Extended-release Naltrexone and Care Management for Alcohol Dependent Frequent Emergency Department Users
Status: | Recruiting |
---|---|
Conditions: | Hospital, Psychiatric, Psychiatric |
Therapuetic Areas: | Psychiatry / Psychology, Other |
Healthy: | No |
Age Range: | 18 - 80 |
Updated: | 7/8/2018 |
Start Date: | July 2015 |
End Date: | January 2023 |
Contact: | Ryan P McCormack, MD |
Email: | ryan.mccormack@nyumc.org |
Phone: | 212-263-2862 |
Novel Interventions for Alcohol Dependent Frequent Emergency Department Users: Phase IV, Randomized, Open-label, Non-placebo-controlled Study of Extended-release Naltrexone and Care Management on Healthcare Use, Drinking, & Quality of Life
Our primary aim is to assess the feasibility of initiating treatment in the ED with
extended-release naltrexone (XR-NTX) plus care management (CM) vs. standard care and
continuing care in cooperation with clinic providers as well as how best to assess outcomes.
Secondarily, the investigators will explore its effect on various health outcomes (healthcare
utilization and engagement, expenditures, drinking and consequences, quality of life) as well
as the association of patient-level characteristics (e.g. sex, race, baseline drinking,
health and psychosocial factors, mu opioid receptor genotype) with effectiveness. Determining
both how to implement XR-NTX+CM and rigorously test its effects in the ED (phase 1) is
essential before planning a large-scale effectiveness trial (phase 2).
extended-release naltrexone (XR-NTX) plus care management (CM) vs. standard care and
continuing care in cooperation with clinic providers as well as how best to assess outcomes.
Secondarily, the investigators will explore its effect on various health outcomes (healthcare
utilization and engagement, expenditures, drinking and consequences, quality of life) as well
as the association of patient-level characteristics (e.g. sex, race, baseline drinking,
health and psychosocial factors, mu opioid receptor genotype) with effectiveness. Determining
both how to implement XR-NTX+CM and rigorously test its effects in the ED (phase 1) is
essential before planning a large-scale effectiveness trial (phase 2).
Aim #1: To conduct a feasibility and acceptability study of XR-NTX+CM treatment in alcohol
dependent patients with frequent ED use.
Hypothesis: Enrollment of a limited number of subjects will allow identification of optimal
processes for a definitive trial.
Aim #2: To conduct an analysis of the effect of this intervention on healthcare utilization
and engagement, drinking outcomes, quality of life, and consequences of drinking (initial
analysis will be exploratory).
Hypothesis: Measuring changes in healthcare utilization, drinking metrics, and indicators of
quality of life and consequences will provide preliminary data on intervention effect size on
various outcomes of interest to inform the second phase, definitive trial.
Aim #3: To identify patient-level characteristics associated with effectiveness.
Hypothesis: Exploratory analysis of patient and system-level characteristics possibly
associated with effectiveness will inform treatment choice to maximize the probability of
successful outcome. Factors assessed will include data collected in ongoing investigations of
pharmacotherapy for alcohol dependence, including mu opioid receptor (OPRM1) genotypes, to
facilitate comparison across study populations and settings.
This a phase IV, randomized, open-label, non-placebo-controlled, single-center study of the
feasibility, acceptability, and effect of initiating treatment in the ED with
extended-release naltrexone 380mg intramuscular injection compared to standard care in
subjects with severe alcohol use disorders (i.e. alcohol dependence) and frequent emergency
department use. In the first two years, we will finalize study preparations, recruit and
randomize 50 subjects for the pilot phase of this study. The duration of each subject's
participation will be 12 months. Thereafter, in the second phase of study, we will enroll an
additional 250 subjects (for a total of 300 subjects) to address remaining feasibility and
acceptability concerns and test effects.
The study investigators (PI and RA) will collect process data, including barriers and
facilitators encountered in the completion of all study procedures. For the following study
procedures, study investigators (the PI and RAs) will enter data directly into New York
University Langone Medical Center (NYULMC) internal REDCap system for use on portable tablet
computers.
Synopsis of Study Procedures:
The following study procedures are described in greater detail elsewhere in this protocol.
Patients will be prescreened for potential eligibility and added to an automated alert system
linked to ED registration by Bellevue Care Managers as part of an ongoing quality improvement
initiative. When a potentially eligible patient presents to the ED, an automated page will be
delivered to the study PI and Bellevue ED social work and care management staff, prompting
consultation and potential referral of the patient to study investigators (PI/RA) for
recruitment (See 4.3 Subject Recruitment and Screening). ED medical providers (inclusive of
ED physicians, nurses, social workers, and care managers) will notify study investigators
(PI/RA) when potentially eligible patients are present in the ED. The medical provider will
introduce the PI/RA to clinically sober and medically stable patients who have given their
permission to be approached. The PI/RA will describe the study, confirm capacity to consent
using the University of California San Diego Brief Assessment of Capacity to Consent to
Research (UBACC), and obtain written informed consent. The PI/RA will confirm eligibility by
performing a chart and laboratory review (liver enzymes, pregnancy, urine drug screen),
history and examination, and diagnostic interview to confirm alcohol dependence and assess
for opioid use and chronic pain. The PI/RA will conduct research intake assessments and
interview and collect blood for biomarker (5mL) and genetic (10mL) analyses. The PI/RA will
randomize subjects to intervention (XR-NTX+CM) or Standard Care using a random number
generator with randomly permuted blocks with allocations contained within opaque sealed
envelopes.
