L. Storti scite author profile

SummaryBackground The rationale for combining anticancer drugs has not been applied consistently to use of intravesical agents for treatment of superficial bladder cancer, for which immunotherapeutic BCG and chemotherapeutic mitomycin seem to be a potentially effective combination. We aimed to do a prospective, randomised comparison of BCG alone with that of sequential BCG and electromotive mitomycin in patients with stage pT1 bladder cancer.Methods After transurethral resection and multiple biopsies, 212 patients with stage pT1 bladder cancer were randomly assigned to: 81 mg BCG infused over 120 min once a week for 6 weeks (n=105); or to 81 mg BCG infused over 120 min once a week for 2 weeks, followed by 40 mg electromotive mitomycin (intravesical electric current 20 mA for 30 min) once a week as one cycle for three cycles (n=107). Complete responders underwent maintenance treatment: those assigned BCG alone had one infusion of 81 mg BCG once a month for 10 months, and those assigned BCG and mitomycin had 40 mg electromotive mitomycin once a month for 2 months, followed by 81 mg BCG once a month as one cycle for three cycles. The primary endpoint was disease-free interval; secondary endpoints were time to progression; overall survival; and disease-specific survival. Analyses were done by intention to treat. This trial has been submitted for registration at the US National Cancer Institute website http://clinicaltrials.gov. Findings

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Transdermal electromotive administration of verapamil and dexamethasone for Peyronie's disease

Stasi

Giannantoni

Capelli

et al. 2003

BJU International

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OBJECTIVETo evaluate the effects of the transdermal electromotive administration of verapamil and dexamethasone on plaque size, penile deviation, pain, erectile function and capacity for vaginal penetration in patients with Peyronie's disease. PATIENTS AND METHODSForty-nine patients were treated four times weekly for six consecutive weeks. During each session the drug mixture was administered from a receptacle fixed to the skin overlying the plaques, using 2.4 mA pulsed current for 20 min. Plaque size and penile deviation were evaluated by dynamic penile duplex ultrasonography, X-ray and photographs; pain, erectile function and capacity for vaginal penetration were assessed using a questionnaire. Vital signs and side-effects were recorded. Differences before and after treatment were assessed. RESULTSThe plaque disappeared in 8% of patients, with a measurable reduction in volume in 74% and no change in 18% ( P < 0.001). Penile deviation resolved in 10% of the men, decreased in 74% and remained unchanged in 16% ( P < 0.001). The plaque volume was halved in two-thirds of the men, to a mean ( SD ) of 515 (301) mm 3 , and the penile deviation halved in 45% of patients, to 24 (5) ∞ ; pain was completely eliminated in 88% ( P < 0.001). Erectile function was completely restored in 42% of patients with initial erectile dysfunction and improved in 17% ( P < 0.001); vaginal penetration improved in 73%. No toxicity was noted, except for a transient skin erythema at the site of the penile and dispersive electrodes.

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Intravesical Oxybutynin: Mode of Action Assessed by Passive Diffusion and Electromotive Administration With Pharmacokinetics of Oxybutynin and N-Desethyl Oxybutynin

et al. 2001

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Purpose: A proportion of patients with detrusor hyperreflexia who are unresponsive to oral oxybutynin often benefit from intravesical oxybutynin instillation. To our knowledge the precise mode of action of this method is obscure.Materials and Methods: In 12 patients with detrusor hyperreflexia who were previously unresponsive to oral and intravesical passive diffusion of 5 mg. oxybutynin we administered 5 mg. oxybutynin orally as well as increased doses of 15 mg. oxybutynin intravesically with passive diffusion and with 15 mA. associated electric current. Each administration mode per patient was associated with an 8-hour urodynamic monitoring session during which oxybutynin and N-desethyl oxybutynin plasma levels, and intravesical oxybutynin uptake were measured.Results: A dose of 5 mg. oxybutynin orally induced no urodynamic improvement with an area under the plasma concentration time curve of combined N-desethyl oxybutynin plus oxybutynin of 16,297 ng./8 hours and an area under the curve ratio of N-desethyl oxybutynin-to-oxybutynin of 11:1. Passive diffusion oxybutynin resulted in 12 mg. oxybutynin intravesical uptake and significant improvement in 3 of 8 urodynamic measurements, although the area under the curve of combined N-desethyl oxybutynin plus oxybutynin was only 2,123 ng./8 hours and the N-desethyl oxybutynin-to-oxybutynin ratio was 1.1:1.0. Electromotive administration of oxybutynin resulted in almost complete intravesical uptake of the 15 mg. dose, significant improvement in all 8 urodynamic measurements and an increased oxybutynin level versus oral and passive diffusion, although the area under the curve of combined N-desethyl oxybutynin plus oxybutynin was 4,574 ng./8 hours and the N-desethyl oxybutynin-to-oxybutynin ratio was inverted at 1.0:1.4. The oral dose of 5 mg. oxybutynin caused anticholinergic side effects in 8 of the 12 patients. Neither intravesical passive diffusion nor electromotive administration caused side effects with an uptake of 12 and 15 mg., respectively.Conclusions: A large proportion of intravesical oxybutynin is sequestered, probably in the urothelium. Intravesical oxybutynin administration confers therapeutic benefits via localized direct action within the bladder wall.

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SINGLE IMMEDIATE PREOPERATIVE INSTILLATION OF ELECTROMOTIVE MITOMYCIN-C PLUS TRANSURETHRAL RESECTION VERSUS TRANSURETHAL RESECTION ALONE VERSUS TRANSURETHRAL RESECTION PLUS IMMEDIATE MITOMYCIN-C FOR pTa BLADDER TUMORS: LONG TERM RESULTS OF A PROSPECTIVE RANDOMIZED TRIAL

Stasi¹,

Storti²,

Giurioli³

et al. 2008

Journal of Urology

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Intravesical Oxybutynin:

Stasi¹,

Giannantoni²,

Navarra³

et al. 2001

The Journal of Urology

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L. Storti

Sequential BCG and electromotive mitomycin versus BCG alone for high-risk superficial bladder cancer: a randomised controlled trial

Transdermal electromotive administration of verapamil and dexamethasone for Peyronie's disease

Intravesical Oxybutynin: Mode of Action Assessed by Passive Diffusion and Electromotive Administration With Pharmacokinetics of Oxybutynin and N-Desethyl Oxybutynin

SINGLE IMMEDIATE PREOPERATIVE INSTILLATION OF ELECTROMOTIVE MITOMYCIN-C PLUS TRANSURETHRAL RESECTION VERSUS TRANSURETHAL RESECTION ALONE VERSUS TRANSURETHRAL RESECTION PLUS IMMEDIATE MITOMYCIN-C FOR pTa BLADDER TUMORS: LONG TERM RESULTS OF A PROSPECTIVE RANDOMIZED TRIAL

Intravesical Oxybutynin:

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