Activity refinement of aryl amino acetamides that target the P. falciparum STAR-related lipid transfer 1 protein

William Nguyen; Coralie Boulet; Madeline G. Dans; Katie Loi; Kate E. Jarman; Gabrielle M. Watson; Wai Hong Tham; Kate J. Fairhurst; Tomas Yeo; David A. Fidock; Sergio Wittlin; Mrittika Chowdury; Tania F. de Koning-Ward; Gong Chen; Dandan Yan; Susan A. Charman; Delphine Baud; Stephen Brand; Paul F. Jackson; Alan F. Cowman; Paul R. Gilson; Brad E. Sleebs

doi:10.1016/j.ejmech.2024.116354

Activity refinement of aryl amino acetamides that target the P. falciparum STAR-related lipid transfer 1 protein

William Nguyen, Coralie Boulet, Madeline G. Dans, Katie Loi, Kate E. Jarman, Gabrielle M. Watson, Wai Hong Tham, Kate J. Fairhurst, Tomas Yeo, David A. Fidock, Sergio Wittlin, Mrittika Chowdury, Tania F. de Koning-Ward, Gong Chen, Dandan Yan, Susan A. Charman, Delphine Baud, Stephen Brand, Paul F. Jackson, Alan F. CowmanPaul R. Gilson, Brad E. Sleebs

Centre for Drug Candidate Optimisation

Research output: Contribution to journal › Article › Research › peer-review

7 Citations (Scopus)

Abstract

Malaria is a devastating disease that causes significant morbidity worldwide. The development of new antimalarial chemotypes is urgently needed because of the emergence of resistance to frontline therapies. Independent phenotypic screening campaigns against the Plasmodium asexual parasite, including our own, identified the aryl amino acetamide hit scaffold. In a prior study, we identified the STAR-related lipid transfer protein (PfSTART1) as the molecular target of this antimalarial chemotype. In this study, we combined structural elements from the different aryl acetamide hit subtypes and explored the structure-activity relationship. It was shown that the inclusion of an endocyclic nitrogen, to generate the tool compound WJM-715, improved aqueous solubility and modestly improved metabolic stability in rat hepatocytes. Metabolic stability in human liver microsomes remains a challenge for future development of the aryl acetamide class, which was underscored by modest systemic exposure and a short half-life in mice. The optimized aryl acetamide analogs were cross resistant to parasites with mutations in PfSTART1, but not to other drug-resistant mutations, and showed potent binding to recombinant PfSTART1 by biophysical analysis, further supporting PfSTART1 as the likely molecular target. The optimized aryl acetamide analogue, WJM-715 will be a useful tool for further investigating the druggability of PfSTART1 across the lifecycle of the malaria parasite.

Original language	English
Article number	116354
Number of pages	19
Journal	European Journal of Medicinal Chemistry
Volume	270
DOIs	https://doi.org/10.1016/j.ejmech.2024.116354
Publication status	Published - 15 Apr 2024

Keywords

Antimalarial
Aryl amino acetamide
Malaria
Plasmodium
STAR lipid transfer

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.ejmech.2024.116354Licence: CC BY

Cite this

Nguyen, W., Boulet, C., Dans, M. G., Loi, K., Jarman, K. E., Watson, G. M., Tham, W. H., Fairhurst, K. J., Yeo, T., Fidock, D. A., Wittlin, S., Chowdury, M., de Koning-Ward, T. F., Chen, G., Yan, D., Charman, S. A., Baud, D., Brand, S., Jackson, P. F., ... Sleebs, B. E. (2024). Activity refinement of aryl amino acetamides that target the P. falciparum STAR-related lipid transfer 1 protein. European Journal of Medicinal Chemistry, 270, Article 116354. https://doi.org/10.1016/j.ejmech.2024.116354

