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Efficacy, Safety, and PK of Ascending Dosages of Moxidectin Versus Ivermectin Against Strongyloides Stercoralis (StrongMoxi)

J

Jennifer Keiser

Status and phase

Unknown
Phase 2

Conditions

Strongyloides Stercoralis Infection

Treatments

Drug: Placebo oral tablet
Drug: Moxidectin
Drug: Ivermectin

Study type

Interventional

Funder types

Other

Identifiers

Details and patient eligibility

About

This study is a phase 2, blinded and randomized clinical trial. The phase 2a trial is single blinded and conducted in Lao, while the phase 2b trial is double-blinded and conducted in Lao and Cambodia. The study aims at providing evidence on effective doses and safety of moxidectin in adults against infection with S. stercoralis in Laos (trial 2a) and efficacy and safety of moxidectin compared to ivermectin in adults against infection with S. stercoralis in Laos and Cambodia (trial 2b). The efficacy of the treatment will be assessed by collecting three stool samples once pre-treatment and once 21 days post-treatment. The stool samples will be analyzed by a quantitative Baermann assay.

Full description

This is a phase 2a single-blinded and a phase 2b double-blinded randomized clinical trial, which aims to determine efficacy and safety of (2a) seven ascending oral moxidectin dosages in 210 adults infected with S. stercoralis, namely placebo, 2 mg, 4 mg, 6 mg, 8 mg, 10 mg, 12 mg in Lao and (2b) the recommended dose moxidectin (i.e. the most promising dosage identified in trial A; between 2-12 mg) in comparison to the standard treatment dose of ivermectin (200 µg/kg) in 245 adults infected with S. stercoralis in Lao and Cambodia. Embedded in the trial is a pharmacokinetic/-dynamic study with the goal to measure moxidectin disposition in adults and to determine population pharmacokinetic (PK) parameters of the optimal dose of moxidectin in the treatment of S. stercoralis.

The primary objective is to determine the dose-response of moxidectin based on cure rates (CR) against S. stercoralis and to quantify the efficacy of the recommended dose to the standard treatment (ivermectin) in adults.

The secondary objectives of the trial are: Evaluation of the safety and tolerability of the dose-dependent treatment regimes, evaluation of the safety and tolerability of moxidectin compared to ivermectin, comparison of the larvae reduction rate (LRR) of the different treatment regimens against S. stercoralis (trial 2a,b), determination of an exposure- (including Cmax, area under curve (AUC) and tmax) -response correlation of moxidectin in adults, comparison of the exposure-response of moxidectin using venous and capillary blood, evaluation of the cure rate of the different moxidectin treatment regimens against co-infection and the determination of the population PK parameters of the optimal dose of moxidectin in the treatment of S. stercoralis.

After obtaining informed consent from each individual, the medical history of the participants will be assessed with a standardized questionnaire, in addition to a clinical examination carried out by the study physician before treatment. Enrollment will be based on collection and analysis by a quantitative Baermann method (in duplicates) of three stool samples. Randomization of participants into the different treatment arms will be stratified according to intensity of infection. The adults will also be interviewed before treatment, 3 and 24 hours as well as 21 days after treatment about the occurrence of adverse events (AE). The efficacy of the treatment will be determined 21 days post-treatment by collecting another three stool samples. All stool samples will be examined with duplicate Baermann assays recorded quantitatively. Co-infection with T. trichiura, A. lumbricoides and hookworm infection will be identified using duplicate Kato-Katz thick smears on stool samples.

A subsample of adults will further be sampled using finger pricking for micro sampling at 0, 2, 4, 8, 24, and 72 hours, 7 and 21 days post treatment to evaluate pharmacokinetic parameters (trial phase 2a) and at defined time windows, that are based on the PK model earned from trial 2a (trial phase 2b). For validation of the analytical method the subsample of one study arm (8 mg, trial phase 2a) will undergo venous blood sampling in addition to finger pricking.

An available case analysis (full analysis set according to the intention to treat principle) will be performed, including all subjects with primary end point data. Supplementary, a per-protocol analysis will be conducted. CRs will be calculated as the percentage of larvae-positive subjects at baseline who become larvae-negative after treatment. Larvae per gram (LPG) stool sample will be assessed by calculating the mean of the larvae counts from the three duplicate Baermann assays and divided by the mean weighted amount of these stool samples. The LRR will be calculated following: (LRR = (1-(mean at follow-up/mean at baseline))*100) Geometric and arithmetic mean larvae counts will be calculated for the different treatment arms before and after treatment to assess the corresponding LRRs. Bootstrap resampling method with 2,000 replicates will be used to calculate 95% confidence intervals (CIs) for LRRs. Emax models using the dose finding package of the statistical software environment R will be implemented to predict the dose-response curves in terms of CRs and LRRs.

Enrollment

210 estimated patients

Sex

All

Ages

18 to 60 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

  • Adults (≥ 18 years) infected with S. stercoralis
  • Absence of major systemic illnesses
  • Written informed consent signed by individual

Exclusion criteria

  • Any abnormal medical conditions or chronic disease
  • Negative diagnostic result for S. stercoralis
  • No written informed consent by individual.
  • Pregnant and lactating women.
  • Recent use of anthelmintic drug (within past 4 weeks), attending other clinical trials during the study
  • Known allergy to study medications (i.e. moxidectin, ivermectin)
  • Currently taking medications with known interaction (i.e. for warfarin)

Trial design

Primary purpose

Treatment

Allocation

Randomized

Interventional model

Parallel Assignment

Masking

Single Blind

210 participants in 10 patient groups, including a placebo group

Phase 2a - Arm A
Experimental group
Description:
2 mg Moxidectin at day 0 administered orally
Treatment:
Drug: Moxidectin
Phase 2a - Arm B
Experimental group
Description:
4 mg Moxidectin at day 0 administered orally
Treatment:
Drug: Moxidectin
Phase 2a - Arm C
Experimental group
Description:
6 mg Moxidectin at day 0 administered orally
Treatment:
Drug: Moxidectin
Phase 2a - Arm D
Experimental group
Description:
8 mg Moxidectin at day 0 administered orally
Treatment:
Drug: Moxidectin
Phase 2a - Arm E
Experimental group
Description:
10 mg Moxidectin at day 0 administered orally
Treatment:
Drug: Moxidectin
Phase 2a - Arm F
Experimental group
Description:
12 mg Moxidectin at day 0 administered orally
Treatment:
Drug: Moxidectin
Phase 2a - Arm G
Placebo Comparator group
Description:
matching Placebo tablet(s) at day 0 administered orally
Treatment:
Drug: Placebo oral tablet
Phase 2b - Arm A
Experimental group
Description:
the recommended dose moxidectin (i.e. the most promising dosage identified in trial A; between 2-12 mg) at day 0 administered orally
Treatment:
Drug: Moxidectin
Phase 2b - Arm B
Active Comparator group
Description:
200 µg/kg ivermectin at day 0 administered orally
Treatment:
Drug: Ivermectin
Phase 2b - Arm P
Placebo Comparator group
Description:
matching Placebo tablet(s) at day 0 administered orally
Treatment:
Drug: Placebo oral tablet

Trial contacts and locations

2

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Data sourced from clinicaltrials.gov

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