AI Article Synopsis

  • Researchers are developing a drug to target the CCK1R receptor, potentially helping to prevent and treat obesity by enhancing the natural action of CCK, which promotes feelings of fullness.
  • The study identified promising tetracyclic molecules through high throughput screening and characterized two leading candidates that meet the desired pharmacological profile.
  • They expanded this research by testing 65 analogs, successfully eliminating an unwanted side effect while maintaining the positive allosteric modulation of the CCK1R, paving the way for future clinical trials.

Article Abstract

As part of an ongoing effort to develop a drug targeting the type 1 cholecystokinin receptor (CCK1R) to help prevent and/or treat obesity, we recently performed a high throughput screening effort of small molecules seeking candidates that enhanced the action of the natural agonist, CCK, thus acting as positive allosteric modulators without exhibiting intrinsic agonist action. Such probes would be expected to act in a temporally finite way to enhance CCK action to induce satiety during and after a meal and potentially even modulate activity at the CCK1R in a high cholesterol environment present in some obese patients. The current work focuses on the best scaffold, representing tetracyclic molecules identified through high throughput screening we previously reported. Extensive characterization of the two top "hits" from the previous effort demonstrated them to fulfill the desired pharmacologic profile. We undertook analog-by-catalog expansion of this scaffold using 65 commercially available analogs. In this effort, we were able to eliminate an off-target effect observed for this scaffold while retaining its activity as a positive allosteric modulator of CCK1R in both normal and high cholesterol membrane environments. These insights should be useful in the rational medicinal chemical enhancement of this scaffold and in the future development of candidates to advance to pre-clinical proof-of-concept and to clinical trials.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9964746PMC
http://dx.doi.org/10.3390/membranes13020150DOI Listing

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