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Discovery and Rational Design of Natural-Product-Derived 2‑Phenyl-3,4-dihydro‑2<i>H</i>‑benzo[<i>f</i>]chromen-3-amine Analogs as Novel and Potent Dipeptidyl Peptidase 4 (DPP-4) Inhibitors for the Treatment of Type 2 Diabetes
Starting
from the lead isodaphnetin, a natural product inhibitor
of DPP-4 discovered through a target fishing docking based approach,
a series of novel 2-phenyl-3,4-dihydro-2<i>H</i>-benzoÂ[<i>f</i>]Âchromen-3-amine derivatives as potent DPP-4 inhibitors
are rationally designed utilizing highly efficient 3D molecular similarity
based scaffold hopping as well as electrostatic complementary methods.
Those ingenious drug design strategies bring us approximate 7400-fold
boost in potency. Compounds <b>22a</b> and <b>24a</b> are
the most potent ones (IC<sub>50</sub> ≈ 2.0 nM) with good pharmacokinetic
profiles. Compound <b>22a</b> demonstrated stable pharmacological
effect. A 3 mg/kg oral dose provided >80% inhibition of DPP-4 activity
within 24 h, which is comparable to the performance of the long-acting
control omarigliptin. Moreover, the efficacy of <b>22a</b> in
improving the glucose tolerance is also comparable with omarigliptin.
In this study, not only promising DPP-4 inhibitors as long acting
antidiabetic that are clinically on demand are identified, but the
target fish docking and medicinal chemistry strategies were successfully
implemented