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Safety and Tolerability Study of Acoziborole in g-HAT Seropositive Subjects (OXA004)

Primary Purpose

Trypanosomiasis, African, Trypanosoma Brucei Gambiense; Infection, Sleeping Sickness

Status
Completed
Phase
Phase 2
Locations
International
Study Type
Interventional
Intervention
Acoziborole
Placebo
Sponsored by
Drugs for Neglected Diseases
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Trypanosomiasis, African focused on measuring Human African Trypanosomiasis, Trypanosoma Brucei Gambiense, Sleeping sickness, g-HAT, g-HAT seropositive individuals

Eligibility Criteria

15 Years - undefined (Child, Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  • Signed the informed consent form
  • Male or female
  • 15 years of age or older
  • CATT test or HAT sero-K-set RDT positive
  • Parasitology negative (in blood and/or lymph if lymphadenopathy is present)
  • Karnofsky Performance Status above 70
  • Able to ingest oral tablets
  • Known address and/or contact details provided
  • Must be able to comply with the schedule of follow-up visits and other requirements of the study
  • Agreement to be hospitalised upon enrolment for at least 5 days (in order to receive in-ward post-treatment observational follow-up through the first 5 days after treatment)
  • Agreement to not take part in any other clinical trials during the participation in this study
  • For women of childbearing potential:

    • Must agree to have protected sexual relations to avoid becoming pregnant from enrolment up to 3 months after dosing
    • Negative urine pregnancy tests

Exclusion Criteria:

  • Individuals parasitologically confirmed in blood and/or lymph
  • Previously treated for g-HAT
  • Severe malnutrition, defined as body mass index (BMI) <16 kg/m2
  • Pregnant or breast-feeding women
  • For women of childbearing potential:

    • Urine pregnancy test positive
    • Do not accept contraceptive protection from enrolment up to 3 months after dosing
  • Clinically significant medical condition and/or abnormal laboratory results that could, in the opinion of the Investigator, jeopardise the subject's safety or participation in the study

Additional exclusion criteria for the TrypSkin exploratory sub-study:

  • Rejection to participate in the exploratory sub-study in the signed ICF
  • Known diabetes
  • Known haemophilia

Sites / Locations

  • General Referral Hospital of Bagata
  • Hospital of Dipumba
  • General Referral Hospital of Idiofa
  • General Referral Hospital of Masi-Manimba
  • General Referral Hospital of Kwamouth
  • General Hospital of Bandundu
  • General Referral Hospital of Dubreka

Arms of the Study

Arm 1

Arm 2

Arm Type

Active Comparator

Placebo Comparator

Arm Label

Acoziborole

Placebo

Arm Description

Single dose administration of 3 tablets of 320 mg

Single dose administration of 3 tablets of 320 mg

Outcomes

Primary Outcome Measures

Occurrence of treatment-emergent adverse events (TEAEs)
Occurrence of any Treatment Emergent Adverse Event from investigational product administration to 4 month follow-up visit

Secondary Outcome Measures

Occurrence of adverse events (AEs)
Occurrence of any Adverse Event from Inform Consent signature to 4 month follow-up visit
Change from baseline in biochemistry parameter: Alanine Aminotransferase
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Albumin
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Alkaline Phosphatase
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Aspartate Aminotransferase
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Calcium
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Chloride
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Creatinine
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Glucose
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Potassium
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Sodium
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Total Bilirubin
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Total Carbon Dioxide
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Total Protein
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in biochemistry parameter: Blood Urea Nitrogen
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in hematology parameter: hemoglobin
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in hematology parameter: Platelets
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in hematology parameter: white blood cells
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Change from baseline in ECG (Electrocardiogram) parameter: heart rate (HR)
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Change from baseline in ECG (Electrocardiogram) parameter: RR interval
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Change from baseline in ECG (Electrocardiogram) parameter: PR interval
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Change from baseline in ECG (Electrocardiogram) parameter: QRS interval
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Change from baseline in ECG (Electrocardiogram) parameter: QT interval
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Change from baseline in ECG (Electrocardiogram) parameter: QTc interval
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Blood concentration of acoziborole at Day 5 and Month 1
Concentration of acoziborole in whole blood at Day 5 and Month 1
Correlation between ΔQTc measurements and acoziborole concentrations in blood at Day 5

