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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT04188301
Other study ID # 201910085
Secondary ID
Status Completed
Phase Phase 2
First received
Last updated
Start date December 6, 2019
Est. completion date June 1, 2022

Study information

Verified date June 2024
Source Washington University School of Medicine
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This DOLF study will investigate the safety and effectiveness of IDA treatment in persons with onchocerciasis when it is administered after pre-treatment with ivermectin to clear or greatly reduce microfilariae from the skin and eyes.


Description:

This study will provide preliminary data on the safety of IDA treatment in persons with onchocerciasis when it is administered after pre-treatment with IVM to clear or greatly reduce microfilariae from the skin and eyes. Widespread use of IDA following IVM pretreatment (I/IDA) has the potential to greatly accelerate elimination of lymphatic filariasis (LF) in African countries that are co-endemic for LF and onchocerciasis. study later. This study will also assess the efficacy of IDA for killing and sterilizing adult filarial worms. An improved macrofilaricidal treatment would be a major advance for the global program to eliminate onchocerciasis. Since the safety and efficacy objectives are both very important, we have included dual primary objectives for the study. Primary objectives: - Safety: To compare rates and types of severe adverse events (grade 3 or higher) that occur within 7 days following 1 day or 3 days of treatment with triple drug treatment ("IDA" = diethylcarbamazine (DEC) with ivermectin (IVM) and albendazole (ALB)) with the comparator regimen of 1 day of treatment with ivermectin and albendazole (IA) in persons with active Onchocerca volvulus infections after pretreatment with ivermectin alone. - Efficacy: To compare the effect of three treatment regimens (1 day of IDA, 3 days of IDA, or IA) for killing or sterilizing adult female O. volvulus worms based on the percentage of all adult female worms in nodules that are alive with embryos in the uterus 18 months after treatment. This is an open label, randomized clinical trial.


Recruitment information / eligibility

Status Completed
Enrollment 154
Est. completion date June 1, 2022
Est. primary completion date March 14, 2022
Accepts healthy volunteers No
Gender All
Age group 16 Years to 70 Years
Eligibility Inclusion Criteria: - Men and women who were previously enrolled in the preceding Part I study (Protocol ID#201804116) and residing in the study area - Must have at least palpable subcutaneous nodule (onchocercoma) - Participants with baseline skin Mf counts less than or equal to 3 Mf/mg at the time of enrollment into the Part I study (Protocol ID#201804116) Exclusion Criteria: - Pregnant and breastfeeding mothers within 1 month of giving birth - Severe eye disease at baseline including uveitis, severe glaucoma, severe keratitis, and/or cataracts that interfere with visualization of the posterior segment of the eye as well as the list of ocular diseases as outlined below. All ocular disease exclusion criteria apply to either eye. Bilateral disease is not necessary to exclude a participant. A participant will be excluded if any of the criteria are met for one eye. 1. Any cataract of any type preventing clear visualization of fundus or imaging on Optical Coherence Tomography (OCT). 2. Severe retinal nerve fiber layer thinning in the superior and inferior quadrant analysis on Ocular Coherence Tomography of the optic nerve with a corresponding visual field defect of grade 2 or worse on the same eye.If Ocular Coherence Tomography is not available, the following exclusion criteria will apply: vertical Cup/disc ratio on fundoscopy (not by OCT reading) greater than or equal to 0.80. 3. Intraocular pressure (IOP) greater than or equal to 25 by Goldmann tonometry .12 4. Retinal Detachment or Retinal Break 5. Acute ocular infection (i.e., Viral conjunctivitis, corneal ulcer, endophthalmitis) 6. Optic Atrophy with visual field defect reproducible on confrontation visual field testing.. 7. Exam consistent with Herpes Simplex Virus eye infection 8. Homonymous hemianopsia, quadrantanopsia, bitemporal hemianopsia, or central scotoma related to cerebral vascular disease by Automated Visual Field testing and confrontation visual field testing. 9. Acute Angle Closure Glaucoma 10. Gonioscopy grade 0 (slit) limiting ability to safely dilate patient 11. Severe Tremor, blepharospasm, or other voluntary or involuntary motor condition that prevents ability to examine patient with slit lamp, OCT, gonioscopy, IOP measurement, fundus photography, and Frequency doubling technology perimetry. 12. Cognitive impairment sufficient to prevent ability to understand and perform Visual Acuity Test with Tumbling E chart, confrontation visual field, slit lamp exam, or any other ocular exam component. 13. Optic nerve edema 14. Active retinopathy or retinitis not attributable to onchocercal disease 15. History of uveitis not associated with onchocercal disease 16. Any pre-existing chorioretinal scar or retinal degeneration and other significant retinal pathologies (foveomacular schisis, dystrophies, arterial macroaneurysms etc) involving the macula. 17. Severe ocular pain, that patient rates as 9 or 10 out of 10 pain. 18. Best corrected or pinhole visual acuity worse than 6/60 (20/200) 19. Age related macular degeneration (AMD) - Significant comorbidities such as renal insufficiency, liver failure, or any other acute or chronic illness identified by study clinicians and investigators that interferes with the participant's ability to go to school or work or perform routine household chores. - Prior allergic / hypersensitivity reactions or intolerance to IVM, ALB, or DEC. - Treatment with IVM outside of the study after the pre-treatment clearing dose provided in the Part I study. - >5 motile Mf in the anterior chamber in either eye at the time of enrollment (after pre-treatment with IVM). - Any Mf identified in the posterior segment of the eye at the time of enrollment (six months after pre-treatment with IVM). - Any other condition identified by study clinicians or investigators that may preclude participation in the study.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
IVM w/ ALB
Participants will be given a single dose of oral IVM (150 µg/kg) plus ALB (400 mg) (IVM/ALB)
Single dose of IDA
Participants will be given a single dose of oral IVM (150 µg/kg), DEC (6 mg/kg) and ALB (400 mg)
Three daily doses of IDA
Participants will be given one daily dose for 3 days of oral IVM (150 µg/kg), DEC (6 mg/kg) and ALB (400 mg)

