Efficacy and Cost-Effectiveness of Cost-free Pharmacotherapy for Smoking Cessation for High-risk Smokers With Cerebrovascular Disease

University of Ottawa Heart Institute

Status and phase

Completed

Phase 4

Conditions

Cerebrovascular Disorders

Smoking Cessation

Treatments

Other: Prescription Only Group

Drug: Cost-Free Pharmacotherapy Group

Study type

Interventional

Funder types

Other

Identifiers

NCT00962988

HIPRC-6749

Details and patient eligibility

About

Research Aims

The aims of this research study are to determine whether cost-free smoking cessation pharmacotherapy:

Helps smokers with Transient Ischemic Attack (TIA) or stroke to quit smoking over the long-term, compared to simply providing a prescription for these medications;
Is a more cost-effective alternative to providing a prescription only for these medications in this high risk population.

Hypotheses to be Tested

The hypotheses to be tested include the following:

The CO-validated continuous abstinence rate at weeks 26 and 52 following a target quit date will be at least 10% higher for the cost-free smoking cessation pharmacotherapy intervention group compared to the prescription only usual care group;
Cost-free smoking cessation pharmacotherapy will have a greater cost-effectiveness (i.e., cost/quit) than providing a prescription only.

Full description

Smokers with Transient Ischemic Attack (TIA) or stroke attending a Stroke Prevention Clinic and willing to quit smoking will be randomly assigned (1:1) to either a prescription only (PO) usual care group or a cost-free (CF) pharmacotherapy experimental group. Participants assigned to the prescription only usual care group will be asked to have their prescription for smoking cessation pharmacotherapy filled at their own cost at their local community pharmacy. Participants assigned to the cost-free pharmacotherapy group will be provided with a 12-week supply of NRT, or a 12-week supply of bupropion or varenicline. The pharmacotherapy will be provided by the research nurse to the patient immediately. All participants will receive identical advice regarding smoking from the attending neurologist, nurse counseling for smoking cessation, and follow-up tracking and telephone-based support for up to 26 weeks after the target quit date. Non-treatment follow-up will continue to week 52 after the target quit date.

Enrollment

194 patients

Sex

All

Ages

18+ years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Patient is a current daily smoker (one cigarette per day in the month preceding the visit to the Stroke Prevention Clinic)
Patient has been diagnosed with TIA or stroke at any point in time
Patient is able, in the opinion of the neurologist, to comprehend and participate in the smoking cessation interventions
Patient is 18 years of age or older
Patient is willing to set a quit date
Patient willing to travel to study centre for follow-up visits
Patient is willing to provide informed consent

Exclusion criteria

Patient is unable to understand English or French
Patient is not willing to use pharmacotherapy to quit
Patient has been using smoking cessation medication for more than 6 weeks directly prior to clinic visit or hospital admission.
Patient is pregnant, lactating or planning to become pregnant during the study period
Patient has contraindication(s) to all of the following smoking cessation medications:
- Nicotine replacement therapy (allergy to adhesive, serious cardiac arrhythmias (e.g., tachycardia), vasospastic disease (e.g., Buerger's disease, Prinzmetal's variant angina)
- Bupropion (history of seizure disorder or head trauma; presently taking Wellbutrin; previous reaction to bupropion/Zyban/Wellbutrin; pre-existing or current eating disorder; taking anti-depressants, antipsychotics, corticosteroids, MAO inhibitors, theophylline, cocaine or diet pills; taking a quinalone antibiotic (e.g., ciprofloxacin, levoflozacin); currently using oral hypoglycemic product or insulin; severe hepatic impairment; CNS tumour; and
- Varenicline (renal failure; use of cimetidine; previous reaction to varenicline)