Effectiveness and durability of solifenacin versus percutaneous tibial nerve stimulation versus their combination for the treatment of women with overactive bladder syndrome: a randomized controlled study with a follow-up of ten months

Vecchioli-Scaldazza, Carlo; Morosetti, Carolina

doi:10.1590/S1677-5538.IBJU.2016.0611

ABSTRACT

Purpose

To assess effectiveness and durability of Solifenacin (SS) versus tibial nerve stimulation (PTNS) versus combination therapy (PTNS + SS) in women with overactive bladder syndrome (OAB).

Materials and Methods

105 women with OAB were divided randomly into three groups of 35 patients each. In group A women received SS, in group B women underwent PTNS, in group C women underwent combination of PTNS + SS. Improvements in OAB symptoms were assessed with OABSS questionnaire; patients’ quality of life was assessed with OAB-q SF questionnaire. Evaluation of effectiveness of treatments was performed with PGI-I questionnaire. OABSS and PGI-I were also assessed monthly for ten months.

Results

All treatments were effective on symptoms. PTNS showed a greater effectiveness than SS, but PTNS + SS was more effective than SS and PTNS. Furthermore, PTNS + SS showed a greater duration of effectiveness than PTNS and SS.

Conclusions

Combination of PTNS with SS showed more effectiveness and more durability than PTNS and SS alone.

Keywords
Urinary Bladder; Overactive; Combined Modality Therapy; Solifenacin Succinate

INTRODUCTION

Overactive bladder syndrome (OAB) is a chronic disease characterized by urinary urgency with or without urge incontinence, frequency and nocturia (¹1. Abrams P, Cardozo L, Fall M, Griffiths D, Rosier P, Ulmsten U, et al. The standardisation of terminology of lower urinary tract function: report from the Standardisation Sub-committee of the International Continence Society. Neurourol Urodyn. 2002;21:167-78.) with huge economic burden and detrimental effects on the quality of life of patients (²2. Irwin DE, Milsom I, Hunskaar S, Reilly K, Kopp Z, Herschorn S, et al. Population-based survey of urinary incontinence, overactive bladder, and other lower urinary tract symptoms in five countries: results of the EPIC study. Eur Urol. 2006;50:1306-14.). The prevalence of OAB in women increases with age and is present in approximately 30% of women over the age of 65 years (³3. Stewart WF, Van Rooyen JB, Cundiff GW, Abrams P, Herzog AR, Corey R, et al. Prevalence and burden of overactive bladder in the United States. World J Urol. 2003;20:327-36.) and in the general population it is estimated at 11.8% (⁴4. Irwin DE, Abrams P, Milsom I, Kopp Z, Reilly K; EPIC Study Group. Understanding the elements of overactive bladder: questions raised by the EPIC study. BJU Int. 2008;101:1381-7.). Antimuscarinic agents represent the therapy of choice for the management of OAB, when the conservative treatment is ineffective, but although a long-lasting therapy is required to obtain better control of symptoms, a high percentage of patients discontinue the treatment after a few months (⁵5. Andersson KE, Chapple CR, Cardozo L, Cruz F, Hashim H, Michel MC, et al. Pharmacological treatment of overactive bladder: report from the International Consultation on Incontinence. Curr Opin Urol. 2009;19:380-94., ⁶6. Yu YF, Nichol MB, Yu AP, Ahn J. Persistence and adherence of medications for chronic overactive bladder/urinary incontinence in the california medicaid program. Value Health. 2005;8:495-505.). After failure of a single drug, most practitioners try a different pharmacological treatment and if this second option also fails, more invasive options are considered (⁷7. Bolduc S, Moore K, Lebel S, Lamontagne P, Hamel M. Double anticholinergic therapy for refractory overactive bladder. J Urol. 2009;182(4 Suppl):2033-8.). In recent years several studies have shown that a combination of two different anticholinergic or one anticholinergic combined with the β3-adrenoceptor agonist Mirabegron may improve efficacy in the treatment of OAB symptoms while also reducing the side effects (⁸8. Abrams P, Kelleher C, Staskin D, Rechberger T, Kay R, Martina R, et al. Combination treatment with mirabegron and solifenacin in patients with overactive bladder: efficacy and safety results from a randomised, double-blind, dose-ranging, phase 2 study (Symphony). Eur Urol. 2015;67:577-88.). Furthermore, although the available data does not allow definitive evaluation (⁹9. Rai BP, Cody JD, Alhasso A, Stewart L. Anticholinergic drugs versus non-drug active therapies for non-neurogenic overactive bladder syndrome in adults. Cochrane Database Syst Rev. 2012, 12;12:CD003193.), promising results were observed with an anticholinergic combined with bladder training, electric stimulation or percutaneous tibial nerve stimulation (¹⁰10. Mattiasson A, Blaakaer J, Høye K, Wein AJ; Tolterodine Scandinavian Study Group. Simplified bladder training augments the effectiveness of tolterodine in patients with an overactive bladder. BJU Int. 2003;91:54-60.

