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| ID | Type | Description | Link |
|---|---|---|---|
| R01HD095562 | U.S. NIH Grant/Contract | View source |
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| Name | Class |
|---|---|
| London School of Hygiene and Tropical Medicine | OTHER |
| University of Liverpool | OTHER |
| Research Institute for Tropical Medicine, Philippines | OTHER_GOV |
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The overall goals of this proposal are to conduct a trial to address the significant gaps with respect to our understanding of best approaches to treatment of children ages 1-4 with intestinal schistosomiasis. Over 200 million individuals worldwide are infected with one of three predominant species of schistosomes, with over half of infections occurring in children. Recent studies have highlighted the fact that many children experience first infections before the age of two, with the prevalence of infection among children under four mirroring the prevalence of older children from the same community. Importantly, praziquantel (PZQ), the drug used worldwide for the treatment of schistosomiasis, is only FDA approved among adults and children over the age of four. Only one small study led by co-PI Bustinduy has evaluated the pharmacokinetic/pharmacodynamics (PK/PD) of PZQ in children. That study, conducted among children ages 3-8, strongly suggests that the current dose of 40 mg/kg is insufficient, with lower cure rates than found at 60 mg/kg.
In endemic settings, PZQ is most often administered as part of school based, or community wide preventive chemotherapy campaigns. Currently, none of the 28 schistosomiasis endemic African nations or The Philippines includes children under the age of four in control programs. The reasons for this are multifactorial and include a) lack of sufficient PK/PD data in this age group, with none in children under three, b) lack of safety data at a dose of 80 mg/kg, c) lack of data addressing the impact of treatment on key growth and nutritional outcomes in this vulnerable age group hampering prioritization of treatment, d) no PK/PD studies conducted in the context of pediatric S. japonicum and e) FDA labeling that does not include young children.
The goals of this proposal are to conduct a randomized, controlled Phase II trial to be conducted in an S. mansoni endemic region of Uganda with N=300 children ages 1-4, that will address many of the current gaps that are hindering treatment of young children. Specifically in SA1 we will 1) assess PK/PD of PZQ dosing among children under the age of 4 at doses of 40 versus 80 mg/kg, 2) expand PD endpoints to include state of the art antigen tests and morbidity outcomes, 3) assess the PK/PD of both PZQ enantiomers, and 4) address the innovative hypothesis that environmental enteropathy (EE) contributes to the significant inter-individual variability observed in PZQ PK/PD. In SA2, we will 1) assess the safety of PZQ administered at 80 mg/kg in two large cohorts of very young children, 2) assess the impact of two different treatment intervals (6 vs 12 months) on nutritional status, growth, and anemia risk, and 3) address innovative hypotheses regarding mechanisms through which schistosomiasis contributes to morbidity in this age group including EE and gut microbial translocation with consequent systemic immune activation.
Over 200 million individuals worldwide are infected with one of three predominant species of schistosomes, with over half of infections occurring in children.1 Recent studies have highlighted the fact that many children experience their first infections before the age of two, with the prevalence of infection among children under four mirroring the prevalence of older children and adults from the same community.2 Importantly, schistosomiasis has been implicated as a cause of linear growth stunting, undernutrition, anemia, and deficits in neurodevelopment among children over the age of four, representing a significant proportion of the global burden of disease due to schistosomiasis.3 Little is known with respect to the impact of schistosomiasis on key morbidities among the highly vulnerable group of children under four.
