Anti-schistosomal activities of quinoxaline-containing compounds: From hit identification to lead optimisation

Schistosomiasis is a neglected disease of poverty that is caused by infection with blood fluke species contained within the genus Schistosoma. For the last 40 years, control of schistosomiasis in endemic regions has predominantly been facilitated by administration of a single drug, praziquantel. Due...

Descripción completa

Detalles Bibliográficos
Autores principales: Padalino, Gilda, El-Sakkary, Nelly, Liu, Lawrence J., Liu, Chenxi, Harte, Danielle S.G., Barnes, Rachel E., Sayers, Edward, Forde-Thomas, Josephine, Whiteland, Helen, Bassetto, Marcella, Ferla, Salvatore, Johnson, George, Jones, Arwyn T., Caffrey, Conor R., Chalmers, Iain, Brancale, Andrea, Hoffmann, Karl F.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Editions Scientifiques Elsevier 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8626775/
https://www.ncbi.nlm.nih.gov/pubmed/34536671
http://dx.doi.org/10.1016/j.ejmech.2021.113823
_version_ 1784606724514119680
author Padalino, Gilda
El-Sakkary, Nelly
Liu, Lawrence J.
Liu, Chenxi
Harte, Danielle S.G.
Barnes, Rachel E.
Sayers, Edward
Forde-Thomas, Josephine
Whiteland, Helen
Bassetto, Marcella
Ferla, Salvatore
Johnson, George
Jones, Arwyn T.
Caffrey, Conor R.
Chalmers, Iain
Brancale, Andrea
Hoffmann, Karl F.
author_facet Padalino, Gilda
El-Sakkary, Nelly
Liu, Lawrence J.
Liu, Chenxi
Harte, Danielle S.G.
Barnes, Rachel E.
Sayers, Edward
Forde-Thomas, Josephine
Whiteland, Helen
Bassetto, Marcella
Ferla, Salvatore
Johnson, George
Jones, Arwyn T.
Caffrey, Conor R.
Chalmers, Iain
Brancale, Andrea
Hoffmann, Karl F.
author_sort Padalino, Gilda
collection PubMed
description Schistosomiasis is a neglected disease of poverty that is caused by infection with blood fluke species contained within the genus Schistosoma. For the last 40 years, control of schistosomiasis in endemic regions has predominantly been facilitated by administration of a single drug, praziquantel. Due to limitations in this mono-chemotherapeutic approach for sustaining schistosomiasis control into the future, alternative anti-schistosomal compounds are increasingly being sought by the drug discovery community. Herein, we describe a multi-pronged, integrated strategy that led to the identification and further exploration of the quinoxaline core as a promising anti-schistosomal scaffold. Firstly, phenotypic screening of commercially available small molecules resulted in the identification of a moderately active hit compound against Schistosoma mansoni (1, EC(50) = 4.59 μM on schistosomula). Secondary exploration of the chemical space around compound 1 led to the identification of a quinoxaline-core containing, non-genotoxic lead (compound 22). Compound 22 demonstrated substantially improved activities on both intra-mammalian (EC(50) = 0.44 μM, 0.20 μM and 84.7 nM, on schistosomula, juvenile and adult worms, respectively) and intra-molluscan (sporocyst) S. mansoni lifecycle stages. Further medicinal chemistry optimisation of compound 22, resulting in the generation of 20 additional analogues, improved our understanding of the structure-activity relationship and resulted in considerable improvements in both anti-schistosome potency and selectivity (e.g. compound 30; EC(50) = 2.59 nM on adult worms; selectivity index compared to the HepG2 cell line = 348). Some derivatives of compound 22 (e.g. 31 and 33) also demonstrated significant activity against the two other medically important species, Schistosoma haematobium and Schistosoma japonicum. Further optimisation of this class of anti-schistosomal is ongoing and could lead to the development of an urgently needed alternative to praziquantel for assisting in schistosomiasis elimination strategies.
format Online
Article
Text
id pubmed-8626775
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Editions Scientifiques Elsevier
record_format MEDLINE/PubMed
spelling pubmed-86267752021-12-15 Anti-schistosomal activities of quinoxaline-containing compounds: From hit identification to lead optimisation Padalino, Gilda El-Sakkary, Nelly Liu, Lawrence J. Liu, Chenxi Harte, Danielle S.G. Barnes, Rachel E. Sayers, Edward Forde-Thomas, Josephine Whiteland, Helen Bassetto, Marcella Ferla, Salvatore Johnson, George Jones, Arwyn T. Caffrey, Conor R. Chalmers, Iain Brancale, Andrea Hoffmann, Karl F. Eur J Med Chem Article Schistosomiasis is a neglected disease of poverty that is caused by infection with blood fluke species contained within the genus Schistosoma. For the last 40 years, control of schistosomiasis in endemic regions has predominantly been