Full Information

First Posted
January 17, 2022
Last Updated
August 4, 2023
Sponsor
Drugs for Neglected Diseases
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1. Study Identification

Unique Protocol Identification Number
NCT05256017
Brief Title
Safety and Tolerability Study of Acoziborole in g-HAT Seropositive Subjects
Acronym
OXA004
Official Title
Safety and Tolerability Study of Acoziborole in g-HAT Seropositive Non-parasitologically Confirmed Subjects: a Multicentre Randomised Double-blind Placebo-controlled Study
Study Type
Interventional

2. Study Status

Record Verification Date
August 2023
Overall Recruitment Status
Completed
Study Start Date
December 30, 2021 (Actual)
Primary Completion Date
August 2, 2023 (Actual)
Study Completion Date
August 2, 2023 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Drugs for Neglected Diseases

4. Oversight

Studies a U.S. FDA-regulated Drug Product
No
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
Yes

5. Study Description

Brief Summary
Acoziborole as an oral, single-dose treatment was studied in an open-label pivotal Phase II/III trial (DNDi-OXA-02-HAT) in DRC and Guinea. The safety and efficacy results on g-HAT confirmed cases (all disease stages) from the pivotal study provided data, that allows to envision the treatment of confirmed g-HAT cases but there is still a gap in the management of g-HAT seropositive non-parasitologically confirmed individuals. Indeed, the standard g-HAT case definition implies the demonstration of the parasite in any body fluid via microscopy. However, there are factors such as low parasitaemia and the complexity and low sensitivity of parasitological methods that make such demonstration difficult. It has been demonstrated that a variable proportion (mainly depending on the prevalence) of such g-HAT "sero-suspects" are confirmed cases and, therefore, remaining as potential reservoirs of the parasite and a source of new infections hindering the efforts to eliminate the disease. The present clinical trial intends to expand the safety data of acoziborole and complement the safety profile obtained from the pivotal trial by assessing the safety and tolerability of a single dose of acoziborole compared with placebo in seropositive individuals who are not confirmed parasitologically. In addition to this study, an exploratory sub-study named 'TrypSkin' is planned to assess the presence of extravascular dermal T.b. gambiense in the population enrolled.
Detailed Description
HAT is a neglected tropical disease, transmitted by the bite of a tsetse fly, affecting sub-Saharan African countries. Without prompt diagnosis and treatment, it is usually fatal, as the parasites responsible for HAT (Trypanosoma brucei gambiense [T.b. gambiense or g-HAT] or Trypanosoma brucei rhodesiense [T.b. rhodesiense]) invade the central nervous system (late stage of the disease) causing neurological changes which include among other symptoms sleep disorder, aggression, sensory disturbances, psychosis, seizures, coma, and ultimately death. Eight and a half million people, living mainly in rural parts of East, West, and Central Africa, are situated in areas where g-HAT is still considered a public health problem. Whereas, fifty-three million people are estimated to be at risk of infection on the African continent. Few therapeutic options are currently available to treat g-HAT at either the haemolymphatic (early) stage or meningoencephalitic (late) stage. When early stage g-HAT is diagnosed, patients can be treated in their villages with intramuscular injections of pentamidine for 7 days. In patients with late-stage g-HAT, nifurtimox-eflornithine combination therapy (NECT), a combination of oral nifurtimox for 10 days plus eflornithine, two 2-hour intravenous (IV) infusions daily for 7 days, was found to provide similar cure rates to the standard regimen with eflornithine for 14 days, but with obvious practical advantages, including ease of administration and a shorter duration of treatment. In December 2018, Fexinidazole was approved for the treatment of g-HAT in the Democratic Republic of Congo (DRC), which is an effective 10-day oral treatment, able to cure early and late stage patients, although an increased risk of relapse on very advanced patients keeps NECT as first line treatment for patients showing more than 100 white blood cells (WBC)/µL of cerebrospinal fluid on diagnosis. Whilst the delivery of fexinidazole has improved the management of g-HAT cases and facilitates the integration of HAT treatment into the general health system, Acoziborole (studied in an open-label pivotal Phase II/III trial) as an oral, single-dose treatment envisioned for all stages of g-HAT is expected to improve further the management of g-HAT cases. However, there is still a gap in the management of g-HAT seropositive non-parasitologically confirmed individuals. Indeed, the standard g-HAT case definition implies the demonstration of the parasite in any body fluid via microscopy. But, there are factors such as low parasitaemia and the complexity and low sensitivity of parasitological methods that make such demonstration difficult. It has been demonstrated that a variable proportion (mainly depending on the prevalence) of such g-HAT "sero-suspects" are confirmed cases and, therefore, remaining as potential reservoirs of the parasite and a source of new infections hindering the efforts to eliminate the disease. The present clinical trial intends to expand the safety data of acoziborole and complement the safety profile obtained from the pivotal trial by assessing the safety and tolerability of a single dose of acoziborole compared with placebo in seropositive individuals who are not confirmed parasitologically. In addition to this study, an exploratory sub-study named 'TrypSkin' is planned to assess the presence of extravascular dermal T.b. gambiense in the population enrolled. Indeed, in an observational cohort study conducted in Guinea, the presence of extravascular dermal trypanosomes has been observed in individuals presenting with CATT positive results in plasma dilution ≥1:4 but not confirmed by parasitological examination of blood and lymph. If these dermal trypanosomes correspond to T.b. gambiense subspecies and are able to infect vectors, these individuals could act as reservoirs for the transmission of g-HAT, hampering the elimination goal.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Trypanosomiasis, African, Trypanosoma Brucei Gambiense; Infection, Sleeping Sickness
Keywords
Human African Trypanosomiasis, Trypanosoma Brucei Gambiense, Sleeping sickness, g-HAT, g-HAT seropositive individuals

