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1. Diverse evolutionary pathways challenge the use of collateral sensitivity as a strategy to suppress resistance.

Author

Mandt, Rebecca, Luth, Madeline, Tye, Mark, Mazitschek, Ralph, Ottilie, Sabine, Lafuente-Monasterio, Maria, Gamo, Francisco, Wirth, Dyann, Lukens, Amanda, and Winzeler, Elizabeth

Subjects
P. falciparum, Plasmodium falciparum, dihydroorotate dehydrogenase, drug resistance, evolutionary biology, infectious disease, malaria, microbiology, Animals, Humans, Dihydroorotate Dehydrogenase, Malaria, Falciparum, Oxidoreductases Acting on CH-CH Group Donors, Plasmodium falciparum, Antimalarials, DNA Copy Number Variations, Drug Collateral Sensitivity, Parasites
Abstract

Drug resistance remains a major obstacle to malaria control and eradication efforts, necessitating the development of novel therapeutic strategies to treat this disease. Drug combinations based on collateral sensitivity, wherein resistance to one drug causes increased sensitivity to the partner drug, have been proposed as an evolutionary strategy to suppress the emergence of resistance in pathogen populations. In this study, we explore collateral sensitivity between compounds targeting the Plasmodium dihydroorotate dehydrogenase (DHODH). We profiled the cross-resistance and collateral sensitivity phenotypes of several DHODH mutant lines to a diverse panel of DHODH inhibitors. We focus on one compound, TCMDC-125334, which was active against all mutant lines tested, including the DHODH C276Y line, which arose in selections with the clinical candidate DSM265. In six selections with TCMDC-125334, the most common mechanism of resistance to this compound was copy number variation of the dhodh locus, although we did identify one mutation, DHODH I263S, which conferred resistance to TCMDC-125334 but not DSM265. We found that selection of the DHODH C276Y mutant with TCMDC-125334 yielded additional genetic changes in the dhodh locus. These double mutant parasites exhibited decreased sensitivity to TCMDC-125334 and were highly resistant to DSM265. Finally, we tested whether collateral sensitivity could be exploited to suppress the emergence of resistance in the context of combination treatment by exposing wildtype parasites to both DSM265 and TCMDC-125334 simultaneously. This selected for parasites with a DHODH V532A mutation which were cross-resistant to both compounds and were as fit as the wildtype parent in vitro. The emergence of these cross-resistant, evolutionarily fit parasites highlights the mutational flexibility of the DHODH enzyme.

Published
2023

2. Human nuclear hormone receptor activity contributes to malaria parasite liver stage development.

Author

Mittal, Nimisha, Davis, Chadwick, McLean, Peter, Calla, Jaeson, Godinez-Macias, Karla, Gardner, Alison, Healey, David, Orjuela-Sanchez, Pamela, Ottilie, Sabine, Chong, Yolanda, Gibson, Christopher, and Winzeler, Elizabeth

Subjects
Plasmodium, drug discovery, malaria, nuclear hormone receptors, phenotypic screening, siRNA, Animals, Humans, Hepatocytes, Liver, Malaria, Parasites, Plasmodium berghei
Abstract

Chemical genetic approaches have had a transformative impact on discovery of drug targets for malaria but have primarily been used for parasite targets. To identify human pathways required for intrahepatic development of parasite, we implemented multiplex cytological profiling of malaria infected hepatocytes treated with liver stage active compounds. Some compounds, including MMV1088447 and MMV1346624, exhibited profiles similar to cells treated with nuclear hormone receptor (NHR) agonist/antagonists. siRNAs targeting human NHRs, or their signaling partners identified eight genes that were critical for Plasmodium berghei infection. Knockdown of NR1D2, a host NHR, significantly impaired parasite growth by downregulation of host lipid metabolism. Importantly, treatment with MMV1088447 and MMV1346624 but not other antimalarials, phenocopied the lipid metabolism defect of NR1D2 knockdown. Our data underlines the use of high-content imaging for host-cellular pathway deconvolution, highlights host lipid metabolism as a drug-able human pathway and provides new chemical biology tools for studying host-parasite interactions.

Published
2023

3. Development of Potent and Highly Selective Epoxyketone‐Based Plasmodium Proteasome Inhibitors

Author

Almaliti, Jehad, Fajtová, Pavla, Calla, Jaeson, LaMonte, Gregory M, Feng, Mudong, Rocamora, Frances, Ottilie, Sabine, Glukhov, Evgenia, Boura, Evzen, Suhandynata, Raymond T, Momper, Jeremiah D, Gilson, Michael K, Winzeler, Elizabeth A, Gerwick, William H, and O'Donoghue, Anthony J

Subjects
Chemical Sciences, Orphan Drug, Rare Diseases, Vector-Borne Diseases, Infectious Diseases, Malaria, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Infection, Good Health and Well Being, Mice, Animals, Humans, Proteasome Inhibitors, Proteasome Endopeptidase Complex, Plasmodium, Plasmodium falciparum, Antimalarials, epoxyketone, inhibition, malaria, plasmodium, proteasome, General Chemistry, Chemical sciences
Abstract

Here, we present remarkable epoxyketone-based proteasome inhibitors with low nanomolar in vitro potency for blood-stage Plasmodium falciparum and low cytotoxicity for human cells. Our best compound has more than 2,000-fold greater selectivity for erythrocytic-stage P. falciparum over HepG2 and H460 cells, which is largely driven by the accommodation of the parasite proteasome for a D-amino acid in the P3 position and the preference for a difluorobenzyl group in the P1 position. We isolated the proteasome from P. falciparum cell extracts and determined that the best compound is 171-fold more potent at inhibiting the β5 subunit of P. falciparum proteasome when compared to the same subunit of the human constitutive proteasome. These compounds also significantly reduce parasitemia in a P. berghei mouse infection model and prolong survival of animals by an average of 6 days. The current epoxyketone inhibitors are ideal starting compounds for orally bioavailable anti-malarial drugs.

Published
2023

4. Cytoplasmic isoleucyl tRNA synthetase as an attractive multistage antimalarial drug target

Author

Istvan, Eva S, Guerra, Francisco, Abraham, Matthew, Huang, Kuo-Sen, Rocamora, Frances, Zhao, Haoshuang, Xu, Lan, Pasaje, Charisse, Kumpornsin, Krittikorn, Luth, Madeline R, Cui, Haissi, Yang, Tuo, Palomo Diaz, Sara, Gomez-Lorenzo, Maria G, Qahash, Tarrick, Mittal, Nimisha, Ottilie, Sabine, Niles, Jacquin, Lee, Marcus CS, Llinas, Manuel, Kato, Nobutaka, Okombo, John, Fidock, David A, Schimmel, Paul, Gamo, Francisco Javier, Goldberg, Daniel E, and Winzeler, Elizabeth A

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Genetics, Vector-Borne Diseases, Infectious Diseases, Malaria, Orphan Drug, Rare Diseases, Infection, Good Health and Well Being, Humans, Antimalarials, Isoleucine-tRNA Ligase, Plasmodium falciparum, Malaria, Falciparum, Drug Resistance, Biological Sciences, Medical and Health Sciences, Medical biotechnology, Biomedical engineering
Abstract

Development of antimalarial compounds into clinical candidates remains costly and arduous without detailed knowledge of the target. As resistance increases and treatment options at various stages of disease are limited, it is critical to identify multistage drug targets that are readily interrogated in biochemical assays. Whole-genome sequencing of 18 parasite clones evolved using thienopyrimidine compounds with submicromolar, rapid-killing, pan-life cycle antiparasitic activity showed that all had acquired mutations in the P. falciparum cytoplasmic isoleucyl tRNA synthetase (cIRS). Engineering two of the mutations into drug-naïve parasites recapitulated the resistance phenotype, and parasites with conditional knockdowns of cIRS became hypersensitive to two thienopyrimidines. Purified recombinant P. vivax cIRS inhibition, cross-resistance, and biochemical assays indicated a noncompetitive, allosteric binding site that is distinct from that of known cIRS inhibitors mupirocin and reveromycin A. Our data show that Plasmodium cIRS is an important chemically and genetically validated target for next-generation medicines for malaria.

