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pISSN 2287-4208  eISSN 2287-4690
    World J Mens Health. 2018 May;36(2):161-170. English.
    Published online Sep 06, 2017.
    https://doi.org/10.5534/wjmh.17017
    Copyright © 2018 Korean Society for Sexual Medicine and Andrology
    Original Article

    Safety and Effectiveness of Once-Daily Tadalafil (5 mg) Therapy in Korean Men with Benign Prostatic Hyperplasia/Lower Urinary Tract Symptoms in a Real-World Clinical Setting: Results from a Post-Marketing Surveillance Study

    Ji Eon Won,1 Ji Yeon Chu,1 Hyunah Caroline Choi,1 Yun Chen,2 Hyun Jun Park,3 and Héctor José Dueñas4
      • 1Lilly Korea, Seoul, South Korea.
      • 2Lilly Suzhou Pharmaceutical Company, Shanghai, China.
      • 3Department of Urology, Pusan National University School of Medicine, Busan, Korea.
      • 4Eli Lilly de Mexico, Mexico City, Mexico.
    • Correspondence to: Hyun Jun Park. Department of Urology, Pusan National University Hospital, 179 Gudeok-ro, Seo-gu, Busan 49241, Korea. Tel: +82-51-240-7347, Fax: +82-51-247-5443, Email: joon501@naver.com
    Received May 17, 2017; Revised July 13, 2017; Accepted July 25, 2017.

    This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

    Abstract

    Purpose

    The aim of this study was to investigate the safety and effectiveness of tadalafil 5 mg once daily (quaque die [everyday], QD) among Korean men with benign prostatic hyperplasia (BPH)/lower urinary tract symptoms (LUTS) in a real-world clinical setting.

    Materials and Methods

    This was a single-country, prospective, observational cohort study in which patients newly prescribed tadalafil 5 mg QD for the treatment of BPH/LUTS were followed-up for 12±2 or 24±2 weeks, or to the last treatment, during post-marketing surveillance. Safety was evaluated in terms of the frequency of treatment-emergent adverse events (TEAEs) and serious adverse events (SAEs). Effectiveness was assessed by changes in the International Prostate Symptom Score (IPSS) from baseline to each endpoint.

    Results

    All patients receiving ≥1 dose of tadalafil 5 mg QD (N=637) were included in the safety population. Two percent of patients (n=13) experienced 15 TEAEs of mild (n=10; 66.7%) or moderate (n=5; 33.3%) severity. No severe TEAEs and no SAEs were reported. Effectiveness evaluations included all patients receiving tadalafil who had both baseline and endpoint observations (12-week, N=265; 24-week, N=44). Compared with baseline, the mean IPSS total score (±standard error) significantly improved by 4.7±0.3 and 6.4±0.7 points at the 12- and 24-week endpoints, respectively (p<0.0001), with significant improvements also observed on the storage, voiding, and quality of life subscores. In total, 69.1% of the patients had a clinically meaningful ≥3-point improvement in the IPSS total score.

    Conclusions

    Tadalafil 5 mg QD was well tolerated and effective in Korean men with BPH/LUTS in a real-world clinical setting.

    Keywords
    Lower urinary tract symptoms; Phosphodiesterase 5 Inhibitors; Prostatic hyperplasia; Safety; Tadalafil

    INTRODUCTION

    Lower urinary tract symptoms (LUTS) are frequently associated with benign prostatic hyperplasia (BPH). BPH/LUTS commonly includes both storage symptoms (i.e., daytime urinary frequency, urgency, and nocturia) and voiding symptoms (i.e., straining, intermittent stream, and incomplete emptying), which can negatively affect quality of life (QoL) [1, 2, 3]. BPH/LUTS is common in both Asian and non-Asian men, with higher incidence in older men [4, 5]. A current estimate indicates that the incidence of BPH/LUTS in Korea is 2105 per 100,000 men, which is predicted to rise with an increasingly aged population [5]. Often, men present with both BPH/LUTS and erectile dysfunction (ED), and the similar risk factors for these two conditions suggest shared aspects in their etiology and pathophysiology [3].

