AI Article Synopsis

  • The kidneys regulate fluid balance, maintain acid-base and electrolyte levels, and excrete metabolic waste, highlighting their essential functions in the body.
  • The study investigated the human uric acid transporter 1 (hURAT1) using Xenopus oocytes to test new compounds that inhibit uric acid uptake, which is linked to conditions like gout.
  • Results showed that certain modified benzofuran compounds exhibited strong inhibitory activity on hURAT1, with some achieving submicromolar effectiveness, indicating potential for developing treatments targeting uric acid secretion.

Article Abstract

The kidneys are a vital organ in the human body. They serve several purposes including homeostatic functions such as regulating extracellular fluid volume and maintaining acid-base and electrolyte balance and are essential regarding the excretion of metabolic waste. Furthermore, the kidneys play an important role in uric acid secretion/reabsorption. Abnormalities associated with kidney transporters have been associated with various diseases, such as gout. The current study utilized Xenopus oocytes expressing human uric acid transporter 1 (hURAT1; SLC22A12) as an in vitro method to investigate novel compounds and their ability to inhibit (14)C-uric acid uptake via hURAT1. We have prepared and tested a series of 2-ethyl-benzofuran compounds and probed the hURAT1 in vitro inhibitor structure-activity relationship. As compared to dimethoxy analogues, monophenols formed on the C ring showed the best in vitro inhibitory potential. Compounds with submicromolar (i.e., IC(50) < 1000 nM) inhibitors were prepared by brominating the corresponding phenols to produce compounds with potent uricosuric activity.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3124071PMC
http://dx.doi.org/10.1021/jm1015022DOI Listing

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