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 2, Phase 3
Interventional Study Model
Parallel Assignment
Model Description
2 arms (acoziborole and placebo, ratio 3:1); 5 days post drug administration of hospitalization; follow-up visits at Month 1 and Month 4 (End of Study Visit)
Masking
ParticipantCare ProviderInvestigatorOutcomes Assessor
Allocation
Randomized
Enrollment
1208 (Actual)

8. Arms, Groups, and Interventions

Arm Title
Acoziborole
Arm Type
Active Comparator
Arm Description
Single dose administration of 3 tablets of 320 mg
Arm Title
Placebo
Arm Type
Placebo Comparator
Arm Description
Single dose administration of 3 tablets of 320 mg
Intervention Type
Drug
Intervention Name(s)
Acoziborole
Intervention Description
Acoziborole tablets
Intervention Type
Drug
Intervention Name(s)
Placebo
Intervention Description
matching placebo of acoziborole tablets
Primary Outcome Measure Information:
Title
Occurrence of treatment-emergent adverse events (TEAEs)
Description
Occurrence of any Treatment Emergent Adverse Event from investigational product administration to 4 month follow-up visit
Time Frame
From Investigational Product administration to 4 months follow up visit (End of Study)
Secondary Outcome Measure Information:
Title
Occurrence of adverse events (AEs)
Description
Occurrence of any Adverse Event from Inform Consent signature to 4 month follow-up visit
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Alanine Aminotransferase
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Albumin
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Alkaline Phosphatase
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Aspartate Aminotransferase
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Calcium
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Chloride
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Creatinine
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Glucose
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Potassium
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Sodium
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Total Bilirubin
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Total Carbon Dioxide
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Total Protein
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in biochemistry parameter: Blood Urea Nitrogen
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in hematology parameter: hemoglobin
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in hematology parameter: Platelets
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in hematology parameter: white blood cells
Description
Changes from baseline at D5, M1 and M4 will be will be presented by treatment group and summarized using mean, standard deviation, median, interquartile range (Q1-Q2) and range (minimum - maximum). Changes from baseline will also be presented as shift table expressed by % of subjects with low, normal or high value for each parameter and each timepoint.
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Change from baseline in ECG (Electrocardiogram) parameter: heart rate (HR)
Description
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Time Frame
From Inform Consent signature to Day 5 (end of Hospitalization)
Title
Change from baseline in ECG (Electrocardiogram) parameter: RR interval
Description
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Time Frame
From Inform Consent signature to Day 5 (end of Hospitalization)
Title
Change from baseline in ECG (Electrocardiogram) parameter: PR interval
Description
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Time Frame
From Inform Consent signature to Day 5 (end of Hospitalization)
Title
Change from baseline in ECG (Electrocardiogram) parameter: QRS interval
Description
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Time Frame
From Inform Consent signature to Day 5 (end of Hospitalization)
Title
Change from baseline in ECG (Electrocardiogram) parameter: QT interval
Description
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Time Frame
From Inform Consent signature to Day 5 (end of Hospitalization)
Title
Change from baseline in ECG (Electrocardiogram) parameter: QTc interval
Description
change from baseline (Δ) at D5 will be summarized by treatment group and Placebo -corrected change from baseline (ΔΔ) will be calculated using an analysis of covariance model adjusting for sex and age.
Time Frame
From Inform Consent signature to Day 5 (end of Hospitalization)
Title
Blood concentration of acoziborole at Day 5 and Month 1
Description
Concentration of acoziborole in whole blood at Day 5 and Month 1
Time Frame
Day 5 and 1 month follow-up visit
Title
Correlation between ΔQTc measurements and acoziborole concentrations in blood at Day 5
Time Frame
Day 5
Other Pre-specified Outcome Measures:
Title
Exploratory outcome: occurrence of dermatitis and/or pruritus
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Exploratory outcome: occurrence of positive results on blood and skin samples analyzed by Immuno-Histochemistry (IHC), TBR- PCR and/or 18S-PCR
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Exploratory outcome: occurrence of positive results on blood and skin samples analyzed by qPCRs, multiplex qRT-PCRs and SHERLOCK (Specific High-sensitivity Enzymatic Reporter unlocking)
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Exploratory outcome: descriptive comparisons between groups and timepoints in occurrence of dermatitis, pruritus, positive results in skin and blood samples analyzed by IHC, qPCRs, multiplex qRT-PCRs and SHERLOCK
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)
Title
Exploratory outcome: occurrence comparisons between all diagnostic methods alone or in combination
Time Frame
From Inform Consent signature to 4 months follow up visit (End of Study)