    Until recently, α-blockers and 5-α-reductase inhibitors were the primary medications prescribed for BPH/LUTS in South Korea [6, 7]. However, these treatments are not effective in all patients and are associated with side effects, including sexual dysfunction, that frequently lead to discontinuation of treatment [4, 8, 9]. The selective phosphodiesterase type 5 (PDE-5) inhibitor tadalafil (Cialis®; Eli Lilly and Company, Indianapolis, IN, USA), originally approved in South Korea as a treatment for ED, has been approved since 2012 to treat men with BPH/LUTS with or without ED [10]. The effectiveness and tolerability of tadalafil for this indication has been established in placebo-controlled clinical studies in Asian populations with BPH/LUTS [11, 12, 13, 14]. An integrated analysis of Korean populations from these studies showed that tadalafil 5 mg once daily (quaque die [everyday], QD) produced clinically meaningful improvements in voiding and storage symptoms and QoL over 12 weeks [10]. However, little is known about the safety and effectiveness of tadalafil for the treatment of BPH/LUTS in real-world clinical settings.

    The current paper reports the results of a post-marketing surveillance study conducted between May 21, 2012 and May 20, 2016 to monitor the safety and effectiveness of tadalafil 5 mg QD among Korean men with BPH/LUTS. Our results provide insights into the safety and effectiveness of this treatment in common clinical practice, including measures of patient QoL.

    MATERIALS AND METHODS

    1. Study design and patients

    This was a prospective, non-interventional, post-marketing surveillance study of Korean men being treated with tadalafil 5 mg QD for BPH/LUTS with and without ED, conducted in an ambulatory care setting. The safety population included all patients who received at least 1 dose of tadalafil 5 mg, including those who discontinued early, if safety follow-up occurred within 30 days of discontinuation. Patients were followed-up either to the last treatment (if they discontinued treatment prior to 12 weeks) or for surveillance periods of 12±2 or 24±2 weeks. The study population for the effectiveness analyses included all patients with a baseline and endpoint observation (at 12±2 or 24±2 weeks or at an early discontinuation visit).

    2. Ethics statement

    Each center's institutional review board or independent ethics committee approved this study, and all patients provided their written informed consent, in accordance with the guiding principles of the Declaration of Helsinki. Treatment for BPH was prescribed according to the usual standard of care and was not provided by the study sponsor.

    3. Inclusion and exclusion criteria

    The patients included in the study were ≥19-year-old males who had been diagnosed with BPH/LUTS with or without ED and who were newly prescribed tadalafil 5 mg QD. Patients were excluded if they had taken tadalafil 5 mg in the past, were currently receiving a combination of tadalafil 5 mg and other treatment for ED, or were simultaneously participating in a different study involving an intervention and/or investigational drug. Patients with any of the following contraindications were also excluded: use of any form of organic nitrate, hypersensitivity to tadalafil, diagnosis of hereditary degenerative retinal disorders, hereditary galactose intolerance, Lapp lactase deficiency, glucose-galactose malabsorption, non-arteritic anterior ischemic optic neuropathy, or specified cardiac and cardiovascular diseases. The decision to enroll a patient was made at the discretion of the investigator.

    4. Endpoints

    Data were reported in a case report form by investigators. The primary endpoint was to evaluate the safety of tadalafil 5 mg treatment by analyzing the incidence of treatment-emergent adverse events (TEAEs) and serious adverse events (SAEs). TEAEs were classified according to the Medical Dictionary for Regulatory Activities version 19.0, with System Organ Class and Preferred Terms as the first and second levels, respectively. The secondary end-point was to analyze treatment effectiveness. Investigators used the verified Korean-language version of the International Prostate Symptom Score (IPSS) questionnaire [15] to assess the severity of symptoms at the study baseline and at each endpoint. Each question was scored from 0 to 5 for a total IPSS range of 0 to 35 points, with higher scores representing greater severity. The storage subscore (sum of questions 2, 4, and 7), voiding subscore (sum of questions 1, 3, 5, and 6), and QoL index (score of the QoL question) were also derived. A ≥3-point improvement in total IPSS was considered clinically meaningful [16].