11. Souto SC, Reis LO, Palma T, Palma P, Denardi F. Prospective and randomized comparison of electrical stimulation of the posterior tibial nerve versus oxybutynin versus their combination for treatment of women with overactive bladder syndrome. World J Urol. 2014;32:179-84.-¹²12. Kizilyel S, Karakeçi A, Ozan T, Ünüş İ, Barut O, Onur R. Role of percutaneous posterior tibial nerve stimulation either alone or combined with na anticholinergic agent in treating patients with overactive bladder. Turk J Urol. 2015;41:208-14.). The aim of this study was to assess the efficacy and the long term durability of Solifenacin (SS) and percutaneous tibial nerve stimulation (PTNS) administered alone or in combination in the treatment of women with OAB syndrome.

MATERIALS AND METHODS

From May 2015 to December 2015, 105 consecutive women (mean age 61 years, range 41-73) with symptoms of overactive bladder (urgency, urinary frequency, with or without urge incontinence) were enrolled in this prospective, randomized, controlled study. Women were divided randomly into three groups of 35 patients each using online randomization (Graph Pad Quick Calcs software: http://www.graphad.com/quickcalcs/randomize1) by an independent biostatistician who was unaware of treatments performed by patients and was not involved in the study. In group-A, women received Solifenacin Succinate (SS) 5mg once a day for 12 weeks. In Group-B, women underwent PTNS once a week for 30 min each for a total of 12 weeks. In Group-C, patients underwent PTNS once a week for 30 min each for a total of 8 weeks and SS 5mg on alternate days also for 8 weeks (short-low dose therapy). The treatment was performed with a 34-gauge needle electrode inserted 6-8 centimeters cephalad to the medial malleolus and slightly posterior to the tibia. The electrode was connected to the Urgent PC stimulator and a current level of 0.5 to 9mA at 20Hz was selected based on patient sensory and motor response. Patients with urinary tract infection, neurological disease, bladder lithiasis, genital prolapse higher than stage II on POP-Q system, uncontrolled narrow angle glaucoma, pelvic tumours, post void residual urine ≥100mL, previously treated with radiation therapy, antimuscarinic agents, antidepressants and antianxiety agents, were excluded.

