Technology ID
TAB-4072

Synergistic Use of Exo VII Inhibitors And Quinolone Antibiotics For Treating Bacterial Infection

E-Numbers
E-171-2020-0
Lead Inventor
Pommier, Yves (NCI)
Co-Inventors
Huang, Shar-yin (NCI)
Mitchell, Brianna (NCI)
Applications
Therapeutics
Therapeutic Areas
Infectious Disease
Development Stages
Pre-clinical (in vivo)
Lead IC
NCI
ICs
NCI

Topoisomerase poisons, such as quinolone antibiotics, are widely used as anticancer drugs and antibiotics. Quinolone antibiotics act by trapping prokaryotic type IIA topoisomerases (DNA gyrase and TOPO IV), resulting in irreversible topoisomerase cleavage complexes. However, current U.S. Food and Drug Administration (FDA) guidance reserves the use of quinolones for the most serious bacterial infections due to their associated side effects and to limit the occurrence of drug-resistant bacterial strains. Resistance to available antibiotics in pathogenic bacteria is a global challenge as the number of drug-resistant strains increased dramatically each year. 

Combination of antibiotics with antibiotic adjuvants offers a productive strategy to address the widespread emergence of antibiotic-resistant strains. Exonuclease VII (ExoVII) repairs quinolone-induced DNA damage by excising the tyrosyl-DNA linkage between DNA and trapped DNA gyrase, an essential prokaryotic type II A topoisomerase. Consequently, inactivation of ExoVII results in hypersensitivity to quinolones. Researchers at the NCI have discovered ExoVII inhibitors that synergize with the antimicrobial activity of the quinolone antibiotic ciprofloxacin. These inhibitors present strong potential as antibiotic adjuvants increasing the potency of quinolones – particularly against quinolone-resistant bacterial strains. In addition, the combination of ExoVII inhibitors with quinolones may allow dose reduction – potentially decreasing side-effects.

The NCI seeks co-development partners or licensees to further develop the novel ExoVII inhibitor(s) as antibiotic adjuvants for enhancing the efficacy of quinolone antibiotics, particularly in quinolone-resistant bacterial strains.

Competitive Advantages:

  • ExoVII inhibitor increases the efficacy of quinolone antibiotics, allowing dose reduction for quinolones and potentially decrease side-effects and be well-tolerated
  • Potentially overcome bacterial resistance to quinolones 
  • Lack of inhibitory activity against human tyrosyl-DNA phosphodiesterase (TDP) suggests that inhibitors targeting prokaryotic ExoVII might decrease side-effects and be well-tolerated

Commercial Applications:

  • Antibiotic adjuvant in combination with ciprofloxacin and other quinolone antibiotics 
  • Antibiotic adjuvant in combination with other topoisomerase poisons 

Request More Info

Licensing Contact:
Chang, Kevin
changke@mail.nih.gov

Patents

  • US
    Provisional (PRV) 63/129,271
    Filed on 2020-12-22
  • Patent Cooperation Treaty
    (PCT) PCT/US2021/064996
    Filed on 2021-12-22
  • Canada
    National Stage 3205044
    Filed on 2023-06-12
  • Australia
    National Stage 2021409956
    Filed on 2023-06-25
  • China
    National Stage 202180086835.1
    Filed on 2023-06-21
  • US
    National Stage 18/268,603
    Filed on 2023-06-20
  • European Patent
    National Stage 21851911.4
    Filed on 2023-05-16

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