    Patient demographics, disease duration, BPH treatment history, BPH-relevant surgical history, comorbid diseases, previous PDE-5 inhibitor treatment, concomitant medications, and ≥22-week tadalafil use were assessed in relation to safety and effectiveness.

    5. Statistical analysis

    Descriptive statistics are presented as mean±standard deviation (SD) for continuous variables, unless otherwise indicated, and frequency and percentages are presented for categorical variables. The 95% confidence interval for TEAE incidence was calculated using the Clopper-Pearson exact method. For effectiveness analyses, changes in the IPSS score from baseline to endpoint were analyzed using the paired t-test. As the number of patients completing the 12±2-week follow-up differed from the number completing the 24±2-week follow-up, 2 separate analyses were conducted to determine the effectiveness outcomes. Differences for factors of interest were tested either by the 2-sample t-test or the Fisher exact test for categorical variables. In a sensitivity analysis, the visit windows were extended to 12±6 weeks and 24±6 weeks in order to include more patients. No imputation was applied for missing data or discontinuations. A 2-sided p-value of <0.05 was considered to indicate statistical significance. Due to the exploratory purposes of this study, the multiplicity was not adjusted. All analyses were conducted using SAS ver. 9.2 or higher (SAS Institute Inc., Cary, NC, USA).

    RESULTS

    1. Analysis populations

    A total of 637 patients were included in the safety analysis, and their baseline demographics and clinical characteristics are shown in Table 1. Of these, 265 patients were included in the 12-week effectiveness evaluation, and 44 patients were included in the 24-week surveillance effectiveness analysis (Fig. 1).

    Fig. 1
    Patient populations for the safety and effectiveness analyses. CRF: case report form.

    Table 1
    Baseline demographics and clinical characteristics of the safety population

    2. Demographics, baseline clinical characteristics, concomitant medications, and drug exposure

    The mean age of the safety population was 57.8±9.0 years (Table 1), ranging from 30 to 86 years, with 83.7% (n=533) patients aged ≥50 years and 21.5% (n=137) aged ≥65 years. The majority of patients (65.5%) had BPH/LUTS for <12 weeks prior to initiating treatment, and 18.3% had a history of PDE-5 inhibitor use (Table 1). Common comorbidities included diseases of the genitourinary (72.1%), circulatory (25.9%), and endocrine, nutritional, and metabolic systems (26.1%) (Table 1). In accordance with this, a relatively high number of patients used concomitant medications throughout the study period, the most common of which were for genitourinary system (74.1%) and cardiovascular and hematopoietic system diseases (30.7%) (Table 2). Of the patient population examined in the effectiveness analyses, 27.8% (10 of 36), 73.1% (117 of 160), and 81.2% (56 of 69) had mild (total IPSS ≤7), moderate (total IPSS 8~19), and severe (total IPSS ≥20) BPH/LUTS, respectively, at baseline. Patients received tadalafil 5 mg QD over a mean administration period (±SD) of 15.8±13.3 weeks (Table 3).

    Table 2
    Concomitant medication by medical specialty

    Table 3
    Exposure to tadalafil

    3. Safety: treatment-emergent adverse events

    Two percent of patients (n=13) experienced 15 TEAEs of mild (n=10; 66.7%) or moderate (n=5; 33.3%) severity. No severe TEAEs and no SAEs were reported. Causal relationships between TEAEs and the study medication were considered as ‘possible’ (n=8; 53.3%) or ‘unlikely’ (n=7; 46.7%) by investigators, with no TEAEs classified as ‘certain’ or ‘probable/likely’ associated with the treatment. The most frequently reported TEAEs were headache (0.5%; 3 of 637 patients, 3 events) and hot flashes (0.3%; 2 of 637patients, 2 events) (Table 4). Six patients (6 of 637; 0.9%) reported TEAEs (8 events) as the reason for abandonment at follow-up. No significant differences in the incidence of TEAEs were found when analyzed according to several factors, including age ≥65 years, disease duration, BPH treatment history, BPH-relevant surgical history, comorbid diseases, previous PDE-5 inhibitor treatment, and concomitant medication usage (Table 5). When analyzed by the total duration of tadalafil administration, TEAEs were only found in patients receiving treatment for <22 weeks (N=454) and not in those receiving treatment ≥22 weeks (N=174; p=0.0243; Table 5).