Published
2023

5. The anticancer human mTOR inhibitor sapanisertib potently inhibits multiple Plasmodium kinases and life cycle stages.

Author

Arendse, Lauren, Murithi, James, Qahash, Tarrick, Pasaje, Charisse, Godoy, Luiz, Dey, Sumanta, Gibhard, Liezl, Ghidelli-Disse, Sonja, Drewes, Gerard, Bantscheff, Marcus, Lafuente-Monasterio, Maria, Fienberg, Stephen, Wambua, Lynn, Gachuhi, Samuel, Coertzen, Dina, van der Watt, Mariëtte, Reader, Janette, Aswat, Ayesha, Erlank, Erica, Venter, Nelius, Mittal, Nimisha, Luth, Madeline, Ottilie, Sabine, Winzeler, Elizabeth, Koekemoer, Lizette, Birkholtz, Lyn-Marie, Niles, Jacquin, Llinás, Manuel, Fidock, David, and Chibale, Kelly

Subjects
Animals, Humans, Antimalarials, Plasmodium falciparum, MTOR Inhibitors, 1-Phosphatidylinositol 4-Kinase, Guanosine Monophosphate, Life Cycle Stages, TOR Serine-Threonine Kinases, Plasmodium, Sirolimus, Mammals
Abstract

Compounds acting on multiple targets are critical to combating antimalarial drug resistance. Here, we report that the human mammalian target of rapamycin (mTOR) inhibitor sapanisertib has potent prophylactic liver stage activity, in vitro and in vivo asexual blood stage (ABS) activity, and transmission-blocking activity against the protozoan parasite Plasmodium spp. Chemoproteomics studies revealed multiple potential Plasmodium kinase targets, and potent inhibition of Plasmodium phosphatidylinositol 4-kinase type III beta (PI4Kβ) and cyclic guanosine monophosphate-dependent protein kinase (PKG) was confirmed in vitro. Conditional knockdown of PI4Kβ in ABS cultures modulated parasite sensitivity to sapanisertib, and laboratory-generated P. falciparum sapanisertib resistance was mediated by mutations in PI4Kβ. Parasite metabolomic perturbation profiles associated with sapanisertib and other known PI4Kβ and/or PKG inhibitors revealed similarities and differences between chemotypes, potentially caused by sapanisertib targeting multiple parasite kinases. The multistage activity of sapanisertib and its in vivo antimalarial efficacy, coupled with potent inhibition of at least two promising drug targets, provides an opportunity to reposition this pyrazolopyrimidine for malaria.

Published
2022

6. Reaction hijacking of tyrosine tRNA synthetase as a new whole-of-life-cycle antimalarial strategy.

Author

Xie, Stanley, Metcalfe, Riley, Dunn, Elyse, Morton, Craig, Huang, Shih-Chung, Puhalovich, Tanya, Du, Yawei, Wittlin, Sergio, Nie, Shuai, Luth, Madeline, Ma, Liting, Kim, Mi-Sook, Pasaje, Charisse, Kumpornsin, Krittikorn, Giannangelo, Carlo, Houghton, Fiona, Churchyard, Alisje, Famodimu, Mufuliat, Barry, Daniel, Gillett, David, Dey, Sumanta, Kosasih, Clara, Newman, William, Niles, Jacquin, Lee, Marcus, Baum, Jake, Ottilie, Sabine, Winzeler, Elizabeth, Creek, Darren, Williamson, Nicholas, Parker, Michael, Brand, Stephen, Langston, Steven, Dick, Lawrence, Griffin, Michael, Gould, Alexandra, and Tilley, Leann

Subjects
Adenosine, Animals, Antimalarials, Crystallography, X-Ray, Humans, Malaria, Falciparum, Mice, Molecular Targeted Therapy, Plasmodium falciparum, Protein Biosynthesis, Protein Conformation, Protozoan Proteins, Sulfonic Acids, Tyrosine-tRNA Ligase
Abstract

Aminoacyl transfer RNA (tRNA) synthetases (aaRSs) are attractive drug targets, and we present class I and II aaRSs as previously unrecognized targets for adenosine 5-monophosphate-mimicking nucleoside sulfamates. The target enzyme catalyzes the formation of an inhibitory amino acid-sulfamate conjugate through a reaction-hijacking mechanism. We identified adenosine 5-sulfamate as a broad-specificity compound that hijacks a range of aaRSs and ML901 as a specific reagent a specific reagent that hijacks a single aaRS in the malaria parasite Plasmodium falciparum, namely tyrosine RS (PfYRS). ML901 exerts whole-life-cycle-killing activity with low nanomolar potency and single-dose efficacy in a mouse model of malaria. X-ray crystallographic studies of plasmodium and human YRSs reveal differential flexibility of a loop over the catalytic site that underpins differential susceptibility to reaction hijacking by ML901.

Published
2022

7. The Plasmodium falciparum ABC transporter ABCI3 confers parasite strain-dependent pleiotropic antimalarial drug resistance.

Author

Murithi, James, Deni, Ioanna, Pasaje, Charisse, Okombo, John, Bridgford, Jessica, Gnädig, Nina, Edwards, Rachel, Yeo, Tomas, Mok, Sachel, Burkhard, Anna, Coburn-Flynn, Olivia, Istvan, Eva, Sakata-Kato, Tomoyo, Gomez-Lorenzo, Maria, Cowell, Annie, Wicht, Kathryn, Le Manach, Claire, Kalantarov, Gavreel, Dey, Sumanta, Duffey, Maëlle, Laleu, Benoît, Lukens, Amanda, Ottilie, Sabine, Vanaerschot, Manu, Trakht, Ilya, Gamo, Francisco-Javier, Wirth, Dyann, Goldberg, Daniel, Odom John, Audrey, Chibale, Kelly, Winzeler, Elizabeth, Niles, Jacquin, and Fidock, David

Subjects
ABCI3, CRISPR/Cas9, Plasmodium falciparum malaria, biphasic dose-response curves, cellular accumulation assays, conditional knockdowns, copy-number variations, heme fractionation, pfcrt, ATP-Binding Cassette Transporters, Animals, Antimalarials, Folic Acid Antagonists, Heme, Malaria, Falciparum, Membrane Transport Proteins, Parasites, Plasmodium falciparum, Protozoan Proteins, Quinolines
Abstract

Widespread Plasmodium falciparum resistance to first-line antimalarials underscores the vital need to develop compounds with novel modes of action and identify new druggable targets. Here, we profile five compounds that potently inhibit P. falciparum asexual blood stages. Resistance selection studies with three carboxamide-containing compounds, confirmed by gene editing and conditional knockdowns, identify point mutations in the parasite transporter ABCI3 as the primary mediator of resistance. Selection studies with imidazopyridine or quinoline-carboxamide compounds also yield changes in ABCI3, this time through gene amplification. Imidazopyridine mode of action is attributed to inhibition of heme detoxification, as evidenced by cellular accumulation and heme fractionation assays. For the copy-number variation-selecting imidazopyridine and quinoline-carboxamide compounds, we find that resistance, manifesting as a biphasic concentration-response curve, can independently be mediated by mutations in the chloroquine resistance transporter PfCRT. These studies reveal the interconnectedness of P. falciparum transporters in overcoming drug pressure in different parasite strains.

