- Olu / Okwu: Olu 9: Nke 1
nkịtị
Ihe ndabere na ebumnuche
Internet addiction, sex addiction and compulsive buying are common behavioral problems, which share similarities with gambling disorder and substance use disorders. However, little is known about the efficacy of their treatments. The objective of this meta-analysis was to examine the efficacy of the treatments of such problem behaviors, and to draw parallels to gambling disorder and substance use disorders in terms of treatment response.
ụzọ
Literature search yielded 91 studies totaling 3,531 participants to provide a comprehensive evaluation of the short-term and long-term efficacy of psychological, pharmacological and combined treatments for internet addiction, sex addiction, and compulsive buying.
Results
Psychological, pharmacological, and combined treatments were associated with robust pre-post improvements in the global severity of internet addiction (Hedges’s g: 1.51, 1.13, and 2.51, respectively) and sex addiction (Hedges’s g: 1.09, 1.21, and 1.91, respectively). For compulsive buying, psychological and pharmacological treatments were also associated with a large-sized pre-post reduction in global severity (Hedges’s g: 1.00 and 1.52, respectively). The controlled pre-post and within-group pre-follow-up effect sizes were in the similar range, with few exceptions. Moderator analyses suggest that psychological interventions are effective for reducing compulsive behaviors, especially when delivered face-to-face and conducted over extended periods of time. Combinations of cognitive-behavioral approaches with medications showed an advantage over monotherapies.
Mkparịta ụka na Okwu Mmechi
The results suggest that treatments for common behavioral addictions are effective in the short term, similar to those implemented for gambling disorder and substance use disorders, but more rigorous clinical trials are needed.
Recent research has identified similarities between substance use disorders (SUDs) and behavioral addictions (BAs; e.g., Onyinye, Potenza, Weinstein, & Gorelick, 2010). Accordingly, non-substance related behavioral addictions had been defined based on the criteria for substance use specified in the Diagnostic and Statistical Manual of Mental Disorders (DSM IV; American Psychiatric Association, 1994) including preoccupation with the specific behavior, lack of control over the behavior, tolerance, withdrawal, and continued behavior despite negative consequences (e.g., Grant et al., 2010). Currently, only gambling disorder (GD), which was subsumed under “Impulse-Control Disorders Not Elsewhere Classified” in the DSM IV (American Psychiatric Association, 1994), is categorized under the new section “Substance-related and Addictive Disorders” of the DSM-5 (American Psychiatric Association, 2013). This reorganization has stimulated much debate as to whether further behaviors with diminished impulse control should be considered as possible candidates for BAs (e.g., Grant et al., 2010; Mueller et al., 2019).
Apart from GD, internet gaming disorder (IGD) is the only condition that is placed in the DSM-5 under Section III with the recommendation for further research (American Psychiatric Association, 2013). Supported by experts from various clinical and public health domains (e.g., Rumpf et al., 2018; Saunders et al., 2017), gaming disorder is also considered in the draft of the ICD-11 (Òtù Ahụ Ike Ụwa, 2018). It is important to note that IGD should be distinguished from the global designation internet addiction (IA), as both represent different constructs (e.g., Griffiths & Pontes, 2014; Kiraly et al., 2014). However, since many publications refer to global IA, this term has also been adopted in this paper. Moreover, a distinction should be made between “gaming” and “gambling”: Whereas “gaming is principally defined by its interactivity, predominantly skill-based play, and contextual indicators of progression and success, … gambling is defined by betting and wagering mechanics, predominantly chance-determined outcomes, and monetisation features that involve risk and payout to the player.” (King, Gainsbury, Delfabbro, Hing, & Abarbanel, 2015, p. 216).
Although the inclusion of IGD in the diagnostic manuals is discussed controversially in the scientific literature (King et al., 2019; Petry, Rehbein, Ko, & O'Brien, 2015; Rumpf et al., 2018; Saunders et al., 2017), much research has already been done on IA and IGD, particularly on neurobiological measures suggesting parallels to SUDs (for reviews see Fauth-Buhler & Mann, 2017; Kuss, Pontes, & Griffiths, 2018). Aside from similarities between SUDs and BAs in terms of phenomenological and clinical characteristics, comorbidity and family history, particularly findings from neuroscience research appear essential for identifying indicators of addictive behaviors (e.g., Grant et al., 2010; Potenza, Sofuoglu, Carroll, & Rounsaville, 2011).
In line with this consideration, some progress in the examination of neurobiological commonalities with SUDs has been achieved more recently within the domains of sex addiction (SA) and compulsive buying (CB) by analyzing phenomena traditionally investigated in SUDs such as conditioning processes (e.g., Hoffmann, Goodrich, Wilson, & Janssen, 2014; Snagowski, Laier, Duka, & Brand, 2016), cue reactivity, attentional bias and related neural network activation (e.g., Ahịa, Snagowski, Laier, & Maderwald, 2016; Gola et al., 2017; Jiang, Zhao, na Li, 2017; Laier, Pawlikowski, & Brand, 2014; Laier, Schulte, & Brand, 2013; Lawrence, Ciorciari, & Kyrios, 2014; Mechelmans et al., 2014; Pekal, Laier, Snagowski, Stark, & Brand, 2018; Schmidt et al., 2017; Seok & Sohn, 2015; Starcke, Schlereth, Domass, Schöler, & Brand, 2012; Trotzke, Starcke, Pedersen, & Eke, 2014; Trotzke, Starcke, Pedersen, Müller, & Eke, 2015; Voon et al., 2014), or executive functioning (Derbyshire, Chamberlain, Odlaug, Schreiber, & Grant, 2014; Messina, Fuentes, Tavares, Abdo, & Scanavino, 2017; Uhie, Elger, Neuner, & Weber, 2011; Trotzke et al., 2015). These studies demonstrated that among those conditions that have not yet been officially recognized in the DSM-5 as BAs, the currently available evidence regarding neurobiological indicators for parallels between substance-related and non substance-related behaviors mainly comes from the areas of IA, SA and CB, which are the focus of the present paper. Since these problems are of clinical relevance, and often associated with harmful consequences for affected individuals (e.g., Pontes, Kuss, & Griffiths, 2015), effective treatment options need to be investigated (e.g., Grant et al., 2010). To date, published meta-analyses have primarily been conducted with respect to IA proving the efficacy of various treatment approaches (Chun, Shim, & Kim, 2017; Liu, Liao, & Smith, 2012; Winkler, Doersing, Rief, Shen, & Glombiewski, 2013). Two of the meta-analyses examined psychological, pharmacological and combinations of both interventions, but the evidence was limited to treatment outcome studies in China (Liu et al., 2012), and Korea (Chun et al., 2017). The most comprehensive meta-analytic review supported the evidence for the efficacy of psychotherapy and medical treatments to reduce symptoms of IA including trials from Asian and western countries (Winkler et al., 2013). Combined interventions, however, were not considered. Moreover, the meta-analysis of Winkler et al. (2013) did not include more recent research.
Favorable results for psychological and pharmacological interventions in reducing global severity of CB were also found in another recent meta-analysis (Hague, Hall, & Kellett, 2016). However, the impact of study quality and other moderators on treatment outcomes was not examined. Consequently, a comprehensive investigation of treatment options for IA and CB is still pending. Although SA is considered in the ICD-11 with the term “compulsive sexual behaviour disorder” (Òtù Ahụ Ike Ụwa, 2018), and “self-reported feelings of addiction to pornography are not uncommon” (Grubbs, Kraus, & Perry, 2019, p. 93), treatments for SA have not yet been examined by meta-analytic methods. Additionally, no comparisons have yet been made between IA, or IGD—a candidate for the section “Substance-related and Addictive Disorders” of the DSM—and other possibly addictive behaviors, such as SA and CB, based on treatment response, which is considered an important indicator for parallels between SUDs and BAs (e.g., Grant et al., 2010).
The primary objective of the present meta-analysis, therefore, was to investigate the efficacy of psychological, pharmacological and combined psychological and pharmacological interventions for IA, SA, and CB for reducing (a) the global severity and (b) the frequency of compulsive behaviors after treatment cessation (short-term effects) and at the last reported follow-up period (long-term effects). Based on findings in recent reviews (Hague et al., 2016; Winkler et al., 2013), we expected psychological and pharmacological treatments to be equally effective across the three addiction categories. We further expected that treatment outcomes are similar to those reported for substance use and gambling (Grant et al., 2010; Potenza et al., 2011). In addition, our goal was to identify potential moderators of the effect sizes within each addiction category. The meta-analysis was conducted according to the recommendations of the PRISMA Statement (Moher, Liberati, Tetzlaff, & Altman, 2009).
ụzọ
Ụkpụrụ ruru eru
Studies were considered for inclusion if they (1) employed any kind of psychological, pharmacological, or combined intervention (e.g., psychological and pharmacological interventions applied at the same time); (2) used within-group, randomized, or quasi-randomized controlled study designs including wait-list controls, participants not receiving treatment, alternative active treatments, or a placebo intervention; (3) treated participants with the diagnosis of IA, SA, or CB; (4) measured at least one of the outcome variables (i.e., global severity or frequency); and (5) reported sufficient statistical data for effect size calculations. Studies were excluded if (1) the study was a single case study; (2) the study sample overlapped completely with the sample of another study included in the meta-analysis; (3) the treatment was not described, or (4) no abstract or full text of the study was available. With respect to SA, we only included studies investigating excessive sexual behaviors following the definition proposed by Kafka (2010), and excluded studies focusing treatments of paraphilias that differ from SA in terms of “socially anomalous or ‘deviant’ forms of sexual preference” (Kafka, 2010, p. 392).