In the 1980s, Praziquantel (PZQ) was approved for the treatment of schistosomiasis among adults and children ages four and older, and remains FDA approved only for this age group. In 2008, the WHO funded studies to address the safety and parasitologic efficacy of PZQ in the context of S. haematobium and S. mansoni in young children. Based on these and other studies, the WHO in 2011 issued a report recommending that pre-school age children be treated as part of "regular health services."4 This recommendation was based on studies that did not a) evaluate pharmaco-kinetics/dynamics (PK-PD) in this age group, b) evaluate parasitologic efficacy in S. japonicum or c) evaluate the impact of treatment on key schistosomiasis-related morbidities. Since that time, co-PI Bustinduy led the first study of the PK-PD of PZQ at both 40 and 60 mg/kg dosing among children ages 3-8. Results from that study, albeit small, showed that higher doses are likely needed, particularly for younger children. Authors urged further study of higher doses in this age group, the causes of the significant inter-subject variability in PK-PD, better PD indices linking drug exposure to treatment effects, and enantiomer activity across all three species before introduction of monoenantiomeric formulations.5
Thus, significant lacunae remain with respect to treatment of pre-school age children, which contribute to the persistent exclusion of this vulnerable age group from preventive chemotherapy campaigns, with none of the 28 schistosomiasis endemic African nations or The Philippines currently including children under the age of four in control programs.2 In this application, we propose a trial to investigate the off label use of PZQ in children under the age of four. The trial will be conducted at two sites, with high prevalence of intestinal schistosomiasis due to S. mansoni (Uganda) and S. japonicum (The Philippines) employing a two arm single blind, placebo controlled modified cross-over trial design among N=600 children ages 1-4. Children who are infected with schistosomiasis will be randomized at baseline to receive 40 or 80 mg/kg of PZQ. At six months, we will re-randomize half of each baseline group to receive a treatment at the same dose or placebo. This will allow us to evaluate the impact of 6 versus 12 month treatment intervals on key measures of morbidity which, importantly, will inform frequency of treatment needed in this young age group. Successful execution of the following specific aims for this trial will address the significant aforementioned gaps:
SA1 To assess the PK/PD of PZQ administered at different dose regimens. SA1a To measure drug efficacy as per standard parasitological endpoints (Cure Rate and Egg Reduction Rate) at 4 +/- 1 weeks post-PZQ.
SA1b To expand PD endpoints for drug efficacy to include state-of-the art antigen tests to accurately capture residual worm burden (Circulating Cathodic and Anodic Antigens (CCA and CAA)).
SA1c To evaluate the PK/PD of both PZQ enantiomers given the concern that this varies across species and has varied in studies of S. mansoni.
SA1d To assess the role of environmental enteropathy in inter-individual variability in PZQ area under the curve (AUC) demonstrated in this age group.
SA2 To assess the safety and impact of PZQ treatment (dose and interval) on key measures of morbidity 6 and 12 months after initial treatment and mechanisms mediating morbidity.
SA2a To further evaluate the safety of higher PZQ dosing (60 mg/kg), particularly among the unstudied group of very young children ages 1-2.
SA2b To evaluate the impact of different doses (40 vs. 80 mg/kg) and varying dosing intervals (every 6 or 12 months) on iron status, hemoglobin, and age and gender adjusted longitudinal growth and nutritional status as captured by height and weight for age, and weight for height z-scores as determined by WHO Anthro.
