Multistage and transmission-blocking targeted antimalarials discovered from the open-source MMV Pandemic Response Box

Reader, Janette; Watt, Mariëtte van der; Taylor, Dale; Manach, Claire Le; Mittal, Nimisha; Ottilie, Sabine; Theron, Anjo; Moyo, Phanankosi; Erlank, Erica; Nardini, Luisa; Venter, Nelius; Lauterbach, Sonja; Bezuidenhout, Belinda; Horatscheck, André; Heerden, Ashleigh van; Boyle, Grant A.; Calvo, David; Mancama, D; Coetzer, Thérèsa L.; Winzeler, Elizabeth A.; Duffy, James; Koekemoer, Lizette L.; Basarab, Gregory S.; Chibale, Kelly; Birkholtz, Lyn-Marié

doi:10.1101/2020.06.05.133405

Cited by 13 publications

(32 citation statements)

References 61 publications

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“…Here, we con rmed the dynamic yet stage-speci c nature of H3K36me2&3 (11) and delineate their roles in the transcriptional reprogramming occurring post-commitment in the gametocyte sexual stage of P. falciparum blood-stage development (34). Our chemical interrogation of P. falciparum HDMs supports these conclusions, highlights the importance of the dynamics of histone methylation for transcriptional control and links aberrant H3K36me2&3 patterns with the increased potency of Jumonji HDM inhibitors towards gametocytes reported before (38,65,66).…”

Section: Discussionsupporting

confidence: 68%

“…JIB-04 (pan-selective) and ML324 (targeting KDM4, PfJMJ3) resulted in the hypermethylation of both H3K36me2&3 relative to the untreated controls (36-to 89-fold, Fig. 5b, Figure S6A), similar to hypermethylation of H3K4me3 and H3K9me3 induced by JIB-04 and ML324 in asexual parasites and gametocytes, respectively (38,66). This hypermethylation was not observed for GSK-J4 (KDM6, H3K27me3 selective, (67) or PCPA-2 (targeting LSD1).…”

Section: Inhibition Of H3k36 Demethylation By Jib-04 Is Associated Wimentioning

confidence: 78%

“…To investigate the functional relevance of these enzymes for H3K36me2&3, we chemically interrogated HDM activity and determined the effects of this inhibition on H3K36 methylation levels on days associated with stage II gametocyte development. Jumonji HDM inhibitors with activity against gametocytes (38,65,66). JIB-04 (pan-selective) and ML324 (targeting KDM4, PfJMJ3) resulted in the hypermethylation of both H3K36me2&3 relative to the untreated controls (36-to 89-fold, Fig.…”

Section: Inhibition Of H3k36 Demethylation By Jib-04 Is Associated Wimentioning

confidence: 99%

“…In the asexual parasites, the inhibition of PfJMJ3 by JIB-04 results in transcriptional de-regulation (38). Since this inhibitor is signi cantly more potent towards the sexual stages (38,66), we were particularly interested in the transcriptional effects of JIB-04 in gametocytes since this inhibitor is signi cantly more active against the sexual stages. As such, we performed genome-wide transcriptional pro ling of JIB-04 activity on day 3 and 4 gametocytes each following 24 h treatment with JIB-04 (Additional le 3: Table S6).…”

Section: Inhibition Of H3k36 Demethylation By Jib-04 Is Associated Wimentioning

confidence: 99%

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H3K36 Methylation Reprograms Gene Expression to Drive Early Gametocyte Development in Plasmodium Falciparum

Connacher

Josling

Orchard

et al. 2021

Preprint

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Background: The Plasmodium sexual gametocyte stages are the only transmissible form of the malaria parasite and are thus responsible for the continued transmission of the disease. Gametocytes undergo extensive functional and morphological changes from commitment to maturity, directed by an equally extensive control program. Several interconnected mechanisms governing sexual commitment have been described. However, the processes that drive the subsequent differentiation and development of the gametocyte remain largely unexplored. Using chromatin immunoprecipitation followed by high-throughput sequencing we describe an association between H3K36 di- and tri-methylation (H3K36me2&3) and the global changes in the transcriptional program driving gametocyte development post-commitment. Results: Here, we show that in stage II gametocytes, H3K36me2&3 are associated with an active repression of genes involved in asexual proliferation and sexual commitment, linking H3K36me2&3 to the transition from early gametocyte differentiation to intermediate development. Specifically, we establish a link between H3K36me2&3 and the repression of genes that are upregulated during commitment once terminal differentiation renders their protein products obsolete in developing gametocytes, thereby securing an appropriate transcriptional environment for intermediate gametocyte development. Lastly, we associate the enhanced potency of JIB-04 in gametocytes with the inhibition of H3K36me2&3 demethylation and a disruption of normal transcriptional programs.Conclusions: Taken together, our results provide the first description of an association between global gene expression reprogramming and histone post-translational modifications during P. falciparum sexual development. In addition to fulfilling the same role in virulence gene regulation as in asexual parasites, the stage II gametocyte-specific abundance of H3K36me2/3 manifests as a largely interdependent enrichment of the two modifications targeted towards genes whose functions become obsolete in post-commitment gametocytes. This contrasts with the broad repression associated with wide-spread H3K36me2 occupancy in asexual parasites, highlighting H3K36me2/3 enrichment as a marker of directed transcriptional repression specific to early gametocytes. The importance of such histone methylation during gametocyte development is underscored by the transcriptional disruption associated with histone demethylase inhibition in P. falciparum gametocytes. By demonstrating the participation of H3K36me2&3 in gametocyte development, we provide a more thorough understanding of the link between epigenetic mechanisms and gene expression in the transmissible stages of the malaria parasite.