10. Eligibility

Sex
All
Minimum Age & Unit of Time
15 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: Signed the informed consent form Male or female 15 years of age or older CATT test or HAT sero-K-set RDT positive Parasitology negative (in blood and/or lymph if lymphadenopathy is present) Karnofsky Performance Status above 70 Able to ingest oral tablets Known address and/or contact details provided Must be able to comply with the schedule of follow-up visits and other requirements of the study Agreement to be hospitalised upon enrolment for at least 5 days (in order to receive in-ward post-treatment observational follow-up through the first 5 days after treatment) Agreement to not take part in any other clinical trials during the participation in this study For women of childbearing potential: Must agree to have protected sexual relations to avoid becoming pregnant from enrolment up to 3 months after dosing Negative urine pregnancy tests Exclusion Criteria: Individuals parasitologically confirmed in blood and/or lymph Previously treated for g-HAT Severe malnutrition, defined as body mass index (BMI) <16 kg/m2 Pregnant or breast-feeding women For women of childbearing potential: Urine pregnancy test positive Do not accept contraceptive protection from enrolment up to 3 months after dosing Clinically significant medical condition and/or abnormal laboratory results that could, in the opinion of the Investigator, jeopardise the subject's safety or participation in the study Additional exclusion criteria for the TrypSkin exploratory sub-study: Rejection to participate in the exploratory sub-study in the signed ICF Known diabetes Known haemophilia
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Victor Kande Betu Ku Mesu, Dr.
Organizational Affiliation
Ministry of Public Health, Hygiene and Prevention, Kinshasa
Official's Role
Principal Investigator
Facility Information:
Facility Name
General Referral Hospital of Bagata
City
Kwilu
State/Province
Bandundu
Country
Congo, The Democratic Republic of the
Facility Name
Hospital of Dipumba
City
Mbuji-Mayi
State/Province
Kasai-Oriental
Country
Congo, The Democratic Republic of the
Facility Name
General Referral Hospital of Idiofa
City
Idiofa
State/Province
Kwilu
Country
Congo, The Democratic Republic of the
Facility Name
General Referral Hospital of Masi-Manimba
City
Masi-Manimba
State/Province
Kwilu
Country
Congo, The Democratic Republic of the
Facility Name
General Referral Hospital of Kwamouth
City
Kwamouth
State/Province
Mai-Ndombe
Country
Congo, The Democratic Republic of the
Facility Name
General Hospital of Bandundu
City
Bandundu
Country
Congo, The Democratic Republic of the
Facility Name
General Referral Hospital of Dubreka
City
Dubréka
State/Province
Dubreka
Country
Guinea

12. IPD Sharing Statement

Learn more about this trial

Safety and Tolerability Study of Acoziborole in g-HAT Seropositive Subjects

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