Participants were recruited from SUD treatment facilities by means of therapists’ referral. Inclusion criteria were self-reporting 10 cigarettes per day within the last year, receiving outpatient SUD treatment at the time of the study entry, and being able to attend the full smoking cessation treatment. Exclusion criteria were self-reported diagnosis of severe mental disorder (i.e., active psychotic disorder and/or suicidal ideation); current cannabis use; and current use of pharmacotherapy or behavioral treatment for smoking cessation.

A total of 97 participants were recruited for this randomized control trial, of which 17 were excluded due to cannabis use (n = 8), severe mental disorder (n = 2), not being in receipt of SUD treatment (n = 2), lack of motivation to quit tobacco (n = 2), self-quitting prior to treatment onset (n = 2), and electronic cigarette use (n = 1) (see Fig. 1). A total of 80 participants were randomly assigned to two treatment conditions: CBT (n = 46) or CBT+CM (n = 34). Fifteen participants in CBT and three in CBT+CM refused to participate after the baseline assessment, leaving a total of thirty-one participants in each treatment condition. There were not significant differences in baseline characteristics between treatment conditions (all p-values ≥ 0.115) (Table 1).

Figure 1.

Consort flow diagram of study participants.

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All participants were interviewed in an individual single assessment which gathered data about sociodemographic characteristics (e.g., age, sex, monthly income, marital status), as well as tobacco- and substance-related variables. Variables related to tobacco were number of cigarettes per day, years of regular use, motivation to quit (i.e., pre-contemplation, contemplation, and preparation stages) and previous quit attempts. Nicotine dependence was evaluated through the Fagerström Test for Cigarette Dependence (FTCD; Fagerström, 2012), which consist of 6 items. FTCD scores yield five levels of cigarette dependence: very low (0–2), low (3–4), medium (5), high (6–7), and very high (8–10) (Fagerström & Kozlowski, 1990).

The Structured Clinical Interview for the DSM-5 (SCID-5) was used to assess past year tobacco use disorder. The SCID-5 covers the 11 DSM criteria in a dichotomized scale (i.e., yes/no). SUD severity was interpreted based on the DSM-5 guidelines: absence (0–1), minimal (2–3), moderate (4–5), and severe (6–11). Substance-related variables were assessed as well, including primary and secondary substance of use, substance use abstinence (in days), and substance use treatment length (in days).

Both tobacco and substance use were biochemically verified. Carbon monoxide (CO) was used to assess tobacco use exposure at the baseline assessment and follow-ups, and urine cotinine was used to confirm smoking abstinence status from the sixth session, at the end of treatment, and each of the follow-up assessments. The cut-off for determining smoking abstinence were CO ≤ 4 ppm and urine cotinine ≤ 80 ng/ml. At the baseline assessment and each of the study visits, substance use (cannabis, cocaine, opioids, amphetamines, and methamphetamines) was assessed through test cassettes, and alcohol use was monitored through air expired. Worthy of note is that due to the COVID-19 lockdown (between March and June 2020), abstinence, both from tobacco and other substances, was not verified biochemically.

The treatment protocols and study procedures were approved by the Local Research Ethics Committee (No. 144/16) and registered in the ClinicalTrials-gov database (ref. NCT03551704). All participants provided a written informed consent prior to the baseline assessment.

Both treatment conditions (i.e., CBT and CBT+CM) included an eight-week smoking cessation treatment. Patients had to attend the clinic twice a week, one for the therapy session, with a duration of one hour and half, and the control session, whose objective is to collect biochemical samples.

Cognitive-Behavioral Therapy (CBT). The CBT protocol included several components previously described in standard cognitive-behavioral smoking cessation treatments (Secades-Villa et al., 2014) such as: psychoeducation, biochemical feedback, stimulus control, and training in strategies for reducing impulsivity, dealing with nicotine withdrawal symptoms, relapse prevention, and problem solving, among others. The CBT included a nicotine fading component that consisted of decreasing 20% of nicotine each week. Patients were asked to gradually reduce the number of cigarettes and switch their brand to lower-nicotine-content cigarettes each week. Patients were trained in EFT (the capability to pre-experience and project oneself into specific future events) (Morris et al., 2020). Further details on the EFT procedure may be consulted elsewhere (Aonso-Diego et al., 2021). In brief, participants were trained in the visualization of a total of five situations (one situation in one week, two in two weeks, one in a month, and one in three months), and practice visualizing them at each of the therapy sessions and at home.

Cognitive-Behavioral therapy (CBT) + Contingency Management (CM). This condition included the CBT, as described above, and voucher-based CM component for reinforcing tobacco abstinence. It consisted of providing contingent points (incentives) in exchange for biochemically verified tobacco abstinence (CO ≤ 4 ppm and urine cotinine ≤ 80 ng/ml). Incentives started at 20 points (€20) in the sixth session and increased by 5 points (€5) for each negative sample. Additionally, after each two consecutives negatives samples, patients received an additional 10 points. The reinforcement was continued through follow-ups: 45, 50, and 55 points were given to abstinent patients at one-, two-, and three-month follow-ups, respectively. The total maximum amount of vouchers a patient could earn if abstinent throughout the entire treatment and follow-ups was 340 points.

The primary outcome variable was smoking abstinence, for which two measures were considered: (1) self-reported point-prevalence abstinence (24-hour tobacco abstinence at the end of treatment and 7 days in follow-ups), and (2) days of continuous abstinence (i.e., number of consecutive days without smoking, not even a puff). Substance use abstinence was a secondary study outcome and was operationalized as 7-day point-prevalence, as well as by biochemical analysis. Worthy of note is that some follow-up visits were not collected due to COVID, and abstinence was based on self-report assessments.

