Behavioral therapy and pharmacotherapy for relapse prevention in abstinent smokers: a rapid review and meta-analysis for the Korea Preventive Service Task Force

Article information

Osong Public Health Res Perspect. 2021;12(4):244-253
Publication date (electronic) : 2021 May 27
doi : https://doi.org/10.24171/j.phrp.2021.0017
1Department of Public Health Science, Graduate School of Public Health, Seoul National University, Seoul, Korea
2Department of Family Medicine, Ilsan Paik Hospital, Inje University College of Medicine, Goyang, Korea
3Department of Family Medicine, Seoul National University Hospital, Seoul, Korea
4Department of Family Medicine, Healthcare System Gangnam Center, Seoul National University Hospital, Seoul, Korea
5Biomedical Research Institute, Seoul National University Hospital, Seoul, Korea
Corresponding author: Belong Cho Department of Family Medicine, Seoul National University Hospital, 101 Daehak-ro, Jongno-gu, Seoul 03080, Korea E-mail: belong@snu.ac.kr
Naae Lee and Eon Sook Lee contributed equally as co-first authors.
Received 2021 January 21; Revised 2021 April 12; Accepted 2021 April 15.

Abstract

Objectives

This study aimed to assess the effectiveness of relapse prevention interventions involving behavioral and pharmacological treatment among abstinent smokers.

Methods

This rapid review was conducted using MEDLINE, Cochrane CENTRAL, CINAHL, Embase, KMbase, and KoreaMed to identify studies published until June 20, 2020. The participants were abstinent smokers who quit smoking on their own, due to pregnancy, hospitalization, or by participating in a smoking cessation program. We found a systematic review that fit the objective of this study and included 81 randomized controlled trials (RCTs). Studies that did not present information on smoking cessation status, had no control group, or used reward-based interventions were excluded. Random effect and fixed effect meta-analyses were used to estimate the relative risk (RR) and 95% confidence interval (CI). In subgroup analyses, differences between subgroups were verified based on the participant setting, characteristics, intervention type, and intensity.

Results

Following screening, 44 RCTs were included in the meta-analysis. The review reported no differences in the success rate of relapse prevention between the behavioral interventions. Pharmacotherapy interventions showed higher success rates (RR, 1.15; 95% CI, 1.05−1.26; I2=40.71%), depending on prior abstinence duration and the drug type.

Conclusion

The results indicated that pharmacotherapy has a significant effect on preventing relapse among abstinent smokers.

Introduction

Smoking is one of the major global causes of morbidity and mortality, with about half of smokers dying from smoking-related diseases [1]. Research on the health effects of smoking began in the early 1960s, and in 1964, general surgeons in the United States released a research report [2]; since then, many epidemiological studies have examined the harmful effects of tobacco. According to the World Health Organization, more than 8 million people per year die due to tobacco-related addiction [3]; among these, 7 million deaths can be directly attributed to tobacco. Smoking increases the risk of chronic diseases, such as chronic obstructive pulmonary disease, hypertension, cardiovascular diseases, and susceptibility to cancer [4,5]. The health effects of smoking contribute to the burden of disease nationally and globally, especially in developing countries [6].

According to Statistics Korea, since 2010, the percentage of smokers who have attempted to quit smoking for more than 24 hours in the last year has been steadily increasing, reaching 52.7% in 2018 [7]. According to the findings of the European Network for Smoking and Tobacco Prevention, the relapse rate of smokers who quit smoking unaided tends to increase over time. A study reported complete abstinence rates among abstinent smokers of 19% at 4 weeks after quitting, 10% at 6 months, and 5% at 1 year [8]. Many smokers attempt to quit smoking with a desire to improve their health; however, they are unsuccessful due to severe nicotine withdrawal symptoms [9]. Nicotine dependence has been found to be a strong predictor of the success of smoking cessation [10]. Therefore, the process of abstinence requires multiple attempts, instead of a single trial [11], and it may occur after different durations of cessation attempts [12].

In this study, relapse refers to the phenomenon of recurrence of smoking amidst the process of attempting to quit smoking. During the smoking cessation process, behavioral changes are observed in people who try to quit smoking, which gradually leads to relapse after a period of abstinence [8]. Several interventions can help smokers continue on their path of smoking cessation. Behavioral therapies, such as cognitive-behavioral therapy, and pharmacological approaches are relapse interventions that help abstainers continue on their path of smoking cessation [13]. However, the success rate of abstinence decreases steadily over time due to relapses [14]. In addition, randomized controlled trials (RCTs) have reported mixed findings concerning the efficacy and long-term success of relapse prevention for smoking cessation [15].

