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Inhibitors of the Elastase LasB for the Treatment of Pseudomonas aeruginosa Lung Infections.

Jelena KonstantinovićAndreas Martin KanyAlaa AlhayekAhmed S AbdelsamieAsfandyar SikandarKatrin VoosYiwen YaoAnastasia AndreasRoya ShafieiBrigitta LoretzEsther SchönauerRobert BalsHans BrandstetterRolf Wolfgang HartmannChristian DuchoClaus-Michael LehrChristoph BeisswengerRolf MüllerKatharina RoxJörg HaupenthalAnna Katharina Herta Hirsch
Published in: ACS central science (2023)
Infections caused by the Gram-negative pathogen Pseudomonas aeruginosa are emerging worldwide as a major threat to human health. Conventional antibiotic monotherapy suffers from rapid resistance development, underlining urgent need for novel treatment concepts. Here, we report on a nontraditional approach to combat P. aeruginosa -derived infections by targeting its main virulence factor, the elastase LasB. We discovered a new chemical class of phosphonates with an outstanding in vitro ADMET and PK profile, auspicious activity both in vitro and in vivo . We established the mode of action through a cocrystal structure of our lead compound with LasB and in several in vitro and ex vivo models. The proof of concept of a combination of our pathoblocker with levofloxacin in a murine neutropenic lung infection model and the reduction of LasB protein levels in blood as a proof of target engagement demonstrate the great potential for use as an adjunctive treatment of lung infections in humans.
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