Author:
Rao Komal Umashankar,Henderson Domhnall Iain,Krishnan Nitya,Puthia Manoj,Glegola-Madejska Izabela,Brive Lena,Bjarnemark Fanny,Millqvist Fureby Anna,Hjort Karin,Andersson Dan I.,Tenland Erik,Sturegård Erik,Robertson Brian D.,Godaly Gabriela
Abstract
AbstractAlternative ways to prevent and treat infectious diseases are needed. Previously, we identified a fungal peptide, NZX, that was comparable to rifampicin in lowering M. tuberculosis load in a murine tuberculosis (TB) infection model. Here we assessed the potential synergy between this cationic host defence peptide (CHDP) and the current TB drugs and analysed its pharmacokinetics. We found additive effect of this peptide with isoniazid and ethambutol and confirmed these results with ethambutol in a murine TB-model. In vivo, the peptide remained stable in circulation and preserved lung structure better than ethambutol alone. Antibiotic resistance studies did not induce mutants with reduced susceptibility to the peptide. We further observed that this peptide was effective against nontuberculous mycobacteria (NTM), such as M. avium and M. abscessus, and several Gram-positive bacteria, including methicillin-resistant Staphylococcus aureus. In conclusion, the presented data supports a role for this CHDP in the treatment of drug resistant organisms.
Funder
Royal Physiographic Society of Lund
UK Medical Research Council
Swedish Research Council
Hjärt-Lungfonden
Lund University
Publisher
Springer Science and Business Media LLC
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