Abstract

This retrospective study was performed to verify the efficacy and safety of Onabotulinumtoxin A (BTX-A) in treating children with neurogenic bladder (NB) secondary to myelomeningocele (MMC) with detrusor overactivity/low compliance. From January 2002 to June 2011, 47 patients out of 68 with neuropathic bladder were selected (22 females, 25 males, age range 5–17 years; mean age 10.7 years at first injection). They presented overactive/poor compliant neurogenic bladders on clean intermittent catheterization, and were resistant or non compliant to pharmacological therapy. Ten patients presented second to fourth grade concomitant monolateral/bilateral vesicoureteral reflux (VUR). All patients were incontinent despite catheterization. In the majority of patients Botulinum-A toxin was administered under general/local anesthesia by the injection of 200 IU of toxin, without exceeding the dosage of 12IU/kg body weight, diluted in 20 cc of saline solution in 20 sites, except in the periureteral areas. Follow-up included clinical and ultrasound examination, urodynamics performed at 6, 12 and 24 weeks, and annually thereafter. Seven patients remained stable, 21 patients required a second injection after 6–9 months and 19 a third injection. VUR was corrected, when necessary, in the same session after the BT-A injection, by 1–3 cc of subureteral Deflux®. Urodynamic parameters considered were leak point pressure (LPP), leak point volume (LPV) and specific volume at 20 cm H2O pressure. The results were analyzed using the Wilcoxon test. All patients experienced a significant 66.45% average increase of LPV (Wilcoxon paired rank test = 7169 × 10 −10) and a significant 118.57% average increase of SC 20 (Wilcoxon paired rank test = 2.466 × 10 −12). The difference between preoperative and postoperative LPP resulted not significant (Wilcoxon paired rank test = 0.8858) No patient presented severe systemic complications; 38/47 patients presented slight hematuria for 2–3 days. Two patients had postoperative urinary tract infection. All patients were hospitalized for 24 h with catheterization. Thirty-eight out of 47 patients achieved dryness between CIC; nine patients improved their incontinence but still need pads. Ten patients have resumed anticholinergic agents. Our results suggest that the use of BTX-A is safe and effective in patients with MMC with a positive effect on their dryness and quality of life.

Highlights

  • Current treatment of patients with neurogenic bladder (NB) secondary to myelomeningocele (MMC) is mainly based on Clean Intermittent Catheterization (CIC) and associated anticholinergic agents, or on surgical procedures on the bladder or bladder neck

  • Our results suggest that the use of BTX-A is safe and effective in patients with MMC with a positive effect on their dryness and quality of life

  • In cases where the NB is characterized by overactivity and/or low compliance, the first safeguard is the use of early anticholinergic drugs, such as oxybutynin, tolterodine, or most recently trospium chloride, with the ultimate goal of making the patient dry safeguarding renal function

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Summary

Introduction

Current treatment of patients with neurogenic bladder (NB) secondary to myelomeningocele (MMC) is mainly based on Clean Intermittent Catheterization (CIC) and associated anticholinergic agents, or on surgical procedures on the bladder or bladder neck. If anticholinergics and CIC do not provide the desired result, it is necessary to use more invasive techniques of augmentation in order to transform the bladder into a reservoir with high capacity/low pressure [1]. There is increasing confidence in the use of onabotulinumtoxin A (Botox—BTX-A) in the treatment of NB secondary to MMC as a valid alternative to invasive procedures [2,3,4,5]. We present our experience of a selected a group of patients in whom the clinical and urodynamics assumed the need for augmenting their bladder due to the poor response to drugs, and in whom incontinence and the use of pads between catheterizations strongly influenced their social lives

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