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StrongMoxi_KH: Efficacy, Safety and PK of Moxidectin Versus Ivermectin Against Strongyloides Stercoralis

Sponsor
Jennifer Keiser (Other)
Overall Status
Enrolling by invitation
CT.gov ID
NCT04848688
Collaborator
National Centre for Parasitology, Entomology and Malaria Control, Cambodia (Other)
350
Enrollment
1
Location
2
Arms
9.8
Anticipated Duration (Months)
35.6
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

The study is an extension to the study StrongMoxi NCT04056325 and entails modifications based on the outcome of NCT04056325 part A.

The study is a phase 3, double-blinded and randomized clinical trial conducted in Cambodia. It aims at providing evidence on efficacy, safety and pharmacokinetic measures of 8 mg of moxidectin compared to 200 μg/kg ivermectin in adults infected with S. stercoralis. The efficacy of the treatment will be assessed by collecting three stool samples once per-treatment and once 21-28 days post-treatment. The stool samples will be analyzed by a quantitative duplicate Baermann assay.

Condition or Disease Intervention/Treatment Phase
  • Drug: Moxidectin 2 mg
  • Drug: Ivermectin 3 mg
  • Drug: Placebo
 Phase 3

Detailed Description

The study is a phase 3 trial and will determine the efficacy and safety of:

8 mg of moxidectin in comparison to the standard treatment dose of ivermectin (200 μg/kg) in adults infected with S. stercoralis and to measure moxidectin disposition in adults using a microsampling device.

Our primary objective is to demonstrate non-inferiority in terms of cure rate (CR) against S. stercoralis in adults of an oral 8 mg of moxidectin compared to 200 μg/kg of ivermectin.

The secondary objectives of the trial are:

  1. to evaluate the safety and tolerability of moxidectin

  2. to compare the larval reduction rate (LRR) of the two different treatment groups against

  1. stercoralis

  1. to evaluate the CRs and egg reduction rates (ERRs) of the different treatment drugs and regimens against soil-transmitted helminths (STH) co-infections.

  2. to determine the population pharmacokinetics (popPK) of moxidectin administered to S. stercoralis-infected in adolescents, as well as normal and underweight adults.

  3. to investigate potential extended effects on follow-up helminth prevalence at 42-49 and 63-70 days post-treatment

  4. to relate socioeconomic characteristics (SES), access to sanitation, water facilities, hygiene to baseline infection intensity.

  5. to determine the larval excretion pattern till day 70 in the moxidectin treatment arm, determined at every second day between day zero and 70 post-treatment in a subset of 50 adults.

  6. to determine the origin of the remaining worm burden after treatment to treatment failure and reinfection based on genetic profiling.

Three stool samples will be collected at baseline analysed in duplicates by a quantitative Baermann method for S. stercoralis infection. Co-infection with other Helminths species will be identified using duplicate Kato-Katz thick smears on two stool samples. The medical history of the participants will be assessed with a standardized questionnaire, in addition to a clinical and physical examination carried out by the study physician shortly before the treatment day. Each participant will be asked to provide a finger-prick blood sample for haemoglobin measurements at baseline. Enrolled participants will be treated with either 8 mg of moxidectin or with the standard treatment ivermectin (200 μg/kg). The adults will be interviewed a) before treatment, 3 and 24 hours as well as 21-28, 42-49 and 63-70 days after treatment about the occurrence of adverse events. The efficacy of the treatment will be determined 21-28 days of post-treatment. All stool samples will be examined with quantitative sixtuplicate Baermann assays and quadruplet Kato-Katz thick smears. At 42-49 and 63-70 days post-treatment another three stool samples will be collected and quantified for S. stercoralis larvae using Baermann assay to assess potential long-term benefits of the study drugs and treatment regimen. Of 50 adults in the moxidectin arm only, additional stool samples will be collected every second day between treatment and 70 days post treatment to evaluate larval secretion patterns.

