Aggressive Smoking Cessation Trial (ASAP)

Sir Mortimer B. Davis - Jewish General Hospital

Status and phase

Enrolling

Phase 3

Conditions

Acute Coronary Syndrome

Cardiovascular Diseases

Treatments

Combination Product: Combination Therapy Arm (Varenicline and Nicotine E-Cigarettes Plus Counseling)

Other: Varenicline Plus Counseling

Study type

Interventional

Funder types

Other

Identifiers

NCT05257629

ASAP-001, Version 10

Details and patient eligibility

About

The ASAP Trial is a 5-year, multi-centre, randomized controlled trial that will assess the efficacy, safety, and tolerability of aggressive smoking cessation therapy among people at elevated cardiovascular risk. It will recruit 798 adult patients smoking on average at least 10 conventional (tobacco) cigarettes per day who are motivated to quit smoking and have either been diagnosed with ACS requiring hospitalization or are outpatients at elevated cardiovascular risk. Patients will be randomized (1:1) to one of two treatment arms: (1) combination therapy of varenicline and nicotine e-cigarettes plus counseling or (2) varenicline plus counseling for 12 weeks, with 52-week follow-up.

Full description

Background and Importance:

People who smoke are at an elevated risk of developing cardiovascular disease (CVD). Those who have an acute coronary syndrome (ACS), including myocardial infarction and unstable angina, and continue to smoke have a 35% increased risk of reinfarction or death compared with those who quit. Our previous smoking cessation trials have established varenicline (Champix) as the "gold standard" for patients with CVD. However, more than 50% of patients motivated to quit who receive varenicline for 12 weeks immediately post-ACS will return to smoking within 6 months. Therefore, more effective smoking cessation strategies are needed. Based on newly available data from randomized controlled trials (RCTs), including our E3 Trial, which suggest that nicotine e-cigarettes are more efficacious for smoking cessation than other nicotine replacement therapies and counseling alone, the investigators propose to combine varenicline and nicotine e-cigarettes (aggressive smoking cessation therapy). The proposed aggressive therapy is a novel approach needed now to increase abstinence in people at elevated cardiovascular risk.

Goal(s)/Research Aims:

The Aggressive Smoking Cessation Therapy Among People at Elevated Cardiovascular Risk (ASAP) Trial is a 5-year, multi-centre RCT that will assess the efficacy, safety, and tolerability of aggressive smoking cessation therapy among people at elevated cardiovascular risk. The specific aims are:

To assess the efficacy of combination therapy (varenicline and nicotine e-cigarettes) versus varenicline alone for 12 weeks, in terms of biochemically-validated 7-day point prevalence and continuous smoking abstinence, and ≥50% reduction in daily cigarette consumption at 24 and 52 weeks among people at elevated cardiovascular risk.
To describe the safety and tolerability of varenicline combined with nicotine e-cigarettes, in terms of serious adverse events (SAEs), adverse events (AEs), treatment discontinuation due to side effects, and therapy adherence over the 12-week treatment period.

Methods/Approaches/Expertise:

A total of 798 participants will be randomized 1:1 to: (1) varenicline and nicotine e-cigarettes (aggressive smoking cessation therapy), or (2) varenicline alone for 12 weeks, with follow-up of 52 weeks. Both arms will receive individual smoking cessation counseling. Participants randomized to aggressive therapy (varenicline and nicotine e-cigarette) will be given funds to cover the purchase of e-cigarettes and nicotine cartridges. Funds will be provided at baseline for the first 4 weeks of e-cigarette use. Participants who follow the e-cigarette purchasing instructions and provide receipts at subsequent clinic visits will be provided additional funds at week 4 (for weeks 4 to 8) and reimbursed at week 12 (for weeks 8 to 12). Participants will begin varenicline (titrated to 1.0 mg twice daily) and counseling at baseline, and e-cigarette use (if applicable) after the baseline visit. Eligible people will have or be at elevated risk of developing CVD, self-identify as regular smokers (≥10 cigarettes/day for ≥1 year), and be motivated to quit. They will complete telephone follow-ups at weeks 1, 2, 8, and 18, and clinic visits at weeks 4, 12, 24, and 52. We will collect information about self-reported smoking, treatment adherence, and adverse events. Self-reported smoking abstinence will be biochemically-validated at clinic visits using exhaled carbon monoxide (≤10 ppm). The primary endpoint will be biochemically-validated 7-day point prevalence smoking abstinence at 24 weeks. With 399 participants per arm and an alpha of .05, the investigators will have 80% power to detect a ≥10% difference in abstinence at 24 weeks. The ASAP Trial will be conducted by a highly experienced team of researchers and enrolling centres, who have previously completed three smoking cessation RCTs, including two in cardiac patients.

Expected Outcomes:

Smoking cessation is essential to reduce morbidity and mortality in this high-risk patient population. ASAP will provide regulators, health care professionals, and smokers with important information about the efficacy of aggressive varenicline and nicotine e-cigarettes therapy for smoking cessation in people at an elevated cardiovascular risk.

Enrollment

798 estimated patients

Sex

All

Ages

18+ years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Patients currently hospitalized or being discharged from hospital who have suffered an ACS, defined as follows:

i. MI, defined by positive troponin T, troponin I, or CK-MB levels (as defined by institution-specific cut-offs) and ≥ 1 of the following:
1. Ischemic symptoms for ≥ 20 min;
2. Electrocardiogram (ECG) changes indicative of ischemia (ST-segment elevation or depression);
3. Development of pathological Q waves on the ECG
ii. Unstable angina with significant coronary artery disease, defined by all of the following:
1. Ischemic symptoms for ≥ 20 min;
2. ECG changes indicative of ischemia (ST-segment changes);
3. At least one lesion ≥ 50% on angiogram performed during the current hospitalization.
[Note: patients who undergo cardiac catheterization or percutaneous coronary intervention (PCI) or coronary artery bypass graft (CABG) surgery will be eligible provided they are able to start varenicline in-hospital and nicotine e-cigarette at discharge.]