Published
2022

8. Chemogenomics identifies acetyl-coenzyme A synthetase as a target for malaria treatment and prevention.

Author

Summers, Robert, Pasaje, Charisse, Pisco, Joao, Striepen, Josefine, Luth, Madeline, Kumpornsin, Krittikorn, Carpenter, Emma, Munro, Justin, Lin, De, Plater, Andrew, Punekar, Avinash, Shepherd, Andrew, Shepherd, Sharon, Vanaerschot, Manu, Murithi, James, Rubiano, Kelly, Akidil, Aslı, Ottilie, Sabine, Mittal, Nimisha, Dilmore, A, Won, Madalyn, Mandt, Rebecca, McGowen, Kerry, Owen, Edward, Walpole, Chris, Llinás, Manuel, Lee, Marcus, Fidock, David, Gilbert, Ian, Wirth, Dyann, Niles, Jacquin, Baragaña, Beatriz, Lukens, Amanda, and Winzeler, Elizabeth

Subjects
Plasmodium falciparum, acetyl-CoA synthetase, antimalarial, drug development, drug target identification, histone acetylation, malaria, mechanism of action, Acetate-CoA Ligase, Antimalarials, Enzyme Inhibitors, Humans, Malaria, Models, Molecular, Molecular Structure, Parasitic Sensitivity Tests, Plasmodium falciparum
Abstract

We identify the Plasmodium falciparum acetyl-coenzyme A synthetase (PfAcAS) as a druggable target, using genetic and chemical validation. In vitro evolution of resistance with two antiplasmodial drug-like compounds (MMV019721 and MMV084978) selects for mutations in PfAcAS. Metabolic profiling of compound-treated parasites reveals changes in acetyl-CoA levels for both compounds. Genome editing confirms that mutations in PfAcAS are sufficient to confer resistance. Knockdown studies demonstrate that PfAcAS is essential for asexual growth, and partial knockdown induces hypersensitivity to both compounds. In vitro biochemical assays using recombinantly expressed PfAcAS validates that MMV019721 and MMV084978 directly inhibit the enzyme by preventing CoA and acetate binding, respectively. Immunolocalization studies reveal that PfAcAS is primarily localized to the nucleus. Functional studies demonstrate inhibition of histone acetylation in compound-treated wild-type, but not in resistant parasites. Our findings identify and validate PfAcAS as an essential, druggable target involved in the epigenetic regulation of gene expression.

Published
2022

9. Semi-Synthetic Analogues of Cryptolepine as a Potential Source of Sustainable Drugs for the Treatment of Malaria, Human African Trypanosomiasis, and Cancer.

Author

Abacha, Yabalu, Forkuo, Arnold, Gbedema, Stephen, Mittal, Nimisha, Ottilie, Sabine, Rocamora, Frances, Winzeler, Elizabeth, van Schalkwyk, Donelly, Kelly, John, Taylor, Martin, Reader, Janette, Birkholtz, Lyn-Marie, Lisgarten, David, Cockcroft, Jeremy, Lisgarten, John, Palmer, Rex, Talbert, Rosemary, Shnyder, Steven, and Wright, Colin

Subjects
Plasmodium falciparum, Plasmodium knowlesi, Trypanosoma brucei, halogenation of cryptolepine, ovarian cancer, sustainable pharmaceuticals
Abstract

The prospect of eradicating malaria continues to be challenging in the face of increasing parasite resistance to antimalarial drugs so that novel antimalarials active against asexual, sexual, and liver-stage malaria parasites are urgently needed. In addition, new antimalarials need to be affordable and available to those most in need and, bearing in mind climate change, should ideally be sustainable. The West African climbing shrub Cryptolepis sanguinolenta is used traditionally for the treatment of malaria; its principal alkaloid, cryptolepine (1), has been shown to have antimalarial properties, and the synthetic analogue 2,7-dibromocryptolepine (2) is of interest as a lead toward new antimalarial agents. Cryptolepine (1) was isolated using a two-step Soxhlet extraction of C. sanguinolenta roots, followed by crystallization (yield 0.8% calculated as a base with respect to the dried roots). Semi-synthetic 7-bromo- (3), 7, 9-dibromo- (4), 7-iodo- (5), and 7, 9-dibromocryptolepine (6) were obtained in excellent yields by reaction of 1 with N-bromo- or N-iodosuccinimide in trifluoroacetic acid as a solvent. All compounds were active against Plasmodia in vitro, but 6 showed the most selective profile with respect to Hep G2 cells: P. falciparum (chloroquine-resistant strain K1), IC50 = 0.25 µM, SI = 113; late stage, gametocytes, IC50 = 2.2 µM, SI = 13; liver stage, P. berghei sporozoites IC50 = 6.13 µM, SI = 4.6. Compounds 3-6 were also active against the emerging zoonotic species P. knowlesi with 5 being the most potent (IC50 = 0.11 µM). In addition, 3-6 potently inhibited T. brucei in vitro at nM concentrations and good selectivity with 6 again being the most selective (IC50 = 59 nM, SI = 478). These compounds were also cytotoxic to wild-type ovarian cancer cells as well as adriamycin-resistant and, except for 5, cisplatin-resistant ovarian cancer cells. In an acute oral toxicity test in mice, 3-6 did not exhibit toxic effects at doses of up to 100 mg/kg/dose × 3 consecutive days. This study demonstrates that C. sanguinolenta may be utilized as a sustainable source of novel compounds that may lead to the development of novel agents for the treatment of malaria, African trypanosomiasis, and cancer.

Published
2022

10. Adaptive laboratory evolution in S. cerevisiae highlights role of transcription factors in fungal xenobiotic resistance

Author

Ottilie, Sabine, Luth, Madeline R, Hellemann, Erich, Goldgof, Gregory M, Vigil, Eddy, Kumar, Prianka, Cheung, Andrea L, Song, Miranda, Godinez-Macias, Karla P, Carolino, Krypton, Yang, Jennifer, Lopez, Gisel, Abraham, Matthew, Tarsio, Maureen, LeBlanc, Emmanuelle, Whitesell, Luke, Schenken, Jake, Gunawan, Felicia, Patel, Reysha, Smith, Joshua, Love, Melissa S, Williams, Roy M, McNamara, Case W, Gerwick, William H, Ideker, Trey, Suzuki, Yo, Wirth, Dyann F, Lukens, Amanda K, Kane, Patricia M, Cowen, Leah E, Durrant, Jacob D, and Winzeler, Elizabeth A

Subjects
Microbiology, Biological Sciences, Antimicrobial Resistance, Genetics, Human Genome, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Gene Expression Regulation, Fungal, Saccharomyces cerevisiae, Saccharomyces cerevisiae Proteins, Transcription Factors, Xenobiotics, Biological sciences, Biomedical and clinical sciences
Abstract

In vitro evolution and whole genome analysis were used to comprehensively identify the genetic determinants of chemical resistance in Saccharomyces cerevisiae. Sequence analysis identified many genes contributing to the resistance phenotype as well as numerous amino acids in potential targets that may play a role in compound binding. Our work shows that compound-target pairs can be conserved across multiple species. The set of 25 most frequently mutated genes was enriched for transcription factors, and for almost 25 percent of the compounds, resistance was mediated by one of 100 independently derived, gain-of-function SNVs found in a 170 amino acid domain in the two Zn2C6 transcription factors YRR1 and YRM1 (p

Published
2022

11. Prioritization of Molecular Targets for Antimalarial Drug Discovery.

Author

Forte, Barbara, Ottilie, Sabine, Plater, Andrew, Campo, Brice, Dechering, Koen, Gamo, Francisco, Goldberg, Daniel, Istvan, Eva, Lee, Marcus, Lukens, Amanda, McNamara, Case, Niles, Jacquin, Okombo, John, Pasaje, Charisse, Siegel, Miles, Wirth, Dyann, Wyllie, Susan, Fidock, David, Baragaña, Beatriz, Winzeler, Elizabeth, and Gilbert, Ian

Subjects
Plasmodium, drug discovery, malaria, molecular targets, Antimalarials, Drug Discovery, Humans, Malaria, Plasmodium
Abstract

There is a shift in antimalarial drug discovery from phenotypic screening toward target-based approaches, as more potential drug targets are being validated in Plasmodium species. Given the high attrition rate and high cost of drug discovery, it is important to select the targets most likely to deliver progressible drug candidates. In this paper, we describe the criteria that we consider important for selecting targets for antimalarial drug discovery. We describe the analysis of a number of drug targets in the Malaria Drug Accelerator (MalDA) pipeline, which has allowed us to prioritize targets that are ready to enter the drug discovery process. This selection process has also highlighted where additional data are required to inform target progression or deprioritization of other targets. Finally, we comment on how additional drug targets may be identified.