In this study, we aimed to conduct an updated rapid review and meta-analysis of these RCT studies to examine the effectiveness of relapse prevention interventions in behavioral and pharmacological treatment among abstinent smokers who successfully quit smoking. This review provides updated evidence, including additional studies from another recent review. This study aims to provide sufficient evidence to recommend appropriate relapse prevention interventions for smoking cessation to the Korea Preventive Service Task Force (KPSTF).

Materials and Methods

A rapid review of behavioral therapy and pharmacotherapy for relapse prevention was conducted using the KPSTF’s rapid review method to examine available evidence within a limited timeline [16]. The study protocol was approved by the KPSTF.

Search Strategy

We searched the following electronic international databases: MEDLINE, Cochrane Central Register of Controlled Trials (CENTRAL), Embase, and the Cumulative Index to Nursing and Allied Health Literature (CINAHL). Additionally, domestic databases included KoreaMed and KMbase. The search terms included “relapse prevention,” “recurrence,” “smoking cessation,” “smoke,” “tobacco,” and other relevant terms. As per the process of a rapid review, a systematic review (SR) or meta-analysis of the RCTs was explored initially. If we found an SR that could answer the key questions and aligned well with our inclusion and exclusion criteria, then we selected the most recent published SR fitting those criteria. Additional search strategies employed are provided in the supplementary files (Methods S1). There was no restriction on the publication year, and the most recent search date was June 19, 2020. The studies selected for this review were published in Korean and English.

Inclusion and Exclusion Criteria (PICO)

Studies conducting randomized controlled clinical trials were included in this review, while those with a follow-up period of less than 6 months were excluded.

The participants of the included studies were abstinent smokers, who voluntarily quit smoking (unassisted abstainers) or who quit smoking due to pregnancy, hospitalization, or by participating in a smoking cessation program (assisted abstainers). Abstinent smokers were defined as individuals who did not smoke at all within at least 24 hours. Participants who did not provide smoking cessation status at entry, who served in the military, or who did not report success at quitting smoking within 24 hours before entry were excluded.

Regarding the intervention, RCTs employing behavioral support and extended use of smoking cessation medication intended to prevent relapse were included. Among the included studies, pharmacological intervention studies for smoking cessation used placebos for the control groups, while behavioral intervention studies for smoking cessation used no intervention, regular care, or minimal interventions for the control groups. Intervention studies with reward-based incentives were excluded.

Outcome Measure

The primary outcome was the prolonged or point abstinence rate at 6 months or more of follow-up from RCTs. For trials that reported multiple follow-up studies, we chose the longest follow-up duration for the primary outcome. Biochemical tests involving the exhaled carbon monoxide level or cotinine level in saliva or urine and self-report were employed to verify continuing abstinence. The secondary outcome was the prolonged or point abstinence rate at less than 6 months of follow-up when that was reported.

Data Collection and Processing

While selecting the studies for the rapid review, 2 reviewers identified potentially eligible studies for inclusion. First, the titles were screened, followed by the selection of the abstract and the full text of the articles for the review. SRs were screened by checking the inclusion and exclusion criteria before selecting relevant studies. Two reviewers cross-checked independently, and a third reviewer checked the selected articles and all of them reached a consensus. In order to prevent bias, the findings of all studies were carefully reviewed, and any duplicated research was excluded (Figure 1).

Figure. 1.

Flow diagram of the selection of eligible studies for the systematic review and meta-analysis.

CENTRAL, Cochrane Central Register of Controlled Trial; CINAHL, Cumulative Index to Nursing and Allied Health Literature; RCTs, randomized controlled trials.

After finding the final SR for our study, 2 reviewers cross-checked the included RCTs to verify that they matched the inclusion and exclusion criteria. After selecting the studies, the following data from each RCT were identified: year of publication, author, intervention type, country, setting, number of participants, and abstinence verification method.