To determine the PK parameters of the study drug, a subsample of 10 willing youngest adults (aged 18~20 years old) and voluntary 20 adults (aged 18-65) in the moxidectin arm will further be asked to provide 3 finger pricks of blood per participant. The finger pricks will be collected within three consecutive days of post-treatment application. Not more than two finger pricks will be taken on the same day. To all participating households, a brief questionnaire will be administered assessing information on socioeconomic characteristics (SES) and access to sanitation, water facilities, and hygiene behaviour.

An available case analysis (full analysis set according to the intention to treat principle) will be performed, including all participants with primary endpoint data.

CRs will be calculated as the percentage of larvae-positive subjects at baseline who become larvae-negative after treatment, assessed 21-28 days post-treatment by sextuplicate Baermann. Uncertainty estimates around the differences among CRs will be assessed using melded confidence intervals with mid-p correction. The non-inferiority.

Study Design

Study Type:
Interventional
Anticipated Enrollment :
350 participants
Allocation:
Randomized
Intervention Model:
Parallel Assignment
Intervention Model Description:
Parallel study with 2 treatment armsParallel study with 2 treatment arms
Masking:
Quadruple (Participant, Care Provider, Investigator, Outcomes Assessor)
Masking Description:
Double-blinded (Participant and Care provider) Additionally, the principal investigator and the statistician will be blinded. PK substudy is single-blinded (Participant)
Primary Purpose:
Treatment
Official Title:
Efficacy, Safety and Pharmacokinetics of Moxidectin and Its Comparison to Ivermectin Against Strongyloides Stercoralis in Adults: a Randomized Controlled Non-inferiority Trial
Actual Study Start Date :
Feb 5, 2022
Anticipated Primary Completion Date :
Oct 1, 2022
Anticipated Study Completion Date :
Dec 1, 2022

Arms and Interventions

Arm Intervention/Treatment
Experimental: Moxidectin

8 mg Moxidectin at day 0 administered orally

Drug: Moxidectin 2 mg
Monotherapy, oral administration, single-dose, fixed-dose, 4 tablets a 2 mg to yield an 8 mg final dose.

Drug: Placebo
Monotherapy, oral administration, single dose, matching number of tablets to either moxidectin or ivermectin
Experimental: Ivermectin

200 ug/kg Ivermectin at day 0 administered orally

Drug: Ivermectin 3 mg
Monotherapy, oral administration, single-dose, weight dependent, The number of tablets will be adjusted according to the patients' weight to yield 200 ug/kg final dose.

Drug: Placebo
Monotherapy, oral administration, single dose, matching number of tablets to either moxidectin or ivermectin

Outcome Measures

Primary Outcome Measures

  1. Cure rate against Strongyloides stercoralis [21-28 days after treatment]

    The conversion from being larvae positive pre-treatment to larvae negative post-treatment, or cure rate (CR).

Secondary Outcome Measures

  1. Larvae-reduction rate (LRR) against Strongyloidiasis stercoralis [21-28, 42-49 and 63-70 days after treatment (All) or every second day between day 0 and day 70 (Arm Moxidectin, n=50)]

    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)

  2. CRs against concomitant soil-transmitted helminth infections [21-28 days after treatment]

    CRs will be calculated for T. trichiura, A. lumbricoides and hookworm infections as described in primary outcome.

  3. Number of participants reporting adverse events [3 hours, 24 hours, 21-28 days, 42-49 days , 63-70 days after treatment]

    Subjects will be kept for observation for at least 3 hours following treatment for any acute adverse events. If there is any abnormal finding, the local study physician will perform a full clinical, physical and biochemical examination and findings will be recorded. An emergency kit will be available on-site to treat any medical conditions that warrant urgent medical intervention. In addition, patients will also be interviewed 3 and 24 hours and again at several points after treatment about the occurrence of adverse events. A standardized symptom questionnaire is used, that includes the recording of headache, abdominal pain, itching, nausea, vomiting, diarrhoea, allergic reaction as well as any further mentioned event by the participant.

  4. Maximum concentration (Cmax) of moxidectin in adults, young adults and adults with a BMI <19 [0-24 hours after treatment]

    Upon oral intake moxidectin levels in blood will be quantified with time using a micro sampling device. Moxidectin will be quantified using a validated liquid chromatography tandem mass spectrometry (LC-MS/MS) method. Drug concentrations will be calculated by interpolation from a calibration curve with a foreseen limit of quantification of approximately 5 ng/ml. The PK analysis will be undertaken fitting a structural compartmental PK model.