SA2c To evaluate the mechanistic role of environmental enteropathy (EE) in the pathogenesis of schistosomiasis related morbidities. We will capture state of the art biomarkers of EE including fecal calprotectin, urine lactulose:mannitol ratio, serum endotoxin, serum endotoxin core antibody, and pro-inflammatory cytokines and employ Path Modeling techniques to identify mechanistic pathways.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Praziquantel 40 mg/kg dose only baseline treatment | Active Comparator | 75 children will receive 40 mg/kg Praziquantel at baseline as single treatment and placebo six months following baseline |
|
| Praziquantel 80 mg/kg dose only baseline treatment | Active Comparator | 75 children will receive 80 mg/kg Praziquantel at baseline as single treatment and placebo six months following baseline |
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| Praziquantel 40 mg/kg dose at baseline and 6 months | Active Comparator | 75 children will receive 40 mg/kg Praziquantel at baseline and again six months later. |
|
| Praziquantel 80 mg/kg dose at baseline and 6 months | Active Comparator | 75 children will receive 80 mg/kg Praziquantel at baseline and again six months later. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Praziquantel | Drug | Praziquantel given as crushed tablets (40 or 80 mg/kg) |
|
| Measure | Description | Time Frame |
|---|---|---|
| Treatment Efficacy | Treatment efficacy as captured by egg reduction rate with the post treatment egg count assessed four weeks after treatment baseline treatment only. This is the calculated as 1 - (Post-treatment mean egg count / pre-treatment mean egg count) x 100% | Four weeks after baseline treatment |
| Treatment Efficacy - Cure Rate | Efficacy of treatment as captured by cure rate 4 weeks after treatment at baseline. Cure rate is the percent of participants in a group who have no infection (zero eggs per gram of stool) four weeks after treatment at baseline | Four weeks after baseline treatment |
| Measure | Description | Time Frame |
|---|---|---|
| Hemoglobin | Assess impact of varying doses and frequency of dosing on hemoglobin measured 12 months after baseline treatment | 12 months following treatment at enrollment/baseline |
| Age and Gender Adjusted Linear Growth |
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Inclusion Criteria:
Exclusion Criteria:
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| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Medical Research Council | Entebbe | 3FC6+Q3C, | Uganda | |||
| London School of Tropical Hygiene and Medicine |
| PubMed Identifier | Type | Citation | Retractions |
|---|---|---|---|
| 34488846 | Background | Webb EL, Edielu A, Wu HW, Kabatereine NB, Tukahebwa EM, Mubangizi A, Adriko M, Elliott AM, Hope WW, Mawa PA, Friedman JF, Bustinduy AL. The praziquantel in preschoolers (PIP) trial: study protocol for a phase II PK/PD-driven randomised controlled trial of praziquantel in children under 4 years of age. Trials. 2021 Sep 6;22(1):601. doi: 10.1186/s13063-021-05558-1. | |
| 40412398 | Result | Bustinduy AL, Edielu A, Ayebazibwe GK, Nakyesige R, Anguajibi V, Mpooya S, Nassuna J, Adriko M, Elliott A, van Dam G, Corstjens P, Pach S, Wu H, Colt S, Mawa PA, Muheki E, Kabatereine NB, Webb EL, Friedman JF. Safety and efficacy of praziquantel 40 mg/kg versus 80 mg/kg in preschool-aged children with intestinal schistosomiasis in Uganda: a 2 x 2 factorial, double-blind, placebo-controlled, phase 2 randomised trial. Lancet Glob Health. 2025 Jun;13(6):e1091-e1100. doi: 10.1016/S2214-109X(25)00095-6. |
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Data from the trial will be made available to interested investigators following IRB approval to provide these de-identified data. Specifically, after research data set has been cleaned, finalized, and all identifiers removed, the PIs will provide timely release and sharing of the final research data for use by other researchers. In addition, this study will generate samples collected young children. Upon discussion with the Principal Investigators and based on availability of samples, residual stored samples may be shared following IRB approval to provide these de-identified samples to interested researchers.
Within one year of trial completion and up to five years after.
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| ID | Title | Description |
|---|---|---|
| FG000 | Praziquantel 40 mg/kg Dose Only Baseline Treatment | 75 children will receive 40 mg/kg Praziquantel at baseline as single treatment and placebo six months following baseline Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| FG001 | Praziquantel 80 mg/kg Dose Only Baseline Treatment | 75 children will receive 80 mg/kg Praziquantel at baseline as single treatment and placebo six months following baseline Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| FG002 | Praziquantel 40 mg/kg Dose at Baseline and 6 Months | 75 children will receive 40 mg/kg Praziquantel at baseline and again six months later. Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| FG003 | Praziquantel 80 mg/kg Dose at Baseline and 6 Months | 75 children will receive 80 mg/kg Praziquantel at baseline and again six months later. Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| Title | Milestones | Reasons Not Completed | ||||||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Overall Study |
|
all children enrolled were infected with S. Mansoni as determined by Kato Katz and then randomly allocated to four treatment arms.