Information sources and literature search
We conducted a multilevel literature search using the databases PsycInfo, Medline, PubMed, Psyndex, and ISI Web of Knowledge. The search covered all relevant publications from the first available year until June 30, 2019 using the following disorder-related search terms: Internet addiction, online addict∗, internet gaming disorder, online game addict∗, video game addict∗, videogame addict∗, computer game addict∗, smartphone addict∗, mobile phone addict∗, social media addict∗, facebook addict∗, problem∗ cellular phone; sex∗ addict∗, sex∗ compuls∗, sex∗ impuls∗, hypersex∗, nonparaphilic sex∗, paraphilia-related disorder∗; compulsive shopping, impulsive buy∗, oniomania, shopaholic∗, overshopping combined with the intervention-related key words treatment, intervention, therapy, psychotherapy. The same search terms were used to browse ProQuest Digital Dissertations for unpublished, gray literature. Subsequently, we conducted a thorough examination of the reference lists of review articles, meta-analyses, and original studies retrieved from the databases. Additionally, authors of relevant articles were contacted to ask for missing data and/or unpublished papers suitable for inclusion in the meta-analysis. Chinese publications were translated by two native speakers with an academic background.
Ihe ndi ozo
Following the most commonly reported outcome measures in the original studies, we specified two outcome variables to determine the reduction of pathological symptoms: (1) the global severity, quantified by the use of relevant assessment tools, and (2) the frequency (e.g., number of hours spent online, pornography viewing, or the number of buying episodes in the last week or month), quantified by diary cards or self-reports.
Nhọrọ nhọrọ
Study selection was performed by two independent reviewers (the first and the second authors, MG and ML), and supervised by the last author of this paper (AL). Disagreements between the authors were resolved through discussion.
Data collection process and data extraction
We generated a structured data extraction form that we refined and modified after pilot testing a sample of 10 studies. To calculate pre-post and pre-follow-up within-group effect sizes, numerical data were extracted for each treatment condition and outcome separately. If different psychological or pharmacological treatments were examined within one study, data for each condition were recorded separately and included in the within-group effect sizes for statistical analyses. To calculate pre-post controlled effect sizes, data from wait-list, no treatment, and placebo control groups were included. Additionally, we extracted numerical and categorical data from each study in order to perform moderator analyses. Data extraction was performed by the first author (MG), and validated by the second author (ML). The ratings of the two independent coders focused on the types of treatments, the measurement of the outcome variables, and the reliability and validity of the disorder-specific diagnoses. In the studies, however, the same tools have been applied both for the assessment of disorder-specific diagnoses and the measurement of the outcome variable “global severity” during treatment. Because the rating of the reliability and validity of the tools used for the measurement of the outcome variables was also part of the rating of the risk of bias in individual studies (see below), the interrater reliability quantified by the kappa statistic was performed only for the types of treatments.
Risk of bias in individual studies
We assessed the internal validity of each study using the Quality Assessment Tool for Quantitative Studies, developed by the Effective Public Health Practice Project (EPHPP) (Thomas, Ciliska, Dobbins, & Micucci, 2004). This tool has demonstrated content and construct validity (Thomas et al., 2004) and is recommended for systematic reviews and meta-analyses (Deeks et al., 2003). Each study was rated in a standardized manner on six domains: selection bias, study design, identification and control of confounders, blinding, reliability and validity of data collection tools, and reporting and percentage of withdrawals and dropouts. Each domain was evaluated as strong, moderate, or weak. The global rating was calculated after evaluation of the six domains. The first two authors (MG and ML) independently assessed each study and determined the global score of each trial. Interrater reliability was quantified using the kappa statistic. Disagreements between the authors were resolved through discussion until consensus was reached.
Effect size calculation and quantitative data synthesis
Statistical analysis was performed using the software program Comprehensive Meta-Analysis (CMA) version 2.2.064 (Borenstein, Hedges, Higgins, & Rothstein, 2005). Within each addiction category, we calculated effect sizes for the outcome variables reported in psychological, pharmacological, and combined studies separately for within-group and controlled study designs (see Appendix for formulas). Due to small sample sizes, the effect sizes were corrected for bias using Hedges’s g with the corresponding 95% confidence interval (CI; Hedges & Olkin, 1984). If means and standard deviations were not available, effect sizes were calculated based on equivalent estimation procedures (e.g., t values, or exact probability levels). If an outcome variable was measured by more than one instrument, data from these instruments were entered separately and pooled together for the particular outcome variable (Lipsey & Wilson, 2000). For studies reporting data based on both completers and intention-to-treat (ITT) analyses, the ITT data was taken into account. The direction of the effect was adjusted according to the “success”: the effect size was positive if the treated group performed superior to the control group. According to Cohen’s recommendations (1977), effect sizes of 0.20 to 0.30 can be classified as small, those near 0.50 as medium, and those above 0.80 as large.
Assuming heterogeneity among the studies, we decided to use the random effects model for the integration of effect sizes. Heterogeneity of the effect sizes was investigated using the Q statistic with the corresponding p value, and the I2 statistic, indicating to what extent real differences in effect sizes was reflected by the proportion of the variance (Borenstein, Hedges, Higgins, & Rothstein, 2009; Higgins, Thompson, Deeks, & Altman, 2003); I2 values of 25%, 50%, and 75% were classified as low, moderate, and high, respectively (Higgins et al., 2003).
Risk of bias across studies
To control for publication bias, we conducted a thorough literature search and computed Rosenthal’s fail-safe N (Rosenthal, 1979) and also examined funnel plots (Duval & Tweedie, 2000). Dabere na Rosenthal (1991), effect sizes are considered robust if the number of studies needed to obtain a nonsignificant overall effect is greater than 5k + 10, where k represents the number of studies. Additionally, we used the trim-and-fill method (Duval & Tweedie, 2000) to estimate missing studies and their impact on the ascertained effect sizes. This method is based on the logic of the funnel plot and assumes a symmetrical distribution of the effect sizes for outcome variables in the absence of publication bias. In the case of asymmetrical distribution, the trim-and-fill method adjusts and corrects the effect sizes (Borenstein et al., 2009); we only applied this method if 10 studies were available for the analysis (Sterne, Egger, & Moher, 2011). Funnel plot asymmetry was assessed by using Egger’s test (Egger, Smith, Schneider, na Minder, 1997). As singular extreme effect size values produce misleading interpretations of treatment effects (Lipsey & Wilson, 2000), we used the “one-study-removed” method offered by CMA to examine the impact of each study’s effect size on the overall effect (Borenstein et al., 2005). If the recalculated results did not substantially impact the effect size and remained within the 95% CI, studies were retained in the analyses.
Moderator analysis
To explain heterogeneity among effect sizes, we examined the type of data analysis (ITT vs. completer analysis), and the quality of studies (EPHPP global scores) as possible moderators. Because depression and anxiety were found to be associated with BAs (e.g., González-Bueso et al., 2018; Starcevic & Khazaal, 2017), we examined whether the effect sizes varied as a function of these co-occurring disorders (inclusion vs. exclusion of depression and/or anxiety). Since co-occurring disorders, particularly depression and anxiety, are most common among individuals affected by BAs (Starcevic & Khazaal, 2017), studies that failed to report data on comorbid conditions were assumed to include participants with co-occurring depression and anxiety as well. For psychological studies, we further investigated the mode of treatment (group setting vs. individual counseling vs. other types of settings [e.g., individual and group setting, family setting]), the mode of delivery (face-to-face [FTFTs] vs. self-guided treatments [SGTs]), and the type of psychological intervention. The type of psychological intervention was analyzed by dividing psychological strategies into the following subcategories: (1) CBT, covering cognitive and/or behavioral treatments; (2) integrative treatment involving a variety of different treatment approaches, and (3) psychological therapies that pertain to other categories, such as family therapy, reality therapy, acceptance and commitment therapy, or art therapy. Assuming that a number of studies were conducted in non-western countries, particularly for IA, we followed a previous meta-analysis (Winkler et al., 2013) and explored whether the cultural background (Asian vs. other countries) proved to be a moderator. Since global IA and IGD represent different constructs (e.g., Griffiths & Pontes, 2014), we also examined the differences between studies based on global IA and those, that investigated IGD and other internet-enabled activities (e.g., smartphone addiction, videogame addiction).
For pharmacological treatments, we examined whether antidepressants performed superior to other types of medications or to mixed medications (e.g., antidepressants combined with methylphenidate). For combined studies, we examined both the impact of the types of psychological and pharmacological interventions. Additionally, we investigated whether one of the types of treatment (psychological vs. pharmacological vs. combined interventions) within each addiction category showed an advantage over the others. Finally, we compared the effect sizes of psychological and pharmacological interventions of the different addiction categories. Accounting for the fact that “the internet is just a channel through which individuals may access whatever content they want (e.g., gambling, shopping, chatting, sex)” (Griffiths & Pontes, 2014, p. 2), we subsumed studies that included individuals with excessive sexual or buying behaviors under the categories “sex addiction” and “compulsive buying”, regardless of whether the internet was used or not.
Moderator analyses for categorical variables were conducted using the mixed effects model with pooled estimates of T2 and the Q-test based on analysis of variance with the corresponding p value for the interpretation of the differences between subgroups (Borenstein et al., 2009). In the case of at least 10 available studies (Deeks, Higgins, & Altman, 2011), we further conducted meta-regression analyses using the year of publication and the duration of treatment (assessed with the total number of hours spent in treatment in psychological trials, or with the number of weeks in pharmacological trials). If an insufficient number of psychological studies indicated the number of hours spent in treatment, the number of weeks was used to measure treatment duration. Meta-regression analyses on the mean age and the percentage of male/female participants were not performed because age and sex across studies differ from that within studies hampering reliable interpretation (Thompson & Higgins, 2002).
Results
Nhọrọ nhọrọ
The flow diagram of the study selection process is illustrated in Fig. 1. There were no interrater disagreements regarding the types of treatments.
Characteristics of studies, treatments, and participants
Across all addiction categories, the present sample of studies varied in type of control condition: Half of them implemented no control group (50%) and several studies used waitlist, no treatment, healthy controls, or placebo control groups (30%), or other active treatment comparisons (20%). Results were mainly based on completers (80%). Follow-up data were provided by 32 psychological studies (IA: k = 16 studies with periods ranging from 1 to 6 months; M = 3.53, SD = 2.13; SA: k =11 studies with periods ranging from 1.5 to 6 months; M = 4.27, SD = 1.88; CB: k = 5 studies with periods ranging from 3 to 6 months; M = 5.4, SD = 1.34), by one pharmacological study in the CB category with 12 months follow-up, and by two studies in the IA category which used combined interventions, each collecting data at one month follow-up.
