Differential Effects of Estrogen and Raloxifene on Messendger RNA and Matrix Metalloproteinase 2 Activity in Rat Uterus

doi:10.1095/biolreprod.104.034595

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BOR - Papers in Press, published online ahead of print December 1, 2004.
Biol Reprod 2004, 10.1095/biolreprod.104.034595

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Submitted September 13, 2004
Returned for revision October 11, 2004
Accepted November 10, 2004

Female Reproductive Tract

Differential Effects of Estrogen and Raloxifene on Messendger RNA and Matrix Metalloproteinase 2 Activity in Rat Uterus

L. M. Helvering ^*, M. D. Adrian , A. G. Geiser , S. T. Estrem , T. Wei , S. Huang , P. Chen , E. R. Dow , J. N. Calley , J. A. Dodge , T. A. Grese , S. A. Jones , D. L. Halladay , R. R. Miles , J. E. Onyia , Y. L. Ma , M. Sato , and H. U. Bryant

^* To whom correspondence should be addressed. E-mail: l.helvering{at}lilly.com.

Abstract
A detailed analysis of the differential effects of estrogen(E) compared to raloxifene (Ral), a selective estrogen receptormodulator (SERM), following estrogen receptor binding in gynecologicaltissues was conducted using gene microarrays, northern analysisand MMP2 activity studies. We profiled gene expression in theuterus following acute (1 day) and prolonged daily treatment(5 weeks) of E and Ral in ovariectomized rats. E regulatedtwice as many genes as Ral, largely those associated with catalysisand metabolism, whereas Ral treatment induced genes associatedwith cell death and negative cell regulation. Follow-up studiesconfirmed that genes associated with matrix integrity were differentiallyregulated by Ral and E at various timepoints in uterine andvaginal tissues. Additional experiments were conducted to determinethe levels of MMP2 activity in uterus explants from ovariectomizedrats following 2 weeks of treatment with E, Ral, or one of twoadditional SERMs: lasofoxifene, and levormeloxifene. E andlasofoxifene stimulated uterine MMP2 activity to a level twicethat of Ral while levormeloxifene elevated MMP2 activity toa level 12 times that of Ral. These data show that one of thesignificant differences between E and Ral signaling in the uterusis the regulation of genes and proteins associated with matrixintegrity. This may be a potential key difference between theaction of SERMs in the uterus of postmenopausal women.

Key words: Female Reproductive Tract • Mechanisms of Hormone Action • Estradiol receptor • Uterus • Vagina

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