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| ID | Title | Description |
|---|---|---|
| BG000 | Praziquantel 40 mg/kg Dose Only Baseline Treatment | 75 children will receive 40 mg/kg Praziquantel at baseline as single treatment and placebo six months following baseline Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| BG001 | Praziquantel 80 mg/kg Dose Only Baseline Treatment |
| Units | Counts |
|---|---|
| Participants |
|
| Title | Description | Population Description | Parameter Type | Dispersion Type | Unit of Measure | Calculate Percentage | Denominator Units Selected | Denominators | Classes |
|---|---|---|---|---|---|---|---|---|---|
| Age, Categorical | 12 - 47 months |
| Type | Title | Description | Population Description | Reporting Status | Anticipated Posting Date | Parameter Type | Dispersion Type | Unit of Measure | Calculate Percentage | Time Frame | Units Analyzed | Denominator Units Selected | Arm/Group Information | Denominators | Classes | Analyses | ||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Primary | Treatment Efficacy | Treatment efficacy as captured by egg reduction rate with the post treatment egg count assessed four weeks after treatment baseline treatment only. This is the calculated as 1 - (Post-treatment mean egg count / pre-treatment mean egg count) x 100% | Egg reduction rate at 4 weeks post baseline treatment among subjects who submitted both pre and post treatment stools for assessment | Posted | Geometric Mean | 95% Confidence Interval | percentage change | Four weeks after baseline treatment |
|
For one year during the 12 months following the first treatment at Baseline
Adverse events and serious adverse events were actively ascertained for 18 hours after dosing of the study agent at baseline.
Serious adverse events were ascertained by report of family members following the dosing follow up window for up to one year (study participation time)
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| ID | Title | Description | Deaths (Affected) | Deaths (At Risk) | Serious Events (Affected) | Serious Events (At Risk) | Other Events (Affected) | Other Events (At Risk) |
|---|---|---|---|---|---|---|---|---|
| EG000 | Praziquantel 40 mg/kg Dose Only Baseline Treatment | 75 children will receive 40 mg/kg Praziquantel at baseline as single treatment and placebo six months following baseline Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| Term | Organ System | Source Vocabulary | Assessment Type | Notes | Statistical Information |
|---|---|---|---|---|---|
| malaria | Blood and lymphatic system disorders | MedDRA (10.0) | Systematic Assessment | admitted for two days to hospital for severe malaria |
| Term | Organ System | Source Vocabulary | Assessment Type | Notes | Statistical Information |
|---|---|---|---|---|---|
| liver function tests | Hepatobiliary disorders | MedDRA (10.0) | Systematic Assessment | Elevated liver function tests (AST or ALT or Bilirubin) 12 hours after baseline dosing |
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| Title | Organization | Phone | Extension | |
|---|---|---|---|---|
| Dr. Jennifer Friedman | Center for International Health Research at Brown Health | 401 444 7990 | Jennifer_Friedman@Brown.edu |
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| Type | Includes Protocol | Includes SAP | Includes ICF | Document Label | Document Date | Document Uploaded Date | Document File Name |
|---|---|---|---|---|---|---|---|
| Prot_SAP | Yes | Yes | No | Study Protocol and Statistical Analysis Plan | Mar 3, 2022 | Jul 22, 2025 | Prot_SAP_000.pdf |
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| ID | Term |
|---|---|
| D012552 | Schistosomiasis |
| D012555 | Schistosomiasis mansoni |
| D012554 | Schistosomiasis japonica |
| ID | Term |
|---|---|
| D014201 | Trematode Infections |
| D006373 | Helminthiasis |
| D010272 | Parasitic Diseases |
| D007239 | Infections |
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| ID | Term |
|---|---|
| D011223 | Praziquantel |
| ID | Term |
|---|---|
| D007546 | Isoquinolines |
| D006574 | Heterocyclic Compounds, 2-Ring |
| D000072471 | Heterocyclic Compounds, Fused-Ring |
| D006571 | Heterocyclic Compounds |
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| Medical Research Council |
| OTHER_GOV |
| Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD) | NIH |
Children ages 12-48 months who are infected with S. japonicum (Philippines) or S. mansoni (Uganda) will be randomized to receive either 40 or 60 mg/kg of praziquantel at baseline. Six months later, half of each group will receive second treatment at same dose or placebo.