The majority of psychological studies examined CBT (58%), delivered treatment through group settings (71%), and in face-to-face format (92%). The total number of hours spent in psychological interventions ranged from 15 min to 54 h (M = 12.55 h, SD = 10.49), from one week to 26 weeks (M = 10.44, SD = 6.12), and from 8 weeks to 20 weeks (M = 11.71, SD = 3.90) for the treatment of IA, SA, and CB, respectively. Most pharmacological studies examined antidepressants (85%); the majority of combined trials used CBT in combination with antidepressants (71%). The duration of pharmacological treatments ranged from 6 to 52 weeks (M = 15.67, SD = 17.95), from 12 to 72 weeks (M = 24.83, SD = 23.58), and from 7 to 12 weeks (M = 9.50, SD = 2.20) for the treatment of IA, SA, and CB, respectively.
Across all addiction categories, a total of 3,531 participants were analyzed (IA: n = 2,427; SA: n = 771; CB: n = 333). The majority of the studies included participants with co-occurring depression and anxiety (77%). Trials focusing on IA were mainly conducted in Asian countries (75%). The total sample was predominantly male in studies examining IA (76%) with an average age of 21, and SA (98%) with an average age of 37, but female in studies examining CB (92.45%) with an average age of 42. Detailed information regarding the characteristics of studies is presented in Tables 1–3.
Ntọala 1.Characteristics of studies for internet addiction
Study/Year | Na | Treatment group (N)/Mode of therapy/Mode of deliveryb | Control group (N)/Mode of therapy/Mode of deliveryb | Culture/D/A (+/−)/IA type | Duration t/cc | FU (months) | Outcomes (assessment) | Nyocha data | EPHPP |
Psychological treatments | |||||||||
Anuradha and Singh (2018) | 28 | CBT (28)/I/FTFT | Ọ dịghị onye | Asia/−/IA | NA | Ọ dịghị onye | GS (IADQ) | CO | 3 |
Bai and Fan (2007) | 48 | IT (CBT; self-control; social competence) (24)/G/FTFT | NT (24) | Asia/+/IA | 16 | 1.5 | GS (CIAS-R) | CO | 3 |
Cao et al. (2007) | 57 | CBT (26)/G/FTFT | NT (31) | Asia/+/IA | 10 | Ọ dịghị onye | GS (YDQ, CIAS) | CO | 2 |
Celik (2016) | 30 | EDU (15)/G/FTFT | NT (15) | Turkey/+/IA | 10 | 6 | GS (PIUS) FR (% of Internet game playing among Internet use/w)d | NA | 3 |
Deng et al. (2017) | 63 | CBI (44)/G/FTFT | WL (19) | Asia/+/IGD | 18 | 6 | GS (CIAS) | CO | 2 |
Du et al. (2010) | 56 | IT (CBT; parent training; EDU for teachers) (32)/G/FTFT | NT (24) | Asia/+/IA | 14 | 6 | GS (IOSRS) | CO | 2 |
González-Bueso et al. (2018) | 30 | 1) CBT (15)/I/FTFT 2) IT (CBT+EDU for parents) (15)/I/FTFT | HC (30)e | Spain/−/IGD | 1) 9 2) 9 | Ọ dịghị onye | GS (DQVMIA) | CO | 3 |
Guo et al. (2008) | 28 | 1) CBT (14)/G/FTFT | 2) SUPP (e.g., sharing information on IA; promotion of self-esteem and resources) (14)/G/FTFTf | Asia/+/IA | 1) 8 2) NA | Ọ dịghị onye | GS (CIAS) | CO | 2 |
Han et al. (2012) | 14 | FT (14)/F/FTFT | Ọ dịghị onye | Asia/−/IGD | NA | Ọ dịghị onye | GS (YIAS) FR (h/w) | CO | 3 |
Han et al. (2018) | 26 | CBT (26)/G/FTFT | Ọ dịghị onye | Asia/−/IGD | 24 | Ọ dịghị onye | GS (CIAS) FR (h/w) | CO | 3 |
Hui et al. (2017) | 73 | 1) CBT (37)/G/FTFT | 2) IT (CBT+EA) (36)/I+G/FTFTf | Asia/−/IGD | 1) 5 2) 10 | Ọ dịghị onye | GS (IAD) | CO | 2 |
Ke and Wong (2018) | 157 | CBT (157)G/FTFT | Ọ dịghị onye | Asia/+/IA | 12 | 1 | GS (PIUQ) | CO | 3 |
Khazaei et al. (2017) | 48 | PI (24)/G/FTFT | WL (24) | Iran/+/IA | NA | Ọ dịghị onye | GS (IAT) FR (h/w) | NA | 3 |
Kim (2008) | 25 | RT (13)/G/FTFT | NT (12) | Asia/+/IA | 12.5 | Ọ dịghị onye | GS (K-IAS) | NA | 3 |
King et al. (2017)g | CBT (84 h abstinence) (9)/I/NA | Ọ dịghị onye | Australia/+/IGD | NA | 1 | GS (IGD checklist) FR (h/w) | CO | 3 | |
Lan et al. (2018) | 54 | 1) CBT (27)/G/FTFT | 2) EDU (27)/G/FTFTf | Asia/+/SMA | 1) 8 2) 1 | 3 | GS (MPIAS) FR (h/w) | CO | 2 |
Lee et al. (2016) | 46 | CBT (home-based daily writing) (46)/FTFT/I | Ọ dịghị onye | Asia/+/SMA | NA | Ọ dịghị onye | GS (KSAPS) | CO | |
Li and Dai (2009) | 76 | CBT (38)/I/FTFT | WL (38) | Asia/+/IA | 14 | Ọ dịghị onye | GS (CIAS) | CO | 3 |
Li, Garland et al. (2017) | 30 | 1) MORE (15)/G/FTFT | 2) SUPP (15)/G/FTFTf | USA/−/IGD | 1) 16 2) 16 | 3 | GS (DSM-5 criteria) | ITT | 2 |
Li, Jin et al. (2017) | 73 | 1) CBT (36)/G/FTFT | 2) CBT+EA (37)/I+G/FTFTf | Asia/+/IGD | 1) 5 2) 10 | Ọ dịghị onye | GS (IAT) | CO | 3 |
Liu et al. (2013) | 31 | 1) CBT (16)/G/FTFT | 2) SM (e.g., written records of gambling frequency; determination of target behaviors) (15)/G/SGTf | Asia/−/IA | 1) 54 2) 24 | Ọ dịghị onye | GS (IAT) FR (h/d) | CO | 3 |
Liu et al. (2015) | 46 | FT (21)/G/FTFT | WL (25) | Asia/−/IA | 12 | 3 | GS (APIUS) FR (h/w) | CO | 2 |
Pallesen et al. (2015) | 12 | IT (CBT; FT; SFT; MI) (12)/G/FTFT | Ọ dịghị onye | Norway/+/VGA | NA | Ọ dịghị onye | GS (GASA; PVP) | CO | 3 |
Park, Kim et al. (2016) | 24 | 1) CBT (12)/G/FTFT | 2) VRT (12)/G/SGTf | Asia/−/IGD | 1) 16 2) 4 | Ọ dịghị onye | GS (YIAS) | CO | 3 |
Pornnoppadol et al. (2018) | 54 | 1) IT (CBT+skills+ sports) (24)/G/FTFT | 2) EDU (30)/G/FTFTf | Asia/−/IGD | NA 2) 1 | 6 | GS (GAST) | CO | 2 |
Sakuma et al. (2017)g | 10 | IT (SDiC including CBT; outdoor cooking; walk rally; trekking; woodworking) (10) G/FTFT | Ọ dịghị onye | Asia/−/IGD | NA | 3 | FR (gaming h/d; h/w; d/w) | CO | 3 |
Shek et al. (2009) | 22 | IT (individual and family counseling; peer support) (22)/I/FTFT | Ọ dịghị onye | Asia/+/IA | NA | Ọ dịghị onye | GS (CIA-Y; CIA-G) | CO | 3 |
Sei et al. (2018) | 46 | MI (PFB) (46)/I/SGT | Ọ dịghị onye | Asia/+/IA | NA | Ọ dịghị onye | GS (IAT) | CO | 3 |
Su et al. (2011) | 59 | CBT (online treatment program) 1) LE (17)/I/SGT 2) NE (12)/I/SGT 3) NI (14)/I/SGT | NT (16) | Asia/+/IA | 1) 0.48 2) 0.48 3) 0.26 | Ọ dịghị onye | GS (YDQ) FR (h/w) | CO | 2 |
van Rooij et al. (2012) | 7 | CBT (7)/I/FTFT | Ọ dịghị onye | Netherlands/+/IA | 7.5 | Ọ dịghị onye | GS (CIUS) FR (d/w; h/d) | CO | 3 |
Wartberg et al. (2014) | 18 | CBT (18)/G/FTFT | Ọ dịghị onye | Germany/+/IA | 12 | Ọ dịghị onye | GS (CIUS) FR (h/weekdays; h/weekends) | CO | 3 |
Woelfling et al. (2014) | 42 | CBT (42)/G+I/FTFT | Ọ dịghị onye | Germany/−/IA | 32 | Ọ dịghị onye | GS (AICA-S) FR (h/weekend day) | ITT | 3 |
Yang and Hao (2005) | 52 | IT (SFBT; FT; CT) (52)/I/FTFT | Ọ dịghị onye | Asia/+/IA | NA | Ọ dịghị onye | GS (YDQ) | CO | 3 |
Yang et al. (2017) | 14 | 1) CBT (14)/G+I/FTFT 2) EA (16)h | HC (16)e | Asia/−/IA | 20 | Ọ dịghị onye | GS (IAT) | CO | 2 |
Yao et al. (2017) | 37 | IT (RT; MFM) (18) G/FTFT | NT (19) | Asia/+/IGD | 12 | Ọ dịghị onye | GS (CIAS) | CO | 3 |
Na-eto eto (2007) | 114 | CBT (114)/I/FTFT | Ọ dịghị onye | USA/+/IA | NA | 6 | GS (APA; CCU; MSA; SF) FR (OA) | CO | 3 |
Na-eto eto (2013) | 128 | CBT modified (128)/I/FTFT | Ọ dịghị onye | USA/+/IA | NA | 6 | GS (IADQ) | CO | 3 |
Zhang (2009) | 70 | IT (CBT; sports) (35)/G/FTFT | NT (35) | Asia/+/IA | 24 | Ọ dịghị onye | GS (IAT) | CO | 3 |
Zhang et al. (2009) | 11 | CBT (11)/G/FTFT | Ọ dịghị onye | Asia/+/IA | NA | Ọ dịghị onye | GS (IAT) | CO | 2 |
Zhang et al. (2016) | 36 | IT (CBI+MFTR) (20)/G/FTFT | NT (16) | Asia/+/IGD | 17 | Ọ dịghị onye | GS (CIAS) FR (h/w) | CO | 2 |
Zhong et al. (2011) | 57 | 1) FT (28)/G/FTFT | 2) IT (military training; sports; therapy targeting addictive behaviors) (29)/G/FTFTf | Asia/−/IA | 24.5 2) NA | 3 | GS (OCS) | CO | 2 |
Zhu et al. (2009) | 45 | 1) CBT (22)/G/FTFT | 2) IT (CBT+EA) (23)/I+G/FTFTf | Asia/+/IA | 5 2) 10 | Ọ dịghị onye | GS (ISS) | CO | 2 |
Zhu et al. (2012) | 73 | 1) CBT (36)/G/FTFT | 2) IT (CBT+EA) (37)/I+G/FTFTf | Asia/+/IA | 5 2) 10 | Ọ dịghị onye | GS (IAT) | CO | 2 |
Ọgwụ Farmacological | |||||||||
Bipeta et al. (2015) | 11 | Various antidepressants (after clonazepam was tapered off in 3 weeks) (11) (participants with IA and OCD) | 2) Various antidepressants (after clonazepam was tapered off in 3 weeks) (27) (participants with OCD only)e | India/−/IA | 52 | Ọ dịghị onye | GS (YBOCS; IAT) | NA | 3 |
Dell’Osso et al. (2008) | 17 | Escitalopram (17) | Ọ dịghị onye | USA/+/IA | 10 | Ọ dịghị onye | GS (IC-IUD-YBOCS) FR (h/w) | CO | 3 |