Published
2021

12. Design of proteasome inhibitors with oral efficacy in vivo against Plasmodium falciparum and selectivity over the human proteasome.

Author

Xie, Stanley, Metcalfe, Riley, Mizutani, Hirotake, Puhalovich, Tanya, Hanssen, Eric, Morton, Craig, Du, Yawei, Dogovski, Con, Huang, Shih-Chung, Ciavarri, Jeffrey, Hales, Paul, Griffin, Robert, Cohen, Lawrence, Chuang, Bei-Ching, Wittlin, Sergio, Deni, Ioanna, Yeo, Tomas, Ward, Kurt, Barry, Daniel, Liu, Boyin, Gillett, David, Crespo-Fernandez, Benigno, Ottilie, Sabine, Mittal, Nimisha, Churchyard, Alisje, Ferguson, Daniel, Aguiar, Anna, Guido, Rafael, Baum, Jake, Hanson, Kirsten, Winzeler, Elizabeth, Gamo, Francisco-Javier, Fidock, David, Baud, Delphine, Parker, Michael, Brand, Stephen, Dick, Lawrence, Griffin, Michael, Gould, Alexandra, and Tilley, Leann

Subjects
Plasmodium, antimalarial drug, cryo-EM, peptide boronate, proteasome, Administration, Oral, Animals, Boron Compounds, Catalytic Domain, Humans, Malaria, Falciparum, Mice, Mice, Inbred NOD, Mice, SCID, Models, Molecular, Plasmodium falciparum, Proteasome Endopeptidase Complex, Proteasome Inhibitors
Abstract

The Plasmodium falciparum proteasome is a potential antimalarial drug target. We have identified a series of amino-amide boronates that are potent and specific inhibitors of the P. falciparum 20S proteasome (Pf20S) β5 active site and that exhibit fast-acting antimalarial activity. They selectively inhibit the growth of P. falciparum compared with a human cell line and exhibit high potency against field isolates of P. falciparum and Plasmodium vivax They have a low propensity for development of resistance and possess liver stage and transmission-blocking activity. Exemplar compounds, MPI-5 and MPI-13, show potent activity against P. falciparum infections in a SCID mouse model with an oral dosing regimen that is well tolerated. We show that MPI-5 binds more strongly to Pf20S than to human constitutive 20S (Hs20Sc). Comparison of the cryo-electron microscopy (EM) structures of Pf20S and Hs20Sc in complex with MPI-5 and Pf20S in complex with the clinically used anti-cancer agent, bortezomib, reveal differences in binding modes that help to explain the selectivity. Together, this work provides insights into the 20S proteasome in P. falciparum, underpinning the design of potent and selective antimalarial proteasome inhibitors.

Published
2021

13. Pan-active imidazolopiperazine antimalarials target the Plasmodium falciparum intracellular secretory pathway.

Author

LaMonte, Gregory M, Rocamora, Frances, Marapana, Danushka S, Gnädig, Nina F, Ottilie, Sabine, Luth, Madeline R, Worgall, Tilla S, Goldgof, Gregory M, Mohunlal, Roxanne, Santha Kumar, TR, Thompson, Jennifer K, Vigil, Edgar, Yang, Jennifer, Hutson, Dylan, Johnson, Trevor, Huang, Jianbo, Williams, Roy M, Zou, Bing Yu, Cheung, Andrea L, Kumar, Prianka, Egan, Timothy J, Lee, Marcus CS, Siegel, Dionicio, Cowman, Alan F, Fidock, David A, and Winzeler, Elizabeth A

Subjects
Endoplasmic Reticulum, Plasmodium falciparum, Saccharomyces cerevisiae, Pyrazoles, Protozoan Proteins, Antimalarials, Chromatography, High Pressure Liquid, Inhibitory Concentration 50, Mass Spectrometry, Secretory Pathway, Malaria, Rare Diseases, Infectious Diseases, HIV/AIDS, Vector-Borne Diseases, 2.1 Biological and endogenous factors, 2.2 Factors relating to the physical environment, 5.1 Pharmaceuticals, Infection
Abstract

A promising new compound class for treating human malaria is the imidazolopiperazines (IZP) class. IZP compounds KAF156 (Ganaplacide) and GNF179 are effective against Plasmodium symptomatic asexual blood-stage infections, and are able to prevent transmission and block infection in animal models. But despite the identification of resistance mechanisms in P. falciparum, the mode of action of IZPs remains unknown. To investigate, we here combine in vitro evolution and genome analysis in Saccharomyces cerevisiae with molecular, metabolomic, and chemogenomic methods in P. falciparum. Our findings reveal that IZP-resistant S. cerevisiae clones carry mutations in genes involved in Endoplasmic Reticulum (ER)-based lipid homeostasis and autophagy. In Plasmodium, IZPs inhibit protein trafficking, block the establishment of new permeation pathways, and cause ER expansion. Our data highlight a mechanism for blocking parasite development that is distinct from those of standard compounds used to treat malaria, and demonstrate the potential of IZPs for studying ER-dependent protein processing.

Published
2020

14. Open-source discovery of chemical leads for next-generation chemoprotective antimalarials

Author

Antonova-Koch, Yevgeniya, Meister, Stephan, Abraham, Matthew, Luth, Madeline R, Ottilie, Sabine, Lukens, Amanda K, Sakata-Kato, Tomoyo, Vanaerschot, Manu, Owen, Edward, Jado, Juan Carlos, Maher, Steven P, Calla, Jaeson, Plouffe, David, Zhong, Yang, Chen, Kaisheng, Chaumeau, Victor, Conway, Amy J, McNamara, Case W, Ibanez, Maureen, Gagaring, Kerstin, Serrano, Fernando Neria, Eribez, Korina, Taggard, Cullin McLean, Cheung, Andrea L, Lincoln, Christie, Ambachew, Biniam, Rouillier, Melanie, Siegel, Dionicio, Nosten, François, Kyle, Dennis E, Gamo, Francisco-Javier, Zhou, Yingyao, Llinás, Manuel, Fidock, David A, Wirth, Dyann F, Burrows, Jeremy, Campo, Brice, and Winzeler, Elizabeth A

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, HIV/AIDS, Infectious Diseases, Vector-Borne Diseases, Rare Diseases, Malaria, Orphan Drug, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Infection, Good Health and Well Being, Antimalarials, Chemoprevention, Drug Discovery, Drug Evaluation, Preclinical, Humans, Mitochondria, Plasmodium, General Science & Technology
Abstract

To discover leads for next-generation chemoprotective antimalarial drugs, we tested more than 500,000 compounds for their ability to inhibit liver-stage development of luciferase-expressing Plasmodium spp. parasites (681 compounds showed a half-maximal inhibitory concentration of less than 1 micromolar). Cluster analysis identified potent and previously unreported scaffold families as well as other series previously associated with chemoprophylaxis. Further testing through multiple phenotypic assays that predict stage-specific and multispecies antimalarial activity distinguished compound classes that are likely to provide symptomatic relief by reducing asexual blood-stage parasitemia from those which are likely to only prevent malaria. Target identification by using functional assays, in vitro evolution, or metabolic profiling revealed 58 mitochondrial inhibitors but also many chemotypes possibly with previously unidentified mechanisms of action.