Locations

Country Name City State
Ghana University of Health and Allied Sciences Hohoe

Sponsors (3)

Lead Sponsor Collaborator
Washington University School of Medicine Case Western Reserve University, University of Health and Allied Sciences

Country where clinical trial is conducted

Ghana, 

References & Publications (41)

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* Note: There are 41 references in allClick here to view all references

Outcome

Type Measure Description Time frame Safety issue
Primary Rates of Severe Adverse Events (SAEs) Across Study Arms Rates of severe adverse events (grade 3 or higher) following 1-day or 3-day triple drug treatment will be compared against those of the comparator regimen of 1 day of IVM/ALB. Within 7 days following end of treatment
Primary Percentage of Worms Killed Across Study Arms The effect of three treatment regimens for killing adult female O. volvulus worms will be compared based on the percentage of all adult female worms in nodules that are alive with embryos in the uterus 18 months after treatment. 18 months following treatment.
Primary Percentage of Worms Sterilized Across Study Arms The effect of three treatment regimens for sterilizing adult female O. volvulus worms will be compared based on the percentage of all adult female worms that are fertile in the nodules 18 months after treatment. 18 months following treatment.
Secondary Rates of SAEs by Treatment Group in Those With Intraocular Microfilariae Just Prior to Treatment With IDA Rates of adverse events grade 3 or higher that occur within 7 days of treatment in the subset of participants who have intraocular microfilariae just prior to treatment with IDA will be compared by treatment group. within 7 days following end of treatment
Secondary Rates of Ocular Adverse Events (Any Grade) by Treatment Group Rates of ocular adverse events of any grade within 3 months will be compared by treatment group. within 3 months of treatment with IDA
Secondary Effectiveness of Killing Adult Female Worms The effectiveness of three treatment regimens for killing adult female O. volvulus worms based on the percentage of all adult female worms in nodules that are alive 18 months after treatment. 18 months following treatment
Secondary Effectiveness of Clearing Microfilariae From Skin by Skin Snips The effectiveness of three treatment regimens for complete clearance of microfilariae from the skin as determined by skin snips at 3, 12, and 18 months after treatment with IDA will be compared by treatment arm. Baseline, 3 months, 12 months, & 18 months following treatment.
Secondary Effectiveness for Preventing Reappearance of Microfilariae in the Skin by Skin Snips The effectiveness of three treatment regimens for preventing reappearance of microfilariae in the skin as determined by skin snips at 12 and 18 months after treatment will be compared by treatment arm. Measured by the presence of microfilariae in skin snips. Baseline, 12 months, and 18 months following treatment
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