AI Article Synopsis

  • The combination of Conjugated Estrogens (CE) and Bazedoxifene (BZA) aims to relieve menopause symptoms in women but its effects on gut microbiome and enzyme activity have not been previously studied.
  • A mouse study revealed that while CE+BZA didn't significantly alter the overall gut microbiome, it did reduce the abundance of Akkermansia, associated with weight gain, and lowered fecal GUS activity linked to Lactobacillaceae abundance.
  • This research suggests that long-term estrogen supplementation can directly influence gut microbial activity and composition, potentially optimizing the metabolism of estrogens for better health outcomes in postmenopausal women or breast cancer patients.

Article Abstract

Conjugated estrogens (CE) and Bazedoxifene (BZA) combination is used to alleviate menopause-associated symptoms in women. CE+BZA undergo first-pass-metabolism in the liver and deconjugation by gut microbiome via β-glucuronidase (GUS) enzyme inside the distal gut. To date, the impact of long-term exposure to CE+BZA on the gut microbiome or GUS activity has not been examined. Our study using an ovariectomized mouse model showed that CE+BZA administration did not affect the overall cecal or fecal microbiome community except that it decreased the abundance of Akkermansia, which was identified as a fecal biomarker correlated with weight gain. The fecal GUS activity was reduced significantly and was positively correlated with the abundance of Lactobacillaceae in the fecal microbiome. We further confirmed in Escherichia coli K12 and Lactobacillus gasseri ADH that Tamoxifen-, 4-hydroxy-Tamoxifen- and Estradiol-Glucuronides competed for GUS activity. Our study for the first time demonstrated that long-term estrogen supplementation directly modulated gut microbial GUS activity. Our findings implicate that long-term estrogen supplementation impacts composition of gut microbiota and microbial activity, which affects estrogen metabolism in the gut. Thus, it is possible to manipulate such activity to improve the efficacy and safety of long-term administered estrogens for postmenopausal women or breast cancer patients.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5970144PMC
http://dx.doi.org/10.1038/s41598-018-26506-1DOI Listing

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