Han et al. (2009) | 21 | Methylphenidate (21) (Concerta) | Ọ dịghị onye | Asia/−/IGD | 8 | Ọ dịghị onye | GS (YIAS-K) FR (h/d) | CO | 3 |
Han et al. (2010) | 11 | Bupropion SR (11) | Ọ dịghị onye | Asia/−/IGD | 6 | Ọ dịghị onye | GS (YIAS) FR (h/d) | CO | 3 |
Park, Lee et al. (2016) | 86 | 1) Methylphenidate (44) | 2) Atomoxetine (42)f 10–60 mg/d | Asia/−/IGD | 12 | Ọ dịghị onye | GS (YIAS) | CO | 3 |
Song et al. (2016) | 119 | 1) Bupropion SR (44) 2) Escitalopram (42) | NT (33) | Asia/−/IGD | 6 | Ọ dịghị onye | GS (YIAS) | CO | 2 |
Combined treatments | |||||||||
Han and Renshaw (2012) | 25 | 1) Bupropion+8 sessions EDU (25) | 2) Placebo+8 sessions EDU (25)e | Asia/+/IGD | 8 | 1 | GS (YIAS) FR (h/w) | CO | 2 |
Kim et al. (2012) | 32 | 1) Bupropion+8 sessions CBT (32) | 2) Bupropion+10 min. weekly interviews (33)e | Asia/+/IGD | 8 | 1 | GS (YIAS) FR (h/w) | CO | 2 |
Li et al. (2008) | 48 | Diverse antidepressants +CBT+FT (48) | Ọ dịghị onye | Asia/+/IA | 4 | Ọ dịghị onye | GS (IRQ) | CO | 3 |
Nam et al. (2017) | 30 | 1) Bupropion+EDU (15) | 2) Escitalopram+EDU (15)f | Asia/+/IGD | 12 | Ọ dịghị onye | GS (YIAS) | CO | 2 |
Santos et al. (2016) | 39 | Mixed medications+10 sessions modified CBT (39) | Ọ dịghị onye | Brazil/+/IA | 10 | Ọ dịghị onye | GS (IAT) | CO | 3 |
Yang et al. (2005) | 18 | CBT+parent training+Fluoxetine (18) | Ọ dịghị onye | Asia/+/IA | 10.5 | Ọ dịghị onye | GS (CIUS) | CO | 3 |
Note.
aNumber of subjects included in the analysis.
bThe moderators “mode of therapy” and “mode of delivery” were applied for psychological treatments only.
cFor psychological studies, the duration of treatment was measured using the total number of hours spent in treatment for treatment (t) and control groups (c). For pharmacological and combined studies, the duration of treatment was measured using the number of weeks.
dData for the outcome variable “frequency” were available only for the treatment group.
eThe control condition was excluded from the analyses due to the incompatibility with the selection criteria.
fThe control condition was considered as a separate treatment arm.
gThe study reported data from pretreatment to follow-up only.
hThe treatment condition was excluded from the analyses due to the incompatibility with the selection criteria.
Ntọala 2.Characteristics of studies for sex addiction
Study/Year | Total Na | Treatment group (N)/Mode of therapy/Mode of deliveryb | Control group (N) Mode of therapy/Mode of deliveryb | Duration t/cc/D/A (+/−) | FU (months) | Outcomes (assessment) | Nyocha data | EPHPP |
Psychological treatments | ||||||||
Crosby (2012) | 27 | ACT (14)/I/FTFT | WL (13) | 12 / + | 5d | GS (SCS) FR (pornography viewing hours/w; modified version of the DDQ) | CO | 2 |
Hallberg et al. (2017) | 10 | CBT (10)/G/FTFT | Ọ dịghị onye | 8/− | 6 | GS (HD:CAS; HDSI) | ITT | 3 |
Hallberg et al. (2019) | 137 | CBT (70)/G/FTFT | WL (67) | 8/− | 6 | GS (HD:CAS; SCS) | ITT | 2 |
Hardy et al. (2010) | 138 | CBT (Candeo online program) (138)/I/SGT | Ọ dịghị onye | 26 / + | Ọ dịghị onye | GS (PDR) FR (pornography use/m; masturbation/m) | CO | 3 |
Hart et al. (2016) | 49 | MI (49)/G/FTFT | Ọ dịghị onye | 7 / + | 3 | GS (SCS) | CO | 3 |
Hartman et al. (2012)e | 57 | IT (program for SA and SA-SUD)/ I+G/FTFT (57) | Ọ dịghị onye | 13 / + | 6 | GS (CSBI) | CO | 3 |
Klontz et al. (2005) | 38 | 1) IT (EXPT; CBT; EDU; M-Medit.), males (28)/G/FTFT 2) IT (EXPT; CBT; EDU; M-Medit.), females (10)/G/FTFT | Ọ dịghị onye | 1) 1/+ 2) 1/+ | 6 | GS (GSBI; CGI) | CO | 3 |
Levin et al. (2017) | 11 | ACT (SHWB)(11)/I/SGT | Ọ dịghị onye | 8 / + | 1.5 | GS (CPUI) FR (pornography viewing h/w) | CO | 3 |
Minarcik (2016) | 12 | CBT (12)/I/FTFT | Ọ dịghị onye | 12 / + | Ọ dịghị onye | GS (CLAPS; HBI; SCS) FR (pornography viewing min./w) | CO | 3 |
Orzack et al. (2006) | 35 | IT (RtC; CBT; MI) (35)/G/FTFT | Ọ dịghị onye | 16 / + | Ọ dịghị onye | FR (pornography viewing/w; OTIS) | CO | 3 |
Pachankis et al. (2015) | 63 | CBT (ESTEEM-SC based on the UP) (32)/I/FTFT | WL (31) | 12 / + | 3 | GS (SCS) | ITT | 2 |
Parsons et al. (2017) | 11 | CBT (ESTEEM-SC based on the UP) (11)/I/FTFT | Ọ dịghị onye | 12 / + | Ọ dịghị onye | GS (SCS) | CO | 3 |
Quadland (1985)e | 15 | 1) GPT/G/FTFT (15) | 2) PT for participants affected by other problems/I/FTFT (14)f | 20 / + | 6 | FR (n of different sexual partners/last 3 months; % of sexual partners seen only once; % of sex with one partner; % of sex in public settings) | CO | 3 |
Sadiza et al. (2011) | 10 | CBT (10)/G/FTFT | Ọ dịghị onye | 12 / + | Ọ dịghị onye | GS (SCS) | CO | 3 |
Abụọ na Crosby (2010) | 6 | ACT (6)/I/FTFT | Ọ dịghị onye | 8 / + | 3 | FR (pornography viewing h/d) | CO | 3 |
Wilson (2010) | 54 | 1) Art therapy (27)/G/FTFT | 2) modified CBT (TCA) (27)/G/FTFTg | 1) 6/+ 2) 6/+ | 1.5 | GS (HBI-19) | CO | 2 |
Ọgwụ Farmacological | ||||||||
Kafka (1991) | 10 | Diverse antidepressants +Lithium (10) | Ọ dịghị onye | 12 / + | Ọ dịghị onye | GS (SOI) | CO | 3 |
Kafka and Prentky (1992) | 16 | Fluoxetine (16) | Ọ dịghị onye | 12 / + | Ọ dịghị onye | GS (SOI) | CO | 3 |
Kafka (1994) | 11h | Sertraline (11) | Ọ dịghị onye | 17 / + | Ọ dịghị onye | GS (SOI) FR (fantasizing, urges, sexual activities min./d) | CO | 3 |
Kafka and Hennen (2000) | 26 | Diverse antidepressants+ methylphenidate (26) | Ọ dịghị onye | 72 / + | Ọ dịghị onye | GS (TSO) FR (fantasizing, urges, sexual activities min./w) | ITT | 3 |
Wainberg et al. (2006) | 28 | Citalopram (13) | PLA (15) | 12/− | Ọ dịghị onye | GS (YBOCS-CSB; CSBI; CGI-CSB) FR (masturbation, internet use, pornography use h/w) | ITT | 2 |
Combined treatments | ||||||||
Gola and Potenza (2016) | 3 | CBT+Paroxetine (3) | Ọ dịghị onye | 10 / + | Ọ dịghị onye | FR (pornography use/w) | CO | 3 |
Scanavino et al. (2013) | 4 | STPGP+various medications (4) | Ọ dịghị onye | 16 / + | Ọ dịghị onye | GS (SCS) | CO | 3 |
Note. A = anxiety; ACT = Acceptance and Commitment Therapy; BSI = Brief Symptom Inventory; CBT = cognitive-behavioral therapy; CGI-CSB = Clinical Global Impression Scale adopted for compulsive sexual behavior; CLAPS = Clear Lake Addiction to Pornography Scale; CO = completers only; CPUI = Cyber-Pornography Use Inventory; CSBI = Compulsive Sexual Behavior Inventory; D = depression; d = day; DDQ = Daily Drinking Questionnaire; EDU = psychoeducation; EPHPP = Effective Public Health Practice Project (1 = strong, 2 = moderate, 3 = weak rating); ESTEEM = Effective Skills to Empower Effective Men; EXPT = experiential therapy; FR = frequency; FTFT = face-to-face treatment; FU = follow-up; G = group setting; GPT = group psychotherapy; GS = global severity; GSBI = Garos Sexual Beavior Inventory; h = hours; HBI = Hypersexual Behavior Inventory; HD:CAS = Hypersexual Disorder:Current Assessment Scale; HDSI = Hypersexual Disorder Screening Inventory; I = individual counseling; IT = integrative treatment; ITT = intention-to-treat; m = month; M-Medit. = mindfulness meditation; MI = Motivational Interviewing; NA = not available; OTIS = Orzack Time Intensity Survey; PDR = psychological dimensions of recovery (obsessive sexual thoughts, constructive reactions to recovery, positive affect, negative affect, perceptions of agency over the addiction, tendency to deny responsibility for the addiction, meaning in life, connection to others, feelings of being forgiven, awareness of thoughts and tempting situations, healthy pleasure outlets); PLA = placebo; PT = psychotherapy; RtC = Readiness to Change; SA = sexual addiction; SA-SUD = comorbid sexual and substance addiction; SC = sexual compulsivity; SCS = Sexual Compulsivity Scale; SGT = self-guided treatment; SHWB = self-help workbook; SOI = Sexual Outlet Inventory ; STPGP = short-term psychodynamic group psychotherapy; TCA = Task Centered Approach; TSO = Total sexual outlet; UP = Unified Protocol for the Transdiagnostic Treatment of Emotional Disorders; W = waitlist; w = week; YBOCS-CSB = Yale-Brown Obsessive Compulsive Scale modified for compulsive sexual behavior.
