AI Article Synopsis

  • * Adding a sulfate group to bile acids can lower their absorption and increase the amount excreted in feces, making them better for targeting the gut.
  • * For IBD treatment, a different strategy is used where a 7-methoxy group increases potency at the TGR5 receptor, and a methyl-d-glucamine group is added to balance receptor activity with low absorption and good fecal recovery.

Article Abstract

Bile acid derivatives have been investigated as possible therapeutics for a wide array of conditions, including several for which gut-restricted analogs would likely be preferred. These include the prevention of infection (CDI) and the treatment of inflammatory bowel disease (IBD). The design of gut-restricted bile acid analogs, however, is complicated by the highly efficient enterohepatic circulation system that typically reabsorbs these compounds from the digestive tract for subsequent return to the liver. Herein, we report that incorporation of a sulfate group at the 7-position of the bile acid scaffold reduces oral bioavailability and increases fecal recovery in two pairs of compounds designed to inhibit the germination of spores. A different approach was necessary for designing gut-restricted bile acid-based TGR5 agonists for the treatment of IBD, as the incorporation of a 7-sulfate group reduces activity at this receptor. Instead, building on our previous discovery that incorporation of a 7-methoxy group into chenodeoxycholic acid derivatives greatly increases their TGR5 receptor potency, we determined that an -methyl-d-glucamine group could be conjugated to the scaffold to obtain a compound with an excellent mix of potency at the TGR5 receptor, low oral exposure, and good fecal recovery.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8130628PMC
http://dx.doi.org/10.1039/d0md00425aDOI Listing

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