Rapid Evolution of a Fragment-like Molecule to Pan-Metallo-Beta-Lactamase Inhibitors: Initial Leads toward Clinical Candidates.

Mihirbaran Mandal,William K Hagmann,Haiqun Tang,Edward Dinunzio,Amy Flattery,Winnie Prosise,Ann E Weber,Haifeng Tang,Katherine Young,Rumin Zhang,Alexei V Buevich,Alexander Pasternak,Yuriko Root,Jing Su,Asra Mirza,Inhou Chu,Jacqueline D Hicks,Emma R Parmee,Guoqing Li,Nicholas Murgolo,Giovanna Scapin,Shuzhi Dong,Li Xiao,Alex G Therien,Daniel F Wyss,Donald Chu,Jianping Pan,Jim Tata,Weidong Pan,Artjohn Villafania,Priya Dayananth,Lianzhu Liang,Carrie G Markgraf ,Charles G Garlisi ,Cangming Yang ,Todd Mayhood ,Hai‐Young Kim ,Wei Jin ,Todd A Black ,Payal R Sheth ,Ronald E Painter ,Shu‐Wei Yang ,Reynalda K De Jesus ,Thierry O Fischmann

doi:10.1021/acs.jmedchem.2c00766

Abstract

With the emergence and rapid spreading of NDM-1 and existence of clinically relevant VIM-1 and IMP-1, discovery of pan inhibitors targeting metallo-beta-lactamases (MBLs) became critical in our battle against bacterial infection. Concurrent with our fragment and high-throughput screenings, we performed a knowledge-based search of known metallo-beta-lactamase inhibitors (MBLIs) to identify starting points for early engagement of medicinal chemistry. A class of compounds exemplified by 11, discovered earlier as B. fragilis metallo-beta-lactamase inhibitors, was selected for in silico virtual screening. From these efforts, compound 12 was identified with activity against NDM-1 only. Initial exploration on metal binding design followed by structure-guided optimization led to the discovery of a series of compounds represented by 23 with a pan MBL inhibition profile. In in vivo studies, compound 23 in combination with imipenem (IPM) robustly lowered the bacterial burden in a murine infection model and became the lead for the invention of MBLI clinical candidates.

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