Safety, Tolerability, and Parasite Clearance Kinetics in Controlled Human Malaria Infection after Direct Venous Inoculation of Plasmodium falciparum Sporozoites: A Model for Evaluating New Blood-Stage Antimalarial Drugs.

Adult Animals Antimalarials / adverse effects Artemether / therapeutic use Artemether, Lumefantrine Drug Combination / adverse effects Humans Malaria / drug therapy Parasitemia / drug therapy Parasites Plasmodium falciparum Sporozoites

Journal

The American journal of tropical medicine and hygiene
ISSN: 1476-1645
Titre abrégé: Am J Trop Med Hyg
Pays: United States
ID NLM: 0370507

Informations de publication

Date de publication:
12 10 2022
Historique:
received: 15 12 2021
accepted: 16 03 2022
pubmed: 30 8 2022
medline: 19 10 2022
entrez: 29 8 2022
Statut: epublish

Résumé

Plasmodium falciparum sporozoite (PfSPZ) direct venous inoculation (DVI) using cryopreserved, infectious PfSPZ (PfSPZ Challenge [Sanaria, Rockville, Maryland]) is an established controlled human malaria infection model. However, to evaluate new chemical entities with potential blood-stage activity, more detailed data are needed on safety, tolerability, and parasite clearance kinetics for DVI of PfSPZ Challenge with established schizonticidal antimalarial drugs. This open-label, phase Ib study enrolled 16 malaria-naïve healthy adults in two cohorts (eight per cohort). Following DVI of 3,200 PfSPZ (NF54 strain), parasitemia was assessed by quantitative polymerase chain reaction (qPCR) from day 7. The approved antimalarial artemether-lumefantrine was administered at a qPCR-defined target parasitemia of ≥ 5,000 parasites/mL of blood. The intervention was generally well tolerated, with two grade 3 adverse events of neutropenia, and no serious adverse events. All 16 participants developed parasitemia after a mean of 9.7 days (95% CI 9.1-10.4) and a mean parasitemia level of 511 parasites/mL (95% CI 369-709). The median time to reach ≥ 5,000 parasites/mL was 11.5 days (95% CI 10.4-12.4; Kaplan-Meier), at that point the geometric mean (GM) parasitemia was 15,530 parasites/mL (95% CI 10,268-23,488). Artemether-lumefantrine was initiated at a GM of 12.1 days (95% CI 11.5-12.7), and a GM parasitemia of 6,101 parasites/mL (1,587-23,450). Mean parasite clearance time was 1.3 days (95% CI 0.9-2.1) and the mean log10 parasite reduction ratio over 48 hours was 3.6 (95% CI 3.4-3.7). This study supports the safety, tolerability, and feasibility of PfSPZ Challenge by DVI for evaluating the blood-stage activity of candidate antimalarial drugs.

Identifiants

DOI: 10.4269/ajtmh.21-1297 PMID: 36037868 PMC: PMC9651526
pubmed: 36037868
doi: 10.4269/ajtmh.21-1297
pii: tpmd211297
pmc: PMC9651526
doi:

Substances chimiques

Antimalarials 0
Artemether, Lumefantrine Drug Combination 0
Artemether C7D6T3H22J

Types de publication

Clinical Trial, Phase I Journal Article Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

IM

Pagination

804-814

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Auteurs

M Farouk Chughlay (MF)

Medicines for Malaria Venture, Geneva, Switzerland.

Stephan Chalon (S)

Medicines for Malaria Venture, Geneva, Switzerland.

Myriam El Gaaloul (M)

Medicines for Malaria Venture, Geneva, Switzerland.

Nathalie Gobeau (N)

Medicines for Malaria Venture, Geneva, Switzerland.

Jörg J Möhrle (JJ)

Medicines for Malaria Venture, Geneva, Switzerland.

Pieter-Jan Berghmans (PJ)

SGS Life Sciences, Antwerp, Belgium.

Katrin Van Leuven (K)

SGS Life Sciences, Antwerp, Belgium.

Michael W Marx (MW)

ICON Clinical Research GmbH, Langen, Germany.

Anna Rosanas-Urgell (A)

Department of Biomedical Sciences, Institute of Tropical Medicine, Antwerp, Belgium.

Julia Flynn (J)

Medicines for Malaria Venture, Geneva, Switzerland.

Emilie Escoffier (E)

Medicines for Malaria Venture, Geneva, Switzerland.

Daniel Izquierdo-Juncàs (D)

SGS Life Sciences, Antwerp, Belgium.

Bastiaan Jansen (B)

SGS Life Sciences, Antwerp, Belgium.

Venelin Mitov (V)

IntiQuan GmbH, Basel, Switzerland.

Anne Kümmel (A)

IntiQuan GmbH, Basel, Switzerland.

Jean-Pierre Van Geertruyden (JP)

Global Health Institute, University of Antwerp, Antwerp, Belgium.

Karen I Barnes (KI)

Division of Clinical Pharmacology, Department of Medicine, University of Cape Town, Cape Town, South Africa.
University of Cape Town Medical Research Council Collaborating Centre for Optimizing Antimalarial Therapy, University of Cape Town, Cape Town, South Africa.

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Classifications MeSH

questionsmedicales.fr Personnes Tranches d'âge Adulte Safety, Tolerability, and Parasite Clearance...
questionsmedicales.fr Eucaryotes Animaux Safety, Tolerability, and Parasite Clearance...
questionsmedicales.fr Actions chimiques et utilisations Actions pharmacologiques Utilisations thérapeutiques Anti-infectieux Antiparasitaires Antiprotozoaires Antipaludiques Safety, Tolerability, and Parasite Clearance...
questionsmedicales.fr Composés chimiques organiques Hydrocarbures Terpènes Sesquiterpènes Artémisinines Artéméther Safety, Tolerability, and Parasite Clearance...
questionsmedicales.fr Préparations pharmaceutiques Association médicamenteuse Association d'artéméther et de luméfantrine Safety, Tolerability, and Parasite Clearance...
questionsmedicales.fr Eucaryotes Animaux Chordés Vertébrés Mammifères Eutheria Primates Haplorhini Catarrhini Hominidae Humains Safety, Tolerability, and Parasite Clearance...
questionsmedicales.fr Infection Maladies vectorielles Paludisme Safety, Tolerability, and Parasite Clearance...
questionsmedicales.fr États, signes et symptômes pathologiques Processus pathologiques Inflammation Sepsie Parasitémie Safety, Tolerability, and Parasite Clearance...
questionsmedicales.fr Eucaryotes Animaux Invertébrés Parasites Safety, Tolerability, and Parasite Clearance...
questionsmedicales.fr Eucaryotes Alveolata Apicomplexa Haemosporida Plasmodium Plasmodium falciparum Safety, Tolerability, and Parasite Clearance...
questionsmedicales.fr Phénomènes physiologiques Croissance et développement Morphogenèse Métamorphose biologique Étapes du cycle de vie Oocystes Sporozoïtes Safety, Tolerability, and Parasite Clearance...