Quality Assessment

A Measurement Tool to Assess Systematic Reviews (AMSTAR) helps develop and evaluate SRs; moreover, it helps users focus on their methodological quality [17]. It comprises 11 items with 4 types of responses: “yes,” “no,” “can’t answer,” or “not applicable.” The instrument incorporates the study design, characteristics, and data extraction, literature search including the gray literature, a combination of study results, publication bias, and conflict of interest. AMSTAR quality scores range from 0 to 11, where scores of 0 to 3 indicate low quality, 4 to 7 moderate quality, and 8 to 11 high quality. Finally, 5 SRs were selected; of which 2 that scored a higher rating and a recent Cochrane review published in 2019 were finally selected.

The study of Livingstone-Banks et al. [14], which was published in the Cochrane Library in October 2019 and aimed to assess relapse prevention interventions among recent quitters who relapsed to smoking, was used for this analysis. Studies until May 2019 using randomized or quasi-RCTs with a minimum of 6 months of follow-up from the quitting date were systematically reviewed.

Statistical Analysis

In the meta-analysis, statistical heterogeneity was tested by a graphical representation of study data through the forest plots and the Higgins I2 test statistic. The Higgins I2 test statistic indicates the proportion of variation between the sample estimates; an I2 value ≥50% indicates significant heterogeneity [18]. The Mantel-Haenszel method, which applies a fixed-effect model, is suitable when the number of studies is small. The DerSimonian and Laird method, which uses a random-effects model, has been used for a long time and measures overall effect estimates more accurately even with larger heterogeneity [19]. Considering the characteristics of studies and the statistical tests, a fixed-effects model was used when I2 <50% and a random-effects model was used when I2 >50%.

Publication bias was tested using a funnel plot and the Egger test, which tests the linear relationship between the effect estimate and the standard error [20]. In order to identify significant effects of relapse prevention programs based on behavioral therapy and pharmacotherapy, differences between subgroups were verified according to participants’ recruitment setting and characteristics, publication year and country, the type and intensity of intervention, the verification method of abstinence, publication bias, and reported conflict of interest, as analyzed using the Cochrane Q test. The risk of bias was analyzed using the Cochrane Collaboration’s recommended tool to check the quality of the included studies. All analyses were performed using Stata/MP ver. 16.1 (StataCorp., College Station, TX, USA).

Results

Search Results

A total of 44 RCTs met the inclusion and exclusion criteria of the present study. Overall, 5,838 SRs were retrieved from 4 international databases; 4,630 of these were retained after removing duplicate studies by matching the title with the author. A total of 128 relevant studies were selected by screening the title and abstract, and 1 SR was eventually chosen. For the rapid review process, among the 81 RCTs in the selected SR, 44 RCTs were finally included in the meta-analysis. Figure 1 depicts the literature flow, and an attached supplementary file provides detailed information about the included studies (Table S1).

Effects of the Behavioral Therapy Intervention

Out of the 44 RCTs, 36 with relapse prevention interventions involving behavioral therapy were included; with 4 RCTs evaluating the effects of multiple behavioral therapy interventions. The 38 behavioral interventions resulted in no significant difference in the smoking cessation success rate for the intervention group over 6 months compared to the control group (relative risk [RR], 1.02; 95% confidence interval [CI], 0.98−1.07; I2=21.81%) (Table 1, Figure 2). The funnel plot and Egger test were used to identify publication bias among studies of behavioral therapy. No publication bias was observed after visually evaluating the funnel plot or according to the Egger test (p=0.18), as shown in Figure S1.

Behavioral interventions for relapse prevention in abstinent individuals and subgroup analyses

Figure. 2.

Summary of study findings of behavioral relapse prevention interventions.

CI, confidence interval; I2, Higgins I2 test statistic.

Of the 36 RCTs with 38 intervention groups for the secondary outcome, 12 RCTs reported outcomes at less than 6 months. The success rate of smoking cessation of the intervention group was not significantly higher than that of the control group (RR, 1.04; 95% CI, 0.98−1.10; I2=23.77%). Furthermore, no publication bias was detected (p=0.29) using the Egger test.

Effects of Pharmacotherapy Interventions

There were 10 RCTs on relapse prevention interventions based on pharmacotherapy, with 3 RCTs evaluating the effect of multiple interventions. Seventeen pharmacotherapy intervention groups showed significant effects on the success rate of smoking cessation compared to the control groups (RR, 1.15; 95% CI, 1.05−1.26; I2=40.71%) (Table 2, Figure 3). There was no publication bias in the funnel plot (Figure S1) or in the Egger test (p=0.46).