Endpoints

Improvements in OAB symptoms, including day time frequency, night time frequency, urgency and urge incontinence were considered the primary efficacy end point. The impact of OAB symptoms on patient's quality of life (QoL) and the patient impression of improvement were considered the secondary end point. The primary efficacy end point was evaluated with Overactive Bladder Symptom Score (OABSS) questionnaire. It consists of 4 items related to OAB syndrome symptoms. The score of the first item (day time frequency) ranges from 0 to 2; the score of the second item (night time frequency) ranges from 0 to 3; the scores of the third and fourth items (urgency and urge incontinence respectively) range from 0 to 5. A greater score represents worsening of symptoms. The secondary end point was assessed with the Overactive Bladder questionnaire Short Form (OAB-q SF). The questionnaire consists of 6 items related to symptoms with 6 possible options ranging from “not at all” (score 1) to “a very great deal” (score 6), and a health-related quality of life scale with 13 items, with 6 response options ranging from “none of the time” (score 1) to “all of the time” (score 6). Improvement was evaluated with the Patient Global Impression of Improvement questionnaire (PGI-I). The PGI-I is a validated generic tool for assessment of the overall improvement or deterioration that patients experience following the treatment. It is a 7-point scale from “very much improved” (score 1), to “very much worse” (score 7). OABSS and PGI-I were performed before, at the end of each treatment and thereafter every month with a maximum follow-up of 10 months. OAB-q SF was performed before and after treatment. The study was conducted in accordance with the ethical principles of the Declaration of Helsinki and the protocol was approved by the local ethics committee. All patients signed informed consent before starting treatment. The results were assessed by a researcher blinded to treatment performed by patients.

Statistical analysis

Statistical analysis was performed using the MedCalc software (version 12.7.7). Data in each group was assessed by D'Agostino-Pearson test. After having checked the normal distribution, data was processed using parametric tests: paired sample t test or independent sample t test. If normality was rejected, data was processed using non-parametric tests: Wilcoxon test for paired sample and Mann-Whitney for independent sample. Data was expressed as means±SD. A p value <0.05 was considered significant.

RESULTS

Of the 35 women initially enrolled in group A, 8 patients suspended therapy because of side effects (dry mouth, constipation); therefore, 27 patients (mean age 62 years, range 41-70) were evaluable for the study. In Group-B, only one woman suspended therapy before the end of treatment without a specific reason; therefore. 34 patients (mean age 60 years, range 45-73) were evaluable for the study. In Group-C, two women suspended therapy: one because of side effects and one without a specific reason; therefore, 33 patients (mean age 63 years, range 43-72) were evaluable. Improvements with statistically significant differences were found in all the items assessed with OABSS questionnaire in the three groups of patients: day time frequency, night time frequency, urgency and urge incontinence (Table-1). No statistical difference was found between SS versus PTNS in daily and night time micturition, whereas a significant difference was found between combination therapy versus SS (P value: 0.0167). No significant difference was found between SS versus PTNS in urgency and urge incontinence, whereas significant differences were found in those items between the group of patients who underwent combination therapy and women treated with SS and women treated with PTNS (P values: 0.0005; 0.0225 and 0.0003; 0.0015 respectively) (Table-1). Significant improvements in quality of life of patients (OAB-q SF, 6 and 13 items) were found after treatment in all groups evaluated. However, no significant difference was found between SS versus PTNS, but combination therapy showed statistically significant differences both versus SS and versus PTNS (P values: 0.0168; 0.0287 and 0.0049; 0.0561 respectively) (Table-2). Improvements in PGI-I assessed at the end of treatment were found in all groups of patients. In any case, no significance was found between SS versus PTNS, whereas combination therapy showed significant improvements both versus SS and versus PTNS (P values: 0.0017; 0.0468 respectively). Evaluation of long term durability showed persistence of improvements of SS, PTNS and combination therapy assessed with OABSS questionnaire, respectively for 0.9, 2.5 and 5.9 months; the persistence of the improvements assessed with PGI-I questionnaire was respectively 0.7, 2.1, 5.6 months (Table-3). Statistical analysis showed a significant difference respectively in PTNS versus SS, in combination therapy versus SS and versus PTNS (p values: 0.0039; <0.0001; 0.0009 respectively) (Table-3).

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Table 1
OAB symptoms assessed with OABSS questionnaire in patients treated with Solifenacin (SS), Percutaneous Tibial Nerve Stimulation (PTNS) and Solifenacin + Percutaneous Tibial Nerve Stimulation (SS + PTNS) at the end of treatment.

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Table 2
Improvements assessed with Quality of Life questionnaire (6 and 13 items) (OAB-q SF 6 and 13) and Patient Global Impression of Improvement questionnaire (PGI-I) at the end of treatment.