Published
2018

15. Mapping the malaria parasite druggable genome by using in vitro evolution and chemogenomics

Author

Cowell, Annie N, Istvan, Eva S, Lukens, Amanda K, Gomez-Lorenzo, Maria G, Vanaerschot, Manu, Sakata-Kato, Tomoyo, Flannery, Erika L, Magistrado, Pamela, Owen, Edward, Abraham, Matthew, LaMonte, Gregory, Painter, Heather J, Williams, Roy M, Franco, Virginia, Linares, Maria, Arriaga, Ignacio, Bopp, Selina, Corey, Victoria C, Gnädig, Nina F, Coburn-Flynn, Olivia, Reimer, Christin, Gupta, Purva, Murithi, James M, Moura, Pedro A, Fuchs, Olivia, Sasaki, Erika, Kim, Sang W, Teng, Christine H, Wang, Lawrence T, Akidil, Aslı, Adjalley, Sophie, Willis, Paul A, Siege, Dionicio, Tanaseichuk, Olga, Zhong, Yang, Zhou, Yingyao, Llinás, Manuel, Ottilie, Sabine, Gamo, Francisco-Javier, Lee, Marcus CS, Goldberg, Daniel E, Fidock, David A, Wirth, Dyann F, and Winzeler, Elizabeth A

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Vector-Borne Diseases, Prevention, Biodefense, Infectious Diseases, Genetics, Orphan Drug, Malaria, Rare Diseases, Human Genome, Emerging Infectious Diseases, Antimicrobial Resistance, Vaccine Related, 2.2 Factors relating to the physical environment, Aetiology, Infection, Good Health and Well Being, Activation, Metabolic, Alleles, Antimalarials, DNA Copy Number Variations, Directed Molecular Evolution, Drug Resistance, Drug Resistance, Multiple, Genes, Protozoan, Genome, Protozoan, Metabolomics, Mutation, Plasmodium falciparum, Selection, Genetic, Transcription Factors, General Science & Technology
Abstract

Chemogenetic characterization through in vitro evolution combined with whole-genome analysis can identify antimalarial drug targets and drug-resistance genes. We performed a genome analysis of 262 Plasmodium falciparum parasites resistant to 37 diverse compounds. We found 159 gene amplifications and 148 nonsynonymous changes in 83 genes associated with drug-resistance acquisition, where gene amplifications contributed to one-third of resistance acquisition events. Beyond confirming previously identified multidrug-resistance mechanisms, we discovered hitherto unrecognized drug target-inhibitor pairs, including thymidylate synthase and a benzoquinazolinone, farnesyltransferase and a pyrimidinedione, and a dipeptidylpeptidase and an arylurea. This exploration of the P. falciparum resistome and druggable genome will likely guide drug discovery and structural biology efforts, while also advancing our understanding of resistance mechanisms available to the malaria parasite.

Published
2018

16. MalDA, Accelerating Malaria Drug Discovery

Author

Yang, Tuo, Ottilie, Sabine, Istvan, Eva S., Godinez-Macias, Karla P., Lukens, Amanda K., Baragaña, Beatriz, Campo, Brice, Walpole, Chris, Niles, Jacquin C., Chibale, Kelly, Dechering, Koen J., Llinás, Manuel, Lee, Marcus C.S., Kato, Nobutaka, Wyllie, Susan, McNamara, Case W., Gamo, Francisco Javier, Burrows, Jeremy, Fidock, David A., Goldberg, Daniel E., Gilbert, Ian H., Wirth, Dyann F., and Winzeler, Elizabeth A.

Published
2021
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17. Development of a Potent Inhibitor of the Plasmodium Proteasome with Reduced Mammalian Toxicity

Author

LaMonte, Gregory M, Almaliti, Jehad, Bibo-Verdugo, Betsaida, Keller, Lena, Zou, Bing Yu, Yang, Jennifer, Antonova-Koch, Yevgeniya, Orjuela-Sanchez, Pamela, Boyle, Colleen A, Vigil, Edgar, Wang, Lawrence, Goldgof, Gregory M, Gerwick, Lena, O’Donoghue, Anthony J, Winzeler, Elizabeth A, Gerwick, William H, and Ottilie, Sabine

Subjects
Biotechnology, Rare Diseases, Orphan Drug, Vector-Borne Diseases, Infectious Diseases, Malaria, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Infection, Good Health and Well Being, Antimalarials, Artemisinins, Dipeptides, Drug Design, Enzyme Assays, Hep G2 Cells, Humans, Molecular Docking Simulation, Oligopeptides, Plasmodium falciparum, Proteasome Endopeptidase Complex, Proteasome Inhibitors, Saccharomyces cerevisiae, Medicinal and Biomolecular Chemistry, Organic Chemistry, Pharmacology and Pharmaceutical Sciences, Medicinal & Biomolecular Chemistry
Abstract

Naturally derived chemical compounds are the foundation of much of our pharmacopeia, especially in antiproliferative and anti-infective drug classes. Here, we report that a naturally derived molecule called carmaphycin B is a potent inhibitor against both the asexual and sexual blood stages of malaria infection. Using a combination of in silico molecular docking and in vitro directed evolution in a well-characterized drug-sensitive yeast model, we determined that these compounds target the β5 subunit of the proteasome. These studies were validated using in vitro inhibition assays with proteasomes isolated from Plasmodium falciparum. As carmaphycin B is toxic to mammalian cells, we synthesized a series of chemical analogs that reduce host cell toxicity while maintaining blood-stage and gametocytocidal antimalarial activity and proteasome inhibition. This study describes a promising new class of antimalarial compound based on the carmaphycin B scaffold, as well as several chemical structural features that serve to enhance antimalarial specificity.

Published
2017

18. Rapid Chagas Disease Drug Target Discovery Using Directed Evolution in Drug-Sensitive Yeast

Author

Ottilie, Sabine, Goldgof, Gregory M, Calvet, Claudia Magalhaes, Jennings, Gareth K, LaMonte, Greg, Schenken, Jake, Vigil, Edgar, Kumar, Prianka, McCall, Laura-Isobel, Lopes, Eduardo Soares Constantino, Gunawan, Felicia, Yang, Jennifer, Suzuki, Yo, Siqueira-Neto, Jair L, McKerrow, James H, Amaro, Rommie E, Podust, Larissa M, Durrant, Jacob D, and Winzeler, Elizabeth A

Subjects
Biological Sciences, Medicinal and Biomolecular Chemistry, Chemical Sciences, Rare Diseases, Orphan Drug, Infectious Diseases, Vector-Borne Diseases, Genetics, Biotechnology, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Infection, Good Health and Well Being, 14-alpha Demethylase Inhibitors, Amino Acid Sequence, Chagas Disease, Crystallography, X-Ray, Directed Molecular Evolution, Dose-Response Relationship, Drug, Drug Discovery, Gas Chromatography-Mass Spectrometry, Molecular Docking Simulation, Plasmodium falciparum, Saccharomyces cerevisiae, Spectrophotometry, Ultraviolet, Sterol 14-Demethylase, Trypanocidal Agents, Trypanosoma cruzi, Organic Chemistry, Biological sciences, Chemical sciences
Abstract

Recent advances in cell-based, high-throughput phenotypic screening have identified new chemical compounds that are active against eukaryotic pathogens. A challenge to their future development lies in identifying these compounds' molecular targets and binding modes. In particular, subsequent structure-based chemical optimization and target-based screening require a detailed understanding of the binding event. Here, we use directed evolution and whole-genome sequencing of a drug-sensitive S. cerevisiae strain to identify the yeast ortholog of TcCyp51, lanosterol-14-alpha-demethylase (TcCyp51), as the target of MMV001239, a benzamide compound with activity against Trypanosoma cruzi, the etiological agent of Chagas disease. We show that parasites treated with MMV0001239 phenocopy parasites treated with another TcCyp51 inhibitor, posaconazole, accumulating both lanosterol and eburicol. Direct drug-protein binding of MMV0001239 was confirmed through spectrophotometric binding assays and X-ray crystallography, revealing a binding site shared with other antitrypanosomal compounds that target Cyp51. These studies provide a new probe chemotype for TcCyp51 inhibition.

Published
2017

19. Inhibition of Resistance-Refractory P. falciparum Kinase PKG Delivers Prophylactic, Blood Stage, and Transmission-Blocking Antiplasmodial Activity

Author

Vanaerschot, Manu, Murithi, James M., Pasaje, Charisse Flerida A., Ghidelli-Disse, Sonja, Dwomoh, Louis, Bird, Megan, Spottiswoode, Natasha, Mittal, Nimisha, Arendse, Lauren B., Owen, Edward S., Wicht, Kathryn J., Siciliano, Giulia, Bösche, Markus, Yeo, Tomas, Kumar, T.R. Santha, Mok, Sachel, Carpenter, Emma F., Giddins, Marla J., Sanz, Olalla, Ottilie, Sabine, Alano, Pietro, Chibale, Kelly, Llinás, Manuel, Uhlemann, Anne-Catrin, Delves, Michael, Tobin, Andrew B., Doerig, Christian, Winzeler, Elizabeth A., Lee, Marcus C.S., Niles, Jacquin C., and Fidock, David A.

