The goal of this observational study is to learn about how long-acting injectable antipsychotic (LAIA) medications are affected by the changes that take place in the body during pregnancy, and how much an unborn baby is exposed to. The investigators are also interested in the amount of these drugs that enters into breastmilk and taken by babies during breastfeeding. In addition to their regular clinic visits to receive long-acting mental health medicine injection, participants will be invited for up to four study visits between day 2 and 14 after the injection. This will happen only once during pregnancy, and once during the breastfeeding period to collect a few drops of blood on special filter paper card from the finger using safety lancet. A few drops of breastmilk will also be collected. Immediately after delivery, a few drops of blood will be collected from the mother, umbilical cord and the baby heel. The investigators will use these samples to determine the amount of the drug in the body during pregnancy and compare this to the amount during the breastfeeding period. Additionally, every month during the third trimester, and during the first 3 months postpartum, participants will complete a questionnaire (using the Liverpool University Neuroleptic Side Effect Scale) to document how they are feeling. Clinical improvement will be documented by the primary care provider using the Clinical Global Impressions Scale. Findings from this study are expected to help healthcare providers to understand these drugs better so that they can make informed decisions about if and how to use these drugs in women who become pregnant or are breastfeeding.
Primary Objectives 1. To determine the magnitude of changes (if any) in the pharmacokinetics of selected LAIAs during pregnancy and assess the extent of fetal exposure at delivery. 2. To describe breastmilk pharmacokinetics of selected LAIAs and the extent of breastfed infant exposure. Secondary Objectives 1. To assess safety and clinical outcomes following LAIA use during pregnancy and postpartum. 2. To explore sources of variability in maternal and fetal/breastfed infant LAIA exposure.
Study Type
OBSERVATIONAL
Enrollment
125
Federal Medical Centre
Makurdi, Benue State, Nigeria
RECRUITINGFederal Neuropsychiatric Hospital
Kaduna, Kaduna State, Nigeria
RECRUITINGFederal Neuropsychiatric Hospital
Yaba, Lagos, Nigeria
RECRUITINGNeuropsychiatric Hospital
Abeokuta, Ogun State, Nigeria
RECRUITINGNeuropsychiatric Specialist Hospital
Akure, Ondo State, Nigeria
RECRUITINGObafemi Awolowo University Teaching Hospital
Ile-Ife, Osun State, Nigeria
NOT_YET_RECRUITINGMinimum plasma drug concentration (Cmin) during pregnancy and postpartum
Determined from sampling at the end of a dosing interval during pregnancy, and postpartum
Time frame: During gestation weeks 33-36 and weeks 9-12 weeks postpartum
Minimum breastmilk drug concentration (Cmin)
Determined from sampling at the end of a postpartum dosing interval
Time frame: During weeks 9-12 weeks postpartum
Maximum plasma drug concentration (Cmin) during pregnancy and postpartum
Highest concentration during a dosing interval during pregnancy, and postpartum
Time frame: During gestation weeks 33-36 and weeks 9-12 weeks postpartum
Maximum breastmilk drug concentration (Cmin)
Highest concentration during a postpartum dosing interval
Time frame: During weeks 9-12 weeks postpartum
Area under the plasma concentration-time curve (AUC)
For assessment of overall drug exposure in plasma
Time frame: During gestation weeks 33-36 and weeks 9-12 weeks postpartum
Area under the breastmilk concentration-time curve (AUC)
For assessment of overall drug exposure in breastmilk
Time frame: During weeks 9-12 weeks postpartum
Breastfed infant to maternal plasma LAIA concentration ratio
To determine the level of breastfed infant LAIA exposure and elimination
Time frame: During weeks 9-12 weeks postpartum
Newborn to maternal plasma LAIA concentration ratio
To determine the extent of in utero fetal drug exposure and elimination
Time frame: As soon as possible after delivery
LAIA associated symptoms
To monitor LAIA side effects during and postpartum using the Liverpool University Neuroleptic Side Effect Rating Scale (LUNSERS)
Time frame: From gestation week 28 to postpartum week 12
Clinical improvement
To monitor illness severity, improvement and LAIA efficacy during pregnancy and postpartum using the Clinical Global Impressions Scale.
Time frame: From gestation week 28 to postpartum week 12
Single nucleotide polymorphisms in drug disposition genes
To explore genetic sources of interindividual variability in maternal and fetal/breastfed infant drug exposure
Time frame: From gestation week 28 to postpartum week 12
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