aNumber of subjects included in the analysis.
bThe moderators “mode of therapy” and “mode of delivery” were only applied for psychological treatments.
cThe duration of treatment was measured by using the number of weeks.
dData from pretreatment to follow-up were available only for the outcome variable “frequency”.
eThe study reported data from pretreatment to follow-up only.
fThe control condition was excluded from the analyses due to the incompatibility with the selection criteria.
gThe control condition was considered as a treatment arm.
hOnly participants diagnosed with paraphilia-related disorders were included in the analyses.
Ntọala 3.Characteristics of studies for compulsive buying
Study/Year | Total Na | Treatment group (N)/Mode of therapy/Mode of deliveryb | Control group (N) | Duration t/cc/D/A (+/−) | FU (months) | Outcomes (assessment) | Nyocha data | EPHPP |
Psychological treatments | ||||||||
Armstrong (2012) | 10 | MBSR (4)/G/FTFT | NT (6) | 8 / + | 3 | GS (CBS; YBOCS-SV; IBS) | CO | 2 |
Benson et al. (2014) | 11 | IT (CBT, PSYDYN, PSYEDU, MI, ACT, mindfulness elements) (6)/G/FTFT | WL (5) | 12 / + | 6 | GS (mod. VCBS; RCBS; CBS; YBOCS-SV) FR (min./w spent on buying; buying episodes/w)d | CO | 2 |
Filomensky & Tavares (2009) | 9 | CBT (9)/G/FTFT | Ọ dịghị onye | 20 / + | Ọ dịghị onye | GS (YBOCS-SV) | CO | 3 |
Mitchell et al. (2006) | 35 | CBT (28)/G/FTFT | WL (7) | 10 / + | 6e | GS (YBOCS-SV; CBS) FR (buying episodes/w; h spent buying/w) | ITT | 2 |
Mueller et al. (2008) | 60 | CBT (31)/G/FTFT | WL (29) | 12 / + | 6e | GS (CBS; YBOCS-SV; G-CBS) | ITT | 2 |
Mueller et al. (2013) | 56 | 1) CBT (22)/G/FTFT 2) GSH-program (CBT WB+5 telephone sessions) (20)/I/SGT | WL (14) | 1) 10/+ 2) 10/+ | 6 | GS (CBS; YBOCS-SV) | ITT | 2 |
Ọgwụ Farmacological | ||||||||
Black et al. (1997) | 10 | Fluvoxamine (10) | Ọ dịghị onye | 9/− | Ọ dịghị onye | GS (YBOCS-SV) | CO | 2 |
Black et al. (2000) | 23 | Fluvoxamine (12) | PLA (11) | 9/− | Ọ dịghị onye | GS (YBOCS-SV) | ITT | 2 |
Grant et al. (2012) | 9 | Memantine (9) | Ọ dịghị onye | 8/− | Ọ dịghị onye | GS (YBOCS-SV; mod. CB-SAS) | CO | 2 |
Koran et al. (2002) | 24 | Citalopram (24) | Ọ dịghị onye | 12 / + | Ọ dịghị onye | GS (YBOCS-SV) | ITT | 2 |
Koran et al. (2003) | 23 | Citalopram (23) | Ọ dịghị onye | 7 / + | Ọ dịghị onye | GS (YBOCS-SV; CBS; IBTS) | ITT | 2 |
Koran et al. (2007) | 26 | Escitalopram (26) | Ọ dịghị onye | 7 / + | Ọ dịghị onye | GS (YBOCS-SV) | ITT | 3 |
Ninan et al. (2000) | 37 | Fluvoxamine (20) | PLA (17) | 12 / + | Ọ dịghị onye | GS (YBOCS-SV) | ITT | 3 |
Note. A = anxiety; ACT = Acceptance and Commitment Therapy; CBS = Compulsive Buying Scale; CB-SAS = Compulsive Buying Symptom Assessment Scale (modified version of the Gambling Symptom Assessment Scale; CBT = cognitive-behavioral therapy; CO = completers only; D = depression; EPHPP = Effective Public Health Practice Project (1 = strong, 2 = moderate, 3 = weak rating); FTFT = face-to-face treatment; FR = frequency; FU = follow-up; G = group setting; G-CBS = Canadian Compulsive Buying Measurement Scale, German version; GS = global severity; GSH = guided self-help; h = hours; I = individual counseling; IBS = Impulsive Buying Scale; IBTS = Impulse Buying Tendency Scale; ITT = intention to treat analysis; MBSR = mindfulness-based stress reduction; MI = Motivational Interviewing; NA = not available; NT = no treatment; PLA = placebo control group; PSYDYN = psychodynamic; PSYEDU = psycho-educational; RCBS = Richmond Compulsive Buying Scale; SGT = self-guided treatment; VCBS = Valence Compulsive Buying Scale; WB = workbook; WL = waitlist; w = week; YBOCS-SV = Yale-Brown Obsessive Compulsive Scale-Shopping Version.
aNumber of subjects included in the analysis.
bThe moderators “mode of therapy” and “mode of delivery” were only applied for psychological treatments.
cThe duration of treatment was measured by using the number of weeks.
dData for the outcome variable “frequency” were available only for the treatment group.
eThe studies were excluded from FU analyses, because only data from posttreatment to FU were reported.
Risk of bias within studies
The global EPHPP scores for the studies included in the different addiction categories are outlined in the Tables 1–3. Validity assessment was conducted by two independent raters yielding an interrater reliability of κ = 0.73 for studies in the IA and SA categories, and κ = 0.75 for studies in the CB category.
Synthesis of results and risk of bias across studies
The pooled effect sizes for all types of addictions and treatments separately for within-group and controlled study designs on all outcomes at posttreatment and follow-up, the 95% CI, and the significance tests are outlined in Isiokwu 4. The forest plots on the within-group effect sizes for each condition, treatment, and outcome at posttreatment are presented in Fig. 2.
