Efficacy of Cipargamin (KAE609) in a Randomized, Phase II Dose-Escalation Study in Adults in Sub-Saharan Africa With Uncomplicated <i>Plasmodium falciparum</i> Malaria

Schmitt, E.; Ndayisaba, Gilles; Yeka, Adoke; Asante, Kwaku Poku; Grobusch, Martin P.; Karita, Etienne; Mugerwa, Henry; Asiimwe, Stephen; Oduro, Abraham; Fofana, Bakary; Doumbia, Seydou; Su, Guoqin; Renner, Katalin Csermak; Venishetty, Vinay Kumar; Sayyed, Sarfaraz; Straimer, Judith; Demin, Ivan; Barsainya, Sarita; Boulton, Caroline; Gandhi, Preetam

doi:10.1093/cid/ciab716

Cited by 30 publications

(30 citation statements)

References 22 publications

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“…There was no obvious relationship between LFT abnormalities and cipargamin dose or exposure. Exposure to cipargamin in this trial was higher or comparable to previous trials [ 1 ], with no evidence of an increase in hepatic events. In addition, patients receiving both cipargamin and artemether–lumefantrine during the study did not show an increased rate of LFT abnormalities.…”

Section: Discussionsupporting

confidence: 73%

“…This study paves the way for the further development of this novel anti-malarial. In addition to the good tolerability of cipargamin, this study has confirmed its potency and rapid onset of parasiticidal activity with parasite clearance times of around 8 h for doses of 50 mg or higher [ 1 ]. Furthermore, cipargamin is potent against artemisinin-resistant parasites including the R561H mutant, which is spreading in Rwanda [ 2 ].…”

Section: Discussionmentioning

confidence: 64%

“…Furthermore, cipargamin is potent against artemisinin-resistant parasites including the R561H mutant, which is spreading in Rwanda [ 2 ]. However, when used as monotherapy, treatment-emerging mutations were detected in patients experiencing recrudescences [ 1 ]. Cipargamin will be developed in fixed-dose combination with a partner drug and liver safety aspects remain to be considered for selection of partner compounds and monitored in future clinical trials.…”

Section: Discussionmentioning

confidence: 99%

“…Secondary objectives included overall safety and tolerability, pharmacokinetic parameters and efficacy. Here, hepatic and general safety assessments are described, while efficacy and pharmacokinetics are reported elsewhere [ 1 ].…”

Section: Methodsmentioning

confidence: 99%

“…There is a need to develop new anti-malarials as emerging resistance to artemisinin derivatives threatens to undermine progress in malaria control. Cipargamin (KAE609/NITD609) is a novel anti-malarial spiroindolone analogue compound with promising and potent activity in clinical studies [ 1 – 3 ]. Spiroindolones disrupt sodium and osmotic homeostasis in Plasmodium species by inhibiting PfATP4, a plasma membrane Na+-ATPase [ 4 ].…”

Section: Introductionmentioning

confidence: 99%

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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

Ndayisaba¹,

Yeka

Asante

et al. 2021

Malar J

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Background The novel anti-malarial cipargamin (KAE609) has potent, rapid activity against Plasmodium falciparum. Transient asymptomatic liver function test elevations were previously observed in cipargamin-treated subjects in two trials: one in malaria patients in Asia and one in volunteers with experimentally induced malaria. In this study, the hepatic safety of cipargamin given as single doses of 10 to 150 mg and 10 to 50 mg once daily for 3 days was assessed. Efficacy results, frequency of treatment-emerging mutations in the atp4 gene and pharmacokinetics have been published elsewhere. Further, the R561H mutation in the k13 gene, which confers artemisinin-resistance, was associated with delayed parasite clearance following treatment with artemether–lumefantrine in Rwanda in this study. This was also the first study with cipargamin to be conducted in patients in sub-Saharan Africa. Methods This was a Phase II, multicentre, randomized, open-label, dose-escalation trial in adults with uncomplicated falciparum malaria in five sub-Saharan countries, using artemether–lumefantrine as control. The primary endpoint was ≥ 2 Common Terminology Criteria for Adverse Events (CTCAE) Grade increase from baseline in alanine aminotransferase (ALT) or aspartate transaminase (AST) during the 4-week trial. Results Overall, 2/135 patients treated with cipargamin had ≥ 2 CTCAE Grade increases from baseline in ALT or AST compared to 2/51 artemether–lumefantrine patients, with no significant difference between any cipargamin treatment group and the control group. Cipargamin exposure was comparable to or higher than those in previous studies. Hepatic adverse events and general safety and tolerability were similar for all cipargamin doses and artemether–lumefantrine. Cipargamin was well tolerated with no safety concerns. Conclusions This active-controlled, dose escalation study was a detailed assessment of the hepatic safety of cipargamin, across a wide range of doses, in patients with uncomplicated falciparum malaria. Comparison with previous cipargamin trials requires caution as no clear conclusion can be drawn as to whether hepatic safety and potential immunity to malaria would differ with ethnicity, patient age and or geography. Previous concerns regarding hepatic safety may have been confounded by factors including malaria itself, whether natural or experimental infection, and should not limit the further development of cipargamin. Trial registration ClinicalTrials.gov number: NCT03334747 (7 Nov 2017), other study ID CKAE609A2202