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Table 3
Persistence of improvements in months, assessed with Overactive Bladder Symptoms Score (OAB-SS) and Patient Global Impression of Improvement (PGI-I) questionnaire (follow-up of 10 months).

DISCUSSION

The study showed a significant effectiveness with improvement in all parameters evaluated with OABSS questionnaire at the end of treatment, with all the treatments performed. Combination therapy was always statistically more effective than SS and it showed a significant improvement in urgency and urge incontinence, also when compared to PTNS. Improvement in women’ quality of life was observed in all groups assessed. However, combination therapy was statistically more effective than SS and PTNS. PGI-I evaluated at the end of the treatments showed an increase in perception of improvement in all groups of women. However, combination therapy was statistically more effective compared to SS and PTNS. We considered this PTNS + SS combination therapy, a short low dose treatment. The therapy was short due to the number of PTNS treatments performed (8 treatments instead of the usual 12) and the therapy was low dose due to the administration of SS on alternate days for 8 weeks. In addition to its effectiveness, this therapeutic scheme was developed to obtain a greater adherence especially in regard to a reduction in side effects and cost.

Studies performed on combination therapy in patients with OAB showed its effectiveness without demonstrating an increase in side effects: Bolduc et al., Kosilov et al. (⁷7. Bolduc S, Moore K, Lebel S, Lamontagne P, Hamel M. Double anticholinergic therapy for refractory overactive bladder. J Urol. 2009;182(4 Suppl):2033-8., ¹³13. Kosilov KV, Loparev SA, Ivanovskaya MA, Kosilova LV. Comparative effectiveness of combined low- and standarddose trospium and solifenacin for moderate overactive bladder symptoms in elderly men and women. Urol Int. 2014;93:470-3.), assessed combination of two anticholinergic drugs; Abrams et al. (⁸8. Abrams P, Kelleher C, Staskin D, Rechberger T, Kay R, Martina R, et al. Combination treatment with mirabegron and solifenacin in patients with overactive bladder: efficacy and safety results from a randomised, double-blind, dose-ranging, phase 2 study (Symphony). Eur Urol. 2015;67:577-88.) assessed the combination of an anticholinergic with the β3-adrenoceptor agonist Mirabegron. Mattiasson et al. (¹⁰10. Mattiasson A, Blaakaer J, Høye K, Wein AJ; Tolterodine Scandinavian Study Group. Simplified bladder training augments the effectiveness of tolterodine in patients with an overactive bladder. BJU Int. 2003;91:54-60.) combined tolterodine with simplified bladder training with an improvement on voiding frequency and voided volume; Curran et al. (¹⁴14. Curran MJ, Kaefer M, Peters C, Logigian E, Bauer SB. The overactive bladder in childhood: long-term results with conservative management. J Urol. 2000;163:574-7.) achieved better results by combining anticholinergic with behavioural modifications; Souto et al., Kikilyel et al. (¹¹11. Souto SC, Reis LO, Palma T, Palma P, Denardi F. Prospective and randomized comparison of electrical stimulation of the posterior tibial nerve versus oxybutynin versus their combination for treatment of women with overactive bladder syndrome. World J Urol. 2014;32:179-84., ¹²12. Kizilyel S, Karakeçi A, Ozan T, Ünüş İ, Barut O, Onur R. Role of percutaneous posterior tibial nerve stimulation either alone or combined with na anticholinergic agent in treating patients with overactive bladder. Turk J Urol. 2015;41:208-14.), assessed combination of electrical stimulations of the posterior tibial nerve versus respectively, oxybutinin and tolterodine. Amend et al. (¹⁵15. Amend B, Hennenlotter J, Schäfer T, Horstmann M, Stenzl A, Sievert KD. Effective treatment of neurogenic detrusor dysfunction by combined high-dosed antimuscarinics without increased side-effects. Eur Urol. 2008;53:1021-8.) and Abrams et al. (⁸8. Abrams P, Kelleher C, Staskin D, Rechberger T, Kay R, Martina R, et al. Combination treatment with mirabegron and solifenacin in patients with overactive bladder: efficacy and safety results from a randomised, double-blind, dose-ranging, phase 2 study (Symphony). Eur Urol. 2015;67:577-88.) explained the success respectively of the combination of two anticholinergic drugs and of an anticholinergic with the β3-adrenoceptor agonist Mirabegron, by different receptor selectivity and by receptor interaction on different bladder wall regions. Improvements observed with the combination of PTNS with SS in this study can be explained by the blocking of muscarinic receptors that are responsible for vesical contractions caused by Solifenacine and by the effect of neuromodulation. The mechanism of bladder neuromodulation, although not completely clear, is different from that of drugs: its effect is possibly mediated through a combination of increasing cerebral endorphins, stimulation of somatic sacral and lumbar afferent fibers, and activation of efferent fibers to the striated urethral sphincter. The result of this possible mechanism is the inhibition of detrusor activity (¹⁶16. Groen J, Bosch JL. Neuromodulation techniques in the treatment of the overactive bladder. BJU Int. 2001;87:723-31.). The synergic effect of the combination therapy makes it possible to decrease the dose of each drug delivering an improved tolerability profile compared with monotherapy without compromising efficacy (¹³13. Kosilov KV, Loparev SA, Ivanovskaya MA, Kosilova LV. Comparative effectiveness of combined low- and standarddose trospium and solifenacin for moderate overactive bladder symptoms in elderly men and women. Urol Int. 2014;93:470-3.

