Optimization of
Chromeno[2,3‑c]pyrrol-9(2H)‑ones as Highly Potent, Selective,
and Orally Bioavailable PDE5 Inhibitors: Structure–Activity
Relationship, X‑ray Crystal Structure, and Pharmacodynamic
Effect on Pulmonary Arterial Hypertension

Wu, Deyan; Huang, Yadan; Chen, Yiping; Huang, Yi-You; Geng, Haiju; Zhang, Tianhua; Zhang, Chen; Li, Zhe; Guo, Lei; Chen, Jianwen; Luo, Hai-Bin

doi:10.1021/acs.jmedchem.8b01209.s001

jm8b01209_si_001.pdf (4.55 MB)

Optimization of Chromeno[2,3‑c]pyrrol-9(2H)‑ones as Highly Potent, Selective, and Orally Bioavailable PDE5 Inhibitors: Structure–Activity Relationship, X‑ray Crystal Structure, and Pharmacodynamic Effect on Pulmonary Arterial Hypertension

journal contribution

posted on 2018-08-27, 00:00 authored by Deyan Wu, Yadan Huang, Yiping Chen, Yi-You Huang, Haiju Geng, Tianhua Zhang, Chen Zhang, Zhe Li, Lei Guo, Jianwen Chen, Hai-Bin Luo

To further explore the structure–activity relationship around the chromeno[2,3-c]pyrrol-9(2H)-one scaffold, 19 derivatives as inhibitors against PDE5 were discovered. The most potent inhibitor 3 has an IC₅₀ of 0.32 nM with remarkable selectivity and druglike profile. Oral administration of 3 (1.25 mg/kg) caused comparable therapeutic effects to sildenafil (10.0 mg/kg) against pulmonary arterial hypertension. Further, different binding patterns from sildenafil were revealed in cocrystal structures, which provide structural templates for discovery of highly potent PDE5 inhibitors.