    Table 4
    TEAEs by MedDRA system organ class and preferred terms

    Table 5
    TEAEs by factors

    4. Effectiveness: International Prostate Symptom Score

    The mean IPSS scores and change from baseline were plotted for each endpoint (Fig. 2). Statistically significant changes from baseline were observed for the IPSS total score at both the 12- and 24-week endpoints, as well as for the IPSS storage subscore, voiding subscore, and QoL subscore (Fig. 2B). Regardless of baseline BPH/LUTS severity, the majority (69.1%; 183 of 265) of patients had a ≥3 score decrease in their total IPSS, which was considered a clinically meaningful improvement. The effectiveness of tadalafil was not found to be influenced by advanced age (≥65 years of age), disease duration, BPH-relevant surgical history, or previous PDE-5 inhibitor usage for either surveillance period (data not shown). Statistically significant changes were found at 12 weeks for patients with a BPH treatment history (140 of 265 vs. 125 of 265 with no history; mean change in total IPSS [±standard error, SE] −5.2±0.4 vs. −4.0±0.4, respectively; p=0.0308) and patients taking concomitant medications (179 of 265 vs. 86 of 265 not on concomitant medication; mean change in total IPSS change [±SE] −5.1±0.4 vs. −3.7±0.4, respectively; p=0.0217). The most common concomitant medications in the latter analysis were for genitourinary (140 of 179), cardiovascular and hematopoietic (54 of 179), and gastrointestinal and hepatobiliary system (35 of 179) disorders. Further, patients receiving treatment for ≥ 22 weeks (113 of 264) showed a greater improvement in the total IPSS than those in the <22 weeks group (151 of 264) (mean change in total IPSS [±SE] −6.0±0.5 vs. −3.7±0.3, respectively; p<0.0001). Significantly greater improvements in symptoms were also found at the 24-week endpoint for those patients with a comorbidity (38 of 44 vs 6 of 44 without a comorbidity; mean change in total IPSS [±SE] −7.0±0.7 vs. −2.5±0.9, respectively; p=0.0154), with the comorbidities primarily comprising genitourinary diseases (31 of 44). In the sensitivity analysis (endpoints ±6 weeks), statistically significant changes in the IPSS total score and subscores were observed at both endpoints, consistent with the original analyses (data not shown).

    Fig. 2
    Change in IPSS scores as a measure of treatment effectiveness. (A) Mean IPSS total score and subscores for the 12-week (N=265) and 24-week surveillance groups (N=44). Mean±SD is shown. (B) Mean change from baseline on all IPSS scores. Error bars represent±SE. ***p<0.0001. IPSS: International Prostate Symptom Score, SD: standard deviation, QoL: quality of life, SE: standard error.

    DISCUSSION

    This study demonstrates that tadalafil 5 mg QD for the treatment of BPH/LUTS had favorable safety and effectiveness in a real-world clinical setting. A relatively low number of mild to moderate TEAEs were reported, with their incidence not significantly associated with any baseline parameter. In contrast to other drug therapies available in South Korea for BPH/LUTS, such as α-blockers and 5-α-reductase inhibitors [7, 17], none of the TEAEs were associated with sexual dysfunction, supporting results from previous clinical studies [11, 12, 13, 14, 18, 19, 20, 21]. Currently, tadalafil is the only drug available in South Korea for the treatment of both BPH/LUTS and ED that is not associated with sexual dysfunction side effects, and it is the only daily treatment approved for BPH/LUTS [17]. Interestingly, TEAEs were reported only by patients receiving treatment for <22 weeks and not by those receiving ≥22 weeks of treatment. This suggests that tadalafil use for ≥22 weeks may be well tolerated; however, this finding is confounded by the fact that the <22-week group contained a greater proportion of the safety population than the ≥22-week group.