14. Curran MJ, Kaefer M, Peters C, Logigian E, Bauer SB. The overactive bladder in childhood: long-term results with conservative management. J Urol. 2000;163:574-7.

15. Amend B, Hennenlotter J, Schäfer T, Horstmann M, Stenzl A, Sievert KD. Effective treatment of neurogenic detrusor dysfunction by combined high-dosed antimuscarinics without increased side-effects. Eur Urol. 2008;53:1021-8.

16. Groen J, Bosch JL. Neuromodulation techniques in the treatment of the overactive bladder. BJU Int. 2001;87:723-31.

17. MacDiarmid SA, Peters KM, Shobeiri SA, Wooldridge LS, Rovner ES, Leong FC, et al. Long-term durability of percutaneous tibial nerve stimulation for the treatment of overactive bladder. J Urol. 2010;183:234-40.-⁸8. Abrams P, Kelleher C, Staskin D, Rechberger T, Kay R, Martina R, et al. Combination treatment with mirabegron and solifenacin in patients with overactive bladder: efficacy and safety results from a randomised, double-blind, dose-ranging, phase 2 study (Symphony). Eur Urol. 2015;67:577-88.) with a greater adherence by the patient to therapy allowing its use even in elderly patients (⁸8. Abrams P, Kelleher C, Staskin D, Rechberger T, Kay R, Martina R, et al. Combination treatment with mirabegron and solifenacin in patients with overactive bladder: efficacy and safety results from a randomised, double-blind, dose-ranging, phase 2 study (Symphony). Eur Urol. 2015;67:577-88.). In this study, we assessed with particular attention the duration of effectiveness of treatments performed. SS showed a short therapeutic efficacy with a mean of improvement after discontinuation of therapy of 0.9 months. A meta-analysis conducted by Rai et al. (⁹9. Rai BP, Cody JD, Alhasso A, Stewart L. Anticholinergic drugs versus non-drug active therapies for non-neurogenic overactive bladder syndrome in adults. Cochrane Database Syst Rev. 2012, 12;12:CD003193.) of 23 trials of anticholinergic drugs versus non-drug active therapies for non-neurogenic overactive bladder syndrome, about the permanence of the therapeutic effect of anticholinergic drugs, emphasized how “it is unlikely that the effects of anticholinergics persist after stopping treatment”. PTNS administered in monotherapy or in combination with SS showed a longer duration of effectiveness with a mean of improvement after discontinuation respectively of 2.5 and 5.8 months. A longer duration of effectiveness of PTNS was described by MacDiarmid et al. (¹⁷17. MacDiarmid SA, Peters KM, Shobeiri SA, Wooldridge LS, Rovner ES, Leong FC, et al. Long-term durability of percutaneous tibial nerve stimulation for the treatment of overactive bladder. J Urol. 2010;183:234-40.). Therefore, combination therapy showed the longest therapeutic efficacy. Souto et al. assessed the effectiveness of TENS and oxybutynin alone or in combination therapy, underlining that TENS alone or in association presented longer lasting results than oxybutynin monotherapy. The choice of therapy should be based on several factors including co-morbidities, mental status, age, education and motivation (¹¹11. Souto SC, Reis LO, Palma T, Palma P, Denardi F. Prospective and randomized comparison of electrical stimulation of the posterior tibial nerve versus oxybutynin versus their combination for treatment of women with overactive bladder syndrome. World J Urol. 2014;32:179-84.). However, in clinical practice, antimuscarinic agents are considered the first-line pharmacotherapy for OAB, although a high percentage of patients discontinue the treatment after a few months especially for poor efficacy, side effects and costs (⁵5. Andersson KE, Chapple CR, Cardozo L, Cruz F, Hashim H, Michel MC, et al. Pharmacological treatment of overactive bladder: report from the International Consultation on Incontinence. Curr Opin Urol. 2009;19:380-94., ⁶6. Yu YF, Nichol MB, Yu AP, Ahn J. Persistence and adherence of medications for chronic overactive bladder/urinary incontinence in the california medicaid program. Value Health. 2005;8:495-505.). Therefore, the search for a therapeutic strategy that improves adherence of patients to treatment depends on its efficacy and the reduction of side effects and cost.

