Literature DB >> 17000691

In vivo efficacy of STX213, a second-generation steroid sulfatase inhibitor, for hormone-dependent breast cancer therapy.

Paul A Foster1, Simon P Newman, Surinder K Chander, Chloe Stengel, Roma Jhalli, Lawrence L W Woo, Barry V L Potter, Michael J Reed, Atul Purohit.   

Abstract

PURPOSE: Steroid sulfatase (STS) inhibitors that can decrease or prevent the biosynthesis of estrogenic steroids via the sulfatase route may play an important role in the treatment of breast cancer. We compare the in vivo efficacy of two potent STS inhibitors, STX64 and STX213, in a xenograft breast cancer model. EXPERIMENTAL
DESIGN: MCF-7 cells stably expressing STS cDNA (MCF-7STS) were generated. Ovariectomized MF-1 female nude mice receiving s.c. injections of estradiol sulfate (E2S) and bearing both MCF-7STS and wild-type MCF-7 (MCF-7WT) tumors were orally treated with STX64 and STX213. Treatment was given for 49 days followed by a recovery period of 35 days in which animals received only E2S. Mice were weighed, and tumor measurements were taken weekly.
RESULTS: STX64 and STX213 exhibited potent STS inhibition in vivo. However, STX213 showed a greater duration of activity. In vehicle-treated nude mice receiving E2S, tumor volumes increased 5.5-fold for MCF-7WT and 3.8-fold for MCF-7STS after 49 days compared with day 0. MCF-7WT tumor growth was reduced by 56% by STX213 over the dosing period, and subsequent growth was retarded during the recovery period. All treatments fully inhibited growth of MCF-7STS tumors, and recovery of these tumors was significantly retarded (P<0.01). All compounds completely inhibited liver and tumor STS activity. Additionally, STS mRNA expression in the MCF-7STS tumors directly correlated with the corresponding STS enzyme activity.
CONCLUSIONS: This study indicates that STS inhibitors attenuate hormone-dependent human breast cancer growth and therefore offer a potentially novel treatment for this condition.

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Year:  2006        PMID: 17000691     DOI: 10.1158/1078-0432.CCR-06-0632

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


  12 in total

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3.  The use of steroid sulfatase inhibitors as a novel therapeutic strategy against hormone-dependent endometrial cancer.

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Review 4.  Oestrogen and colorectal cancer: mechanisms and controversies.

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Review 5.  Phase two steroid metabolism and its roles in breast and prostate cancer patients.

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Review 7.  Steroid Sulphatase and Its Inhibitors: Past, Present, and Future.

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Review 8.  The Regulation of Steroid Action by Sulfation and Desulfation.

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9.  The Role of Steroid Sulfatase as a Prognostic Factor in Patients with Endometrial Cancer.

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10.  Design, synthesis, and biological evaluation of new arylamide derivatives possessing sulfonate or sulfamate moieties as steroid sulfatase enzyme inhibitors.

Authors:  Mohammed I El-Gamal; Mohammad H Semreen; Paul A Foster; Barry V L Potter
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