Prior to characterization of antifungal inhibitors that target this enzyme, Trichophyton rubrum CYP51 was expressed in Escherichia coli, purified and characterized. T. rubrum CYP51 bound lanosterol, obtusifoliol and eburicol with similar affinities (Kd values 22.7, 20.3 and 20.9 μM), but displayed substrate specificity insofar as only eburicol was demethylated in CYP51 reconstitution assays (turnover number 1.55 min-1, Km value 2 μM). The investigational agent VT-1161 bound tightly to T. rubrum CYP51 (Kd = 242 nM) with similar affinity as clotrimazole, fluconazole, ketoconazole and voriconazole (Kd values 179, 173, 312, and 304 nM, respectively), and with lower affinity than itraconazole (Kd = 53 nM). IC50 determinations using 0.5 μM CYP51 showed VT-1161 was a tight-binding inhibitor of T. rubrum CYP51 activity yielding an IC50 value of 0.14 μM compared to 0.26, 0.4 and 0.6 μM for itraconazole, fluconazole and ketoconazole, respectively. When tested against 34 clinical isolates, VT-1161 was a potent inhibitor of T. rubrum growth with MIC50, MIC90, and geometric mean MIC values of ≤0.03, 0.06, and 0.033 μg ml-1, respectively. With its selectivity versus human CYP51 and drug metabolizing CYPs having already been established, VT-1161 should prove safe and effective in combating T. rubrum infections in patients.
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