Ntọala 4.Effect sizes for all types of addictions, outcomes and study designs at posttreatment and at follow-up
Ihe | Type of effect | k | g | 95% CI | z | p | I2 | FS N |
Ịgba ahụ n'Intanet | ||||||||
Psychological treatments | ||||||||
Global severity | within-group (post) | 54 | 1.51 | [1.29, 1.72] | 13.79 | 93.66 | 18,317 | |
controlled (post) | 15 | 1.84 | [1.37, 2.31] | 7.268 | 83.56 | 1,254 | ||
within-group (FU) | 17 | 1.48 | [1.11, 1.85] | 7.92 | 94.61 | 4,221 | ||
Frequency | within-group (post) | 17 | 1.09 | [0.73, 1.49] | 6.02 | 92.54 | 1,801 | |
controlled (post) | 6 | 1.12 | [0.41, 1.83] | 3.08 | 78.05 | 69 | ||
within-group (FU) | 6 | 1.06 | [0.12, 2.00] | 2.21 | 97.30 | 259 | ||
Pharmacological Treatments | ||||||||
Global severity | within-group (post) | 8 | 1.13 | [0.85, 1.42] | 7.78 | 78.76 | 564 | |
controlled (post) | 2 | 1.28 | [0.85, 1.71] | 5.85 | 0.00 | -a | ||
within-group (FU) | NA | |||||||
Frequency | within-group (post) | 3 | 0.72 | [0.49, 0.96] | 6.01 | 0.00 | 27 | |
controlled (post) | NA | |||||||
within-group (FU) | NA | |||||||
Combined Treatments | ||||||||
Global severity | within-group (post) | 7 | 2.51 | [1.70, 3.33] | 6.03 | 92.99 | 756 | |
controlled (post) | NA | |||||||
within-group (FU) | 2 | 2.15 | [0.66, 3.65] | 2.82 | 93.55 | -a | ||
Frequency | within-group (post) | 2 | 2.77 | [2.29, 3.24] | 11.39 | 14.43 | -a | |
controlled (post) | NA | |||||||
within-group (FU) | 2 | 2.69 | [2.06, 3.32] | 8.43 | 49.72 | -a | ||
Mmekọahụ Mmekọahụ | ||||||||
Ọgwụ Psychology | ||||||||
Global severity | within-group (post) | 14 | 1.09 | [0.74, 1.45] | 6.03 | 92.54 | 1,311 | |
controlled (post) | 3 | 0.70 | [0.42, 0.99] | 4.87 | 7.02 | 19 | ||
within-group (FU) | 10 | 1.00 | [0.67, 1.32] | 6.02 | 90.02 | 760 | ||
Frequency | within-group (post) | 6 | 0.75 | [0.46, 1.03] | 5.10 | 70.96 | 177 | |
controlled (post) | 1 | 1.67 | [0.82, 2.53] | 3.83 | 0.00 | -a | ||
within-group (FU) | 4 | 0.83 | [0.37, 1.29] | 3.57 | 71.59 | 45 | ||
Ọgwụ Farmacological | ||||||||
Global severity | within-group (post) | 5 | 1.21 | [0.88, 1.54] | 7.12 | 50.42 | 134 | |
controlled (post) | 1 | 0.14 | [−0.58, 0.87] | 0.38 | 0.70 | 0.00 | -a | |
within-group (FU) | NA | |||||||
Frequency | within-group (post) | 3 | 0.87 | [0.63, 1.12] | 6.92 | 0.00 | 33 | |
controlled (post) | 1 | 0.79 | [0.04, 1.55] | 2.06 | 0.00 | -a | ||
within-group (FU) | NA | |||||||
Combined treatments | ||||||||
Global severity | within-group (post) | 1 | 1.91 | [0.75, 3.08] | 3.22 | 0.00 | -a | |
controlled (post) | NA | |||||||
within-group (FU) | NA | |||||||
Frequency | within-group (post) | 1 | 1.04 | [0.22,1.85] | 2.49 | 0.00 | -a | |
controlled (post) | NA | |||||||
within-group (FU) | NA | |||||||
Ịzụta mmanye | ||||||||
Psychological treatments | ||||||||
Global severity | within-group (post) | 7 | 1.00 | [0.75, 1.25] | 7.88 | 46.43 | 210 | |
controlled (post) | 6 | 0.75 | [0.42, 1.08] | 4.45 | 0.00 | 27 | ||
within-group (FU) | 4 | 1.36 | [0.88, 1.84] | 5.57 | 53.65 | 66 | ||
Frequency | within-group (post) | 2 | 0.97 | [0.68; 1.26] | 6.55 | 0.00 | -a | |
controlled (post) | 1 | 2.48 | [1.46, 3.49] | 4.76 | 0.00 | -a | ||
within-group (FU) | 1 | 1.01 | [0.47, 1.55] | 3.68 | 0.00 | -a | ||
Ọgwụ Farmacological | ||||||||
Global severity | within-group (post) | 7 | 1.52 | [1.18, 1.86] | 8.84 | 63.17 | 386 | |
controlled (post) | 2 | -0.13 | [−0.82, 0.57] | -0.35 | 0.724 | 0.00 | -a | |
within-group (FU) | 1 | -0.49 | [−1.00, 0.03] | -1.86 | 0.063 | 0.00 | -a | |
Frequency | within-group (post) | NA | ||||||
controlled (post) | NA | |||||||
within-group (FU) | NA |
Note. k = number of treatment conditions; g = Hedges’s g; CI = confidence interval; I2 = percentage of total variation across studies; FS N = Fail-safe N (number of studies needed to obtain a nonsignificant treatment effect); NA = not available.
aỌdịda-mma N was not calculated because fewer than 3 studies were available.
Effect sizes for psychological treatments at posttreatment and follow-up
Psychological treatments across addiction categories yielded short-term effect sizes ranging from medium to large in both study designs. Long-term effect sizes in all addiction categories indicated that treatment effects were maintained. As depicted in Isiokwu 4, predominantly high heterogeneity across studies was observed for the outcome variables within the IA and SA categories, and moderate heterogeneity or homogeneity was observed in the CB category.
Within the IA category, the trim-and-fill method identified 17 studies causing funnel plot asymmetry for the reduction of global severity and one study for the reduction of frequency in within-group study designs. The analyses with these filled studies suggested slightly reduced effect sizes (global severity: g = 0.87; 95% CI [0.82, 0.92]; Egger’s test p < 0.001; frequency: g = 0.93; 95% CI [0.84, 1.03]; Egger’s test p = 0.282) suggesting a nonsignificant impact of publication bias. No indication for publication bias was found for the reduction of global severity based on controlled study designs (Egger’s test p = 0.067). Within the SA category, the trim-and-fill method identified one study causing funnel plot asymmetry for the reduction of global severity leading to a slightly reduced effect size for this outcome variable (g = 0.88; 95% CI [0.79; 0.97], Egger’s test p = 0.318).Whenever fail-safe N analyses were conducted, the effect sizes across all addiction categories were considered robust for the outcome variables, except for the controlled effect size regarding the reduction of global severity in the SA and CB categories, which were not robust.
Effect sizes of pharmacological treatments at posttreatment and follow-up
At posttreatment, the within-group effect sizes across all addiction categories were medium and large. Controlled effect sizes were mainly based on single trials ranging from large in the IA category to small and negative in the SA and CB categories. The lack of follow-up data precluded the interpretation of long-term effect sizes. High and moderate heterogeneity across studies was observed for the outcome variables within the addiction categories. The fail-safe N analyses performed for the available data suggested the robustness of the effect sizes.
Effect sizes of combined treatments at posttreatment and follow-up
Combined interventions were implemented only for the treatment of IA and SA based on within-group study designs yielding large short-term effect sizes. Follow-up data were available only in the IA category producing equally large effect sizes. High heterogeneity across the studies was observed for the reduction of global severity in the IA category; however the fail-safe N indicated the robustness of the effect size.
Outlier identification through the one-study-removed procedure showed no impact of any single study on the overall effects for psychological, pharmacological, and combined treatments.
Moderator analyses
Moderator analyses were conducted for within-group effect sizes. The results for categorical variables at posttreatment are presented in Isiokwu 5.
Ntọala 5.Moderator analyses for categorical variables for all types of addictions, and outcomes
IA | SA | CB | |||||
Onye njikwa oge | Outcome variable | Qbet | p(Q) | Qbet | p(Q) | Qbet | p(Q) |
Psychological treatments | |||||||
Type of psychological treatment (CBT vs. IT vs. other) | |||||||
GS | 4.24 | 0.120 | 4.50 | 0.105 | 0.34 | 0.945 | |
FR | 0.11 | 0.947 | 15.67 | a | - | - | |
Mode of treatment (group vs. individual vs. other) | |||||||
GS | 0.47 | 0.792 | 0.11 | 0.741b | 0.44 | 0.508b | |
FR | 0.55 | 0.761 | 14.55 | b | |||
Mode of delivery (FTFT vs. SGT) | |||||||
GS | 9.15 | 0.56 | 0.453 | 0.44 | 0.508 | ||
FR | 2.03 | 0.154 | 0.76 | 0.384 | - | - | |
Comorbidity (D/A included vs. excluded) | |||||||
GS | 0.02 | 0.898 | 0.84 | 0.360 | 0.00 | 1.00 | |
FR | 1.13 | 0.289 | 0.00 | 1.00 | - | - | |
Data analysis (completer vs. ITT)c | |||||||
GS | 0.30 | 0.586 | 0.99 | 0.320 | 0.007 | 0.933 | |
FR | 0.09 | 0.771 | 0.00 | 1.00 | - | - | |
EPHPP (1 = strong vs. 2 = moderate vs. 3 = weak internal validity)d | |||||||
GS | 1.14 | 0.285 | 2.24 | 0.134 | 0.02 | 0.903 | |
FR | 1.94 | 0.164 | 0.53 | 0.466 | - | - | |
Culture (Asian vs. Western countries) | |||||||
GS | 0.54 | 0.461 | - | - | - | - | |
FR | 0.58 | 0.447 | - | - | - | - | |
IA type (global IA vs. IGD vs. other) | |||||||
GS | 1.63 | 0.653 | - | - | - | - | |
FR | 4.21 | 0.122 | - | - | - | - | |
Ọgwụ Farmacologicale | |||||||
Type of pharmacological treatment (AD vs. mixed or other) | |||||||
GS | 5.62 | f | 0.09 | 0.765 | 0.65 | 0.421g | |
Comorbidity (D/A included vs. excluded) | |||||||
GS | 0.73 | 0.392 | -h | -h | 0.22 | 0.642 | |
Data analysis (completer vs. ITT) | |||||||
GS | 0.00 | 1.00 | 0.76 | 0.383 | 4.89 | ||
EPHPP (1 = strong vs. 2 = moderate vs. 3 = weak internal validity)d | |||||||
GS | 0.47 | 0.493 | -h | -h | 2.52 | 0.112 | |
Culture (Asian vs. Western countries) | |||||||
GS | 7.32 | - | - | - | - | ||
IA type (global IA vs. IGD vs. other) | |||||||
GS | 7.32 | i | - | - | - | - | |
Combined treatmentse | |||||||
Type of pharmacological treatment (AD vs. mixed or other) | |||||||
GS | 0.83 | 0.362j | - | - | - | - | |
Type of psychological treatment (CBT vs. IT vs. other) | |||||||
GS | 20.81 | k | - | - | - | - | |
Mode of psychological treatment (group vs. individual vs. other) | |||||||
GS | 0.29 | 0.592b | - | - | - | - | |
Comorbidity (D/A included vs. excluded) | |||||||
GS | 0.00 | 1.00 | - | - | - | - | |
Data analysis (completer vs. ITT) | |||||||
GS | 0.00 | 1.00 | - | - | - | - | |
EPHPP (1 = strong vs. 2 = moderate vs. 3 = weak internal validity)d | |||||||
GS | 6.06 | - | - | - | - | ||
Culture (Asian vs. Western countries) | |||||||
GS | 0.83 | 0.362 | - | - | - | - | |
IA type (global IA vs. IGD vs. other) | |||||||
GS | 6.06 | i | - | - | - | - |
Note. A = anxiety; AD = antidepressants; CB = compulsive buying; CBT = cognitive behavioral therapy; D = depression; EPHPP = Effective Public Health Practice Project (quality assessment tool for quantitative studies); GS = global severity; FR = frequency; FTFT = face-to-face treatment; IA = internet addiction; IGD = internet gaming disorder; IT = integrative treatment; ITT = intention to treat analysis; Qbet = homogeneity statistic for differences between subgroups; SA = sex addiction; SGT = self-guided treatment.