@article{75a90757f89644cfbb9cef0a1d7134b6,

title = "Activity refinement of aryl amino acetamides that target the P. falciparum STAR-related lipid transfer 1 protein",

abstract = "Malaria is a devastating disease that causes significant morbidity worldwide. The development of new antimalarial chemotypes is urgently needed because of the emergence of resistance to frontline therapies. Independent phenotypic screening campaigns against the Plasmodium asexual parasite, including our own, identified the aryl amino acetamide hit scaffold. In a prior study, we identified the STAR-related lipid transfer protein (PfSTART1) as the molecular target of this antimalarial chemotype. In this study, we combined structural elements from the different aryl acetamide hit subtypes and explored the structure-activity relationship. It was shown that the inclusion of an endocyclic nitrogen, to generate the tool compound WJM-715, improved aqueous solubility and modestly improved metabolic stability in rat hepatocytes. Metabolic stability in human liver microsomes remains a challenge for future development of the aryl acetamide class, which was underscored by modest systemic exposure and a short half-life in mice. The optimized aryl acetamide analogs were cross resistant to parasites with mutations in PfSTART1, but not to other drug-resistant mutations, and showed potent binding to recombinant PfSTART1 by biophysical analysis, further supporting PfSTART1 as the likely molecular target. The optimized aryl acetamide analogue, WJM-715 will be a useful tool for further investigating the druggability of PfSTART1 across the lifecycle of the malaria parasite.",

keywords = "Antimalarial, Aryl amino acetamide, Malaria, Plasmodium, STAR lipid transfer",

author = "William Nguyen and Coralie Boulet and Dans, \{Madeline G.\} and Katie Loi and Jarman, \{Kate E.\} and Watson, \{Gabrielle M.\} and Tham, \{Wai Hong\} and Fairhurst, \{Kate J.\} and Tomas Yeo and Fidock, \{David A.\} and Sergio Wittlin and Mrittika Chowdury and \{de Koning-Ward\}, \{Tania F.\} and Gong Chen and Dandan Yan and Charman, \{Susan A.\} and Delphine Baud and Stephen Brand and Jackson, \{Paul F.\} and Cowman, \{Alan F.\} and Gilson, \{Paul R.\} and Sleebs, \{Brad E.\}",

note = "Funding Information: The authors declare the following financial interests/personal relationships which may be considered as potential competing interests:Brad Sleebs reports financial support was provided by National Health and Medical Research Council. Susan Charman reports financial support was provided by National Health and Medical Research Council. Paul Gilson reports financial support was provided by National Health and Medical Research Council. Alan Cowman reports financial support was provided by National Health and Medical Research Council. William Nguyen reports financial support was provided by National Health and Medical Research Council. Tania de Koning Ward reports financial support was provided by National Health and Medical Research Council. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper.This work was funded by the National Health and Medical Research Council of Australia (Development Grant 1135421 to B.E.S. and A.F.C. Ideas Grant 2001073 to W.N. and P.R.G, and Synergy Grant 1185354 to S.A.C, P. R. G. and T.F dK-W), the Victorian State Government Operational Infrastructure Support and Australian Government NHMRC IRIISS. B.E.S. and D.A.F. acknowledge the support from the Medicines for Malaria Venture. We thank the Australian Lifeblood for the provision of fresh red blood cells. We thank Christian Scheurer for technical assistance with the P. falciparum in vitro studies performed with the panel of clinical isolates and lab-generated resistant strains. A.F.C. is a Howard Hughes International Scholar and an Australia Fellow of the NHMRC. B.E.S. is a Corin Centenary Fellow. Funding Information: This work was funded by the National Health and Medical Research Council of Australia (Development Grant 1135421 to B.E.S. and A.F.C. Ideas Grant 2001073 to W.N. and P.R.G, and Synergy Grant 1185354 to S.A.C, P. R. G. and T.F dK-W), the Victorian State Government Operational Infrastructure Support and Australian Government NHMRC IRIISS . B.E.S. and D.A.F. acknowledge the support from the Medicines for Malaria Venture . We thank the Australian Lifeblood for the provision of fresh red blood cells. We thank Christian Scheurer for technical assistance with the P. falciparum in vitro studies performed with the panel of clinical isolates and lab-generated resistant strains. A.F.C. is a Howard Hughes International Scholar and an Australia Fellow of the NHMRC. B.E.S. is a Corin Centenary Fellow. Publisher Copyright: {\textcopyright} 2024 The Authors",

