AI Article Synopsis

  • Treatment with CB-154 and Tamoxifen significantly decreased the incidence of mammary carcinomas in female rats exposed to the carcinogen DMBA, with reductions of 58% and 49%, respectively, after 33 days of administration.
  • Combining CB-154 and Tamoxifen further enhanced the cancer prevention effects, reducing incidence rates by an additional 50-59%.
  • While Tamoxifen alone continued to show strong effectiveness in later stages of carcinogenesis, CB-154 did not show significant benefits, indicating that Tamoxifen is more effective during certain phases of cancer prevention.

Article Abstract

Daily treatment of female Sprague-Dawley rats with CB-154 (prolactin suppressor) or Tamoxifen (estrogen antagonist) for 33 days before and after 7,12-dimethylbenzanthracene (DMBA) administration reduced (p less than 0.005) the incidence of mammary carcinomas by 58 and 49%, respectively. A combination of CB-154 and Tamoxifen further reduced (p less than 0.005) mammary carcinoma incidence by an additional 50-59%. Treatment with Tamoxifen for 66 days beginning 33 days after carcinogen treatment reduced (p less than 0.05) the incidence of mammary carcinomas by 65%; CB-154 treatment, during the same time period, did not significantly effect the final yield of mammary carcinomas. The combination of Tamoxifen and CB-154 was comparable to Tamoxifen alone in suppressing the incidence of mammary carcinomas in the latter study. These results demonstrate a substantial suppressive and synergistic effect of Tamoxifen and CB-154 in the initiating phases of mammary carcinogenesis while in the early promoting phases of this oncogenic process, short-term treatment with Tamoxifen was superior to CB-154 treatment; no synergism between these clinically important compounds was observed.

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http://dx.doi.org/10.1159/000225613DOI Listing

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