OR

Outpatients with the following diagnoses/conditions:

i. Cardiovascular:
1. Coronary artery disease documented with angiography or coronary CT;
2. Previous ACS, MI, stable or UA;
3. Previous coronary revascularization (e.g. PCI or CABG). ii. Renovascular:
a. Chronic kidney disease. iii. Cerebrovascular:

a. Previous cerebral infarction or transient cerebral ischemic attack. iv. Peripheral vascular:
1. Abdominal aortic aneurysm > 3.0 cm or previous aortic aneurysm surgery;
2. Ankle-brachial pressure index of < 0.9 or intermittent claudication;
3. Documented carotid artery disease;
4. Lower-limb amputation;
5. Previous lower-limb bypass surgery or angioplasty.
v. ≥1 risk factors:
1. BMI ≥ 27 kg/m2;
2. Dyslipidemia;
3. Family history (first degree relative: parents or siblings only) of coronary heart disease or stroke before the age of 60 years;
4. Hypertension;
5. Males aged ≥ 55 years/females aged ≥ 60 years;
6. Diabetes mellitus. vi. Heart-related conditions:

1. Atrial fibrillation or flutter;
2. Cardiomyopathy;
3. Heart failure;
4. Left ventricular hypertrophy (evidenced by echocardiography or ECG);
5. Valvular disease (evidenced by echocardiography).
Smoked on average ≥ conventional cigarettes/day for the past year;
Age ≥18 years;
Motivated to quit smoking according to the Motivation To Stop Scale (MTSS) (≥ level 5);
Able to understand and provide informed consent in English or French;
If randomized to the combination arm (varenicline and e-cigarette plus counseling), willing and able to purchase e-cigarettes with the following properties: rechargeable, closed system that uses sealed cartridges or pods, tobacco or no flavor only, and nicotine strength of 20 mg/ml (2%) or less;
Likely to be available for 52 weeks of follow-up.

Exclusion criteria

Pregnant or lactating females;
Use of any of the following in the 30 days prior to eligibility assessment:

i. Varenicline or bupropion for smoking cessation; ii. Nicotine or non-nicotine e-cigarettes; iii. Other anti-craving medication (e.g., naltrexone, acamprosate) with the potential to alter substance-seeking behaviors;
Use of nicotine replacement therapy (NRT) in the 7 days prior to eligibility assessment [Note: If participant is prescribed non-study NRT while hospitalized, they can continue using the non-study NRT until being discharged, even while taking the investigational products. Upon discharge, use of the non-study NRT should be stopped.];
Use of varenicline or e-cigarettes (nicotine or non-nicotine) for ≥14 days consecutively in the past year;
Previous serious adverse reaction to varenicline and/or e-cigarettes (nicotine or non-nicotine);
NYHA or Killip Class III or IV at the time of randomization;
Any unstable psychiatric disorder (as per enrolling physician);
Renal impairment with creatinine levels ≥2 times upper limit of normal or eGFR ≤15;
Use of any illegal drugs in the past year;
Planned use of cannabis (smoked) or other tobacco products (smoked or other) during the study period. [Note: use of cannabis which is not smoked is permitted (e.g., edibles, ingested or vaped oils). However, methods which involve combustion could invalidate biochemical validation via exhaled carbon monoxide.]

Trial design

Primary purpose

Prevention

Allocation

Randomized

Interventional model

Parallel Assignment

Masking

None (Open label)

798 participants in 2 patient groups

Combination Therapy Arm (Varenicline and Nicotine E-Cigarettes Plus Counseling)

Active Comparator group

Description:

Patients in the combination therapy arm will be supplied funds and instructions for the purchase of e-cigarettes and cartridges/pods upon hospital discharge and at the week 4 and 12 clinic visits. As with standard NRTs such as the gum, inhaler, and lozenge, the investigators expect smokers will self-regulate administration according to their withdrawal symptoms. Use will be monitored via self-report for telephone follow-ups. At clinic visits, patients will be asked to bring their e-cigarettes, used and unused cartridges/pods, and purchasing receipts. Patients will be advised regarding the signs and symptoms of nicotine toxicity and of an allergic reaction.

Treatment:

Combination Product: Combination Therapy Arm (Varenicline and Nicotine E-Cigarettes Plus Counseling)

Varenicline Plus Counseling

Other group

Description:

All patients will begin varenicline in-hospital upon randomization. For the first 3 days, patients will take a 0.5 mg tablet once a day. They will then take a 0.5 mg tablet twice a day for the following 4 days, and one 1 mg tablet twice a day from day 8 onward for the remainder of the 12-week treatment. Use will be monitored via self-report for telephone follow-ups and return of all unused tablets at the end of the treatment period. Should a patient experience severe side effects (such as headache, nausea, vomiting, dizziness, dyspepsia, fatigue, insomnia, abnormal dreams, constipation, or flatulence) on day 8 onward, the varenicline dose should be reduced from 1 mg twice daily to 0.5 mg twice daily prior to study medication discontinuation.

Treatment:

Other: Varenicline Plus Counseling

Trial contacts and locations

Central trial contact

Tabitha Finch; Carole Bohbot

Data sourced from clinicaltrials.gov

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