aCBT: g = 0.98; 95% CI [0.83, 1.13]; p ≤ 0.001; IT: g = 0.25; 95% CI [−0.08, 0.58]; p = 0.132; Other treatments (i.e., acceptance and commitment therapy): g = 0.80; 95% CI [0.51, 1.10]; p ≤ 0.001.
bModerator analysis included only two subgroups (group vs. individual).
cOnly studies which indicated the type of data analysis were included in the analyses (see Isiokwu 1).
dModerator analysis included only two subgroups (2 = moderate; 3 = weak).
eModerator analyses on the outcome variable “frequency” were not conducted due to the insufficient number of studies.
fModerator analysis included only two subgroups (AD vs. other medications [i.e., methylphenidate, atomoxetine]).
gModerator analysis included only two subgroups (AD vs. other medications [i.e., memantine]).
hThe results of moderator analyses were not interpreted, because only one study remained in one of the two subgroups.
iModerator analysis included only two subgroups (IA vs. IGD).
jModerator analysis included only two subgroups (AD vs. mixed).
kModerator analysis included only two subgroups (CBT vs. other treatments [i.e., education program]).
Effect sizes across all types of addictions and interventions remained unaffected by the quality of studies, co-occurring depression and anxiety, and the year of publication (IA: global severity: β = −0.02; SE = 0.03; p = 0.417; frequency: β = −0.09; SE = 0.05; p = 0.075; SA: global severity: β = −0.03; SE = 0.04; p = 0.519).
In regards to IA, significantly larger effect sizes were found for FTFTs compared to SGTs, and for interventions including a higher number of hours in treatment for the reduction of global severity (β = 0.04; SE = 0.01; p < 0.01) and frequency (β = 0.03; SE = 0.009; p < 0.01). For the reduction of global severity in pharmacological studies, larger effect sizes emerged for antidepressants compared to other chemical agents (i.e., methylphenidate, atomoxetine), for those implemented in other countries compared to Asian countries, and examining global IA compared to IGD and smart phone addiction.
With respect to SA, CBT and other psychological treatments (i.e., acceptance and commitment therapy) showed an advantage over integrative interventions and of individual counseling over group settings for the reduction of frequency. Within the CB category, pharmacological trials using completer analyses produced larger effect sizes than those based on ITT analyses regarding the reduction of global severity.
Moderator analyses on combined treatments were conducted only for the IA category. The results demonstrated that larger effect sizes were associated with CBT-combinations, lower-quality trials, and those examining global IA.
Psychological vs. pharmacological vs. combined treatments
Regarding IA, combined treatments produced larger effect sizes compared to psychological and pharmacological interventions for the reduction of global severity (psychological vs. combined: Qn'etiti = 7.80, p < 0.01; pharmacological vs. combined: Qn'etiti = 14.69, p < 0.001), and frequency (psychological vs. combined: Qn'etiti = 8.73, p < 0.01; pharmacological vs. combined: Qn'etiti = 63.02, p < 0.001). Nonsignificant results were found between the effect sizes of pure psychological and pharmacological treatments (global severity: p = 0.173; frequency: p = 0.492). Considering CB, pharmacological treatments showed an advantage over psychological treatments for the reduction of global severity (Qn'etiti = 5.45, p < 0.05). No other significant differences between the types of treatments were observed.
Differences between the addiction categories
Comparisons of the effect sizes across the addiction categories yielded nonsignificant results with respect to psychological interventions (global severity: p = 0.174; frequency: p = 0.559) and pharmacological interventions (global severity: p = 0.203; frequency: p = 0.389).
Nkwurịta
The objective of this paper was to investigate the efficacy of psychological, pharmacological and combined treatments for IA, SA and CB and to identify possible predictors of treatment outcome. Moreover, comparisons between the three types of BAs based on the effect sizes for psychological and pharmacological treatments have been performed for the first time, with the further aim of drawing parallels to disordered gambling and SUDs in terms of treatment response.
We found that psychological treatments effectively reduced the global severity and frequency of IA and SA with the treatment response being maintained over longer periods of time. For CB, psychological treatments were also associated with a large-sized pre-post and pre-follow-up reduction in global severity. Large and moderate short-term gains in terms of both outcome variables were confirmed in controlled study designs, especially regarding IA and in individual studies in the SA and CB categories. These results are in the same range as those obtained in meta-analyses that examined psychological treatments for disordered gambling (Cowlishaw et al., 2012; Gooding & Tarrier, 2009; Goslar, Leibetseder, Muench, Hofmann, & Laireiter, 2017; Leibetseder, Laireiter, Vierhauser, & Hittenberger, 2011; Pallesen, Mitsem, Kvale, Johnsen, & Molde, 2005) and SUDs (Dutra et al., 2008; Tripodi, Bender, Litschge, & Vaughn, 2010).
Although CBT was most commonly used across the three addiction categories, a variety of other psychological approaches proved to be equally effective for reducing problematic behaviors irrespective of the mode of treatment and—particularly with regard to IA—the cultural background. These findings differ from those reported in a recent meta-analysis, which discovered an advantage of CBT over other psychological treatments for the reduction of time spent online, individual counseling, and for studies conducted in the US (Winkler et al., 2013). Discrepancies, however, may be due to the fact that moderator analyses were conducted on pooled within-group and controlled effect sizes and to the addition of the latest research results in our meta-analysis. Among these, the most commonly used approaches included family therapy, which in view of a variety of dysfunctional familial conditions (e.g., Schneider, King, & Delfabbro, 2017) appear beneficial not only for adolescent problematic internet gamers (e.g., Han, Kim, Lee, & Renshaw, 2012), but also for adolescents with SUDs (for a review see Filges, Andersen, & Jørgensen, 2018). Similarly, mindfulness based programs successfully applied for ameliorating symptoms of IA (Li, Garland, et al., 2017) and CB (Armstrong, 2012), and acceptance and commitment therapy implemented for the treatment of SA (e.g., Crosby, 2012) have proven valuable to reduce symptoms of disordered gambling and SUDs (A-tjak et al., 2015; Li, Howard, Garland, McGovern, & Lazar, 2017; Maynard, Wilson, Labuzienski, & Whiting, 2018). Integrative programs, which mostly contained CBT elements, produced equally large effect sizes across the three addiction categories, except for the reduction of the frequency of compulsive sexual behaviors. This result, however, was based on a single trial that differed from the others by utilizing the Orzack Time Inventory Survey (OTIS; Orzack, 1999) that appeared “not sufficiently inclusive” (Orzack, Voluse, Wolf, & Hennen, 2006, p. 354) to measure the frequency of maladaptive computer use. Because Orzack et al. (2006) delivered treatment in group settings, the low effect size of this study also accounted for the disadvantage of group setting compared to individual counseling underlining the importance of using reliable and valid measurement tools (see also Nko, Reid, Penberthy, Davis, & Jennings, 2014). Furthermore, treatment response appeared to be independent from the type of delivery, with one exception: IA affected individuals receiving FTFTs seemed to profit more from therapy than those included in SGTs. SGTs implemented for the treatment of IA, however, included a considerably lower number of sessions than FTFTs. Therefore, the duration rather than the type of delivery may account for these between-group differences, supporting the results of a recent meta-analysis (Goslar et al., 2017) which indicated that brief SGTs may produce lower levels of improvement than high-intensity, structured self-help programs. Evidence for this finding was provided by more intensive SGTs implemented for the treatment of SA (Hardy, Ruchty, Hull, & Hyde, 2010; Levin, Heninger, Pierce, & Twohig, 2017) and CB (Mueller, Arikian, de Zwaan, & Mitchell, 2013), yielding effect sizes comparable to those found for FTFTs. Accordingly, treatment success increased with the duration of psychotherapy, particularly with regard to the reduction of global severity and frequency of IA. A similar, but nonsignificant result was also observed for the reduction of the global severity of SA. These findings are consistent with those from Asian IA research (Chun et al., 2017), and with those gained from disordered gambling (Goslar et al., 2017; Leibetseder et al., 2011; Pallesen et al., 2005), suggesting that the manifestation of addictive behaviors requires more intensive treatment to achieve improvement.
As with psychological therapies, pharmacological treatments showed large and robust pre-post reductions in pathological symptoms across the three addiction categories. No conclusions, however, can be drawn with respect to the durability of treatment response and the short-term gains of medications over placebo due to the limited amount of data. Moreover, placebo-controlled trials conducted for the treatment of SA and CB were flawed by additional support such as regular therapist contacts including reflection about problematic behaviors (Black, Gabel, Hansen, & Schlosser, 2000; Wainberg et al., 2006) or concomitant strategies such as keeping shopping diaries (e.g., Black et al., 2000; Ninan et al., 2000) contributing to small between-group differences, and concealing the effect of chemical agents (Black et al., 2000; Ninan et al., 2000; Wainberg et al., 2006). For comparison, short-term gains of pharmacological treatments over placebo for gambling disorder were in the medium range (Goslar, Leibetseder, Muench, Hofmann, & Laireiter, 2018), similar to those reported for alcohol use disorder, and for a variety of medical diseases and mental health disorders (e.g., Jonas et al., 2014; Leucht, Hierl, Kissling, Dold, & Davis, 2012).