Published
2020
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22. Multistage and transmission-blocking targeted antimalarials discovered from the open-source MMV Pandemic Response Box

Author

Reader, Janette, van der Watt, Mariëtte E., Taylor, Dale, Le Manach, Claire, Mittal, Nimisha, Ottilie, Sabine, Theron, Anjo, Moyo, Phanankosi, Erlank, Erica, Nardini, Luisa, Venter, Nelius, Lauterbach, Sonja, Bezuidenhout, Belinda, Horatscheck, Andre, van Heerden, Ashleigh, Spillman, Natalie J., Cowell, Anne N., Connacher, Jessica, Opperman, Daniel, Orchard, Lindsey M., Llinás, Manuel, Istvan, Eva S., Goldberg, Daniel E., Boyle, Grant A., Calvo, David, Mancama, Dalu, Coetzer, Theresa L., Winzeler, Elizabeth A., Duffy, James, Koekemoer, Lizette L., Basarab, Gregory, Chibale, Kelly, and Birkholtz, Lyn-Marié

Published
2021
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23. Advances in malaria pharmacology and the online guide to MALARIA PHARMACOLOGY: IUPHAR review 38

Author

Armstrong, Jane F, Campo, Brice, Alexander, Stephen PH, Arendse, Lauren B, Cheng, Xiu, Davenport, Anthony P, Faccenda, Elena, Fidock, David A, Godinez-Macias, Karla P, Harding, Simon D, Kato, Nobutaka, Lee, Marcus CS, Luth, Madeline R, Mazitschek, Ralph, Mittal, Nimisha, Niles, Jacquin C, Okombo, John, Ottilie, Sabine, Pasaje, Charisse Flerida A, Probst, Alexandra S, Rawat, Mukul, Rocamora, Frances, Sakata-Kato, Tomoyo, Southan, Christopher, Spedding, Michael, Tye, Mark A, Yang, Tuo, Zhao, Na, Davies, Jamie A, Armstrong, Jane F [0000-0002-0524-0260], Alexander, Stephen PH [0000-0003-4417-497X], Harding, Simon D [0000-0002-9262-8318], Pasaje, Charisse Flerida A [0000-0002-9780-3680], Spedding, Michael [0000-0002-1248-8221], and Apollo - University of Cambridge Repository

Subjects
Plasmodium, Antimalarials, Drug Discovery, malaria, Humans, bioinformatics, database, molecular target, High-Throughput Screening Assays
Abstract

Antimalarial drug discovery has until recently been driven by high-throughput phenotypic cellular screening, allowing millions of compounds to be assayed and delivering clinical drug candidates. In this review, we will focus on target-based approaches, describing recent advances in our understanding of druggable targets in the malaria parasite. Targeting multiple stages of the Plasmodium lifecycle, rather than just the clinically symptomatic asexual blood stage, has become a requirement for new antimalarial medicines, and we link pharmacological data clearly to the parasite stages to which it applies. Finally, we highlight the IUPHAR/MMV Guide to MALARIA PHARMACOLOGY, a web resource developed for the malaria research community that provides open and optimized access to published data on malaria pharmacology.

Published
2023

24. Advances in malaria pharmacology and the online guide to MALARIA PHARMACOLOGY: IUPHAR review 38

Author

Armstrong, Jane F., primary, Campo, Brice, additional, Alexander, Stephen P. H., additional, Arendse, Lauren B., additional, Cheng, Xiu, additional, Davenport, Anthony P., additional, Faccenda, Elena, additional, Fidock, David A., additional, Godinez‐Macias, Karla P., additional, Harding, Simon D., additional, Kato, Nobutaka, additional, Lee, Marcus C. S., additional, Luth, Madeline R., additional, Mazitschek, Ralph, additional, Mittal, Nimisha, additional, Niles, Jacquin C., additional, Okombo, John, additional, Ottilie, Sabine, additional, Pasaje, Charisse Flerida A., additional, Probst, Alexandra S., additional, Rawat, Mukul, additional, Rocamora, Frances, additional, Sakata‐Kato, Tomoyo, additional, Southan, Christopher, additional, Spedding, Michael, additional, Tye, Mark A., additional, Yang, Tuo, additional, Zhao, Na, additional, and Davies, Jamie A., additional

Published
2023
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26. Advances in Malaria Pharmacology and the online Guide to MALARIA PHARMACOLOGY:IUPHAR review 38

Author

Armstrong, Jane, Campo, Brice, Alexander, Stephen P H, Arendse, Lauren B, Cheng, Xiu, Davenport, Anthony P, Faccenda, Elena, Fidock, David A, Godinez-Macias, Karla P, Harding, Simon D, Kato, Nobutaka, Lee, Marcus CS, Luth, Madeline R, Mazitschek, Ralph, Mittal, Nimisha, Niles, Jacquin C, Okombo, John, Ottilie, Sabine, Pasaje, Charisse Flerida A, Probst, Alexandra S, Rawat, Mikul, Rocamora, Frances, Sakata-Kato, Tomoyo, Southan, Christopher, Spedding, Michael, Tye, Mark A, Yang, Tuo, Zhao, Na, and Davies, Jamie A

Abstract

Antimalarial drug discovery has until recently been driven by high-throughput phenotypic cellular screening, allowing millions of compounds to be assayed and delivering clinical drug candidates. In this review, we will focus on target-based approaches, describing recent advances in our understanding of druggable targets in the malaria parasite. Targeting multiple stages of the Plasmodium lifecycle, rather than just the clinically symptomatic asexual blood stage, has become a requirement for new antimalarial medicines, and we link pharmacological data clearly to the parasite stages to which it applies. Finally, we highlight the IUPHAR/MMV Guide to MALARIA PHARMACOLOGY, a web resource developed for the malaria research community that provides open and optimized access to published data on malaria pharmacology.

Published
2023

27. Advances in Malaria Pharmacology and the online Guide to MALARIA PHARMACOLOGY: IUPHAR Review X

Author

Armstrong, Jane F, Campo, Brice, Alexander, Stephen PH, Arendse, Lauren B, Cheng, Xiu, Davenport, Anthony P, Faccenda, Elena, Fidock, David A, Godinez-Macias, Karla P, Harding, Simon D, Kato, Nobutaka, Lee, Marcus CS, Luth, Madeline R, Mazitschek, Ralph, Mittal, Nimisha, Niles, Jacquin C, Okombo, John, Ottilie, Sabine, Pasaje, Charisse Flerida A, Probst, Alexandra S, Rawat, Mukul, Rocamora, Frances, Sakata-Kato, Tomoyo, Southan, Christopher, Spedding, Michael, Tye, Mark A, Yang, Tuo, Zhao, Na, Davies, Jamie A, Armstrong, Jane F [0000-0002-0524-0260], Alexander, Stephen PH [0000-0003-4417-497X], Harding, Simon D [0000-0002-9262-8318], Pasaje, Charisse Flerida A [0000-0002-9780-3680], Spedding, Michael [0000-0002-1248-8221], and Apollo - University of Cambridge Repository

Subjects
Plasmodium, malaria, bioinformatics, database, drug discovery, molecular target
Abstract

Antimalarial drug discovery has until recently been driven by high-throughput phenotypic cellular screening, allowing millions of compounds to be assayed and delivering clinical drug candidates. In this review, we will focus on target-based approaches, describing recent advances in our understanding of druggable targets in the malaria parasite. Targeting multiple stages of the Plasmodium lifecycle, rather than just the clinically symptomatic asexual blood stage, has become a requirement for new antimalarial medicines, and we link pharmacological data clearly to the parasite stages to which it applies. Finally, we highlight the IUPHAR/MMV Guide to MALARIA PHARMACOLOGY, a web resource developed for the malaria research community that provides open and optimized access to published data on malaria pharmacology.