CONCLUSIONS

The combination of SS and PTNS in the treatment of OAB symptoms was an effective and well-tolerated therapy with greater improvements and longer lasting effects than single treatments. It allowed the use of lower amounts of drug with a smaller number of PTNS treatments. The low sample size of patients and the follow-up of ten months represent biases that do not allow definitive conclusions to be drawn. Further studies on a greater number of patients would be desirable to confirm this data.

Published as Ahead of Print: August 30, 2017

REFERENCES

¹
Abrams P, Cardozo L, Fall M, Griffiths D, Rosier P, Ulmsten U, et al. The standardisation of terminology of lower urinary tract function: report from the Standardisation Sub-committee of the International Continence Society. Neurourol Urodyn. 2002;21:167-78.
²
Irwin DE, Milsom I, Hunskaar S, Reilly K, Kopp Z, Herschorn S, et al. Population-based survey of urinary incontinence, overactive bladder, and other lower urinary tract symptoms in five countries: results of the EPIC study. Eur Urol. 2006;50:1306-14.
³
Stewart WF, Van Rooyen JB, Cundiff GW, Abrams P, Herzog AR, Corey R, et al. Prevalence and burden of overactive bladder in the United States. World J Urol. 2003;20:327-36.
⁴
Irwin DE, Abrams P, Milsom I, Kopp Z, Reilly K; EPIC Study Group. Understanding the elements of overactive bladder: questions raised by the EPIC study. BJU Int. 2008;101:1381-7.
⁵
Andersson KE, Chapple CR, Cardozo L, Cruz F, Hashim H, Michel MC, et al. Pharmacological treatment of overactive bladder: report from the International Consultation on Incontinence. Curr Opin Urol. 2009;19:380-94.
⁶
Yu YF, Nichol MB, Yu AP, Ahn J. Persistence and adherence of medications for chronic overactive bladder/urinary incontinence in the california medicaid program. Value Health. 2005;8:495-505.
⁷
Bolduc S, Moore K, Lebel S, Lamontagne P, Hamel M. Double anticholinergic therapy for refractory overactive bladder. J Urol. 2009;182(4 Suppl):2033-8.
⁸
Abrams P, Kelleher C, Staskin D, Rechberger T, Kay R, Martina R, et al. Combination treatment with mirabegron and solifenacin in patients with overactive bladder: efficacy and safety results from a randomised, double-blind, dose-ranging, phase 2 study (Symphony). Eur Urol. 2015;67:577-88.
⁹
Rai BP, Cody JD, Alhasso A, Stewart L. Anticholinergic drugs versus non-drug active therapies for non-neurogenic overactive bladder syndrome in adults. Cochrane Database Syst Rev. 2012, 12;12:CD003193.
¹⁰
Mattiasson A, Blaakaer J, Høye K, Wein AJ; Tolterodine Scandinavian Study Group. Simplified bladder training augments the effectiveness of tolterodine in patients with an overactive bladder. BJU Int. 2003;91:54-60.
¹¹
Souto SC, Reis LO, Palma T, Palma P, Denardi F. Prospective and randomized comparison of electrical stimulation of the posterior tibial nerve versus oxybutynin versus their combination for treatment of women with overactive bladder syndrome. World J Urol. 2014;32:179-84.
¹²
Kizilyel S, Karakeçi A, Ozan T, Ünüş İ, Barut O, Onur R. Role of percutaneous posterior tibial nerve stimulation either alone or combined with na anticholinergic agent in treating patients with overactive bladder. Turk J Urol. 2015;41:208-14.