Moderator analyses showed no significant differences between the classes of medication, although treatment gain for the reduction of global severity for CB appeared to be overestimated due to larger effect sizes based on completers observed in two trials (Black, Monahan, & Gabel, 1997; Grant, Odlaug, Mooney, O’Brien, & Kim, 2012) compared to those obtained from ITT analyses. These trials have also determined the superiority of pharmacological over psychological treatments for the reduction of global severity supporting the use of ITT analysis, which represents a pragmatic statistical approach reflecting more realistic conditions in the context of treatments (e.g., Sedgwick, 2015). Only within the IA category, antidepressants appeared superior to other medications. A closer examination of the data, however, revealed that the subgroup with the higher treatment gain covered adult participants with comorbid depression, and obsessive-compulsive disorders treated with antidepressants, and included the trial with the largest effect size (g = 2.54; Dell'Osso et al., 2008). The subgroup with the reduced treatment gain, in turn, included adolescents with comorbid attention deficit hyperactivity disorder (ADHD) treated with psychostimulants (methylphenidate), and contained the trial with the lowest effect size examining individuals with low baseline severity of IA (g = 0.57; Han et al., 2009). These differences have also affected the moderators “culture” and “IA type”. With the two studies removed from moderator analyses, the advantage of antidepressants, and the significant results for the moderators “culture”, and “IA type” disappeared. Although treatments in both subgroups yielded beneficial results, differences appeared to be driven by single trials. Therefore, interactions between co-occurring ADHD, medication treatment, age, and culture need investigation if a higher number of studies will be available. Aside from comorbid ADHD, however, disorder-specific improvement was independent from comorbid depression and anxiety, supporting the findings from earlier IA (e.g., Han & Renshaw, 2012) and disordered gambling research (for a review see Dowling, Merkouris, & Lorains, 2016).
Across the three addiction categories, mainly serotonin selective reuptake inhibitors (SSRIs) have been examined based on high proportions of comorbid mood disorders (e.g., Kafka, 1991) and—particularly with respect to SA—the inhibitory properties of serotonin on sexual behaviors (e.g., Kafka & Prentky, 1992). Opioid antagonists (e.g., naltrexone) and glutamatergic medications (e.g., topiramate) were considered only in case studies for treating SA (e.g., Grant & Kim, 2001; Khazaal & Zullino, 2006) and CB (e.g., Ego, 2003; Guzman, Filomensky, & Tavares, 2007) demonstrating beneficial results. Because opioid antagonists and glutamatergic agents proved favorable treatment options for SUDs (Guglielmo et al., 2015; Jonas et al., 2014; Minarini et al., 2017) and disordered gambling (Bartley & Bloch, 2013; Goslar et al., 2018), these types of drugs seem promising for investigation in larger-scaled and controlled study designs, particularly in the light of high rates of comorbid SUDs observed in BAs (e.g., Grant et al., 2010).
Combined treatments for IA, especially medications in combination with CBT, produced enhanced training effects compared to pure psychological and pharmacological interventions supporting the recommendation of a recent review on IA treatment outcome studies (Przepiorka, Blachnio, Miziak, & Czuczwar, 2014). The superiority of CBT combinations over those combined with other psychological strategies was assumed to be based on a single trial yielding a very large effect size (g = 5.31; Yang, Shao, & Zheng, 2005), affecting also the moderators “quality” and “IA type”. With this study removed from subgroup analyses, however, only the advantage of CBT combinations remained significant.
Although most information was provided by IA treatment outcome studies, and data from controlled trials is still limited, psychological and pharmacological approaches showed favorable short-term effects across the three conditions, which are comparable to those applied for substance use and disordered gambling (e.g., Goslar et al., 2017; Grant et al., 2010) supporting our hypotheses. These findings are not sufficient for clarifying the classification of IA, SA and CB within the spectrum of psychiatric disorders due to missing validation of diagnostic criteria, and limited epidemiological, genetic and neurobiological data (e.g., Grant et al., 2010). However, they suggest, that individuals respond equally well to treatments irrespective of the type of addiction. These results fit well into theoretical models of addictive disorders that delineate common underlying mechanisms for both substance-related disorders and BAs (Griffiths, 2005; Jacobs, 1986; Orford, 2001; Shaffer et al., 2004), which can be modified by applying psychological and pharmacological treatments (Potenza et al., 2011). In the light of impaired prefrontal functioning and reward circuits during chronic use of drugs and behaviors (e.g., Nestler, 2005), psychological treatments, particularly CBT-based options, have the potential to alter dysfunctional cognitions and maladaptive behaviors (Kim & Hodgins, 2018), and to strengthen self-control mechanisms by targeting prefrontal brain areas (Potenza et al., 2011). Pharmacological treatments, in turn, aim at reducing craving and withdrawal symptoms by targeting the reward pathways and neurotransmitter systems (Potenza et al., 2011). Moreover, as observed for the treatment of IA, combinations of CBT and pharmacological treatments may have an additive effect, although the interactions between the two are still unclear (Potenza et al., 2011).
The following limitations should be noted: First, as is true for most meta-analytic reviews, the included studies differed in their methodological quality, although when addressed statistically, we did not observe a systematic bias in the effect sizes due to differences in the quality of the studies. None of the studies, however, achieved the highest rating reflecting limited quality of evidence with respect to selection bias and—due to the preponderance of within-group study designs—to the identification and control of confounders, and blinding. Therefore, rigorously designed RCTs are necessary, including the monitoring of additional psychosocial support and follow-up data, particularly with respect to pharmacological trials. Moreover, most IA studies included diverse behaviors acted out over the internet (e.g., online gaming, pornography viewing), although research demonstrated differences between the more general concept of IA and specific types of addictive behaviors driven by the internet (Montag et al., 2015). However, we tried to overcome this problem by grouping the studies according to the respective behavior, regardless of the medium used. With regard to co-occurring disorders, we limited moderator analyses to depression and anxiety not only due to their high prevalence among behavioral addictions (e.g., Starcevic & Khazaal, 2017), but also because these data were most clearly identifiable from the exclusion criteria of the primary studies. Since other conditions often co-occur with BAs (e.g., Grant et al., 2010), and treatment response may be influenced by the nature of comorbidity (Dowling et al., 2016), further studies are encouraged to systematically report the types and rates of co-occurring disorders in order to evaluate this information in future meta-analyses. Most studies also failed to provide information on how the diagnoses had been obtained. The mode of determining the diagnoses, however, may influence their validity (Carlbring et al., 2002; lee kwa Andersson & Titov, 2014). Future studies should therefore report whether the diagnoses were obtained by clinicians, self-report, face-to-face, or over the internet. Moreover, future studies are encouraged to directly compare the impact of treatments for individuals with BAs and SUDs in order to investigate similarities and differences between substance-related and non substance-related BAs in terms of treatment response.
Despite these limitations, the results of the present meta-analysis suggest that a variety of psychological interventions are effective for reducing symptoms of IA, especially when delivered face-to-face and conducted over an extended period of time. Although antidepressants and psychostimulants for individuals with co-occurring ADHD improved IA symptoms, CBT combined with antidepressants showed an advantage over monotherapies. Based on the current state of research, CBT and antidepressants appear efficacious for the treatment of SA and CB. Given the demand for treatment, neurobiological research should continue in order to identify parallels between substance-related disorders and possibly addictive behaviors, and to further improve the treatments for these disabling conditions (Grant et al., 2010; Potenza et al., 2011).
Isi mmalite ego
This research did not receive direct financial support from any funding agencies in the public, commercial, or not-for-profit sectors.
Ntinye aka onye odee
Martina Goslar conducted the literature search, extracted the data and performed the analyses. Papers for inclusion in the meta-analysis were screened by Martina Goslar and Max Leibetseder who also validated the data extraction. Anton-Rupert Laireiter supervised these processes. Martina Goslar and Max Leibetseder rated the validity of the studies. Hannah M. Muench supported the organization of the data and gave statistical advice. The manuscript was written by Martina Goslar with comments provided by Hannah M. Muench, Anton-Rupert Laireiter, and Stefan G. Hofmann. All authors contributed to and approved the final manuscript.
Esemokwu mmasị
Martina Goslar declares that she has no conflict of interest. Max Leibetseder declares that he has no conflict of interest. Hannah M. Muench declares that she has no conflict of interest. Dr. Hofmann receives financial support from the Alexander von Humboldt Foundation (as part of the Humboldt prize), NIH/NCCIH (R01AT007257), NIH/NIMH (R01MH099021, U01MH108168), and the James S. McDonnell Foundation 21st Century Science Initiative in Understanding Human Cognition – Special Initiative. He receives compensation for his work as editor from Springer Nature and the Association for Psychological Science, and as an advisor from the Palo Alto Health Sciences and for his work as a Subject Matter Expert from John Wiley & Sons, Inc. and SilverCloud Health, Inc. He also receives royalties and payments for his editorial work from various publishers. Anton-Rupert Laireiter declares that he has no conflict of interest.
Nkweta
The authors wish to thank Mrs Xuan Wang und Mrs Yang Zhang who translated the Chinese publications.
Formulas for the Effect Size Calculations
To compute the within-group effect sizes, the following formulas were utilized (Borenstein et al, 2005, 2009):
dị otú ahụ Y¯¯¯1 reflects the pretreatment mean, Y¯¯¯2 reflects the post-treatment mean, Siche reflects the standard deviation of the difference, and r reflects the correlation between pretreatment and posttreatment scores. Due to small sample sizes, all effect sizes were corrected for bias using Hedges’s g which was computed by multiplying d with the correction factor
dị otú ahụ df represents the degrees of freedom to estimate the within-group standard deviation. These formulas were also applied for the calculation of effect sizes from pretreatment to the latest follow-up. The controlled effect sizes were computed using the following formula:
dị otú ahụ Δ ¯¯¯¯ is the mean pre- to post-treatment change, SD is the standard deviation of post-treatment scores, n is the sample size, TREAT refers to the active treatment condition, and CONT refers to the control condition. Following Rosenthal (1991), we estimated the pre-post correlation to be r = 0.70.
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