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Tablets will be crushed and given with orange juice
Assess impact of varying doses and frequency of dosing on linear growth as captured by Z-score. A Z-score is the standard deviation from age (months) and sex mean from the World Health Organization's (WHO) Multicentre Growth Reference Study which derived the WHO "Anthro" reference. That reference assessed approximately 8500 children from widely different ethnic backgrounds and cultural settings (Brazil, Ghana, India, Norway, Oman and the USA) and provides a single international standard that represents the best description of physiological growth for all children from birth to five years of age and to establish the breastfed infant as the normative model for growth and development.
For Z-scores presented, 0 represents the population mean for the healthy Anthro reference curve and positive values are taller children while negative are shorter. A Z score of -2.0 or below defines "stunting" or children -2 standard deviations below this healthy reference population.
| 12 months following treatment at enrollment/baseline |
| Age and Gender Adjusted Nutritional Status | Assess impact of varying doses and frequency of dosing on nutritional as captured by weight for height Z-score. A Z-score is the standard deviation from age (months) and sex mean from the World Health Organization's (WHO) Multicentre Growth Reference Study which derived the WHO "Anthro" reference. That reference assessed approximately 8500 children from widely different ethnic backgrounds and cultural settings (Brazil, Ghana, India, Norway, Oman and the USA) and provides a single international standard that represents the best description of physiological growth for all children from birth to five years of age and to establish the breastfed infant as the normative model for growth and development. For Z-scores presented, 0 represents the population mean for the healthy Anthro reference curve and positive values are better nourished children. A Z score of -2.0 or below defines "wasting" or children -2 standard deviations below mean of health reference | 12 months following treatment at enrollment/baseline |
| Fecal Calprotectin | A measure of gut inflammation that is measured on stool samples and captures intestinal inflammation largely caused by neutrophils that migrate to the gut | 12 months following treatment at enrollment/baseline |
| London |
| United Kingdom |
75 children will receive 80 mg/kg Praziquantel at baseline as single treatment and placebo six months following baseline Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| BG002 | Praziquantel 40 mg/kg Dose at Baseline and 6 Months | 75 children will receive 40 mg/kg Praziquantel at baseline and again six months later. Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| BG003 | Praziquantel 80 mg/kg Dose at Baseline and 6 Months | 75 children will receive 80 mg/kg Praziquantel at baseline and again six months later. Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| BG004 | Total | Total of all reporting groups |
| Participants |
| No |
|
| Sex: Female, Male | Count of Participants | Participants |
|
| Race (NIH/OMB) | Count of Participants | Participants |
|
| Region of Enrollment | Number | participants |
|
| Praziquantel 80 mg/kg Dose Only Baseline Treatment |
75 children will receive 80 mg/kg Praziquantel at baseline as single treatment and placebo six months following baseline Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| OG002 | Praziquantel 40 mg/kg Dose at Baseline and 6 Months | 75 children will receive 40 mg/kg Praziquantel at baseline and again six months later. Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
| OG003 | Praziquantel 80 mg/kg Dose at Baseline and 6 Months | 75 children will receive 80 mg/kg Praziquantel at baseline and again six months later. Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) |
|
|
| Primary | Treatment Efficacy - Cure Rate | Efficacy of treatment as captured by cure rate 4 weeks after treatment at baseline. Cure rate is the percent of participants in a group who have no infection (zero eggs per gram of stool) four weeks after treatment at baseline | Subjects who submitted stool for assessment 4 weeks after baseline treatment | Posted | Number | Percent of participants | Four weeks after baseline treatment |