facilitated by administration of a single drug, praziquantel. Due to limitations in this mono-chemotherapeutic approach for sustaining schistosomiasis control into the future, alternative anti-schistosomal compounds are increasingly being sought by the drug discovery community. Herein, we describe a multi-pronged, integrated strategy that led to the identification and further exploration of the quinoxaline core as a promising anti-schistosomal scaffold. Firstly, phenotypic screening of commercially available small molecules resulted in the identification of a moderately active hit compound against Schistosoma mansoni (1, EC(50) = 4.59 μM on schistosomula). Secondary exploration of the chemical space around compound 1 led to the identification of a quinoxaline-core containing, non-genotoxic lead (compound 22). Compound 22 demonstrated substantially improved activities on both intra-mammalian (EC(50) = 0.44 μM, 0.20 μM and 84.7 nM, on schistosomula, juvenile and adult worms, respectively) and intra-molluscan (sporocyst) S. mansoni lifecycle stages. Further medicinal chemistry optimisation of compound 22, resulting in the generation of 20 additional analogues, improved our understanding of the structure-activity relationship and resulted in considerable improvements in both anti-schistosome potency and selectivity (e.g. compound 30; EC(50) = 2.59 nM on adult worms; selectivity index compared to the HepG2 cell line = 348). Some derivatives of compound 22 (e.g. 31 and 33) also demonstrated significant activity against the two other medically important species, Schistosoma haematobium and Schistosoma japonicum. Further optimisation of this class of anti-schistosomal is ongoing and could lead to the development of an urgently needed alternative to praziquantel for assisting in schistosomiasis elimination strategies. Editions Scientifiques Elsevier 2021-12-15 /pmc/articles/PMC8626775/ /pubmed/34536671 http://dx.doi.org/10.1016/j.ejmech.2021.113823 Text en © 2021 The Author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Padalino, Gilda
El-Sakkary, Nelly
Liu, Lawrence J.
Liu, Chenxi
Harte, Danielle S.G.
Barnes, Rachel E.
Sayers, Edward
Forde-Thomas, Josephine
Whiteland, Helen
Bassetto, Marcella
Ferla, Salvatore
Johnson, George
Jones, Arwyn T.
Caffrey, Conor R.
Chalmers, Iain
Brancale, Andrea
Hoffmann, Karl F.
Anti-schistosomal activities of quinoxaline-containing compounds: From hit identification to lead optimisation
title Anti-schistosomal activities of quinoxaline-containing compounds: From hit identification to lead optimisation
title_full Anti-schistosomal activities of quinoxaline-containing compounds: From hit identification to lead optimisation
title_fullStr Anti-schistosomal activities of quinoxaline-containing compounds: From hit identification to lead optimisation
title_full_unstemmed Anti-schistosomal activities of quinoxaline-containing compounds: From hit identification to lead optimisation
title_short Anti-schistosomal activities of quinoxaline-containing compounds: From hit identification to lead optimisation
title_sort anti-schistosomal activities of quinoxaline-containing compounds: from hit identification to lead optimisation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8626775/
https://www.ncbi.nlm.nih.gov/pubmed/34536671
http://dx.doi.org/10.1016/j.ejmech.2021.113823
work_keys_str_mv AT padalinogilda antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT elsakkarynelly antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT liulawrencej antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT liuchenxi antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT hartedaniellesg antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT barnesrachele antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT sayersedward antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT fordethomasjosephine antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT whitelandhelen antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT bassettomarcella antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT ferlasalvatore antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT johnsongeorge antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT jonesarwynt antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT caffreyconorr antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT chalmersiain antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT brancaleandrea antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation
AT hoffmannkarlf antischistosomalactivitiesofquinoxalinecontainingcompoundsfromhitidentificationtoleadoptimisation

Ejemplares similares