¹³
Kosilov KV, Loparev SA, Ivanovskaya MA, Kosilova LV. Comparative effectiveness of combined low- and standarddose trospium and solifenacin for moderate overactive bladder symptoms in elderly men and women. Urol Int. 2014;93:470-3.
¹⁴
Curran MJ, Kaefer M, Peters C, Logigian E, Bauer SB. The overactive bladder in childhood: long-term results with conservative management. J Urol. 2000;163:574-7.
¹⁵
Amend B, Hennenlotter J, Schäfer T, Horstmann M, Stenzl A, Sievert KD. Effective treatment of neurogenic detrusor dysfunction by combined high-dosed antimuscarinics without increased side-effects. Eur Urol. 2008;53:1021-8.
¹⁶
Groen J, Bosch JL. Neuromodulation techniques in the treatment of the overactive bladder. BJU Int. 2001;87:723-31.
¹⁷
MacDiarmid SA, Peters KM, Shobeiri SA, Wooldridge LS, Rovner ES, Leong FC, et al. Long-term durability of percutaneous tibial nerve stimulation for the treatment of overactive bladder. J Urol. 2010;183:234-40.

Publication Dates

Publication in this collection
Jan-Feb 2018

History

Received
30 Nov 2016
Accepted
21 June 2017

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[1] Published as Ahead of Print: August 30, 2017

Patients N°	SS			PTNS			SS + PTNS
Patients N°	27			34			33
Age	62(41-70)			60 (45-73)			63 (43-72)
Age	before	after	p value	before	after	p value	before	after	p value
OABSS	1.19±0.39	0.71±0.45	0.0020^* * Wilcoxon test (paired samples);	1.24±0.42	0.47±0.50	<0.0001^ Paired samples t-test;	1.22±0.42	0.33±0.47	<0.0001^* * Wilcoxon test (paired samples);
Day-time	SS after		vs	PTNS after		0.1334^* ***** Independent samples t-test;
frequency	SS after		vs	SS + PTNS after		0.0167^* ***** Independent samples t-test;
	PTNS after		vs	SS + PTNS after		0.4224^* ***** Independent samples t-test;
Night-time frequency (score 0-3)	2.62±0.79	1.76±1.31	0.0078^* * Wilcoxon test (paired samples);	2.71±0.67	1.41±1.19	0.0010^* * Wilcoxon test (paired samples);	2.89±0.31	0.89±0.87	<0.0001^* * Wilcoxon test (paired samples);
	SS after		vs	PTNS after		0.4110^* ***** Independent samples t-test;
	SS after		vs	SS + PTNS after		0.0243^* ***** Independent samples t-test;
	PTNS after		vs	SS + PTNS after		0.1585^* ***** Independent samples t-test;
Urgency (score 0-5)	4.29±0.63	3.43±1.09	0.0002^* * Wilcoxon test (paired samples);	4.35±0.59	3.00±1.14	<0.0001^ Paired samples t-test;	4.44±0.68	2.11±0.99	<0.0001^ Paired samples t-test;
	SS after		vs	PTNS after		0.2586^* ***** Independent samples t-test;
	SS after		vs	SS + PTNS after		0.0005^* ***** Independent samples t-test;
	PTNS after		vs	SS + PTNS after		0.0225^* ***** Independent samples t-test;
Urge incontinence (score 0-5)	3.71±1.12	2.67±1.49	0.0005^* * Wilcoxon test (paired samples);	4.00±0.69	2.24±1.35	0.0001^* * Wilcoxon test (paired samples);	3.44±1.5	0.56±1.26	<0.0001^* * Wilcoxon test (paired samples);
	SS after		vs	PTNS after		0.3742^* ***** Independent samples t-test;
	SS after		vs	SS + PTNS after		0.0003^** ****** Mann-Whitney test (independent samples)
	PTNS after		vs	SS + PTNS after		0.0015^** ****** Mann-Whitney test (independent samples)