1. For subjects randomized to the Intervention Arm, the PI/RA will confirm the drug screen
is negative for opioids prior to administering XR-NTX 380mg as an intramuscular gluteal
injection. The PI/RA will facilitate a person-centered, harm-reduction-based
motivational interview, , and psychosocial assessment/interview to inform subjects'
care-management plans. Subjects will receive a one-week referral to Bellevue ambulatory
care for initial Alcohol-Medical Management (MM) and will also be scheduled every 4
weeks (after most recent XR-NTX injection) for MM and XR-NTX injections. When possible,
participants who miss MM-injection visits will be navigated to clinic upon their next ED
presentation and/or may receive MM and XR-NTX in the ED. XR-NTX will be administered by
the PI or a provider (physician, physician assistant, or registered nurse) who is
trained in the administration of XR-NTX. The schedule for MM-Injection visits is weeks
4, 8, 12, 16, 20, and 24. Participants may be offered to continue XR-NTX treatment
through this study for as many has 12 injections in total as we explore the feasibility,
acceptability and potential benefits of extending treatment duration to 12 months. The
schedule for potential additional MM-Injection visits is weeks 28, 32, 36, 40, and 44.
Research assessment visits will occur at weeks 12, 24, and 48 and may be conducted up to
28 days prior to- or 90 days after- date in which research visits are due. During
research visits, the PI/RA will repeat the assessments that were conducted at the
initial enrollment visit plus adverse events and participant satisfaction and we will
collect a 5mL blood sample to examine alcohol consumption biomarkers. Subject
participation ends after the week-48 research visit.
2. For subjects randomized to the Standard care arm, the PI/RA will provide referral to
Bellevue ambulatory care for MM without further intervention. Research assessment visits
will occur at weeks 12, 24, and 48 and may be conducted up to 28 days prior to- or 90
days after- date in which research visits are due. During research visits, the PI/RA
will repeat the assessments that were conducted at the initial enrollment visit plus
adverse events and participant satisfaction and we will collect a 5mL blood sample to
examine alcohol consumption biomarkers. Subject participation ends after the week-48
research visit.
dependent patients with frequent ED use.
Hypothesis: Enrollment of a limited number of subjects will allow identification of optimal
processes for a definitive trial.
Aim #2: To conduct an analysis of the effect of this intervention on healthcare utilization
and engagement, drinking outcomes, quality of life, and consequences of drinking (initial
analysis will be exploratory).
Hypothesis: Measuring changes in healthcare utilization, drinking metrics, and indicators of
quality of life and consequences will provide preliminary data on intervention effect size on
various outcomes of interest to inform the second phase, definitive trial.
Aim #3: To identify patient-level characteristics associated with effectiveness.
Hypothesis: Exploratory analysis of patient and system-level characteristics possibly
associated with effectiveness will inform treatment choice to maximize the probability of
successful outcome. Factors assessed will include data collected in ongoing investigations of
pharmacotherapy for alcohol dependence, including mu opioid receptor (OPRM1) genotypes, to
facilitate comparison across study populations and settings.
This a phase IV, randomized, open-label, non-placebo-controlled, single-center study of the
feasibility, acceptability, and effect of initiating treatment in the ED with
extended-release naltrexone 380mg intramuscular injection compared to standard care in
subjects with severe alcohol use disorders (i.e. alcohol dependence) and frequent emergency
department use. In the first two years, we will finalize study preparations, recruit and
randomize 50 subjects for the pilot phase of this study. The duration of each subject's
participation will be 12 months. Thereafter, in the second phase of study, we will enroll an
additional 250 subjects (for a total of 300 subjects) to address remaining feasibility and
acceptability concerns and test effects.
The study investigators (PI and RA) will collect process data, including barriers and
facilitators encountered in the completion of all study procedures. For the following study
procedures, study investigators (the PI and RAs) will enter data directly into New York
University Langone Medical Center (NYULMC) internal REDCap system for use on portable tablet
computers.
Synopsis of Study Procedures:
The following study procedures are described in greater detail elsewhere in this protocol.
