and negatively regulated by Sp3; 6) The expression of 15- LOX2 and its multiple splice variants in NHP cells is cell-autonomously induced and is correlated with and causally involved in the senescence of NHP cells; 7) Transgenic expression of 15-LOX2, or its splice variant, 15-LOX2sv-b, in mouse prostate induces unique gene expression profile and causes degenerative prostate overgrowth; and 8) Finally, 15-LOX2 transgene expression inhibits TRAMP tumor development in the compound mice. These observations togetogether support initial hypothesis that 15-LOX2 represents a functional prostate tumor suppressor, whose loss of expression contributes to PCa development. We initially proposed two Specific Aims: 1) to test the hypothesis that15-LOX2 inhibits PCa development in an orthotopic implantation model using an inducible 15-LOX2 exprexpression systemd 2) to test the hypothesis that 15-LOX2 inhibits PCa development in newly developed prosprostate specific transgenicmal models. We have now accomplished both Specific Aims (see detailed Progress Report).

Document Details

Document Type

Technical Report

Publication Date

Mar 01, 2006

Accession Number

ADA572304

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