year = "2024",

month = apr,

day = "15",

doi = "10.1016/j.ejmech.2024.116354",

language = "English",

volume = "270",

journal = "European Journal of Medicinal Chemistry",

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Nguyen, W, Boulet, C, Dans, MG, Loi, K, Jarman, KE, Watson, GM, Tham, WH, Fairhurst, KJ, Yeo, T, Fidock, DA, Wittlin, S, Chowdury, M, de Koning-Ward, TF, Chen, G, Yan, D, Charman, SA, Baud, D, Brand, S, Jackson, PF, Cowman, AF, Gilson, PR & Sleebs, BE 2024, 'Activity refinement of aryl amino acetamides that target the P. falciparum STAR-related lipid transfer 1 protein', European Journal of Medicinal Chemistry, vol. 270, 116354. https://doi.org/10.1016/j.ejmech.2024.116354

TY - JOUR

T1 - Activity refinement of aryl amino acetamides that target the P. falciparum STAR-related lipid transfer 1 protein

AU - Nguyen, William

AU - Boulet, Coralie

AU - Dans, Madeline G.

AU - Loi, Katie

AU - Jarman, Kate E.

AU - Watson, Gabrielle M.

AU - Tham, Wai Hong

AU - Fairhurst, Kate J.

AU - Yeo, Tomas

AU - Fidock, David A.

AU - Wittlin, Sergio

AU - Chowdury, Mrittika

AU - de Koning-Ward, Tania F.

AU - Chen, Gong

AU - Yan, Dandan

AU - Charman, Susan A.

AU - Baud, Delphine

AU - Brand, Stephen

AU - Jackson, Paul F.

AU - Cowman, Alan F.

AU - Gilson, Paul R.

AU - Sleebs, Brad E.

N1 - Funding Information: The authors declare the following financial interests/personal relationships which may be considered as potential competing interests:Brad Sleebs reports financial support was provided by National Health and Medical Research Council. Susan Charman reports financial support was provided by National Health and Medical Research Council. Paul Gilson reports financial support was provided by National Health and Medical Research Council. Alan Cowman reports financial support was provided by National Health and Medical Research Council. William Nguyen reports financial support was provided by National Health and Medical Research Council. Tania de Koning Ward reports financial support was provided by National Health and Medical Research Council. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper.This work was funded by the National Health and Medical Research Council of Australia (Development Grant 1135421 to B.E.S. and A.F.C. Ideas Grant 2001073 to W.N. and P.R.G, and Synergy Grant 1185354 to S.A.C, P. R. G. and T.F dK-W), the Victorian State Government Operational Infrastructure Support and Australian Government NHMRC IRIISS. B.E.S. and D.A.F. acknowledge the support from the Medicines for Malaria Venture. We thank the Australian Lifeblood for the provision of fresh red blood cells. We thank Christian Scheurer for technical assistance with the P. falciparum in vitro studies performed with the panel of clinical isolates and lab-generated resistant strains. A.F.C. is a Howard Hughes International Scholar and an Australia Fellow of the NHMRC. B.E.S. is a Corin Centenary Fellow. Funding Information: This work was funded by the National Health and Medical Research Council of Australia (Development Grant 1135421 to B.E.S. and A.F.C. Ideas Grant 2001073 to W.N. and P.R.G, and Synergy Grant 1185354 to S.A.C, P. R. G. and T.F dK-W), the Victorian State Government Operational Infrastructure Support and Australian Government NHMRC IRIISS . B.E.S. and D.A.F. acknowledge the support from the Medicines for Malaria Venture . We thank the Australian Lifeblood for the provision of fresh red blood cells. We thank Christian Scheurer for technical assistance with the P. falciparum in vitro studies performed with the panel of clinical isolates and lab-generated resistant strains. A.F.C. is a Howard Hughes International Scholar and an Australia Fellow of the NHMRC. B.E.S. is a Corin Centenary Fellow. Publisher Copyright: © 2024 The Authors

