Harnessing cholesterol uptake of malaria parasites for therapeutic applications

Merryn Fraser; Blake Curtis; Patrick Phillips; Patrick A. Yates; Kwong Sum Lam; Otto Netzel; Giel G. van Dooren; Alyssa Ingmundson; Kai Matuschewski; Malcolm D. McLeod; Alexander G. Maier

doi:10.1038/s44321-024-00087-1

Harnessing cholesterol uptake of malaria parasites for therapeutic applications

Merryn Fraser, Blake Curtis, Patrick Phillips, Patrick A. Yates, Kwong Sum Lam, Otto Netzel, Giel G. van Dooren, Alyssa Ingmundson, Kai Matuschewski, Malcolm D. McLeod^*, Alexander G. Maier^*

^*Corresponding author for this work

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

Abstract

Parasites, such as the malaria parasite P. falciparum, are critically dependent on host nutrients. Interference with nutrient uptake can lead to parasite death and, therefore, serve as a successful treatment strategy. P. falciparum parasites cannot synthesise cholesterol, and instead source this lipid from the host. Here, we tested whether cholesterol uptake pathways could be ‘hijacked’ for optimal drug delivery to the intracellular parasite. We found that fluorescent cholesterol analogues were delivered from the extracellular environment to the intracellular parasite. We investigated the uptake and inhibitory effects of conjugate compounds, where proven antimalarial drugs (primaquine and artesunate) were attached to steroids that mimic the structure of cholesterol. These conjugated antimalarial drugs improved the inhibitory effects against multiple parasite lifecycle stages, multiple parasite species, and drug-resistant parasites, whilst also lowering the toxicity to human host cells. Steroids with introduced peroxides also displayed antimalarial activity. These results provide a proof-of-concept that cholesterol mimics can be developed as a drug delivery system against apicomplexan parasites with the potential to improve drug efficacy, increase therapeutic index, and defeat drug resistance.

Original language	English
Pages (from-to)	1515-1532
Number of pages	18
Journal	EMBO Molecular Medicine
Volume	16
Issue number	7
DOIs	https://doi.org/10.1038/s44321-024-00087-1
Publication status	Published - 15 Jul 2024

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title = "Harnessing cholesterol uptake of malaria parasites for therapeutic applications",

abstract = "Parasites, such as the malaria parasite P. falciparum, are critically dependent on host nutrients. Interference with nutrient uptake can lead to parasite death and, therefore, serve as a successful treatment strategy. P. falciparum parasites cannot synthesise cholesterol, and instead source this lipid from the host. Here, we tested whether cholesterol uptake pathways could be {\textquoteleft}hijacked{\textquoteright} for optimal drug delivery to the intracellular parasite. We found that fluorescent cholesterol analogues were delivered from the extracellular environment to the intracellular parasite. We investigated the uptake and inhibitory effects of conjugate compounds, where proven antimalarial drugs (primaquine and artesunate) were attached to steroids that mimic the structure of cholesterol. These conjugated antimalarial drugs improved the inhibitory effects against multiple parasite lifecycle stages, multiple parasite species, and drug-resistant parasites, whilst also lowering the toxicity to human host cells. Steroids with introduced peroxides also displayed antimalarial activity. These results provide a proof-of-concept that cholesterol mimics can be developed as a drug delivery system against apicomplexan parasites with the potential to improve drug efficacy, increase therapeutic index, and defeat drug resistance.",

keywords = "cholesterol, drug-delivery, drug-resistance, malaria, Plasmodium falciparum",

author = "Merryn Fraser and Blake Curtis and Patrick Phillips and Yates, {Patrick A.} and Lam, {Kwong Sum} and Otto Netzel and {van Dooren}, {Giel G.} and Alyssa Ingmundson and Kai Matuschewski and McLeod, {Malcolm D.} and Maier, {Alexander G.}",

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doi = "10.1038/s44321-024-00087-1",

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T1 - Harnessing cholesterol uptake of malaria parasites for therapeutic applications

AU - Fraser, Merryn

AU - Curtis, Blake

AU - Phillips, Patrick

AU - Yates, Patrick A.

AU - Lam, Kwong Sum

AU - Netzel, Otto

AU - van Dooren, Giel G.

AU - Ingmundson, Alyssa

AU - Matuschewski, Kai

AU - McLeod, Malcolm D.

AU - Maier, Alexander G.

N1 - Publisher Copyright: © The Author(s) 2024.

PY - 2024/7/15

Y1 - 2024/7/15

N2 - Parasites, such as the malaria parasite P. falciparum, are critically dependent on host nutrients. Interference with nutrient uptake can lead to parasite death and, therefore, serve as a successful treatment strategy. P. falciparum parasites cannot synthesise cholesterol, and instead source this lipid from the host. Here, we tested whether cholesterol uptake pathways could be ‘hijacked’ for optimal drug delivery to the intracellular parasite. We found that fluorescent cholesterol analogues were delivered from the extracellular environment to the intracellular parasite. We investigated the uptake and inhibitory effects of conjugate compounds, where proven antimalarial drugs (primaquine and artesunate) were attached to steroids that mimic the structure of cholesterol. These conjugated antimalarial drugs improved the inhibitory effects against multiple parasite lifecycle stages, multiple parasite species, and drug-resistant parasites, whilst also lowering the toxicity to human host cells. Steroids with introduced peroxides also displayed antimalarial activity. These results provide a proof-of-concept that cholesterol mimics can be developed as a drug delivery system against apicomplexan parasites with the potential to improve drug efficacy, increase therapeutic index, and defeat drug resistance.

AB - Parasites, such as the malaria parasite P. falciparum, are critically dependent on host nutrients. Interference with nutrient uptake can lead to parasite death and, therefore, serve as a successful treatment strategy. P. falciparum parasites cannot synthesise cholesterol, and instead source this lipid from the host. Here, we tested whether cholesterol uptake pathways could be ‘hijacked’ for optimal drug delivery to the intracellular parasite. We found that fluorescent cholesterol analogues were delivered from the extracellular environment to the intracellular parasite. We investigated the uptake and inhibitory effects of conjugate compounds, where proven antimalarial drugs (primaquine and artesunate) were attached to steroids that mimic the structure of cholesterol. These conjugated antimalarial drugs improved the inhibitory effects against multiple parasite lifecycle stages, multiple parasite species, and drug-resistant parasites, whilst also lowering the toxicity to human host cells. Steroids with introduced peroxides also displayed antimalarial activity. These results provide a proof-of-concept that cholesterol mimics can be developed as a drug delivery system against apicomplexan parasites with the potential to improve drug efficacy, increase therapeutic index, and defeat drug resistance.

KW - cholesterol

KW - drug-delivery

KW - drug-resistance

KW - malaria

KW - Plasmodium falciparum

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JO - EMBO Molecular Medicine

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ER -

Harnessing cholesterol uptake of malaria parasites for therapeutic applications

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