  5. Time to reach Cmax (tmax) of moxidectin in adults, young adults and adults with a BMI <19 [0-24 hours after treatment]

    Upon oral intake moxidectin levels in blood will be quantified with time using a micro sampling device. Moxidectin will be quantified using a validated liquid chromatography tandem mass spectrometry (LC-MS/MS) method. Drug concentrations will be calculated by interpolation from a calibration curve with a foreseen limit of quantification of approximately 5 ng/ml. The PK analysis will be undertaken fitting a structural compartmental PK model.

  6. Area under the curve (AUC) of moxidectin in adults, young adults and adults with a BMI <19 [0-24 hours after treatment]

    Upon oral intake, moxidectin levels in the blood will be quantified with time using a microsampling device. Moxidectin will be quantified using a validated liquid chromatography tandem mass spectrometry (LC-MS/MS) method. Drug concentrations will be calculated by interpolation from a calibration curve with a foreseen limit of quantification of approximately 5 ng/ml. The pharmacokinetic analysis will be undertaken fitting a structural compartmental PK model.

  7. Elimination half life (t1/2) of moxidectin in adults, young adults and adults with a BMI <19 [0-24 hours after treatment]

    Upon oral intake, moxidectin levels in the blood will be quantified with time using a microsampling device. Moxidectin will be quantified using a validated liquid chromatography tandem mass spectrometry (LC-MS/MS) method. Drug concentrations will be calculated by interpolation from a calibration curve with a foreseen limit of quantification of approximately 5 ng/ml. The pharmacokinetic analysis will be undertaken fitting a structural compartmental pharmacokinetic model.

  8. Genetic profiling of S. stercoralis positive stool samples [Pre-treatment]

    From all S. stercoralis positive stool samples, the extracted larvae will be stored in 70% Ethanol after examination by Baermann. Samples will be shipped to the investigating laboratory (La Trobe University) at room temperature.

  9. Socioeconomic characteristics (SES) [Pre-treatment]

    To all participating households, a brief questionnaire will be administered assessing information on socioeconomic characteristics (SES) and access to sanitation, water facilities, and hygiene behaviour.

Eligibility Criteria

Criteria

Ages Eligible for Study:
18 Years to 65 Years
Sexes Eligible for Study:
All
Accepts Healthy Volunteers:
No
Inclusion Criteria:

  • Adults (18-65 years)

  • Infected with S. stercoralis (positive)

  • Absence of major systemic illnesses

  • Written informed consent

Exclusion Criteria:

  • Any abnormal medical conditions or chronic disease

  • Negative diagnostic result for S. stercoralis

  • No written informed consent by the individual.

  • Pregnant and lactating women.

  • Recent use of an 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)

Contacts and Locations

Locations

Site City State Country Postal Code
1 National Centre for Parasitology, Entomology and Malaria Control Phnom Penh Cambodia

Sponsors and Collaborators

  • Jennifer Keiser
  • National Centre for Parasitology, Entomology and Malaria Control, Cambodia

Investigators

  • Principal Investigator: Jennifer Keiser, Prof. Dr, STPH

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.
Responsible Party:
Jennifer Keiser, Prof. Jennifer Keiser, PhD, Swiss Tropical & Public Health Institute
ClinicalTrials.gov Identifier:
NCT04848688
Other Study ID Numbers:
  • 4
First Posted:
Apr 19, 2021
Last Update Posted:
Jun 13, 2022
Last Verified:
Jun 1, 2022
Individual Participant Data (IPD) Sharing Statement:
Undecided
Plan to Share IPD:
Undecided
Studies a U.S. FDA-regulated Drug Product:
No
Studies a U.S. FDA-regulated Device Product:
No
Additional relevant MeSH terms:
Strongyloidiasis
Ivermectin
Moxidectin

Study Results

No Results Posted as of Jun 13, 2022