Hepatic safety and tolerability of cipargamin (KAE609), in adult patients with Plasmodium falciparum malaria: a randomized, phase II, controlled, dose-escalation trial in sub-Saharan Africa

Ndayisaba, Gilles; Yeka, Adoke; Asante, Kwaku Poku; Grobusch, Martin P.; Karita, Etienne; Mugerwa, Henry; Asiimwe, Stephen; Oduro, Abraham; Fofana, Bakary; Doumbia, Seydou; Jain, Jay Prakash; Barsainya, Sarita; Kullak‐Ublick, Gerd A.; Su, Guoqin; Schmitt, E.; Csermak, Katalin; Gandhi, Preetam; Hughes, David

doi:10.1186/s12936-021-04009-1

Cited by 14 publications

(8 citation statements)

References 17 publications

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“…The simulated 8-patient PK datasets provided a good visual match to the trial data from McCarthy et al [14] (Figure S1). The PK model was incorporated into a Bayesian hierarchical framework, and fitted to each of the 1000 simulated datasets, restricting data to the cipargamin concentrations which correspond to the sampling times of the original Phase 2 trial (1,2,3,4,6,8,12,16,24,36,48,72,96 and 120 hours post-treatment), and the posterior median estimate of each population PK parameter obtained. To evaluate how accurately this model can estimate PK parameters, we calculated the difference (absolute and relative bias) between the posterior median estimate of the population-level PK parameter, and the value used to simulate the data (i.e., the 'true' value).…”

Section: Pharmacokinetic Modelmentioning

confidence: 99%

“…The journey from early phase clinical trials to Phase 3 clinical trials in patients, to then drug registration, can take many years [9]. Cipargamin is a promising candidate antimalarial drug that has transitioned from early phase studies [10] to Phase 2 clinical trials of adult patients with falciparum malaria [11, 12]. In particular, it is a rapidly acting parenteral agent with promise to replace artemisinin [13].…”

Section: Introductionmentioning

confidence: 99%

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Evaluation of a Bayesian hierarchical pharmacokinetic-pharmacodynamic model for predicting parasitological outcomes in Phase 2 studies of new antimalarial drugs

Tully,

Dini,

Flegg

et al. 2024

Preprint

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The rise of multidrug resistant malaria requires accelerated development of novel antimalarial drugs. Pharmacokinetic-pharmacodynamic (PK-PD) models relate blood antimalarial drug concentrations with the parasite-time profile to inform dosing regiments. We performed a simulation study to assess the utility of a Bayesian hierarchical mechanistic PK-PD model for predicting parasite-time profiles for a Phase 2 study of a new antimalarial drug, cipargamin. We simulated cipargamin concentration- and malaria parasite-profiles based on a Phase 2 study of 8 volunteers who received cipargamin 7 days after inoculation with malaria parasites. The cipargamin profiles were generated from a 2-compartment PK model, and parasite profiles from a previously published biologically informed PD model. One-thousand PK-PD datasets of 8 patients were simulated, following the sampling intervals of the Phase 2 study. The mechanistic PK-PD model was incorporated in a Bayesian hierarchical framework and the parameters estimated. Population PK model parameters describing absorption, distribution and clearance were estimated with minimal bias (mean relative bias ranged from 1.7 to 8.4\%). The PD model was fitted to the parasitaemia profiles in each simulated dataset using the estimated PK parameters. Posterior predictive checks demonstrate that our PK-PD model successfully captures both the pre- and post-treatment simulated PD profiles. The bias of the estimated population average PD parameters was low-moderate in magnitude. This simulation study demonstrates the viability of our PK-PD model to predict parasitological outcomes in Phase 2 volunteer infection studies. This work will inform the dose-effect relationship of cipargamin, guiding decisions on dosing regimens to evaluate in Phase 3 trials.

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Section: Pharmacokinetic Modelmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Evaluation of a Bayesian hierarchical pharmacokinetic-pharmacodynamic model for predicting parasitological outcomes in Phase 2 studies of new antimalarial drugs

Tully,

Dini,

Flegg

et al. 2024

Preprint

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“…This is considered a promising agent to combat the artemisinin resistance parasite [ 62 ]. Hepatic safety behavior was achieved through clinical studies (phase II) across wide-range doses [ 63 , 64 ].…”

Section: Synthetic Spirooxindolesmentioning

confidence: 99%

Spirooxindole: A Versatile Biologically Active Heterocyclic Scaffold

et al. 2023

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Spirooxindoles occupy an important place in heterocyclic chemistry. Many natural spirooxindole-containing compounds have been identified as bio-promising agents. Synthetic analogs have also been synthesized utilizing different pathways. The present article summarizes the recent development of both natural and synthetic spirooxindole-containing compounds prepared from isatin or its derivatives reported in the last five years. The spirooxindoles are categorized based on their mentioned biological properties.

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“…NITD609 clears P. berghei from mice very rapidly (faster than artemisinin derivatives), has a favourable safety profile (Rottmann et al, 2010) and is effective in several human clinical trials (e.g. Ndayisaba et al, 2021). Mutations in PfATP4 have been identified in parasites resistant to NITD609 through gradual exposure to increasing concentrations of the compound, and overexpression of the mutated PfATP4 protein in parasites confirmed the resistance phenotype.…”

Section: Progress Towards the Discovery Of New Antimalarial Therapies...mentioning

confidence: 99%

“…falciparum and P. vivax with low nanomolar range IC 50 , block gametocyte development in vitro and oocyst development in mosquitoes(Rottmann et al, 2010;van Pelt-Koops et al, 2012). NITD609 clears P. berghei from mice very rapidly (faster than artemisinin derivatives), has a favourable safety profile(Rottmann et al, 2010) and is effective in several human clinical trials (e.g Ndayisaba et al, 2021)…”

mentioning

confidence: 99%

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

Armstrong

Campo

Alexander

et al. 2023

British J Pharmacology

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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 PHAR-MACOLOGY, a web resource developed for the malaria research community that provides open and optimized access to published data on malaria pharmacology.

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Hepatic safety and tolerability of cipargamin (KAE609), in adult patients with Plasmodium falciparum malaria: a randomized, phase II, controlled, dose-escalation trial in sub-Saharan Africa

Cited by 14 publications

References 17 publications

Evaluation of a Bayesian hierarchical pharmacokinetic-pharmacodynamic model for predicting parasitological outcomes in Phase 2 studies of new antimalarial drugs

Evaluation of a Bayesian hierarchical pharmacokinetic-pharmacodynamic model for predicting parasitological outcomes in Phase 2 studies of new antimalarial drugs

Spirooxindole: A Versatile Biologically Active Heterocyclic Scaffold

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

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