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2 research outputs found

Topoisomerase Inhibitors Addressing Fluoroquinolone Resistance in Gram-Negative Bacteria.

Author: Armstrong Duncan
Balibar Carl
Bauer Daniel
Bellamacina Cornelia
Benton Bret
Bussiere Dirksen
Dangi Veer
De Pascale Gianfranco
De Vicente Fidalgo Javier
Dean Charles
Dhumale Bhavesh
Fuller John
Fulsunder Mangesh
Holder Lauren
Hu Cheng
Kantariya Bhavin
Lapointe Guillaume
Leeds Jennifer
Li Xiaolin
Lu Peichao
Lvov Anatoli
Ma Sylvia
Madhavan Shravanthi
Malekar Swapnil
Mark Fisher
Mckenney David
Mergo Wosenu
Metzger Iv Louis
Moser Heinz
Mutnick Daniel
Noeske Jonas
Osborne Colin
Pal Arani
Patel Ashish
Patel Darshit
Patel Tushar
Prajapati Krunal
Prosen Katie
Reck Folkert
Richie Daryl
Rico Alice
Rivkin Alexey
Sanderson Mark
Satasia Shailesh
Sawyer William
Selvarajah Jogitha
Shafer Cynthia
Shah Nirav
Shangavi Kartik
Shu Wei
Skepper Colin
Thompson Katherine
Vala Anand
Veselkov Dennis
Vo Jason
Wang Michael
Widya Marcella
Williams Sarah
Xu Yongjin
Yue Qin
Zhang Richard
Zhou Bo
Publication venue: 'American Chemical Society (ACS)'
Publication date: 01/01/2020
Field of study

Since their discovery over 5 decades ago, quinolone antibiotics have found enormous success as broad spectrum agents that exert their activity through dual inhibition of bacterial DNA gyrase and topoisomerase IV. Increasing rates of resistance, driven largely by target-based mutations in the GyrA/ParC quinolone resistance determining region, have eroded the utility and threaten the future use of this vital class of antibiotics. Herein we describe the discovery and optimization of a series of 4-(aminomethyl)quinolin-2(1H)-ones, exemplified by 34, that inhibit bacterial DNA gyrase and topoisomerase IV and display potent activity against ciprofloxacin-resistant Gram-negative pathogens. X-ray crystallography reveals that 34 occupies the classical quinolone binding site in the topoisomerase IV-DNA cleavage complex but does not form significant contacts with residues in the quinolone resistance determining region

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Two Distinct Mechanisms of Inhibition of LpxA Acyltransferase Essential for Lipopolysaccharide Biosynthesis

Author: Benson Timothy
Berminghan Alun
Brenton Bret
Casey Fergal
Chie Leon Barbara
Chiu Chun-Hao
Cho Min-Kyu
Cook Kim
De Pascale Gianfranco
Frank Andreas
Frommlet Alexandra
Han Wooseok
Ho Chi-Min
Jansen Hanneke
Lee Patrick
Li Min
Lingel Andreas
Ma Sylvia
Ma Xiaolei
Merritt Hanne
Ornelas Elizabeth
Prathapam Ramadevi
Prosen Katie
Rasper Dita
Rath Christopher
Sawyer William
Shaul Jacob
Shia Steven
Smith Thomas
Steffek Micah
Subramanian Sharadha
Uehara Tsuyoshi
Vo Jason
Wang Feng
Wartchow Charles
Publication venue: 'American Chemical Society (ACS)'
Publication date: 01/01/2020
Field of study

The lipopolysaccharide biosynthesis pathway is considered an attractive drug target against the rising threat of multi-drug-resistant Gram-negative bacteria. Here, we report two novel small-molecule inhibitors (compounds 1 and 2) of the acyltransferase LpxA, the first enzyme in the lipopolysaccharide biosynthesis pathway. We show genetically that the antibacterial activities of the compounds against efflux-deficient Escherichia coli are mediated by LpxA inhibition. Consistently, the compounds inhibited the LpxA enzymatic reaction in vitro. Intriguingly, using biochemical, biophysical, and structural characterization, we reveal two distinct mechanisms of LpxA inhibition; compound 1 is a substrate-competitive inhibitor targeting apo LpxA, and compound 2 is an uncompetitive inhibitor targeting the LpxA/product complex. Compound 2 exhibited more favorable biological and physicochemical properties than compound 1 and was optimized using structural information to achieve improved antibacterial activity against wild-type E. coli. These results show that LpxA is a promising antibacterial target and imply the advantages of targeting enzyme/product complexes in drug discovery

The Novartis Repository