Exploring ND-011992, a quinazoline-type inhibitor targeting quinone reductases and quinol oxidases

Author:

Kägi Jan,Sloan Willough,Schimpf Johannes,Nasiri Hamid R.ORCID,Lashley DanaORCID,Friedrich ThorstenORCID

Abstract

AbstractBacterial energy metabolism has become a promising target for next-generation tuberculosis chemotherapy. One strategy to hamper ATP production is to inhibit the respiratory oxidases. The respiratory chain of Mycobacterium tuberculosis comprises a cytochrome bcc:aa3 and a cytochrome bd ubiquinol oxidase that require a combined approach to block their activity. A quinazoline-type compound called ND-011992 has previously been reported to ineffectively inhibit bd oxidases, but to act bactericidal in combination with inhibitors of cytochrome bcc:aa3 oxidase. Due to the structural similarity of ND-011992 to quinazoline-type inhibitors of respiratory complex I, we suspected that this compound is also capable of blocking other respiratory chain complexes. Here, we synthesized ND-011992 and a bromine derivative to study their effect on the respiratory chain complexes of Escherichia coli. And indeed, ND-011992 was found to inhibit respiratory complex I and bo3 oxidase in addition to bd-I and bd-II oxidases. The IC50 values are all in the low micromolar range, with inhibition of complex I providing the lowest value with an IC50 of 0.12 µM. Thus, ND-011992 acts on both, quinone reductases and quinol oxidases and could be very well suited to regulate the activity of the entire respiratory chain.

Funder

Reves Center for International Studies

Deutsche Forschungsgemeinschaft

Albert-Ludwigs-Universität Freiburg im Breisgau

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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