Abstract:In recent years the selective inhibition of FKBP51 has emerged as a possible treatment for chronic pain, obesity-induced diabetes, or depression. All currently known advanced FKBP51-selective inhibitors, including the widely used SAFit2, contain a cyclohexyl residue as a key motif for enabling selectivity over the closest homolog and anti-target FKBP52. During a structure-based SAR exploration we surprisingly discovered thiophenes as highly efficient cyclohexyl replacement moieties that retain the strong selec… Show more
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