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Section: Discussionsupporting

confidence: 68%

Section: Inhibition Of H3k36 Demethylation By Jib-04 Is Associated Wimentioning

confidence: 78%

Section: Inhibition Of H3k36 Demethylation By Jib-04 Is Associated Wimentioning

confidence: 99%

Section: Inhibition Of H3k36 Demethylation By Jib-04 Is Associated Wimentioning

confidence: 99%

See 2 more Smart Citations

H3K36 Methylation Reprograms Gene Expression to Drive Early Gametocyte Development in Plasmodium Falciparum

Connacher

Josling

Orchard

et al. 2021

Preprint

Self Cite

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“…Alternative sources are the de novo screen of natural product libraries in medium-to high-throughput format. It is now clearly indicated that driving screens based on asexual stage potency may not identify transmission-blocking specific compounds and as such we recommend parallel screens against different parasite life cycle stages or at the start, screening driven primarily on the transmissible forms, after which activity against other stages can be determined for hits obtained [131,132]. For such natural product libraries, stringent go/no go criteria need to be defined, similar to screening any other small molecule libraries.…”

Section: Future Perspectivesmentioning

confidence: 99%

Natural Products: A Potential Source of Malaria Transmission Blocking Drugs?

et al. 2020

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The ability to block human-to-mosquito and mosquito-to-human transmission of Plasmodium parasites is fundamental to accomplish the ambitious goal of malaria elimination. The WHO currently recommends only primaquine as a transmission-blocking drug but its use is severely restricted by toxicity in some populations. New, safe and clinically effective transmission-blocking drugs therefore need to be discovered. While natural products have been extensively investigated for the development of chemotherapeutic antimalarial agents, their potential use as transmission-blocking drugs is comparatively poorly explored. Here, we provide a comprehensive summary of the activities of natural products (and their derivatives) of plant and microbial origins against sexual stages of Plasmodium parasites and the Anopheles mosquito vector. We identify the prevailing challenges and opportunities and suggest how these can be mitigated and/or exploited in an endeavor to expedite transmission-blocking drug discovery efforts from natural products.

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New Transmission‐Selective Antimalarial Agents through Hit‐to‐Lead Optimization of 2‐([1,1′‐Biphenyl]‐4‐carboxamido)benzoic Acid Derivatives

et al. 2022

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Malaria elimination requires multipronged approaches, including the application of antimalarial drugs able to block humanto-mosquito transmission of malaria parasites. The transmissible gametocytes of Plasmodium falciparum seem to be highly sensitive towards epidrugs, particularly those targeting demethylation of histone post-translational marks. Here, we report exploration of compounds from a chemical library generated during hit-to-lead optimization of inhibitors of the human histone lysine demethylase, KDM4B. Derivatives of 2-([1,1'biphenyl]-4-carboxamido) benzoic acid, around either the amide or a sulfonamide linker backbone (2-(arylcarbox-amido)benzoic acid, 2-carboxamide (arylsulfonamido)benzoic acid and N-(2-(1H-tetrazol-5-yl)phenyl)-arylcarboxamide), showed potent activity towards late-stage gametocytes (stage IV/V) of P. falciparum, with the most potent compound reaching single digit nanomolar activity. Structure-activity relationship trends were evident and frontrunner compounds also displayed microsomal stability and favourable solubility profiles. Simplified synthetic routes support further derivatization of these compounds for further development of these series as malaria transmission-blocking agents.[a] J. Reader, D.

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Multistage and transmission-blocking targeted antimalarials discovered from the open-source MMV Pandemic Response Box

Cited by 13 publications

References 61 publications

H3K36 Methylation Reprograms Gene Expression to Drive Early Gametocyte Development in Plasmodium Falciparum

H3K36 Methylation Reprograms Gene Expression to Drive Early Gametocyte Development in Plasmodium Falciparum

Natural Products: A Potential Source of Malaria Transmission Blocking Drugs?

New Transmission‐Selective Antimalarial Agents through Hit‐to‐Lead Optimization of 2‐([1,1′‐Biphenyl]‐4‐carboxamido)benzoic Acid Derivatives

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Multistage and transmission-blocking targeted antimalarials discovered from the open-source MMV Pandemic Response Box

Cited by 13 publications

References 61 publications

H3K36&nbsp;Methylation Reprograms Gene Expression to Drive Early Gametocyte Development in Plasmodium Falciparum

H3K36&nbsp;Methylation Reprograms Gene Expression to Drive Early Gametocyte Development in Plasmodium Falciparum

Natural Products: A Potential Source of Malaria Transmission Blocking Drugs?

New Transmission‐Selective Antimalarial Agents through Hit‐to‐Lead Optimization of 2‐([1,1′‐Biphenyl]‐4‐carboxamido)benzoic Acid Derivatives

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H3K36 Methylation Reprograms Gene Expression to Drive Early Gametocyte Development in Plasmodium Falciparum

H3K36 Methylation Reprograms Gene Expression to Drive Early Gametocyte Development in Plasmodium Falciparum