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SCOPE: Short Course Primaquine for the Radical Cure of P. Vivax - Papua New Guinea

Sponsor
Macfarlane Burnet Institute for Medical Research and Public Health Ltd (Other)
Overall Status
Not yet recruiting
CT.gov ID
NCT05874271
Collaborator
Papua New Guinea Institute of Medical Research (Other), Papua New Guinea National Department of Health (Other), Menzies School of Health Research (Other), University of Melbourne (Other), Medicines for Malaria Venture (Other), PATH (Other), UNITAID (Other)
5,850
Enrollment
4
Locations
1
Arm
25
Anticipated Duration (Months)
1462.5
Patients Per Site
58.5
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

Significant gains have been made in reducing the overall burden of malaria worldwide, however these have been far greater for Plasmodium falciparum than P. vivax.

  1. vivax remains a major obstacle to malaria control and elimination efforts, largely due to its ability to form dormant liver stages (hypnozoites) that allows it to escape detection and treatment. Importantly, they are susceptible only to 8 aminoquinolines such as primaquine. However, primaquine is associated with risk of haemolysis in individuals with a genetic condition, called glucose-6-phosphate dehydrogenase (G6PD) deficiency. Additionally, the recommended 14-day prolonged treatment regimen is associated with poor treatment adherence, hence ineffective primaquine treatment. Innovative solutions to the radical cure of both the blood and liver stages of P. vivax are urgently required.

The PNG National Department of Health has requested a pragmatic study of the feasibility and cost-effectiveness of implementing point-of-care G6PD testing followed by high-dose, short-course primaquine treatment regimens for patients with P. vivax malaria. This revised case management is to be combined with practicable enhancements to patient education, supervision, malariometric surveillance and pharmacovigilance.

This will be a before-after longitudinal health facility-based study implemented at Napapar and Mugil health centres and Baro and Wirui clinics. A staged approach for the implementation of the revised case management strategy will be used, including patient education and counselling, community-based clinical review, with mixed methods evaluation.

Condition or Disease Intervention/Treatment Phase
  • Combination Product: Revised case management package
 N/A

Study Design

Study Type:
Interventional
Anticipated Enrollment :
5850 participants
Allocation:
N/A
Intervention Model:
Single Group Assignment
Masking:
None (Open Label)
Primary Purpose:
Other
Official Title:
Feasibility of High Daily Dose Short Course Primaquine After G6PD Testing for the Radical Cure of Plasmodium Vivax Malaria
Anticipated Study Start Date :
Jul 1, 2023
Anticipated Primary Completion Date :
May 31, 2025
Anticipated Study Completion Date :
Jul 31, 2025

Arms and Interventions

Arm Intervention/Treatment
Experimental: Revised case management package

Combination Product: Revised case management package
Point-of-care quantitative G6PD testing using G6PD STANDARD (SD Biosensor) prior to use of primaquine (Day 0) Prescription of short course primaquine (7 mg/kg total) (Day 0): PQ7 (1 mg/kg/day for 7 days) if G6PD activity greater than 70 percent PQ14 (0.5 mg/kg/day for 14 days) if G6PD activity is 30-70 percent PQ8w (0.75 mg/kg/week for 8 weeks) if G6DP activity less than 30 percent Participant counselling at the health facility (Day 0): Supervision of first dose of primaquine Education regarding importance and risks of primaquine therapy and necessity to take primaquine with food Community based clinical review on Day 3 (and Day 7 for the first 300 participants) to detect and manage gastrointestinal or haemolytic adverse effects of treatment and encourage adherence to full treatment regime Improved malariometric surveillance and pharmacovigilance to support wider scale use of the revised case management

Outcome Measures

Primary Outcome Measures

  1. Proportion of patients experiencing at least one Serious Adverse Event (SAE) during treatment. [During treatment (up to 8 weeks)]

    SAEs are collected during clinical review using a study-specific questionnaire

  2. Proportion of patients experiencing at least one Adverse Event of Special Interest (AESI) during treatment. [During treatment (up to 8 weeks)]

    AESIs (haemolysis, methaemoglobinaemia and gastrointestinal discomfort) are collected during clinical review using a study-specific questionnaire

  3. Proportion of patients with P. vivax malaria who correctly receive all components of the revised case management package [3 days]