Pharmacotherapy interventions for relapse prevention in abstinent individuals and subgroup analyses

Figure. 3.

Summary of study findings of pharmacotherapy relapse prevention interventions for abstainers.

CI, confidence interval; I2, Higgins I2 test statistic.

Among the 10 RCTs with 17 intervention groups, 7 (12 intervention groups) reported outcomes at less than 6 months as a secondary outcome. The success rate in the intervention group was significantly higher than in the control group (RR, 1.13; 95% CI, 1.02−1.25, I2=57.44%). The Egger test detected no publication bias (p=0.23).

Risk of Bias

A risk of bias assessment was performed on selected documents using the Cochrane Risk of Bias tool [21]. Incomplete outcome data (attrition bias), blinding of outcome assessment (detection bias), blinding participants and personnel (performance bias), allocation concealment (selection bias), and random sequence generation (selection bias) were evaluated using 3 grades: low, high, and unclear risk of bias. Of the studies evaluating behavioral therapy, 1 study was evaluated as having a high risk of bias in random sequence generation, 5 studies in allocation concealment, 2 in blinding participants and personal, and 4 in blinding of outcome assessment. Regarding incomplete outcome data, 9 studies with behavioral interventions were unclear and 1 study reporting a pharmacotherapy intervention had a high risk of bias (Figure S2).

Subgroup Analysis

Subgroup analyses were conducted to assess significant factors associated with the efficacy of relapse prevention interventions. Participants were divided into groups based on their characteristics: participants’ recruitment setting, whether they enrolled in the smoking cessation program, were pregnant or hospitalized, the country of study, publication year, intervention type of behavioral therapy (counseling, self-help materials, or booklets), the intensity of the intervention, prior abstinence, verification method of abstinence, publication bias, and reports of conflicts of interest. There were no statistically significant differences among the subgroups in the behavioral intervention studies.

For the pharmacotherapy interventions, subgroup analyses were conducted among the following groups based on participants’ recruitment setting, the characteristics of participants, whether they enrolled patients in the smoking cessation program or hospitalized inpatients, type of country, publication year, the intensity of the intervention, prior abstinence, verification method of abstinence, publication bias, reports of conflicts of interest, and drug type in pharmacotherapy (nicotine replacement therapy [NRT], bupropion, or varenicline). The success rate of smoking cessation varied depending on the type of drug (p=0.047); while interventions with varenicline showed a significantly higher success rate, other modes of intervention that used different drugs did not show significant differences. Therefore, we excluded studies with varenicline, and no significant results were confirmed (RR, 0.97; 95% CI, 0.97−1.23). In addition, the success rate of smoking cessation varied depending on the duration of prior abstinence (p=0.001); specifically, the success rate of smoking cessation was significantly higher when the baseline abstinence period was less than 4 weeks.

Discussion

We investigated the effectiveness of the relapse prevention program for abstinent smokers based on behavioral therapy or pharmacotherapy using a rapid review to develop a recommendation. Evidence from 44 RCTs reported that relapse prevention programs using pharmacotherapy increased the success rate of smoking cessation compared to control groups who used placebos. However, we could not find any difference in the success rate of smoking cessation between the intervention groups incorporating behavioral therapy and usual care. In this study, a meta‐analysis was conducted by selecting the latest review about interventions for relapse prevention. Although several studies were excluded based on the exclusion criteria, the results from the included SR by Livingstone-Banks et al. [14] were consistent with those of this study. Our selected SR reported that the evidence does not support the use of behavioral interventions for assisted abstainers (RR, 0.98; 95% CI, 0.87−1.11) which is consistent with all previous studies. With pharmacotherapy, extended treatment helps in abstinence, but bupropion was not helpful and not enough evidence was available on NRT. Since we narrowed the scope of inclusion and exclusion criteria compared to the previous SR, we could conclude that the results were consistent.

In this review, a significant effect of existing behavioral interventions for relapse prevention among smoking abstainers was not detected. This indicates that the behavioral interventions provided no worthwhile benefit in preventing relapse in abstainers. However, a review of behavioral interventions of relapse prevention for abstainers by Agboola et al. [22] detected more positive results than those found in the present study. Although there are some discrepancies between prior reviews and this study, the differences in conclusions are not attributable to the included studies and are instead due to decisions related to subgroups and outcomes.