Published
2023

28. Development of Potent and Highly Selective Epoxyketone‐Based Plasmodium Proteasome Inhibitors

Author

Almaliti, Jehad, primary, Fajtová, Pavla, additional, Calla, Jaeson, additional, LaMonte, Gregory M., additional, Feng, Mudong, additional, Rocamora, Frances, additional, Ottilie, Sabine, additional, Glukhov, Evgenia, additional, Boura, Evzen, additional, Suhandynata, Raymond T., additional, Momper, Jeremiah D., additional, Gilson, Michael K., additional, Winzeler, Elizabeth A., additional, Gerwick, William H., additional, and O'Donoghue, Anthony J., additional

Published
2023
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30. Development of Highly Selective Epoxyketone-based Plasmodium Proteasome Inhibitors with Negligible Cytotoxicity

Author

Almaliti, Jehad, primary, Fajtová, Pavla, additional, Calla, Jaeson, additional, LaMonte, Gregory M., additional, Feng, Mudong, additional, Rocamora, Frances, additional, Ottilie, Sabine, additional, Glukhov, Evgenia, additional, Boura, Evzen, additional, Suhandynata, Raymond T., additional, Momper, Jeremiah D., additional, Gilson, Michael K., additional, Winzeler, Elizabeth A., additional, Gerwick, William H., additional, and O’Donoghue, Anthony J., additional

Published
2022
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32. Semi-Synthetic Analogues of Cryptolepine as a Potential Source of Sustainable Drugs for the Treatment of Malaria, Human African Trypanosomiasis, and Cancer

Author

Abacha, Yabalu Z., primary, Forkuo, Arnold Donkor, additional, Gbedema, Stephen Y., additional, Mittal, Nimisha, additional, Ottilie, Sabine, additional, Rocamora, Frances, additional, Winzeler, Elizabeth A., additional, van Schalkwyk, Donelly A., additional, Kelly, John M., additional, Taylor, Martin C., additional, Reader, Janette, additional, Birkholtz, Lyn-Marie, additional, Lisgarten, David R., additional, Cockcroft, Jeremy K., additional, Lisgarten, John N., additional, Palmer, Rex A., additional, Talbert, Rosemary C., additional, Shnyder, Steven D., additional, and Wright, Colin W., additional

Published
2022
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34. Comparative chemical genomics reveal that the spiroindolone antimalarial KAE609 (Cipargamin) is a P-type ATPase inhibitor

Author

Goldgof, Gregory M., Durrant, Jacob D., Ottilie, Sabine, Vigil, Edgar, Allen, Kenneth E., Gunawan, Felicia, Kostylev, Maxim, Henderson, Kiersten A., Yang, Jennifer, Schenken, Jake, LaMonte, Gregory M., Manary, Micah J., Murao, Ayako, Nachon, Marie, Murray, Rebecca, Prescott, Maximo, McNamara, Case W., Slayman, Carolyn W., Amaro, Rommie E., Suzuki, Yo, and Winzeler, Elizabeth A.

Published
2016
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37. PfMFR3: A Multidrug-Resistant Modulator in Plasmodium falciparum

Author

Rocamora, Frances, primary, Gupta, Purva, additional, Istvan, Eva S., additional, Luth, Madeline R., additional, Carpenter, Emma F., additional, Kümpornsin, Krittikorn, additional, Sasaki, Erika, additional, Calla, Jaeson, additional, Mittal, Nimisha, additional, Carolino, Krypton, additional, Owen, Edward, additional, Llinás, Manuel, additional, Ottilie, Sabine, additional, Goldberg, Daniel E., additional, Lee, Marcus C. S., additional, and Winzeler, Elizabeth A., additional

Published
2021
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38. Defining the Yeast Resistome through in vitro Evolution and Whole Genome Sequencing

Author

Ottilie, Sabine, primary, Luth, Madeline R., additional, Hellemann, Erich, additional, Goldgof, Gregory M., additional, Vigil, Eddy, additional, Kumar, Prianka, additional, Cheung, Andrea L., additional, Song, Miranda, additional, Godinez-Macias, Karla P., additional, Carolino, Krypton, additional, Yang, Jennifer, additional, Lopez, Gisel, additional, Abraham, Matthew, additional, Tarsio, Maureen, additional, LeBlanc, Emmanuelle, additional, Whitesell, Luke, additional, Schenken, Jake, additional, Gunawan, Felicia, additional, Patel, Reysha, additional, Smith, Joshua, additional, Love, Melissa S., additional, Williams, Roy M., additional, McNamara, Case W., additional, Gerwick, William H., additional, Ideker, Trey, additional, Suzuki, Yo, additional, Wirth, Dyann F., additional, Lukens, Amanda K., additional, Kane, Patricia M., additional, Cowen, Leah E., additional, Durrant, Jacob D., additional, and Winzeler, Elizabeth A., additional

Published
2021
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39. Identification and Profiling of a Novel Diazaspiro[3.4]octane Chemical Series Active against Multiple Stages of the Human Malaria Parasite Plasmodium falciparum and Optimization Efforts

Author

Le Manach, Claire, primary, Dam, Jean, additional, Woodland, John G., additional, Kaur, Gurminder, additional, Khonde, Lutete P., additional, Brunschwig, Christel, additional, Njoroge, Mathew, additional, Wicht, Kathryn J., additional, Horatscheck, André, additional, Paquet, Tanya, additional, Boyle, Grant A., additional, Gibhard, Liezl, additional, Taylor, Dale, additional, Lawrence, Nina, additional, Yeo, Tomas, additional, Mok, Sachel, additional, Eastman, Richard T., additional, Dorjsuren, Dorjbal, additional, Talley, Daniel C., additional, Guo, Hui, additional, Simeonov, Anton, additional, Reader, Janette, additional, van der Watt, Mariëtte, additional, Erlank, Erica, additional, Venter, Nelius, additional, Zawada, Jacek W., additional, Aswat, Ayesha, additional, Nardini, Luisa, additional, Coetzer, Theresa L., additional, Lauterbach, Sonja B., additional, Bezuidenhout, Belinda C., additional, Theron, Anjo, additional, Mancama, Dalu, additional, Koekemoer, Lizette L., additional, Birkholtz, Lyn-Marie, additional, Wittlin, Sergio, additional, Delves, Michael, additional, Ottilie, Sabine, additional, Winzeler, Elizabeth A., additional, von Geldern, Thomas W., additional, Smith, Dennis, additional, Fidock, David A., additional, Street, Leslie J., additional, Basarab, Gregory S., additional, Duffy, James, additional, and Chibale, Kelly, additional

Published
2021
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41. Multistage and transmission-blocking targeted antimalarials discovered from the open-source MMV Pandemic Response Box

Author

Reader, Janette, primary, van der Watt, Mariёtte E., additional, Taylor, Dale, additional, Le Manach, Claire, additional, Mittal, Nimisha, additional, Ottilie, Sabine, additional, Theron, Anjo, additional, Moyo, Phanankosi, additional, Erlank, Erica, additional, Nardini, Luisa, additional, Venter, Nelius, additional, Lauterbach, Sonja, additional, Bezuidenhout, Belinda, additional, Horatscheck, Andre, additional, van Heerden, Ashleigh, additional, Boyle, Grant A., additional, Calvo, David, additional, Mancama, Dalu, additional, Coetzer, Theresa L., additional, Winzeler, Elizabeth A., additional, Duffy, James, additional, Koekemoer, Lizette L., additional, Basarab, Gregory, additional, Chibale, Kelly, additional, and Birkholtz, Lyn-Marié, additional

Published
2020
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42. Probing the Open Global Health Chemical Diversity Library for Multistage-Active Starting Points for Next-Generation Antimalarials

Author

Abraham, Matthew, primary, Gagaring, Kerstin, additional, Martino, Marisa L., additional, Vanaerschot, Manu, additional, Plouffe, David M., additional, Calla, Jaeson, additional, Godinez-Macias, Karla P., additional, Du, Alan Y., additional, Wree, Melanie, additional, Antonova-Koch, Yevgeniya, additional, Eribez, Korina, additional, Luth, Madeline R., additional, Ottilie, Sabine, additional, Fidock, David A., additional, McNamara, Case W., additional, and Winzeler, Elizabeth A., additional

Published
2020
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43. In vitro selection predicts malaria parasite resistance to dihydroorotate dehydrogenase inhibitors in a mouse infection model

Author

Mandt, Rebecca E. K., primary, Lafuente-Monasterio, Maria Jose, additional, Sakata-Kato, Tomoyo, additional, Luth, Madeline R., additional, Segura, Delfina, additional, Pablos-Tanarro, Alba, additional, Viera, Sara, additional, Magan, Noemi, additional, Ottilie, Sabine, additional, Winzeler, Elizabeth A., additional, Lukens, Amanda K., additional, Gamo, Francisco Javier, additional, and Wirth, Dyann F., additional

Published
2019
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44. Mutational analysis of Cdc19p, a Schizosaccharomyces pombe MCM protein

Author

Forsburg, Susan L., Sherman, Daniel A., Ottilie, Sabine, Yasuda, J. Randy, and Hodson, Jeffrey A.

