To evaluate the efficacy and safety of intravesical instillation of Lipotoxin for the treatment of IC/BPS
Liposome has been proven able to carry botulinum toxin protein across the cell membrane and effect on urothelial receptors in human overactive bladder. However, the therapeutic duration is limited to 1 month. Intravesical BOTOX injection in patients with interstitial cystitis (IC) can effectively decrease pain, improve bladder capacity and decrease frequency. However, the need of cystoscopic injection limits its wide application. A total of 100 eligible women with non-ulcer IC will be enrolled to receive intravesical instillation of Lipotoxin containing 80mg liposomes and 200U BOTOX (treatment group), 200U BOTOX in normal saline (N/S) (active control group) or normal saline (placebo control group) single treatment. At least 90 evaluable patients will be included for the final analysis. All patients should have IC symptoms for at least 6 months, and proven to have grade 2 diffused glomerulations after cystoscopic hydrodistention (HD) within recent 1 year without Hunner's lesion. Patients should not have UTI in recent 12 months, no urinary tract stone. Patients should have been proven free of detrusor overactivity or bladder outlet obstruction. Patients should not receive intravesical hyaluronic acid treatment in recent 6 months, or intravesical Botox injection in recent 12 months. Intravesical instillation of Lipotoxin at OPD and the patient should hold the solution for 2 hours to allow bladder distention. Retreatment with Lipotoxin at 3 months if patient reports ineffective. Primary end-point is the change of the O'Leary-Sant symptom score (including ICSI and ICPI) from baseline to 1 month after treatment. Secondary endpoints include VAS, daily frequency, nocturia and FBC as record in 3-day voiding diary, Qmax, voided volume, PVR and global response assessment (GRA). Four visits are required at baseline screening (before first treatment), treatment (V1), 2 weeks (V2), 4 weeks (V3, primary end-point) and 12 weeks (V4).
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
TRIPLE
Enrollment
90
Liposome encapsulated BoNT-A ( mixed BOTOX 200U/10ml in Liposome 80mg/40ml) in single intravesical instillation
BOTOX 200U in normal saline (BoNT-A/NS) 50ml in single intravesical instillation
Normal saline (N/S) 50ml in single intravesical instillation
Buddhist Tzu Chi General Hospital
Hualien City, Taiwan
Change of the O'Leary-Sant symptom score
Change of the O'Leary-Sant symptom score from baseline to 1 month after the treatment day
Time frame: Baseline and 1 month
Net changes of the Visual Analog Scale (VAS)
Net changes of the Visual Analog Scale from baseline to 1 month after the treatment day Safety (1) Local adverse event incidences (hematuria, miction pain, UTI, urinary retention).
Time frame: Baseline and 1 month
Net changes of the functional bladder capacity (FBC)
Net changes of the functional bladder capacity from baseline to 1 month after the treatment day Safety (1) Local adverse event incidences (hematuria, miction pain, UTI, urinary retention).
Time frame: Baseline and 1 month
Net changes of the voiding frequency at daytime as recorded in 3-day voiding diary
Net changes of the voiding frequency at daytime from baseline to 1 month after the treatment day Safety (1) Local adverse event incidences (hematuria, miction pain, UTI, urinary retention).
Time frame: Baseline and 1 month
Net changes of the voiding frequency at night time as recorded in 3-day voiding diary
Net changes of the voiding night time from baseline to 1 month after the treatment day Safety (1) Local adverse event incidences (hematuria, miction pain, UTI, urinary retention).
Time frame: Baseline and 1 month
Net Change of the Global response assessment (GRA)
Global response assessment (GRA) of therapeutic result by the patient (categorized from -3 to +3, indicating markedly worse to markedly improved) at 3 months after the treatment day. Safety (1) Local adverse event incidences (hematuria, miction pain, UTI, urinary retention).
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Time frame: Baseline and 1 month
Net Change of the maximum flow rate
Net changes of the maximum flow rate from baseline to 1 month after the treatment day. Safety (1) Local adverse event incidences (hematuria, miction pain, UTI, urinary retention).
Time frame: Baseline and 1 month
Net Change of the voided volume
Net changes of the voided volume from baseline to 1 month after the treatment day. Safety (1) Local adverse event incidences (hematuria, miction pain, UTI, urinary retention).
Time frame: Baseline and 1 month
Net Change of the PVR
Net changes of the PVR from baseline to 1 month after the treatment day. Safety (1) Local adverse event incidences (hematuria, miction pain, UTI, urinary retention).
Time frame: Baseline and 1 month
Net Change of the urinary nerve growth factor
Changes of urinary nerve growth factor from baseline to 1 month after treatment day. Safety (1) Local adverse event incidences (hematuria, miction pain, UTI, urinary retention).
Time frame: Baseline and 1 month
Net Change of the cytokines level
Changes of cytokines level from baseline to 1 month after treatment day. Safety (1) Local adverse event incidences (hematuria, miction pain, UTI, urinary retention).
Time frame: Baseline and 1 month