Furthermore, the results for some pharmacotherapies were more encouraging. Our study result reported that the extended use of smoking cessation drugs aided 15% of abstainers in maintaining successful smoking cessation, after 6 months of follow-up. The effect of pharmacological interventions was also observed at a shorter follow-up period, and was more prominent in abstainers at less than 4 weeks since quitting smoking. This might be a period when abstainers suffer from withdrawal symptoms. Some large and well-conducted studies illustrated the beneficial effects of varenicline in preventing relapse. However, studies on NRT or bupropion did not detect an effect on relapse prevention for abstainers. Varenicline is the most frequently prescribed medication for smoking cessation (87.9%) in the smoking cessation support services provided by the National Health Insurance Service [23]. This review provides evidence that pharmacological interventions, especially varenicline prescriptions, help abstinent smokers to continue their path of not smoking for over 6 months.

There are several limitations of this review. Firstly, the type and intensity of the behavioral therapy interventions in each study were highly variable; therefore, these conclusions about behavior therapy cannot be considered conclusive. Future studies should include RCTs with a single type of behavioral therapy intervention to further explore our conclusions about the effects of behavioral therapy on relapse prevention. Some studies applied a single intervention, but there were also complex interventions that applied 2 or more approaches. Accordingly, various subgroup analyses were performed. However, no significant effective specific behavioral therapy could be identified. Further research is required to provide more substantial results.

We intended to conduct a rapid SR that included RCTs conducted in Korea by searching Korean databases, but we could not find and include RCTs using Korean participants; thus, it was not possible to confirm any of these findings of relapse prevention within the Korean context. These findings are meaningful and extracted from Korean databases; however, they indicate the need for an RCT on relapse prevention among the Korean population.

In terms of the limitations of pharmacotherapy, the subgroup analyses confirmed that the effect of pharmacotherapy depends on the drug type; however, it cannot be claimed that varenicline is the only successful drug for relapse prevention. To overcome this limitation, a subgroup analysis was conducted excluding those with varenicline, but no significant results were found. In addition, a combined program (behavioral and pharmacotherapy treatment) was reported to be more effective in smoking cessation than a single independent treatment [8]. However, in this review, no significant effects were revealed through various subgroup analyses. Moreover, it cannot be asserted that combined programs are not effective in preventing relapse, because only a small number of studies used combined programs and those studies used NRT.

Conclusion

In summary, this study confirmed that pharmacotherapy interventions improved the success rate of smoking cessation for abstainers through an analysis of 44 RCTs focusing on relapse prevention programs. To encourage and recommend effective relapse prevention programs, a sufficient number of studies with large populations and long-term follow-up assessments should be conducted using each drug for smoking cessation or combined interventions.

Supplementary Material

Methods S1. Search strategies; Table S1. Characteristics of the included studies on relapse prevention; Figure S1. Funnel plot of the studies; Figure S2. Results of risk of bias among the included studies. Supplementary data are available at https://doi.org/10.24171/j.phrp.2021.0017.

Methods S1.

Search strategies

j-phrp-2021-0017-suppl1.pdf
Table S1.

Characteristics of the included studies on relapse prevention

j-phrp-2021-0017-suppl2.pdf
Figure S1.

Funnel plot of the studies. (A) Behavioral therapy interventions. (B) Pharmacotherapy interventions. CI, confidence interval.

j-phrp-2021-0017-suppl3.pdf
Figure S2.

Results of risk of bias among the included studies. (A) Behavioral therapy interventions. (B) Pharmacotherapy interventions.

j-phrp-2021-0017-suppl4.pdf

Notes

Ethics Approval

Not applicable.

Conflicts of Interest

The authors have no conflicts of interest to declare.

Funding

This article was supported by a Korea Disease Control and Prevention Agency (KDCA) research project, ‘Evidence Evaluation Center Operation Support for Community Chronic Disease Prevention and Control Project’ (Project No: B008011400150), in 2020. The content is solely the responsibility of the authors and does not necessarily represent the official views of the KDCA. We are grateful to Geumju Song for her support and guidance throughout the project.

Availability of Data

All data generated or analyzed during this study are included in this published article. For other data, these may be requested through the corresponding author.

Authors’ Contributions

Conceptualization: all authors; Data curation: NL, EL; Formal analysis: NL, EL; Investigation: all authors; Methodology: all authors; Project administration: BC; Resources: all authors; Software: all authors; Supervision: BC; Validation: all authors; Visualization: all authors; Writing–original draft: NL, EL; Writing–review & editing: all authors.