    Measured by completion of G6PD testing and the correct prescription of primaquine based on G6PD activity, completion of patients counselling and community based follow up on Day 3

Secondary Outcome Measures

  1. The proportion of patients with any AESI during treatment [During treatment (up to 8 weeks)]

    AESIs are collected during clinical review using a study-specific questionnaire

  2. The proportion of patients with a gastrointestinal (GI) AESI during treatment [During treatment (up to 8 weeks)]

    AESIs are collected during clinical review using a study-specific questionnaire

  3. The proportion of patients with an AESI related to haemolysis during treatment [During treatment (up to 8 weeks)]

    AESIs are collected during clinical review using a study-specific questionnaire

  4. The proportion of patients an AESI related to methaemoglobinaemia [During treatment (up to 8 weeks)]

    AESIs are collected during clinical review using a study-specific questionnaire

  5. Proportion of patients permanently stopping PQ before end of treatment [During treatment (up to 8 weeks)]

    Discontinuation of PQ will be assessed using a study-specific questionnaire

  6. The proportion of patients receiving correct treatment based on G6PD activity [1 day]

    This will be assessed by linking patients G6PD activity results measured during study enrolment with primaquine dose prescribed on the same day

  7. Proportion of patients who were reviewed on Day 3 and Day 7 [1 week]

    This will be assessed by linking patients enrolment data with Day 3 and Day 7 clinical review data

  8. Perception of and experience with new radical cure tools among health care providers and community members [6 months]

    This will be assessed using stakeholder interviews

  9. Proportion of health care practitioners who comply with the revised radical cure treatment algorithm [1 day]

    The outcome will be assessed from patients' enrolment data

  10. Proportion of patients receiving a SD Biosensor G6PD test [1 day]

    The outcome will be assessed from patients' enrolment data

  11. Proportion of eligible P. vivax malaria patients receiving the correct dose of primaquine based on the result of the G6PD test [1 day]

    The outcome will be assessed from patients' enrolment data

  12. Proportion of P. vivax malaria patients who are ineligible for daily primaquine and are incorrectly given primaquine (including infants, pregnant females and G6PD deficient patients) [1 day]

    The outcome will be assessed from patients' enrolment data

  13. Proportion of P. vivax malaria patients that are reviewed on Day 3 [3 days]

    This will be assessed by linking patients' enrolment data with clinical review data

  14. Proportion of P. vivax malaria patients that adhere to their prescribed primaquine regimen [3 days]

    This will be assessed by linking patients' enrolment data with clinical review data

  15. Factors influencing acceptability and feasibility of the new radical cure tools among health care providers are identified [3 days]

    This will be assessed using stakeholder interviews, observations and focus groups

  16. Barriers and enablers of uptake and implementation at the sub-national levels are identified [18 months]

    This will be assessed using stakeholder interviews and focus groups

  17. Factors influencing compliance with G6PD testing and perceptions of new drug regimens and serious adverse events among health care providers are identified [18 months]

    This will be assessed using stakeholder interviews and focus groups

  18. Required knowledge, skills, and training to administer the revised case management and patient-counselling identified [18 months]

    This will be assessed using stakeholder interviews and focus groups

  19. Factors influencing the barriers and facilitators to patient adherence to primaquine after the rollout of the revised case management identified [18 months]

    This will be assessed using stakeholder interviews and focus groups

  20. Factors influencing the acceptability and feasibility of community-based clinical review at Day 3 of primaquine treatment identified. [18 months]

    This will be assessed using stakeholder interviews and focus groups

  21. Perceptions of the new radical cure tools and serious adverse events at the community level identified [18 months]

    This will be assessed using stakeholder interviews and focus groups

  22. Local acceptability of the revised case management algorithms among patients, their families, and healthcare workers established [18 months]

    This will be assessed using stakeholder interviews and focus groups

  23. The monthly incidence of confirmed symptomatic P. vivax malaria episodes (mono-infection or mixed) before implementation versus after implementation [18 months]

    This will be assessed by comparing facility surveillance data before implementation with facility surveillance data after implementation

  24. The prevalence of P. vivax parasitaemia in patients presenting with fever before implementation versus after implementation [18 months]

    This will be assessed by comparing cross-sectional data on n=200 patients (per facility) collected before implementation to the prevalence collected in n=200 patients (per facility) after implementation

