Pharmacologically-based Strategies for Opioid Substitution Therapy During Pregnancy

Steve N. Caritis, MD

Status and phase

Terminated

Phase 2

Conditions

Opiate Addiction

Pregnancy

Treatments

Drug: Frequency Group

Drug: Magnitude Group

Study type

Interventional

Funder types

Other

NIH

Identifiers

NCT03831113

R01HD096796 (U.S. NIH Grant/Contract)

STUDY19100128

Details and patient eligibility

About

This study is a pharmacodynamic study in pregnant women evaluating the relationship between buprenorphine concentration and outcome such as opioid withdrawal symptoms , NAS scores, neurodevelopmental and neuroanatomic outcomes. Strategies to reduce opioid exposure will be explored. There are 4 specific aims but only specific aim 4 is a clinical trial and reported here. In specific aim 4, eligible consenting women on buprenorphine in an MAT clinic will be assigned to 2 dose reduction regimens and their response to dose reduction will be measured using a visual analog scale.

Full description

Opioid use has reached a staggering level and the associated deaths, neonatal consequences and economic impact are devastating. Buprenorphine and methadone are the two most commonly used medications for pregnant women in a Medication Assisted Treatment (MAT) program. Yet, the target concentration of these agents is not clearly identified. Furthermore, the relationship between drug exposure and adverse effects such as Neonatal Abstinence Syndrome and neurodevelopmental outcomes is unclear but contemporary thinking is that exposure (defined by maternal dose) is unrelated to adverse outcomes. The benefit of an MAT strategy is based on strong clinical data that demonstrates an improvement in perinatal outcomes in women participating in an MAT program. However, some women prefer to stop opioid medications entirely , but are not afforded this option in many MAT programs. The possibility that MAT is associated with some harms has received little attention but there are data that suggest that opioids adversely affect the fetal brain. If MAT is indeed associated with potential harms, then the option of Medically Supervised Withdrawal could be considered.

This study will assess two dose reduction strategies in a cohort of women who desire a reduction or elimination of their opioid exposure. The magnitude group will reduce the dose by either 1 or 2 mg weekly. The frequency group will reduce their dose by 2 mg alternately in one or 2 weeks

Enrollment

13 patients

Sex

Female

Ages

18 to 45 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

On a stable dosing regimen of BUP for at least 2 weeks as part of an established medication- assisted treatment (MAT) program.
Willingness to undergo supervised dose reduction
Subject willingness to be assigned to either the Magnitude, or Frequency group.
Single gestation between 14-30 weeks at the initiation of the dose reduction
On a BUP dose between 6- 24 mg daily (lower doses will not provide sufficient data points)
Willingness to have urine samples tested for drugs of abuse and blood samples tested for BUP+M concentrations during the Medical Supervised Withdrawal (MSW) clinic appointments
Willingness to attend weekly or biweekly MSW clinic appointments and to have daily contact via text messaging and to complete daily logs of sleep quality, withdrawal symptoms and symptoms of craving.
Willingness to attend psychosocial support meetings as needed.

Exclusion criteria

Current use of cocaine, heroin, benzodiazepines, barbiturates, phencyclidine (PCP), or opioids other than BUP.
Currently taking more than two mental health medications
Active moderately severe depression (PHQ-9 score ≥15 or suicidal ideation)
Current incarceration
Lack of a phone or transportation to and from clinic
Major fetal malformation
Mother with significant vaginal bleeding or serious medical or obstetrical complication that could adversely affect the study
Planned delivery at another institution
HIV or AIDS
Diagnosis of schizoaffective disorder or psychosis