PY - 2024/4/15

Y1 - 2024/4/15

N2 - Malaria is a devastating disease that causes significant morbidity worldwide. The development of new antimalarial chemotypes is urgently needed because of the emergence of resistance to frontline therapies. Independent phenotypic screening campaigns against the Plasmodium asexual parasite, including our own, identified the aryl amino acetamide hit scaffold. In a prior study, we identified the STAR-related lipid transfer protein (PfSTART1) as the molecular target of this antimalarial chemotype. In this study, we combined structural elements from the different aryl acetamide hit subtypes and explored the structure-activity relationship. It was shown that the inclusion of an endocyclic nitrogen, to generate the tool compound WJM-715, improved aqueous solubility and modestly improved metabolic stability in rat hepatocytes. Metabolic stability in human liver microsomes remains a challenge for future development of the aryl acetamide class, which was underscored by modest systemic exposure and a short half-life in mice. The optimized aryl acetamide analogs were cross resistant to parasites with mutations in PfSTART1, but not to other drug-resistant mutations, and showed potent binding to recombinant PfSTART1 by biophysical analysis, further supporting PfSTART1 as the likely molecular target. The optimized aryl acetamide analogue, WJM-715 will be a useful tool for further investigating the druggability of PfSTART1 across the lifecycle of the malaria parasite.

AB - Malaria is a devastating disease that causes significant morbidity worldwide. The development of new antimalarial chemotypes is urgently needed because of the emergence of resistance to frontline therapies. Independent phenotypic screening campaigns against the Plasmodium asexual parasite, including our own, identified the aryl amino acetamide hit scaffold. In a prior study, we identified the STAR-related lipid transfer protein (PfSTART1) as the molecular target of this antimalarial chemotype. In this study, we combined structural elements from the different aryl acetamide hit subtypes and explored the structure-activity relationship. It was shown that the inclusion of an endocyclic nitrogen, to generate the tool compound WJM-715, improved aqueous solubility and modestly improved metabolic stability in rat hepatocytes. Metabolic stability in human liver microsomes remains a challenge for future development of the aryl acetamide class, which was underscored by modest systemic exposure and a short half-life in mice. The optimized aryl acetamide analogs were cross resistant to parasites with mutations in PfSTART1, but not to other drug-resistant mutations, and showed potent binding to recombinant PfSTART1 by biophysical analysis, further supporting PfSTART1 as the likely molecular target. The optimized aryl acetamide analogue, WJM-715 will be a useful tool for further investigating the druggability of PfSTART1 across the lifecycle of the malaria parasite.

KW - Antimalarial

KW - Aryl amino acetamide

KW - Malaria

KW - Plasmodium

KW - STAR lipid transfer

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U2 - 10.1016/j.ejmech.2024.116354

DO - 10.1016/j.ejmech.2024.116354

M3 - Article

AN - SCOPUS:85189082857

SN - 0223-5234

VL - 270

JO - European Journal of Medicinal Chemistry

JF - European Journal of Medicinal Chemistry

M1 - 116354

ER -

Activity refinement of aryl amino acetamides that target the P. falciparum STAR-related lipid transfer 1 protein

Abstract

Keywords

UN SDGs

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Multidisciplinary catalyst to discover and progress novel antimalarial drugs

Cite this

Activity refinement of aryl amino acetamides that target the P. falciparum STAR-related lipid transfer 1 protein

Abstract

Keywords

UN SDGs

Access to Document

Other files and links

Projects

Multidisciplinary catalyst to discover and progress novel antimalarial drugs

Cite this