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|
|
| Secondary | Hemoglobin | Assess impact of varying doses and frequency of dosing on hemoglobin measured 12 months after baseline treatment | subjects present for close out at 12 months | Posted | Mean | Standard Deviation | grams/decilter | 12 months following treatment at enrollment/baseline |
|
|
|
| Secondary | Age and Gender Adjusted Linear Growth | Assess impact of varying doses and frequency of dosing on linear growth as captured by Z-score. A Z-score is the standard deviation from age (months) and sex mean from the World Health Organization's (WHO) Multicentre Growth Reference Study which derived the WHO "Anthro" reference. That reference assessed approximately 8500 children from widely different ethnic backgrounds and cultural settings (Brazil, Ghana, India, Norway, Oman and the USA) and provides a single international standard that represents the best description of physiological growth for all children from birth to five years of age and to establish the breastfed infant as the normative model for growth and development. For Z-scores presented, 0 represents the population mean for the healthy Anthro reference curve and positive values are taller children while negative are shorter. A Z score of -2.0 or below defines "stunting" or children -2 standard deviations below this healthy reference population. | Subjects present at study close out at 12 months | Posted | Mean | Standard Deviation | Z score | 12 months following treatment at enrollment/baseline |
|
|
|
| Secondary | Age and Gender Adjusted Nutritional Status | Assess impact of varying doses and frequency of dosing on nutritional as captured by weight for height Z-score. A Z-score is the standard deviation from age (months) and sex mean from the World Health Organization's (WHO) Multicentre Growth Reference Study which derived the WHO "Anthro" reference. That reference assessed approximately 8500 children from widely different ethnic backgrounds and cultural settings (Brazil, Ghana, India, Norway, Oman and the USA) and provides a single international standard that represents the best description of physiological growth for all children from birth to five years of age and to establish the breastfed infant as the normative model for growth and development. For Z-scores presented, 0 represents the population mean for the healthy Anthro reference curve and positive values are better nourished children. A Z score of -2.0 or below defines "wasting" or children -2 standard deviations below mean of health reference | Weight for height z score (WHZ) at 12 months | Posted | Mean | Standard Deviation | Z score | 12 months following treatment at enrollment/baseline |
|
|
|
| Secondary | Fecal Calprotectin | A measure of gut inflammation that is measured on stool samples and captures intestinal inflammation largely caused by neutrophils that migrate to the gut | Calprotectin about 50 ug/g 12 months post baseline | Posted | Number | percentage with calprotectin >50 ug/g | 12 months following treatment at enrollment/baseline |
|
|
|
| 0 |
| 88 |
| 0 |
| 88 |
| 9 |
| 88 |
| EG001 | Praziquantel 80 mg/kg Dose Only Baseline Treatment | 75 children will receive 80 mg/kg Praziquantel at baseline as single treatment and placebo six months following baseline Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) | 1 | 86 | 1 | 86 | 8 | 86 |
| EG002 | Praziquantel 40 mg/kg Dose at Baseline and 6 Months | 75 children will receive 40 mg/kg Praziquantel at baseline and again six months later. Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) | 0 | 89 | 0 | 89 | 10 | 89 |
| EG003 | Praziquantel 80 mg/kg Dose at Baseline and 6 Months | 75 children will receive 80 mg/kg Praziquantel at baseline and again six months later. Praziquantel: Praziquantel given as crushed tablets (40 or 80 mg/kg) | 0 | 91 | 0 | 91 | 8 | 91 |
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| D000079426 |
| Vector Borne Diseases |