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Article information Continued

Figure. 1.

Flow diagram of the selection of eligible studies for the systematic review and meta-analysis.

CENTRAL, Cochrane Central Register of Controlled Trial; CINAHL, Cumulative Index to Nursing and Allied Health Literature; RCTs, randomized controlled trials.

Figure. 2.

Summary of study findings of behavioral relapse prevention interventions.

CI, confidence interval; I2, Higgins I2 test statistic.

Figure. 3.

Summary of study findings of pharmacotherapy relapse prevention interventions for abstainers.

CI, confidence interval; I2, Higgins I2 test statistic.

Table 1.

Behavioral interventions for relapse prevention in abstinent individuals and subgroup analyses

Subgroup Population (intervention-arm) RR (95% CI) I2 Subgroup difference (p-value)
Overall effect 13,494 (38) 1.02 (0.98−1.07) 21.81 -
Setting 0.43
 Hospital/clinic 2,608 (6) 0.97 (0.87−1.09) 60.36
 Community 7,015 (17) 1.02 (0.96−1.09) 20.96
 Premature clinic 3,871 (15) 1.06 (0.99−1.15) 0
Characteristics of participants 0.09
 Unassisted abstainers 2,763 (7) 0.92 (0.84−1.01) 3.59
 Assisted abstainers 5,541 (11) 1.05 (0.97−1.13) 25.63
 Pregnant and postpartum women 4,122 (16) 1.07 (1.00−1.15) 0
 Hospitalized 1,068 (4) 1.02 (0.85−1.22) 68.51
Type of intervention 0.89
 Direct counseling 649 (3) 1.00 (0.86−1.67) 31.14
 Indirect counseling 2,022 (4) 0.98 (0.86−1.12) 0
 Self-help materials 3,898 (8) 1.03 (0.95−1.11) 47.80
 Multiple interventions 6,925 (23) 1.04 (0.97−1.10) 21.81
Intensity of intervention 0.81
 High 4,070 (15) 1.01 (0.93−1.11) 31.62
 Low 9,424 (23) 1.03 (0.93−1.11) 40.26
Duration of prior abstinence 0.67
 Less than 4 wk 6,458 (16) 1.03 (0.96−1.09) 41.72
 Unclear 5,912 (14) 1.05 (0.96−1.14) 25.48
 More than 4 wk 1,124 (8) 0.99 (0.90−1.09) 50.14

RR, relative risk; CI, confidence interval; I2, Higgins I2 test statistic.

Table 2.

Pharmacotherapy interventions for relapse prevention in abstinent individuals and subgroup analyses

Subgroup Population (intervention-arm) RR (95% CI) I2 Subgroup difference (p-value)
Overall effect 4,051 (17) 1.15 (1.05−1.26) 40.71 -
Setting 0.26
 Hospital/clinic 1,948 (4) 1.21 (1.06−1.37) 0
 Community 2,103 (13) 1.09 (0.96−1.24) 42.94
Characteristics of participants 0.14
 Unassisted abstainers 2,016 (12) 1.04 (0.91−1.19) 0.17
 Assisted abstainers 1,473 (3) 1.25 (1.09−1.42) 66.42
 Hospitalized 562 (2) 1.26 (0.89−1.79) 0
Type of intervention 0.047
 NRT 1,575 (7) 1.19 (0.99−1.44) 27.10
 NRT+bupropion 161 (2) 0.83 (0.64−1.07) 0
 Varenicline 1,297 (2) 1.23 (1.08−1.41) 82.28
 Bupropion 1,018 (6) 1.05 (0.88−1.26) 26.16
Duration of prior abstinence 0.001
 Less than 4 wk 2,752 (7) 1.23 (1.10−1.38) 12.74
 Unclear 1,010 (7) 1.11 (0.89−1.38) 0
 More than 4 wk 289 (3) 0.86 (0.75−0.99) 0
Combination of intervention 0.47
 Combined (behavioral+pharmacotherapy) 517 (2) 1.34 (0.87−2.05) 0
  Only pharmacotherapy 3,534 (15) 1.14 (1.04−1.25) 45.42

RR, relative risk; CI, confidence interval; I2, Higgins I2 test statistic; NRT, nicotine replacement therapy.