New antibiotic class effective against multidrug-resistant bacteria

Pressmeddelande

Scientists at Uppsala University have discovered a new class of antibiotics with potent activity against multi-drug resistant bacteria, and have shown that it cures bloodstream infections in mice. The new antibiotic class is described in an article in the scientific journal PNAS.

Peer review/Experimental study/Animals

Antibiotics are the foundation of modern medicine and over the last century have dramatically improved the lives of people around the world. Nowadays we tend to take antibiotics for granted and rely heavily on them to treat or prevent bacterial infections, including for example, to reduce the risk of infections during cancer therapy, during invasive surgery and transplants, and in mothers and preterm babies. Increasingly though, the global rise in antibiotic resistance threatens their effectiveness. In order to ensure access to effective antibiotics in the future, development of novel therapeutics to which there is no existing resistance is essential.

Researchers at Uppsala University have recently published their work in the Proceedings of the National Academy of Sciences of the USA describing a new class of antibiotics developed as a part of multi-national consortia. The class of compounds they describe target a protein, LpxH, which is used in a pathway by Gram-negative bacteria to synthesize their outermost layer of protection from the environment, called lipopolysaccharide. Not all bacteria produce this layer, but those that do include the organisms that have been identified by the World Health Organization as being the most critical to develop novel treatments for, including Escherichia coli and Klebsiella pneumoniae that have already developed resistance to available antibiotics.

The researchers were able to show that this new antibiotic class is highly active against multidrug-resistant bacteria and was able to treat bloodstream infections in a mouse model, demonstrating the promise of this class. Importantly, since this compound class is completely new and the protein LpxH has not yet been exploited as a target for antibiotics there is no pre-existing resistance to this class of compounds. This is in contrast to the many ‘me-too’ antibiotics of existing classes currently in clinical development. While the current results are very promising there will be considerable additional work required before compounds of this class will be ready for clinical trials.

The work to discover and develop this new class of antibiotics was supported by the EU project ENABLE which was funded through the Innovative Medicines Initiative’s New Drugs 4 Bad Bugs program (ND4BB). The ENABLE project, led by researchers at Uppsala University and the pharmaceutical company GlaxoSmithKline, brought together stakeholders from across Europe representing academia and large and small pharmaceutical companies to pool resources and expertise to advance early-stage antibiotic development. This antibiotic class now continues to be developed in the follow-on project, ENABLE-2, an antibiotic drug discovery platform funded by Swedish Research Council, the National Research Programme on Antibiotic Resistance and Sweden’s innovation agency Vinnova to continue the momentum generated by the original ENABLE project.

About ENABLE
In ENABLE, over 50 European partners from academia and industry, co-led by GlaxoSmithKline and Uppsala University, joined forces in a 7-year project funded by the Innovative Medicines Initiative (IMI) to develop novel antibiotics against key Gram-negative bacteria such as E. coli, K. pneumoniae, P. aeruginosa and A. baumannii.
The research leading to these results has received funding from the Innovative Medicines Initiative Joint Undertaking under grant agreement n°115583, resources of which are composed of financial contribution from the European Union’s Seventh Framework Programme (FP7/2007-2013) and EFPIA companies’ in-kind contribution. The ENABLE project is also financially supported by contributions from Academic and SME partners.
For more information about IMI, visit www.imi.europa.eu

About ENABLE-2

ENABLE-2 has built an antibacterial drug discovery platform based on the learnings from the IMI project ENABLE with focus on the early stages of antibiotic discovery and development.
ENABLE-2 is supported by the Swedish Research Council, the National Research
Programme on Antibiotic Resistance and Sweden’s innovation agency Vinnova.
For more information about ENABLE-2, visit www.ilk.uu.se/enable2

Article: Antibiotic class with potent in vivo activity targeting lipopolysaccharide synthesis in Gram-negative bacteria, Proceedings of the National Academy of Sciences U.S.A., DOI: 10.1073/pnas.2317274121/

For more information, please contact:
Dr. Douglas L. Huseby, Dept. Medical Biochemistry and Microbiology, Uppsala University, Email: douglas.huseby@imbim.uu.se
or
Prof. Anders Karlén, Dept. Medicinal Chemistry, Drug Design and Discovery, Uppsala University, Email: anders.karlen@ilk.uu.se
or
Prof. Diarmaid Hughes, Dept. Medical Biochemistry and Microbiology, Uppsala University, Email: diarmaid.hughes@imbim.uu.se

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