Design and Evaluation of New Quinazolin-4(3H)-one Derived PqsR Antagonists as Quorum Sensing Quenchers in Pseudomonas aeruginosa | Zendy

Fadi Soukarieh | Zendy; Alaa Mashabi | Zendy; William Richardson | Zendy; Eduard Vico-Oton | Zendy; Manuel Romero | Zendy; Shaun N. Roberston | Zendy; Scott Grossman | Zendy; Tomás Sou | Zendy; Ruiling Liu | Zendy; Nigel Halliday | Zendy; Iréna Kukavica-Ibrulj | Zendy; Roger C. Lévesque | Zendy; Christel A. S. Bergström | Zendy; Barrie Kellam | Zendy; Jonas Emsley | Zendy; Stephan Heeb | Zendy; Paul Williams | Zendy; Michael J. Stocks | Zendy; Miguel Cámara | Zendy

Open Access

Design and Evaluation of New Quinazolin-4(3H)-one Derived PqsR Antagonists as Quorum Sensing Quenchers in Pseudomonas aeruginosa

Author(s) -

Fadi Soukarieh,

Alaa Mashabi,

William Richardson,

Eduard Vico-Oton,

Manuel Romero,

Shaun N. Roberston,

Scott Grossman,

Tomás Sou,

Ruiling Liu,

Nigel Halliday,

Iréna Kukavica-Ibrulj,

Roger C. Lévesque,

Christel A. S. Bergström,

Barrie Kellam,

Jonas Emsley,

Stephan Heeb,

Paul Williams,

Michael J. Stocks,

Miguel Cámara

Publication year - 2021

Publication title -

acs infectious diseases

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.324

H-Index - 39

ISSN - 2373-8227

DOI - 10.1021/acsinfecdis.1c00175

Subject(s) - quorum sensing , pseudomonas aeruginosa , virulence , chemistry , microbiology and biotechnology , quorum quenching , isothermal titration calorimetry , cross resistance , biology , biochemistry , bacteria , genetics , gene

P. aeruginosa (PA) continues to pose a threat to global public health due to its high levels of antimicrobial resistance (AMR). The ongoing AMR crisis has led to an alarming shortage of effective treatments for resistant microbes, and hence there is a pressing demand for the development of novel antimicrobial interventions. The potential use of antivirulence therapeutics to tackle bacterial infections has attracted considerable attention over the past decades as they hamper the pathogenicity of target microbes with reduced selective pressure, minimizing the emergence of resistance. One such approach is to interfere with the PA pqs quorum sensing system which upon the interaction of PqsR, a Lys-R type transcriptional regulator, with its cognate signal molecules 4-hydroxy-2-heptylquinoline (HHQ) and 2-heptyl-3-hydroxy-4-quinolone (PQS), governs multiple virulence traits and host-microbe interactions. In this study, we report the hit identification and optimization of PqsR antagonists using virtual screening coupled with whole cell assay validation. The optimized hit compound 61 (( R )-2-(4-(3-(6-chloro-4-oxoquinazolin-3(4 H )-yl)-2-hydroxypropoxy)phenyl)acetonitrile) was found to inhibit the expression of the PA P pqsA promoter controlled by PqsR with an IC 50 of 1 μM. Using isothermal titration calorimetry, a K d of 10 nM for the PqsR ligand binding domain (PqsR LBD ) was determined for 61. Furthermore, the crystal structure of 61 with PqsR LBD was attained with a resolution of 2.65 Å. Compound 61 significantly reduced levels of pyocyanin, PQS, and HHQ in PAO1-L, PA14 lab strains and PAK6085 clinical isolate. Furthermore, this compound potentiated the effect of ciprofloxacin in early stages of biofilm treatment and in Galleria mellonella infected with PA. Altogether, this data shows 61 as a potent PqsR inhibitor with potential for hit to lead optimization toward the identification of a PA QS inhibitor which can be advanced into preclinical development.

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