The present systematic review of randomized controlled trials (RCTs) was performed using the Preferred Reporting Items for Systematic Reviews and Meta-analyses checklist (14).

The MEDLINE (January 1992 to December 2018), EMBASE (January 1995 to December 2018) and the Cochrane controlled trials register databases were searched to compare the effects of dutasteride and finasteride in BPH treatment. The following search terms were used: [‘finasteride’ (MeSH terms) OR ‘finasteride’ (all fields)] AND [‘dutasteride’ (MeSH terms) OR ‘dutasteride’ (all fields)] AND [‘prostatic hyperplasia’ (MeSH terms) OR [‘prostatic’ (all fields) AND ‘hyperplasia’ (all fields)] OR ‘prostatic hyperplasia’ (all fields) OR [‘benign’ (all fields) AND ‘prostatic’ (all fields) AND ‘hyperplasia’ (all fields)] OR ‘benign prostatic hyperplasia’ (all fields). All publications were browsed independently by all authors. The study was limited to published research with no restrictions on language. Reviews and summaries presented at meetings were excluded. Authors were contacted to obtain further information when necessary. The references of relevant publications were also searched.

The inclusion criteria for the publications were as follows: i) Dutasteride vs. finasteride in treating BPH were evaluated; ii) the content and associated data of the publication were available; iii) the data provided by the publication were valid and valuable, including the overall number of events and valuable results for each indicator; iv) the design of the study was that of an RCT; v) the treatment duration was ≥6 months. If the results of a trial were published by two or more studies, the latest publication was selected. However, if a group of patients was included in two or more studies, each of the studies may have been analyzed in the present study. It was also checked whether the cohorts overlapped and no overlaps were found. The flow diagram of the study selection and elimination is presented in Fig. 1.

The quality of the studies selected was evaluated using the Jadad scale (15). In addition, a number of strategies of assessment were applied to determine the quality of individual studies, including the distribution method of participants, blinding regarding the distribution process, double-blinding and the number of patients lost at follow-up. Subsequently, individual studies were assessed following the principles derived from the Cochrane Handbook for Systematic Reviews of Interventions v5.10(16). Each publication was evaluated and three quality classification standards were assigned: a) When a study satisfied the majority of the quality criteria, it was considered to have a low probability of bias; b) when the quality criteria were partially satisfied or unclear, the study was considered to have a moderate probability of bias; and c) when the criteria were barely satisfied, the study was considered to have a high probability of bias. All authors participated in the quality assessment of the RCTs retrieved and eventually agreed with the results of the assessment. All reviewers independently assessed whether each study satisfied the criteria and extracted the data from the selected studies. Any discrepancies were recorded, discussed and settled by negotiation.

Two authors independently collected data from the publications based on predetermined criteria. The following usable data were extracted from the studies included: i) Publication year; ii) the first author's name; iii) details on patient treatment; iv) number of participants; and v) international prostate symptom score (IPSS), prostate volume (PV), maximum urine flow rate (Qmax), post-void residual volume (PVRV), prostate-specific antigen (PSA), adverse events (AEs), decreased libido and impotence. These results were considered clinically significant as their impact on patients was measurable. No ethical approval was required for this study.

The primary outcomes were IPSS and PSA. High IPSS indicated more severe symptoms. Data on secondary outcomes, including PV, Qmax and PVRV were reported with acceptable consistency among the studies to allow for analysis. In addition, the number of any AEs, decreased libido and impotence were also analyzed between the two groups of patients receiving different treatments.

The analysis of the study was performed using RevMan version 5.3.0 (Cochrane Collaboration) (16). Fixed or random-effects models were used to evaluate the publications. The mean difference (MD) was used to analyze continuous data and the odds ratio (OR) was calculated for dichotomous results with the corresponding 95% CI (17). The results of analysis showed that the P-value >0.05 for the I² statistic, the study was considered to be homogeneous and the fixed-effects model was used for the analysis. Inconsistency was analyzed by the I² statistic, which reflected the proportion of heterogeneity across trials. A random-effects model was used for studies with an I² value >50%, suggesting significant heterogeneity. P<0.05 was considered to indicate a statistically significant difference.

