grant

A Translational Randomized Clinical Trial of Varenicline Sampling to Promote Smoking Cessation and Scalable Treatment Dissemination

Organization MEDICAL UNIVERSITY OF SOUTH CAROLINALocation CHARLESTON, UNITED STATESPosted 8 Jul 2020Deadline 30 Jun 2026
NIHUS FederalResearch GrantFY2024Active Follow-upAddressAgonistArchivesAttitudeBehaviorBehavioralBiochemicalBiologicalCancer ControlCancer Control ScienceCancersClinicClinicalCuesDataDoseDrug PrescribingDrug PrescriptionsDrug TherapyDrugsExerciseFaceFailureFatigueFutureGoalsGuidelinesHandHealth Care ProvidersHealth Care TechnologyHealth PersonnelHealth TechnologyHealthcare ProvidersHealthcare TechnologyHealthcare workerIncidenceInstructionInternal MedicineInterventionIntervention StrategiesLack of EnergyMalignant NeoplasmsMalignant TumorMeasurableMediatorMedicalMedicationMethodologyMethodsMorbidityMorbidity - disease rateMotivationNicotine Replacement TherapyOutcomeParticipantPenetrancePharmaceutical PreparationsPharmacotherapyPhysiciansPopulationPrevention ResearchProceduresProcessPublic HealthPublicationsRandomizedReactionRecommendationResearchResearch ResourcesResourcesRisk FactorsRisk ReductionRoleSafetySamplingSampling StudiesScientific PublicationSelf EfficacySmokerSmokingSmoking BehaviorSouth CarolinaTestingTherapy trialTimeTobaccoWorkactive followupantagonismantagonistbiologicbrief advicecancer preventioncatalystcease smokingclinical significanceclinically significantcomparator groupcomparison groupdesigndesigningdiariesdrug treatmentdrug/agentevidence basefacesfacialfollow upfollow-upfollowed upfollowuphandshealth care personnelhealth care workerhealth providerhealth workforcehealthcare personnelinnovateinnovationinnovativeinterventional strategym-HealthmHealthmalignancymedical personnelmedication prescriptionmindfulnessmobile healthmortalityneoplasm/cancernicotine replacementoptimismpharmacologicpopulation basedpositive attitudepragmatic interventionprescribed medicationprimary care settingprogramspsychologicpsychologicalquit linequit smokingquitlinerandomisationrandomizationrandomized, clinical trialsrandomly assignedrecruitreduce riskreduce risksreduce that riskreduce the riskreduce these risksreduces riskreduces the riskreducing riskreducing the riskrisk-reducingsecondary outcomeside effectsmoking cessationsocial rolestop smokingtobacco controltooltreatment provideruptakevarenicline
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Full Description

Abstract: Smoking is the leading risk factor for preventable morbidity and mortality, and smoking cessation
remains the primary goal for population-based tobacco and cancer control. Many smokers lack resources to

initiate and sustain a successful quit attempt. For the last decade we have been testing innovative approaches

for delivery of pharmacotherapies that allow smokers to try evidence-based cessation medications and self-

determine their goals and pace for cessation. Medication sampling is a brief, concrete, and easily understood

exercise that often induces attitudinal shifts in favor of quitting smoking, and more importantly promotes quit

attempts and actual cessation. Medication sampling is also favored by healthcare providers, augmenting their

brief advice as per clinical guidelines. We have conducted three trials of nicotine replacement therapy (NRT)

sampling (N=157, 849, 1245), all of which were remote, and some of which have been applied within medical

settings. Each trial demonstrated increases in cessation behavior. Our prior work on NRT sampling creates a

compelling question as to whether varenicline sampling would have similar, or potentially better, effects.

Varenicline is inarguably the most effective single cessation medication available, superior to other

monotherapy options. As a prescription medication, whether varenicline is suitable for sampling is unclear but

worth testing empirically. On one hand, unstructured use, over a brief time, may not deliver sufficient

pharmacologic benefit. Prescription delivery incurs its own barriers to widespread dissemination (which can be

overcome). On the other hand, much like NRT sampling, it could provide a tangible cue to action that provides

psychological engagement (motivation, confidence, autonomy) to sustain subsequent use and ultimately

enhance cessation. A trial of varenicline sampling is not merely a routine extension of NRT trials, yet the

significance is even more compelling given evidence of its unique benefits. We therefore propose a

randomized clinical trial with primary aims to determine the 1) use, 2) consequences (on cessation), and 3)

mechanisms of varenicline sampling. A demographically diverse sample of 648 smokers will be recruited

across South Carolina and randomized (2:1:1) to receive I) a 4-week sample of varenicline, II) a 4-week supply

of NRT, or III) nothing. Thus, our design is strengthened by both active and inactive comparison groups.

Outcomes will be assessed through 6 months of follow-up. We employ innovations in mobile health

technologies throughout to enhance methodological rigor, including remote biological verification of smoking

behavior. If varenicline sampling were to show promise through this and future trials, this would offer great

dissemination appeal to physicians, quitlines, etc in that, much like our NRT work, varenicline sampling could

be a pragmatic strategy to engage more smokers in better treatments, sooner. Ultimately, the population

impact of medication/varenicline sampling could be profound, offering a significant and measurable opportunity

to lessen the impact of tobacco on public health and to reduce the risk, incidence and mortality of cancer.

Grant Number: 5R01CA246729-05
NIH Institute/Center: NIH

Principal Investigator: Matthew Carpenter

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