Following an intent-to-treat approach, participants with missed study follow-up visits were considered as smokers. It is worth noting that the intention-to-treat approach was not considered for substance use outcomes (other than cigarette smoking). This means that missing participants were not considered as actively using substances (other than nicotine) at their corresponding follow-ups but were removed from the analyses. As participants were receiving treatment at the time of the smoking cessation trial, interpretations of the ‘true’ effects of study treatments were less straightforward and considering an intent-to-treat approach would unequivocally lead to high rates of false positives.

Bivariate analyses and descriptive statistics were performed to examine differences in baseline characteristics and abstinence rates. Differences between the two treatment conditions in continuous variables were examined with t-tests, while chi-square analyses were run for categorical variables. Risk ratios (RR) were performed to determine the risk of being a smoker in the follow-ups compared to end of treatment. The RR was estimated by dividing the incidence in the exposed group (i.e., smokers) by the cumulative incidence.

To support methodological convergence, a set of three generalized estimating equations (GEEs) were conducted to examine the efficacy of the tested interventions across time. The first one was performed to assess the main effects of treatment condition (i.e., CBT+CM vs. CBT) and time (i.e., end-of-treatment, 3-, 6-, and 12-month follow-up), as well as its interactive effect, in predicting point-prevalence smoking abstinence. The second and third GEE were aimed at examining the predictive capability of point-prevalence smoking abstinence and treatment conditions on substance abstinence at medium-term (i.e., 3 and 6 months) and long-term (i.e., 12 months). Given that both dependent variables (i.e., smoking abstinence and substance use abstinence) were dichotomous, the model was adjusted using logit link function, assuming a binomial distribution for the random component and with an unstructured working correlation.

Descriptive analyses were conducted using SPSS (version 24, Inc., Chicago, IL, USA), whereas the GEE was implemented through the PROC GENMOD procedure using SAS software version 9.4 (SAS Institute, Cary, NC). The confidence level for all the analyses was set at a 95% level.

At the end of treatment, the 24-h point-prevalence was 30.65% (19/62). Nearly twice as many of the participants in CBT+CM vs. CBT attained at least 24-h tobacco abstinence (41.94% vs. 19.35%; p = .049; φ = 0.245). Smoking abstinence rates by treatment condition at follow-ups are displayed in Table 2. Seven-day point-prevalence tobacco abstinence rates were 14.52% at 3-month follow-up (CBT: 12.90%; CBT+CM: 16.13%; p = .354), and 6.45% at 6- and 12-month follow-up (CBT: 6.45%; CBT+CM: 6.45%; p = 1).

Although both smoking cessation treatments produced positive effects on smoking abstinence, the GEE revealed a non-significant effect of treatment condition over point-prevalence smoking abstinence across time (see Table 3), meaning no additive effects of CM over CBT beyond treatment termination. The main effect of time was statistically significant, meaning that the odds of abstinence progressively declined across follow-ups. Lastly, the interaction between treatment and time did not yield statistical significance (β = −0.205, p = .260). For the whole sample, the risk of being a smoker steadily increased at sixth months (RR = 3.30, 95%CI 1.33, 8.17), and remained stable at one year. An analysis by treatment condition revealed that such risk was statistically significantly higher at 6 and 12 months, only in CM condition (RR = 4.62; 95%CI 1.249, 17.146) (see Fig. 2).

Figure 2.

Risk estimates for cigarette smoking across follow-ups (3-, 6-, and 12-month) in the whole sample and by treatment arm. Note. Risk estimates (RR) are provided for each follow-up assessment in comparison to the end-of-treatment smoking status. * p ≤ 0.05. CBT = cognitive-behavioral treatment; CM = contingency management.

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At the end of treatment, 79.54% (35/44) of the participants remained abstinent from their primary and secondary substance (CBT: 76.19%; CBT+CM: 82.61%; p = .668). At three-month follow-up, 88.24% (30/34) maintained substance abstinence (CBT: 84.21%; CBT+CM: 93.33%; p = .464), at six-month follow-up, 80% (24/30) (CBT: 76.92%; CBT+CM: 82.35%; p = .764), and at twelve-month follow-up 91.18% (31/34) (CBT: 94.12%; CBT+CM: 88.24%; p = .579).

A total of 63.16% (12/19) of those who quitted tobacco at end of treatment, remained abstinent from their primary and secondary substance in all follow-ups while 36.84% (7/19) of those who quitted were using substances at either follow-up. Among participants who did not successfully quit smoking, 55.17% (16/29) sustained substance abstinence across the entire study period (RR = 1.14, 95%CI 0.71, 1.84). An analysis by treatment condition suggested no significant increased risks in substance use as a result of quitting smoking [CBT: RR = 1.11, 95%CI 0.57, 2.17; CBT+CM: RR = 1.38, 95%CI 0.59, 3.23].

The GEE modeling the main effects of smoking abstinence, treatment condition, and its interaction with time (see Table 4) showed a non-significant effect of point-prevalence tobacco abstinence across time, neither medium-term (β = 0.489, p = .488) nor long-term (β = −0.456, p = .532). Similarly, the interaction between smoking abstinence and time was not significant (p ≥ .352). Neither the main effects of treatment condition (p ≥ .740) nor its interaction with time (p ≥ .548) were statistically significant.