Targeting malaria parasites with novel derivatives of azithromycin

INTRODUCTION: The spread of artemisinin resistant Plasmodium falciparum parasites is of global concern and highlights the need to identify new antimalarials for future treatments. Azithromycin, a macrolide antibiotic used clinically against malaria, kills parasites via two mechanisms: ‘delayed death...

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Autores principales: Burns, Amy L., Sleebs, Brad E., Gancheva, Maria, McLean, Kimberley T., Siddiqui, Ghizal, Venter, Henrietta, Beeson, James G., O’Handley, Ryan, Creek, Darren J., Ma, Shutao, Frölich, Sonja, Goodman, Christopher D., McFadden, Geoffrey I., Wilson, Danny W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Cellular and Infection Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9748569/
https://www.ncbi.nlm.nih.gov/pubmed/36530422
http://dx.doi.org/10.3389/fcimb.2022.1063407
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author Burns, Amy L.
Sleebs, Brad E.
Gancheva, Maria
McLean, Kimberley T.
Siddiqui, Ghizal
Venter, Henrietta
Beeson, James G.
O’Handley, Ryan
Creek, Darren J.
Ma, Shutao
Frölich, Sonja
Goodman, Christopher D.
McFadden, Geoffrey I.
Wilson, Danny W.
author_facet Burns, Amy L.
Sleebs, Brad E.
Gancheva, Maria
McLean, Kimberley T.
Siddiqui, Ghizal
Venter, Henrietta
Beeson, James G.
O’Handley, Ryan
Creek, Darren J.
Ma, Shutao
Frölich, Sonja
Goodman, Christopher D.
McFadden, Geoffrey I.
Wilson, Danny W.
author_sort Burns, Amy L.
collection PubMed
description INTRODUCTION: The spread of artemisinin resistant Plasmodium falciparum parasites is of global concern and highlights the need to identify new antimalarials for future treatments. Azithromycin, a macrolide antibiotic used clinically against malaria, kills parasites via two mechanisms: ‘delayed death’ by inhibiting the bacterium-like ribosomes of the apicoplast, and ‘quick-killing’ that kills rapidly across the entire blood stage development. METHODS: Here, 22 azithromycin analogues were explored for delayed death and quick-killing activities against P. falciparum (the most virulent human malaria) and P. knowlesi (a monkey parasite that frequently infects humans). RESULTS: Seventeen analogues showed improved quick-killing against both Plasmodium species, with up to 38 to 20-fold higher potency over azithromycin after less than 48 or 28 hours of treatment for P. falciparum and P. knowlesi, respectively. Quick-killing analogues maintained activity throughout the blood stage lifecycle, including ring stages of P. falciparum parasites (<12 hrs treatment) and were >5-fold more selective against P. falciparum than human cells. Isopentenyl pyrophosphate supplemented parasites that lacked an apicoplast were equally sensitive to quick-killing analogues, confirming that the quick killing activity of these drugs was not directed at the apicoplast. Further, activity against the related apicoplast containing parasite Toxoplasma gondii and the gram-positive bacterium Streptococcus pneumoniae did not show improvement over azithromycin, highlighting the specific improvement in antimalarial quick-killing activity. Metabolomic profiling of parasites subjected to the most potent compound showed a build-up of non-haemoglobin derived peptides that was similar to chloroquine, while also exhibiting accumulation of haemoglobin-derived peptides that was absent for chloroquine treatment. DISCUSSION: The azithromycin analogues characterised in this study expand the structural diversity over previously reported quick-killing compounds and provide new starting points to develop azithromycin analogues with quick-killing antimalarial activity.
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spelling pubmed-97485692022-12-15 Targeting malaria parasites with novel derivatives of azithromycin Burns, Amy L. Sleebs, Brad E. Gancheva, Maria McLean, Kimberley T. Siddiqui, Ghizal Venter, Henrietta Beeson, James G. O’Handley, Ryan Creek, Darren J. Ma, Shutao Frölich, Sonja Goodman, Christopher D. McFadden, Geoffrey I. Wilson, Danny W. Front Cell Infect Microbiol Cellular and Infection Microbiology INTRODUCTION: The spread of artemisinin resistant Plasmodium falciparum parasites is of global concern and highlights the need to identify new antimalarials for future treatments. Azithromycin, a macrolide antibiotic used clinically against malaria, kills parasites via two mechanisms: ‘delayed death’ by inhibiting the bacterium-like ribosomes of the apicoplast, and ‘quick-killing’ that kills rapidly across the entire blood stage development. METHODS: Here, 22 azithromycin analogues were explored for delayed death and quick-killing activities against P. falciparum (the most virulent human malaria) and P. knowlesi (a monkey parasite that frequently infects humans). RESULTS: Seventeen analogues showed improved quick-killing against both Plasmodium species, with up to 38 to 20-fold higher potency over azithromycin after less than 48 or 28 hours of treatment for P. falciparum and P. knowlesi, respectively. Quick-killing analogues maintained activity throughout the blood stage lifecycle, including ring stages of P. falciparum parasites (<12 hrs treatment) and were >5-fold more selective against P. falciparum than human cells. Isopentenyl pyrophosphate supplemented parasites that lacked an apicoplast were equally sensitive to quick-killing analogues, confirming that the quick killing activity of these drugs was not directed at the apicoplast. Further, activity against the related apicoplast containing parasite Toxoplasma gondii and the gram-positive bacterium Streptococcus pneumoniae did not show improvement over azithromycin, highlighting the specific improvement in antimalarial quick-killing activity. Metabolomic profiling of parasites subjected to the most potent compound showed a build-up of non-haemoglobin derived peptides that was similar to chloroquine, while also exhibiting accumulation of haemoglobin-derived peptides that was absent for chloroquine treatment. DISCUSSION: The azithromycin analogues characterised in this study expand the structural diversity over previously reported quick-killing compounds and provide new starting points to develop azithromycin analogues with quick-killing antimalarial activity. Frontiers Media S.A. 2022-11-30 /pmc/articles/PMC9748569/ /pubmed/36530422 http://dx.doi.org/10.3389/fcimb.2022.1063407 Text en Copyright © 2022 Burns, Sleebs, Gancheva, McLean, Siddiqui, Venter, Beeson, O’Handley, Creek, Ma, Frölich, Goodman, McFadden and Wilson https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cellular and Infection Microbiology
Burns, Amy L.
Sleebs, Brad E.
Gancheva, Maria
McLean, Kimberley T.
Siddiqui, Ghizal
Venter, Henrietta
Beeson, James G.
O’Handley, Ryan
Creek, Darren J.
Ma, Shutao
Frölich, Sonja
Goodman, Christopher D.
McFadden, Geoffrey I.
Wilson, Danny W.
Targeting malaria parasites with novel derivatives of azithromycin
title Targeting malaria parasites with novel derivatives of azithromycin
title_full Targeting malaria parasites with novel derivatives of azithromycin
title_fullStr Targeting malaria parasites with novel derivatives of azithromycin
title_full_unstemmed Targeting malaria parasites with novel derivatives of azithromycin
title_short Targeting malaria parasites with novel derivatives of azithromycin
title_sort targeting malaria parasites with novel derivatives of azithromycin
topic Cellular and Infection Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9748569/
https://www.ncbi.nlm.nih.gov/pubmed/36530422
http://dx.doi.org/10.3389/fcimb.2022.1063407
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