    In terms of effectiveness, both the general population and patients aged ≥65 years showed significant improvements in the total IPSS, IPSS subscores, and the QoL index, which were sustained in the 24-week surveillance group. The current data indicate that a prior history of BPH treatment and concomitant medication usage at the 12-week endpoint and comorbidity at the 24-week endpoint may be favorably associated with tadalafil-mediated improvement of BPH/LUTS. Since the concomitant medications and comorbidities were largely related to urogenital disorders, these findings are not surprising given the known or suspected broad actions of tadalafil across the lower urinary tract (e.g., vasodilation, anti-inflammatory, and antiproliferative actions) [4, 8, 22]. However, due to the relatively small study populations, particularly in the 24-week analyses (largely due to many study sites [22 of 29] opting not to participate in the longer surveillance period), the clinical relevance of these findings is not yet clear.

    Due to the inherently observational nature of post-marketing surveillance studies, additional limitations on the interpretation of the current data exist. Notably, the study lacked parallel control and comparator groups within the same study cohort, and the safety and effectiveness outcomes of tadalafil 5 mg QD could only be determined based on the change from baseline for each patient. However, the safety and effectiveness demonstrated for tadalafil 5 mg QD treatment in this BPH/LUTS Korean patient population is consistent with that observed in previous randomized, placebo-controlled clinical studies investigating 12-week tadalafil 5 mg treatment in Asian [11, 12, 13, 14] and Caucasian [18, 19, 20, 21] populations with BPH/LUTS. A series of analyses integrating the data pooled from different subsets of these clinical trials consistently found that tadalafil 5 mg QD progressively and significantly improved IPSS total scores over 12 weeks compared to placebo, simultaneously improving ED, with no serious safety concerns [10, 22, 23, 24]. In the future, larger studies are desirable in order to determine the potential influences of specific additional BPH medications (e.g., α-blockers and 5-α-reductase inhibitors) and other functional bladder diseases (e.g., neurogenic bladder and overactive bladder) on the effectiveness of tadalafil.

    CONCLUSIONS

    This study adds to the existing data on tadalafil 5 mg QD for the treatment of BPH/LUTS, demonstrating that the favorable safety and effectiveness observed in clinical studies for tadalafil extends to a real-world clinical setting. Further, this study reinforces the data on tadalafil 5 mg QD as a safe and effective treatment for the management of patients with BPH/LUTS with and without ED as a comorbidity.

    Notes

    Disclosure:The authors have no potential conflicts of interest to disclose.

    Author Contribution:Research conception & design: Won JE, Chu JY, Choi HC, Chen Y, Park HJ, Dueñas HJ. Performing the experiments: Won JE, Choi HC, Park HJ. Data acquisition: Chu JY, Choi HC, Chen Y, Dueñas HJ. Data analysis and interpretation: Choi HC, Chen Y, Dueñas HJ. Statistical analysis: Choi HC, Chen Y, Dueñas HJ. Drafting of the manuscript: Choi HC, Chen Y, Dueñas HJ. Critical revision of the manuscript: Won JE, Chu JY, Choi HC, Park HJ. Approval of final manuscript: all authors.

    ACKNOWLEDGEMENTS

    We thank the patients, their families, the study sites, and the study personnel who participated in this post-marketing surveillance study. This study and production of this manuscript were sponsored by Eli Lilly and Company. Medical writing (Marissa Philpott, Prudence Stanford, and Kaye Stenvers) and editorial support (Antonia Baldo and Teri Tucker) was provided by inVentiv Health Clinical and funded by Eli Lilly and Company.

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    MeSH Terms
    Cohort Studies
    Humans
    Lower Urinary Tract Symptoms
    Male
    Phosphodiesterase 5 Inhibitors
    Prospective Studies
    Prostate
    Prostatic Hyperplasia
    Quality of Life
    Tadalafil*
    Urinary Tract*
    Metrics
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