  25. Cumulative risk of representation to the same clinic with symptomatic P. vivax malaria within 6 months [18 months]

    This will be assessed by linking patients' enrolment data

  26. Costs of implementing policy from a healthcare provider perspective, including health systems strengthening processes [18 months]

    This will be assessed from health system data collected throughout the study

  27. Household costs per P. vivax episode [3 days]

    This will be assessed from a household cost survey on a subset of patients

  28. Overall cost-effectiveness of changing policy if revised case management is effective [18 months]

    This will be assessed from health system data collected throughout the study

  29. Cost per episode of P. vivax malaria from the healthcare provider and societal perspectives [18 months]

    This will be assessed from health system data collected throughout the study

  30. Cost per component of the revised case management package [18 months]

    This will be assessed from health system data collected throughout the study

  31. If revised case management package is effective (significantly reduces the incidence of malaria), then the cost-effectiveness of implementing the revised case management as compared with usual care [18 months]

    This will be assessed from health system data collected throughout the study

  32. Proportion of CHWs who correctly act on early signs of haemolytic anaemia and GI events (i.e. refer patients for further medical review, instruct patient to discontinue treatment) [3 days]

    This will be assessed from clinical review data and study-specific questionnaire

  33. Number of patients with an SAE who are identified by community or clinic staff follow-up and referred to hospital for further management [During treatment (up to 8 weeks)]

    This will be assessed by linking clinical review data, study specific questionnaire and SAE form

  34. The proportion of patients eligible to receive PQ who had a SAE during treatment [During treatment (up to 8 weeks)]

    This will be assessed by linking enrolment data, clinical review, study specific questionnaire and SAE form

  35. Prevalence of severe anaemia in patients presenting with fever before and after implementation [18 months]

    This will be assessed by comparing the facility surveillance data before implementation with facility surveillance data after implementation

Eligibility Criteria

Criteria

Ages Eligible for Study:
12 Months and Older
Sexes Eligible for Study:
All
Accepts Healthy Volunteers:
No
Inclusion Criteria:
  • Patients with vivax malaria
Exclusion Criteria:

  • Patients who are pregnant

  • Patients who are breastfeeding

  • Patients with a Hb <8g/dL

  • Patients with a previous adverse reaction to primaquine

  • Patient with severe malaria

Contacts and Locations

Locations

Site City State Country Postal Code
1 Napapar Health Centre Kokopo East New Britain Papua New Guinea
2 Wirui Clinic Wewak East Sepik Papua New Guinea
3 Baro Clinic Vanimo West Sepik Papua New Guinea
4 Mugil Health Centre Madang Papua New Guinea

Sponsors and Collaborators

  • Macfarlane Burnet Institute for Medical Research and Public Health Ltd
  • Papua New Guinea Institute of Medical Research
  • Papua New Guinea National Department of Health
  • Menzies School of Health Research
  • University of Melbourne
  • Medicines for Malaria Venture
  • PATH
  • UNITAID

Investigators

  • Principal Investigator: Moses Laman, Dr, Papua New Guinea Institute of Medical Research
  • Principal Investigator: Leanne Robinson, Prof, Macfarlane Burnet Institute for Medical Research and Public Health
  • Principal Investigator: Leo Makita, Papua New Guinea National Department of Health
  • Principal Investigator: William Pomat, Prof, Papua New Guinea Institute of Medical Research

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.
Responsible Party:
Macfarlane Burnet Institute for Medical Research and Public Health Ltd
ClinicalTrials.gov Identifier:
NCT05874271
Other Study ID Numbers:
  • MMV_PQ_21_02
  • U1111-1285-4864
First Posted:
May 24, 2023
Last Update Posted:
May 24, 2023
Last Verified:
May 1, 2023
Individual Participant Data (IPD) Sharing Statement:
Yes
Plan to Share IPD:
Yes
Studies a U.S. FDA-regulated Drug Product:
No
Studies a U.S. FDA-regulated Device Product:
No
Keywords provided by Macfarlane Burnet Institute for Medical Research and Public Health Ltd
primaquine
Additional relevant MeSH terms:
Malaria
Malaria, Vivax
Glucosephosphate Dehydrogenase Deficiency

Study Results

No Results Posted as of May 24, 2023