Patients will be prescreened for potential eligibility and added to an automated alert system
linked to ED registration by Bellevue Care Managers as part of an ongoing quality improvement
initiative. When a potentially eligible patient presents to the ED, an automated page will be
delivered to the study PI and Bellevue ED social work and care management staff, prompting
consultation and potential referral of the patient to study investigators (PI/RA) for
recruitment (See 4.3 Subject Recruitment and Screening). ED medical providers (inclusive of
ED physicians, nurses, social workers, and care managers) will notify study investigators
(PI/RA) when potentially eligible patients are present in the ED. The medical provider will
introduce the PI/RA to clinically sober and medically stable patients who have given their
permission to be approached. The PI/RA will describe the study, confirm capacity to consent
using the University of California San Diego Brief Assessment of Capacity to Consent to
Research (UBACC), and obtain written informed consent. The PI/RA will confirm eligibility by
performing a chart and laboratory review (liver enzymes, pregnancy, urine drug screen),
history and examination, and diagnostic interview to confirm alcohol dependence and assess
for opioid use and chronic pain. The PI/RA will conduct research intake assessments and
interview and collect blood for biomarker (5mL) and genetic (10mL) analyses. The PI/RA will
randomize subjects to intervention (XR-NTX+CM) or Standard Care using a random number
generator with randomly permuted blocks with allocations contained within opaque sealed
envelopes.
1. For subjects randomized to the Intervention Arm, the PI/RA will confirm the drug screen
is negative for opioids prior to administering XR-NTX 380mg as an intramuscular gluteal
injection. The PI/RA will facilitate a person-centered, harm-reduction-based
motivational interview, , and psychosocial assessment/interview to inform subjects'
care-management plans. Subjects will receive a one-week referral to Bellevue ambulatory
care for initial Alcohol-Medical Management (MM) and will also be scheduled every 4
weeks (after most recent XR-NTX injection) for MM and XR-NTX injections. When possible,
participants who miss MM-injection visits will be navigated to clinic upon their next ED
presentation and/or may receive MM and XR-NTX in the ED. XR-NTX will be administered by
the PI or a provider (physician, physician assistant, or registered nurse) who is
trained in the administration of XR-NTX. The schedule for MM-Injection visits is weeks
4, 8, 12, 16, 20, and 24. Participants may be offered to continue XR-NTX treatment
through this study for as many has 12 injections in total as we explore the feasibility,
acceptability and potential benefits of extending treatment duration to 12 months. The
schedule for potential additional MM-Injection visits is weeks 28, 32, 36, 40, and 44.
Research assessment visits will occur at weeks 12, 24, and 48 and may be conducted up to
28 days prior to- or 90 days after- date in which research visits are due. During
research visits, the PI/RA will repeat the assessments that were conducted at the
initial enrollment visit plus adverse events and participant satisfaction and we will
collect a 5mL blood sample to examine alcohol consumption biomarkers. Subject
participation ends after the week-48 research visit.
2. For subjects randomized to the Standard care arm, the PI/RA will provide referral to
Bellevue ambulatory care for MM without further intervention. Research assessment visits
will occur at weeks 12, 24, and 48 and may be conducted up to 28 days prior to- or 90
days after- date in which research visits are due. During research visits, the PI/RA
will repeat the assessments that were conducted at the initial enrollment visit plus
adverse events and participant satisfaction and we will collect a 5mL blood sample to
examine alcohol consumption biomarkers. Subject participation ends after the week-48
research visit.
Inclusion Criteria
Subjects must meet all of the following criteria to be eligible for study enrollment:
1. English or Spanish speaking*
*Non-English Spanish speaking patients will not be enrolled initially until study
documents have been translated, back translated, and approved by the Institutional
Review Board (IRB).
2. Emergency Department patient
3. Aged 18-80
4. Have had >4 emergency department visits within 12 months for 2 consecutive 12-month
periods. Period of time can be extended by up to 6 months if incarcerated or
institutionalized for ≥ 6 months.
5. Meet Diagnostic and Statistical Manual version IV (DSM-IV) criteria for alcohol
dependence or & DSM-V criteria for alcohol use disorder, severe.
6. Have ≥2 days/week of heavy drinking (>4 drinks/day)
7. Capable of giving informed consent.
Exclusion Criteria
Subjects who meet any of the following criteria will be ineligible for study enrollment:
1. Active opioid dependence
2. Acute or chronic pain requiring opioid treatment
3. Acute liver injury (liver aminotransferase concentrations >5 times the upper limit of
normal)
4. Health condition considered unsafe for inclusion (at discretion of PI and/or attending
physician)
5. Lack of capacity or willingness to consent
6. Currently prescribed pharmacotherapy for alcohol dependence (not including treatment
of acute alcohol withdrawal syndrome)
7. Previous significant adverse reaction to naltrexone or diluent
8. Pregnant, nursing, or not using effective methods of birth control
9. Prisoners (as defined by Office of Human Research Protection) at the time of
enrollment ARE NOT ELIGIBLE for study entry. However, subjects who become prisoners
after being enrolled will be included and not be withdrawn from the study. Patients on
parole or probation are eligible for enrollment.
We found this trial at
1
site
New York, New York 10016
Principal Investigator: Ryan P McCormack, MD
Phone: 212-263-2862
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