@article{Bjedov_Bekić_Marinović_Škorić_Pavlović_Ćelić_Petri_Sakač_2022, place={Belgrade, Serbia}, title={Screening the binding affinity of bile acid derivatives for the glucocorticoid receptor ligand-binding domain: Scientific paper}, volume={88}, url={https://shd-pub.org.rs/index.php/JSCS/article/view/12062}, DOI={10.2298/JSC220912078B}, abstractNote={<p>The necessity of anti-inflammatory drugs such as glucocorticoids has been evident during the COVID-19 pandemic. Glucocorticoids, are the stan­dard therapy for the treatment of moderate and severe COVID-19 patients. However, serious side effects limit the use of these drugs, and anti-inflam­matory drugs with better pharmacological properties are urgently required. Bile acids are of interest, because of their anti-inflammatory and immunomodul­atory properties, facilitated through an unclear mechanism involving trans­mem­brane and nuclear receptors. In this work, we screened the binding activity of a number of bile acid deri­vatives, for the ligand-binding domain of glucocor­ticoid receptor (GR-LBD), the most important receptor for anti-inflammatory processes. Tested compounds inc­lude oximes, lactones, lactams, tetrazoles, dienones, C-24 alcohols and cholic acid amides. Cholic acid oxime, deoxy­cho­lic acid dienone, 3-keto-24-cholic alcohol and cholic acid amide showed best binding affinities for GR-LBD among tested compounds. The in silico mole­cular docking explanation is provided. SAR analysis showed that expansion of B and C steroid rings or attachment of hetero­cycle to C ring is not beneficial for binding; side chain should contain hydrogen donor group; the GR-LBD tolerate well different functionalities on C-3 position. These results provide valu­able information toward synthesis of the new gluco­corticoids based on bile acids.</p>}, number={2}, journal={Journal of the Serbian Chemical Society}, author={Bjedov, Srđan and Bekić, Sofija and Marinović, Maja and Škorić, Dušan and Pavlović, Ksenija and Ćelić, Anđelka and Petri, Edward and Sakač, Marija}, year={2022}, month={Dec.}, pages={123–139} }