Clinical Trial Details
— Status: Withdrawn
Administrative data
| NCT number |
NCT04984759 |
| Other study ID # |
MAL21004 |
| Secondary ID |
|
| Status |
Withdrawn |
| Phase |
Phase 4
|
| First received |
|
| Last updated |
|
| Start date |
July 1, 2023 |
| Est. completion date |
June 30, 2025 |
Study information
| Verified date |
March 2024 |
| Source |
University of Oxford |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Each year almost a million infants are born small for gestational age due to malaria
infection in pregnancy. These infants are at risk for stillbirth or neonatal death, and being
born too small predisposes the survivors to increased metabolic diseases later in life.
Plasmodium vivax (PV) is the second most common malaria species globally. Its relapsing
nature results in multiple episodes of PV in a single pregnancy, compounding growth
restriction and stillbirth risk. Women with PV in one pregnancy may harbor dormant parasites
(hypnozoites) in their liver the cause illness and poor fetal growth in a subsequent
pregnancy.
Only radical cure with 8-aminoquinolines (8AQ)- primaquine (PMQ) or tafenoquine (TQ) - can
eliminate hypnozoites, but these drugs are contraindicated in pregnancy. The postpartum
period presents a key window of opportunity for giving radical cure to women of childbearing
age with PV. Pharmacokinetic data is needed to support safe use of these drugs postpartum and
World Health Organization has identified pharmacokinetic studies of 8AQ in lactation as a
research priority.
Primaquine is excreted minimally in mature breast milk, at <1% of the weight-adjusted
relative infant dose (RID). As the main adverse event associated with both 8AQ - hemolysis
glucose-6-phosphate dehydrogenase (G6PD) deficient individuals - is dose-dependent and
negligible at low doses, this finding strongly supports its safe use in later lactation. This
study is needed to determine if primaquine can also be given safely in the early postpartum
period. There is no published data on tafenoquine excretion in breastmilk, and this study
would quantify safety throughout early and late lactation.
Drug safety studies in lactation are essential to ensure medications are not denied and
unnecessary interruption of breastfeeding is avoided. Demonstration of safety of radical cure
for breastfeeding women in the postpartum period would allow women with PV in pregnancy and
lactation to receive 8AQ after delivery, preventing illnesses in the postpartum period and
subsequent pregnancies. Improved uptake of radical cure through elimination of unnecessary
contraindications supports malaria elimination and community health.
The main purpose of this study is to characterize the transfer of tafenoquine and primaquine
in breast milk of mothers receiving radical cure doses of 8AQ throughout the different phases
of lactation - colostrum, transitional milk, and mature milk - in order to determine the
degree of infant exposure.
Description:
The study will take place at clinics of the Shoklo Malaria Research Unit (SMRU),
Mahidol-Oxford Tropical Medicine Research Unit in Tak Province, Thailand. The clinics serve a
population of migrant workers resident along the Thailand-Myanmar border. Non-pregnant
breastfeeding women that access care at SMRU (postnatal care, outpatient, vaccine and routine
baby care departments) will be invited to participate with their breastfed children.
All lactating women and their children will be G6PD phenotypically normal. Participants will
be enrolled as follows; Arm 1: Primaquine mother-neonate pairs Arm 2: Tafenoquine
mother-child pairs Arm 3: Tafenoquine mother-neonate pairs
Pharmacokinetic sampling plan:
- PMQ pharmacokinetic sampling (Mother/Neonate pairs - Arm 1):
- Mothers: Dense pharmacokinetic venous blood and breast milk sampling will be
performed during day 1 and 14; one sample of blood and breast milk will collected
at a single timepoint on days 3, 5 and 8.
- Neonate: One capillary blood sample will be collected on the same days as maternal
sampling.
- TQ pharmacokinetic sampling (Mother/child pairs - Arms 2, and 3):
- Mothers: Dense pharmacokinetic venous blood and breast milk sampling will be
performed during the first day after dosing, followed by one sample of blood and
breast milk at a single time point on days 2, 3, 8, 15, 29, 43 and 75 (allowing a
description of approximately 95% of the total drug exposure).
- Child: One capillary blood sample will be collected on the same days as maternal
sampling.
Mothers and children will be closely monitored for safety throughout the 75 day follow up
period including regular assessments of adverse events, Hb, Hct and MetHb levels.
Pharmacokinetic drug measurements of primaquine, carboxyprimaquine and tafenoquine will be
performed at the Department of Clinical Pharmacology, Mahidol-Oxford Tropical Medicine
Research Unit (MORU), Bangkok, Thailand. Drug concentrations will be quantified by liquid
chromatography coupled with tandem mass spectrometry (LC-MS/MS). Interim data review will be
done by an external drug safety monitoring board (DSMB) before recruitment of Arm 3. The
board will review safety data and any available PK data. If PK data is not yet available and
there are safety concerns, recruitment in Arm 3 may be suspended until PK data from Arms 1
and 2 are available.
Study participants with any adverse events will be followed until the event has stabilized or
resolved (unless the participant refuses such follow up care). Free care will be offered
through SMRU clinics. For severe harm caused by study procedures following this protocol,
Oxford University insurance will support additional health care beyond SMRU's capacity.
This study is funded by Thrasher Research Fund.
