Benzimidazolone as potent chymase inhibitor: modulation of reactive metabolite formation in the hydrophobic (P1) region.

Ho Yin Lo,Peter Allen Nemoto,Jin Mi Kim,Ming-Hong Hao,Kevin Chungeng Qian,Neil A. Farrow,Daniel R. Albaugh,Danielle M. Fowler,Richard D. Schneiderman,E. Michael August,Leslie Martin,Melissa Hill-Drzewi,Steven S. Pullen,Hidenori Takahashi,Stephane De Lombaert

Benzimidazolone as potent chymase inhibitor: modulation of reactive metabolite formation in the hydrophobic (P1) region.

2011

Ho Yin Lo
Peter Allen Nemoto
Jin Mi Kim
Ming-Hong Hao
Kevin Chungeng Qian
Neil A. Farrow
Daniel R. Albaugh
Danielle M. Fowler
Richard D. Schneiderman
E. Michael August
Leslie Martin
Melissa Hill-Drzewi
Steven S. Pullen
Hidenori Takahashi
Stephane De Lombaert

A new class of chymase inhibitor featuring a benzimidazolone core with an acid side chain and a P1 hydrophobic moiety is described. Incubation of the lead compound with GSH resulted in the formation of a GSH conjugate on the benzothiophene P1 moiety. Replacement of the benzothiophene with different heterocyclic systems such as indoles and benzoisothiazole is feasible. Among the P1 replacements, benzoisothiazole prevents the formation of GSH conjugate and an in silico analysis of oxidative potentials agreed with the experimental outcome.

Keywords:

Benzothiophene
Side chain
Serine protease
Organic chemistry
Chymase
Metabolite
Glutathione
Moiety
Biochemistry
Oxidative phosphorylation
Chemistry
Indole test
Stereochemistry
Conjugate
Lead compound

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