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Section: Discussionsupporting

confidence: 73%

Section: Discussionmentioning

confidence: 64%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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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

Ndayisaba¹,

Yeka

Asante

et al. 2021

Malar J

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Catalytic Asymmetric Arylations of Ketimines

Vlahoviček‐Kahlina,

Marijan,

Matišić

et al. 2024

Adv Synth Catal

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Arylation of ketimines is the most straightforward strategy for the construction of chiral α‐tertiary amines, important structural motifs in natural products and biologically active compounds. This comprehensive review highlights the achievements in the transition metal‐catalyzed and organocatalyzed asymmetric arylations of ketimines from the seminal report on catalytic asymmetric arylation of ketimines in 2010 till November 2023. The review is divided into three chapters: (1) Arylation of diaryl ketimines, (2) Arylation of aryl‐alkyl and aryl‐acyl ketimines, and (3) Arylation of acyl‐alkyl and dialkyl ketimines. Each chapter is further divided into transition‐metal catalyzed reactions (grouped by individual metals) and organocatalyzed reactions. Covered literature includes emphasis on the advantages of the reported methodology, its scope and limitations, and the description of the transition state (where applicable).

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Facile Access to Structurally Diverse Antimalarial Indoles Using a One‐Pot A³ Coupling and Domino Cyclization Approach

et al. 2023

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A multistep and diversity‐oriented synthetic route aiming at the A3 coupling/domino cyclization of o‐ethynyl anilines, aldehydes and s‐amines is described. The preparation of the corresponding precursors included a series of transformations, such as haloperoxidation and Sonogashira cross‐coupling reactions, amine protection, desilylation and amine reduction. Some products of the multicomponent reaction underwent further detosylation and Suzuki coupling. The resulting library of structurally diverse compounds was evaluated against blood and liver stage malaria parasites, which revealed a promising lead with sub‐micromolar activity against intra‐erythrocytic forms of Plasmodium falciparum. The results from this hit‐to‐lead optimization are hereby reported for the first time.

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Efficacy of Cipargamin (KAE609) in a Randomized, Phase II Dose-Escalation Study in Adults in Sub-Saharan Africa With Uncomplicated Plasmodium falciparum Malaria

Cited by 30 publications

References 22 publications

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

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

Catalytic Asymmetric Arylations of Ketimines

Facile Access to Structurally Diverse Antimalarial Indoles Using a One‐Pot A³ Coupling and Domino Cyclization Approach

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Efficacy of Cipargamin (KAE609) in a Randomized, Phase II Dose-Escalation Study in Adults in Sub-Saharan Africa With Uncomplicated Plasmodium falciparum Malaria

Cited by 30 publications

References 22 publications

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

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

Catalytic Asymmetric Arylations of Ketimines

Facile Access to Structurally Diverse Antimalarial Indoles Using a One‐Pot A3 Coupling and Domino Cyclization Approach

Contact Info

Product

Resources

About

Facile Access to Structurally Diverse Antimalarial Indoles Using a One‐Pot A³ Coupling and Domino Cyclization Approach