A total of 240 publications were initially retrieved from the databases. Scrutinizing their abstracts and titles resulted in the exclusion of 204 publications. Among the remaining 36 studies, 29 were excluded due to a lack of effective data. In addition, two publications described the same data and one of these publications was excluded. Finally, six publications describing six RCTs (18-23) were included in the present study to compare the effects of dutasteride and finasteride in treating BPH during a treatment period of ≥6 months. The basic features of the six studies are presented in Table I.

All studies included in the meta-analysis were RCTs; however, not all of the studies specified the protocol of randomization. All studies included an appropriate number of participants and one study included an intention-to-treat analysis (21) (Table II). In addition, two studies used a combined medication regimen with α-blockers (19,20) and one study described a post-operative medication regimen (23). However, in these studies, the specific methods of blinding were not explicitly explained and their grade were rated as ‘B’ based on the Cochrane handbook. The plot was highly symmetrical and six squares were contained in the accepted region of the funnel plot, with no evidence of bias being found (Fig. 2). The bias of quality assessment are presented in Fig. 3.

A total of five RCTs including 1,929 patients were used for the IPSS analysis. High heterogeneity among the trials was identified (P<0.00001; I²=88%). The forest plots indicated a significantly greater decrease in IPSS in the dutasteride group compared with that in the finasteride group (MD, -0.86; 95% CI, -1.62 to -0.11; P=0.02; Fig. 4A).

A total of five RCTs including 1,929 patients were used for the analysis of the change of PV. High heterogeneity was identified among the studies in the forest plots (P<0.0001; I²=83%). Dutasteride was not significantly more effective compared with finasteride in reducing the PV (MD, -0.40; 95% CI, -2.11 to 1.30; P=0.64; Fig. 4B).

A total of three RCTs including 1,747 patients contained data on Qmax. Low risk of heterogeneity was identified among the studies (P=0.23; I²=31%). The fixed-effects model demonstrated no significant differences between dutasteride and finasteride in improving the Qmax (MD, 0.16; 95% CI, -0.13 to 0.45; P=0.29; Fig. 4C).

A total of three RCTs including 222 patients were used for the analysis of PVRV. The results of the heterogeneity test were P=0.58 and I²=0%. The fixed-effects model did not identify any statistically significant differences between dutasteride and finasteride in reducing PVRV (MD, -1.92; 95% CI, -4.45 to 0.61; P=0.14; Fig. 5A).

A total of five RCTs including 1,929 patients contained data on PSA. Heterogeneity was identified among the studies (P=0.0008; I²=79%). Dutasteride was significantly more effective compared with finasteride in lowering PSA (MD, -0.13; 95% CI, -0.26 to -0.01; P=0.03; Fig. 5B).

A total of five RCTs with a sample of 1,964 participants evaluated the severity of any AE. The results of the heterogeneity test were P=0.84 and I²=0%. The meta-analysis identified no significant differences between the dutasteride and finasteride groups in the severity of any AE across the five studies (OR, 0.96; 95% CI, 0.80 to 1.15; P=0.66; Fig. 6A).

A total of four RCTs with a sample of 1,919 participants assessed the severity of decreased libido. The results of the heterogeneity test were P=0.93 and I²=0%. The fixed-effects model identified no significant differences between the dutasteride and finasteride groups in the severity of decreased libido among the four studies (OR, 0.85; 95% CI, 0.58 to 1.24; P=0.39; Fig. 6B).

A total of four RCTs with a suitable sample of 1,919 participants analyzed the severity of impotence. The results of the heterogeneity test were P=0.82 and I²=0%. The fixed-effects model identified no statistically significant differences between the dutasteride and finasteride groups in the severity of impotence among the four studies (OR, 0.79; 95% CI, 0.57 to 1.10; P=0.17; Fig. 6C).