Clinical Trial Details
— Status: Active, not recruiting
Administrative data
| NCT number |
NCT04188873 |
| Other study ID # |
2019-0054 |
| Secondary ID |
2P01CA180945A534 |
| Status |
Active, not recruiting |
| Phase |
Phase 4
|
| First received |
|
| Last updated |
|
| Start date |
December 10, 2020 |
| Est. completion date |
May 1, 2025 |
Study information
| Verified date |
June 2024 |
| Source |
University of Wisconsin, Madison |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
This project will use the Multiphase Optimization Strategy (MOST) to guide the development of
optimized treatment strategies for the two most effective smoking cessation medications
(Combination Nicotine Replacement [C-NRT] and varenicline). The investigators will recruit
daily smokers from primary care to participate in a fully crossed, 2x2x2x2 factorial
experiment (N=608) that evaluates 4 different factors: 1) Medication Type (Varenicline vs.
C-NRT), 2) Preparation Medication (4 Weeks vs. Standard), 3) Medication Duration (Extended
[24 weeks] vs. Standard [12 weeks]); and 4) Counseling (Intensive vs. Minimal). Participants
will complete assessments one week pre-quit and then assessments of smoking status, treatment
use, side effects, potential treatment mechanisms (e.g., withdrawal, self-efficacy) during
the first week post-target quit date (TQD) and at Weeks 2, 4, 12, 20, 26, and 52 post-target
quit date. These data will be used to examine the main and interactive effects of these four
factors on various outcomes, with biochemically confirmed 12-month abstinence serving as the
primary outcome. These data will also be used to determine which factors and combinations of
factors are most effective with regard to 12-month biochemically confirmed abstinence and
cost, thereby identifying optimized varenicline and C-NRT treatments, with each developed to
yield especially great benefit. These optimized treatments will then be tested in the
Optimized Care Project. The investigators will also examine the relative effects of each
medication on particular outcomes (e.g., 12-month abstinence).
Description:
Design and Objective: The Cessation Screening Project is a 4-factor factorial screening
experiment (i.e., 2x2x2x2 = 16 experimental conditions) designed to identify the most
promising intervention components that are especially effective and cost-effective with
regard to their main and interactive effects on 12-month biochemically verified abstinence.
This design will allow us to: 1) detect main effects and interactions within the factorial
experiment and identify especially effective regimens for varenicline and for (Combination
Nicotine Replacement) C-NRT; 2) compare the relative effectiveness of varenicline and C-NRT;
and 3) identify the most effective and cost-effective counseling intensity to use with the
optimized medication regimens. Finally, these results will allow us to identify two optimized
treatment packages for use with primary care smokers interested in quitting: packages that
include both counseling and pharmacotherapies optimized on the bases of effectiveness and
cost.
Recruitment and Participants: Participants (N=608) will be primary care patients from 12
primary care clinics in two Wisconsin healthcare systems. Smokers will be identified via the
healthcare system electronic health record (EHR). All EHR-identified smokers in a clinic will
receive a mailed invitation to find out more about smoking treatment by calling a healthcare
system Care Manager (CM). In addition, using an opt-out strategy, Medical Assistants (MAs),
using an EHR-guided prompt, will inform all identified smokers seen at in-person or
tele-health visits that they will be contacted by the CM unless the participant indicates
s/he wants to opt-out. The participant contact information will then be automatically sent to
the CM unless the participant opts out; the investigators have developed and used this
workflow successfully in their past research. The CM will call and tell patients about the
smoking cessation options available for them including the availability of this smoking
cessation study. If patients are interested, the CM will obtain oral assent for screening and
sharing contact, primary care team, and screening data with the research team before
screening patients for eligibility. Eligible patients will learn more about the study and
have a chance to ask questions and provide verbal informed consent. Finally, participants
will complete a brief series of questions and then the CM will schedule a call with the study
staff (i.e., a Health Counselor) in the database to initiate treatment and complete study
assessments. Participants interested in quitting but not eligible for this study will be
electronically referred to the Wisconsin Tobacco Quit Line and/or their primary care provider
(PCP) by the CM.
Those who agree to and pass the screening for the inclusion/exclusion criteria for study
participation will be asked to complete an oral consent and HIPAA authorization process next.
After the patient provides oral consent, the CM will notify the patient's PCP via EHR that
the patient has volunteered for a study with C-NRT or varenicline. The PCP will notify the CM
via the EHR that the patient is medically eligible to receive either agent, as required by
the collaborating healthcare systems. This will occur within 5 business days. The PCP will be
notified via EHR of the patient's treatment assignment and of study-related serious adverse
events or adverse events that prompt medication discontinuation that may occur. Care
coordination with the PCP will occur via Tobacco Care Manager entry of data in the patient
EHR.
Procedures and Measures: At the second study call, participants (N=608) will be randomized to
one level of each of 4 factors: 1) Medication Type (Varenicline vs. C-NRT), 2) Preparation
Medication (4 weeks vs. Standard), 3) Medication Duration (Extended vs. Standard), and 4)
Counseling (Intensive vs. Minimal). Participants will be told their treatment condition at
Call 2, set a target quit date (TQD), and instructed how to use their study medications.
Medications will be mailed following this call, along with a handout that describes: 1) when
to begin taking study medication; 2) the type and doses involved; 3) how and when to obtain
the next month's medication; and 4) complete instructions on proper medication use, including
information from the package insert and contact information if they have questions regarding
their medication and/or symptoms they experience. Participants will be mailed all Preparation
Medication as well as one month of post-quit study medication after Call 2. They will need to
call in to a study line to request that more medication be mailed to them (Standard Duration
participants will call one time to receive their final 2 months of medication; Extended
Duration participants will call once to get 2 additional months of medication and again to
get the remaining 3 months of study medication). Participants will also receive a counseling
handout with their medications; those randomized to intensive counseling will receive a Quit
Plan listing their target quit day and when they start the medications and those randomized
to minimal counseling will receive the mobile health (mHealth) handout.
Participants will complete phone assessments one week pre-quit, during the first week
post-target quit date (TQD) and at Weeks 2, 4, 12, 20, 26, and 52 post-TQD.
Outcomes: The primary outcome for this study is biochemically confirmed, point-prevalence
abstinence at 12 months post-TQD (Primary Aim 1). The secondary outcome is cost effectiveness
in which the costs of implementing each intervention (minus research-related costs) will be
computed from a payer perspective. Costs will be combined with the intent-to-treat
biochemically verified 7-day point prevalence abstinence at 12 months post-TQD to determine
the cost per quit.