	SS			PTNS			SS + PTNS
	before	after	p value	before	after	p value	before	after	p value
OAB-q SF 6	3.85±0.59	3.08±0.95	0.0001^* * Paired samples t-test	4.08±0.32	2.98±0.79	<0.0001^* * Paired samples t-test	4.21±0.24	2.32±0.87	<0.0001^* * Paired samples t-test
	SS after		vs	PTNS after		0.7525^ Independent samples t-test
	SS after		vs	SS + PTNS after		0.0168^ Independent samples t-test
	PTNS after		vs	SS + PTNS after		0.0287^ Independent samples t-test
OAB-q SF 13	3.92±0.62	3.16±0.95	0.0001^* * Paired samples t-test	4.22±0.32	2.96±0.97	<0.0001^* * Paired samples t-test	4.04±0.24	2.27±0.84	<0.0001^* * Paired samples t-test
	SS after		vs	PTNS after		0.5318^ Independent samples t-test
	SS after		vs	SS + PTNS after		0.0049^ Independent samples t-test
	PTNS after		vs	SS + PTNS after		0.0361^ Independent samples t-test
PGI-I		2.81±0.96			2.41±0.84			1.83±0.76
	SS		vs	PTNS		0.1997^ Independent samples t-test
	SS		vs	SS + PTNS		0.0017^ Independent samples t-test
	PTNS		vs	SS + PTNS		0.0468^ Independent samples t-test

Brasil

Brasil

Effectiveness and durability of solifenacin versus percutaneous tibial nerve stimulation versus their combination for the treatment of women with overactive bladder syndrome: a randomized controlled study with a follow-up of ten months

ABSTRACT

Purpose

Materials and Methods

Results

Conclusions

INTRODUCTION

MATERIALS AND METHODS

Endpoints

Statistical analysis

RESULTS

DISCUSSION

CONCLUSIONS

REFERENCES

Publication Dates

History

	SS		PTNS		SS + PTNS
OAB-SS	0.93±1.44		2.50±2.38		5.88±2.20
	Solifenacin	vs	PTNS	p	0.0039^* * Mann-Whitney test (independent samples)
	Solifenacin	vs	Solifenacin + PTNS	p	<0.0001^* * Mann-Whitney test (independent samples)
	PTNS	vs	Solifenacin + PTNS	p	0.0009^* * Mann-Whitney test (independent samples)
PGI-I	0.71±1.13		2.10±1.92		5.63±2.00
	Solifenacin	vs	PTNS	p	0.0017^* * Mann-Whitney test (independent samples)
	Solifenacin	vs	Solifenacin + PTNS	p	<0.0001^* * Mann-Whitney test (independent samples)
	PTNS	vs	Solifenacin + PTNS	p	0.0002^* * Mann-Whitney test (independent samples)