Subjects
Mutation (Biology) -- Analysis, Proteins -- Synthesis, Chromosome replication -- Research, Biological sciences
Abstract

The [cdc19.sup.+] gene encodes an essential member of the MCM family of replication proteins in Schizosaccharomyces pombe. We have examined the structure and function of the Cdc19p protein using molecular and genetic approaches. We find that overproduction of wild-type Cdc19p in wild-type cells has no effect, but cdc19-P1 mutant cells do not tolerate elevated levels of other MCM proteins or overexpression of mutant forms of Cdc19p. We have found genetic interactions between [cdc19.sup.+] and genes encoding subunits of DNA polymerase [Delta] and the replication initiator [cdc18.sup.+]. We have constructed a series of point mutations and sequence deletions throughout Cdc19p, which allow us to distinguish essential from nonessential regions of the protein. Not surprisingly, conserved residues in the MCM homology domain are required for protein function, but some residues outside the core homology domain are dispensable.

Published
1997

45. Pan-active imidazolopiperazine antimalarials target thePlasmodium falciparumintracellular secretory pathway

Author

LaMonte, Gregory M., primary, Marapana, Danushka S., additional, Gnadig, Nina, additional, Ottilie, Sabine, additional, Luth, Madeline R., additional, Worgall, Tilla S., additional, Rocamora, Frances, additional, Goldgof, Gregory M., additional, Mohunlal, Roxanne, additional, Kumar, T.R Santha, additional, Thompson, Jenny K., additional, Vigil, Edgar, additional, Yang, Jennifer, additional, Hutson, Dylan, additional, Johnson, Trevor, additional, Huang, Jianbo, additional, Williams, Roy M., additional, Zou, Bing Yu, additional, Cheung, Andrea L., additional, Kumar, Prianka, additional, Egan, Timothy J., additional, Lee, Marcus C.S., additional, Siegel, Dionicio, additional, Cowman, Alan F., additional, Fidock, David A., additional, and Winzeler, Elizabeth A., additional

Published
2019
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46. Synthesis, Profiling, and in Vivo Evaluation of Cyclopeptides Containing N-Methyl Amino Acids as Antiplasmodial Agents

Author

Fagundez, Catherine, primary, Sellanes, Diver, additional, Peña, Stella, additional, Scarone, Laura, additional, Aguiar, Anna C. C., additional, de Souza, Juliana O., additional, Guido, Rafael V. C., additional, Stewart, Lindsay, additional, Yardley, Vanessa, additional, Ottilie, Sabine, additional, Winzeler, Elizabeth A., additional, Gamo, Francisco-J., additional, Sanz, Laura M., additional, and Serra, Gloria L., additional

Published
2018
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47. Target Validation and Identification of Novel Boronate Inhibitors of the Plasmodium falciparum Proteasome

Author

Xie, Stanley C., primary, Gillett, David L., additional, Spillman, Natalie J., additional, Tsu, Christopher, additional, Luth, Madeline R., additional, Ottilie, Sabine, additional, Duffy, Sandra, additional, Gould, Alexandra E., additional, Hales, Paul, additional, Seager, Benjamin A., additional, Charron, Carlie L., additional, Bruzzese, Frank, additional, Yang, Xiaofeng, additional, Zhao, Xiansi, additional, Huang, Shih-Chung, additional, Hutton, Craig A., additional, Burrows, Jeremy N., additional, Winzeler, Elizabeth A., additional, Avery, Vicky M., additional, Dick, Lawrence R., additional, and Tilley, Leann, additional

Published
2018
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49. Identification and Profiling of a Novel Diazaspiro[3.4]octane Chemical Series Active against Multiple Stages of the Human Malaria Parasite Plasmodium falciparumand Optimization Efforts

Author

Le Manach, Claire, Dam, Jean, Woodland, John G., Kaur, Gurminder, Khonde, Lutete P., Brunschwig, Christel, Njoroge, Mathew, Wicht, Kathryn J., Horatscheck, André, Paquet, Tanya, Boyle, Grant A., Gibhard, Liezl, Taylor, Dale, Lawrence, Nina, Yeo, Tomas, Mok, Sachel, Eastman, Richard T., Dorjsuren, Dorjbal, Talley, Daniel C., Guo, Hui, Simeonov, Anton, Reader, Janette, van der Watt, Mariëtte, Erlank, Erica, Venter, Nelius, Zawada, Jacek W., Aswat, Ayesha, Nardini, Luisa, Coetzer, Theresa L., Lauterbach, Sonja B., Bezuidenhout, Belinda C., Theron, Anjo, Mancama, Dalu, Koekemoer, Lizette L., Birkholtz, Lyn-Marie, Wittlin, Sergio, Delves, Michael, Ottilie, Sabine, Winzeler, Elizabeth A., von Geldern, Thomas W., Smith, Dennis, Fidock, David A., Street, Leslie J., Basarab, Gregory S., Duffy, James, and Chibale, Kelly

Abstract

A novel diazaspiro[3.4]octane series was identified from a Plasmodium falciparumwhole-cell high-throughput screening campaign. Hits displayed activity against multiple stages of the parasite lifecycle, which together with a novel sp3-rich scaffold provided an attractive starting point for a hit-to-lead medicinal chemistry optimization and biological profiling program. Structure–activity-relationship studies led to the identification of compounds that showed low nanomolar asexual blood-stage activity (<50 nM) together with strong gametocyte sterilizing properties that translated to transmission-blocking activity in the standard membrane feeding assay. Mechanistic studies through resistance selection with one of the analogues followed by whole-genome sequencing implicated the P. falciparumcyclic amine resistance locus in the mode of resistance.

Published
2021
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50. Mapping the malaria parasite drug-able genome usingin vitroevolution and chemogenomics

Author

Cowell, Annie N., primary, Istvan, Eva S., additional, Lukens, Amanda K., additional, Gomez-Lorenzo, Maria G., additional, Vanaerschot, Manu, additional, Sakata-Kato, Tomoyo, additional, Flannery, Erika L., additional, Magistrado, Pamela, additional, Abraham, Matthew, additional, LaMonte, Gregory, additional, Williams, Roy M., additional, Franco, Virginia, additional, Linares, Maria, additional, Arriaga, Ignacio, additional, Bopp, Selina, additional, Corey, Victoria C., additional, Gnädig, Nina F., additional, Coburn-Flynn, Olivia, additional, Reimer, Christin, additional, Gupta, Purva, additional, Murithi, James M., additional, Fuchs, Olivia, additional, Sasaki, Erika, additional, Kim, Sang W., additional, Teng, Christine, additional, Wang, Lawrence T., additional, Willis, Paul, additional, Siegel, Dionicio, additional, Tanaseichuk, Olga, additional, Zhong, Yang, additional, Zhou, Yingyao, additional, Ottilie, Sabine, additional, Gamo, Francisco-Javier, additional, Lee, Marcus C.S., additional, Goldberg, Daniel E., additional, Fidock, David A., additional, Wirth, Dyann F., additional, and Winzeler, Elizabeth A., additional

Published
2017
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