Overactive Bladder Clinical Trial
Official title:
Sexual Function Trial of Overactive Bladder: Medication Versus PTNS
Sexual dysfunction affects approximately 45% of women with an even greater incidence reported in women with overactive bladder symptoms, despite this there is a lack of FDA approved treatments for sexual dysfunction in this population. While both medical therapy and electrical neuromodulation have been shown to improve urinary function as well as sexual function, there is a dearth of literature about their comparative effectiveness in the latter. The purpose of this study is to examine the comparative effectiveness of neuromodulation via percutaneous tibial nerve stimulation (PTNS) and medical therapy with anticholinergics or beta-agonists in improving female sexual function. This will be a prospective multi-center cohort study comparing improvement in sexual function as measured by the female sexual function index (FSFI). It is hypothesized that PTNS will improve sexual function to a greater degree than medical therapy as there may be mechanisms by which PTNS directly affects sexual function. Enhanced understanding of the effects of neuromodulation and medical therapy on sexual function may allow for improved patient selection and better outcomes which may lead to widespread use of neuromodulation for female sexual dysfunction.
Specific aims:
Primary aim:
Aim 1: To determine if there is greater improvement in female sexual function as measured by
the female sexual function index (FSFI) with percutaneous tibial nerve stimulation (PTNS) as
compared to medical therapy (MT).
Hypothesis: There will be a greater improvement in overall FSFI with PTNS as compared to MT.
Secondary aims:
Aim 2: To determine if improvement in female sexual function with percutaneous tibial nerve
stimulation or medical therapy is correlated with improvement in urinary symptoms as measured
by the OAB-q questionnaire.
Hypothesis: Improvement in urinary symptoms will be correlated with improvement in sexual
function but that the difference in FSFI between groups will not be solely attributable to
differences in urinary symptom improvement.
Aim 3: To determine if changes in sexual function are greater with beta agonist medications
as compared to anticholinergic medications.
Hypothesis: Beta agonists will result in improved sexual function as compared to
anticholinergics.
Aim 4: To determine if those patients with female sexual dysfunction as defined as an overall
FSFI score below 26.5 have greater improvements than those without.
Hypothesis: Patients with female sexual dysfunction will have a greater improvement in FSFI
than those without.
Female sexual dysfunction (FSD) affects approximately 45% of women with an even greater
incidence reported in women with overactive bladder symptoms, despite this there is a lack of
FDA approved treatments for sexual dysfunction in this population. Female sexual function is
complex and can be affected by pain, depression, and comorbidities as well as bowel and
bladder function. There are numerous treatments for women with overactive bladder (OAB)
defined as urinary urgency, frequency, urge urinary incontinence (UUI) and nocturia. These
treatments include medical therapy (MT) with anticholinergics and beta agonists and
neuromodulation via implantable sacral nerve stimulator (SNM) and percutaneous tibial nerve
stimulation (PTNS). Sexual function, which can be measured by the Female Sexual Function
Index (FSFI) has been shown to improve with both neuromodulation and anticholinergic therapy,
although less is known about the effects of beta agonists. The purpose of this study is to
examine the comparative effectiveness of neuromodulation via percutaneous tibial nerve
stimulation and medical therapy with anticholinergics or beta-agonists in improving female
sexual function. Additionally this study will assess whether improvement in sexual function
is correlated with improvement in urinary symptoms. Furthermore the effectiveness of
anticholinergics as compared to beta agonists with respect to changes in sexual function will
be examined. Lastly patients with sexual dysfunction will be comapred to those without to
determine if patients with female sexual dysfunction have greater improvements than those
without, as this may open the door to future studies using PTNS for the primary indication of
female sexual dysfunction. Enhanced understanding of the effects of neuromodulation and
medical therapy on sexual function may allow for improved patient selection and better
outcomes which may lead to widespread use of neuromodulation for female sexual dysfunction.
This is a prospective multi-center cohort study organized through the American
Urogynecological Society Fellows Pelvic Research Network comparing changes in sexual function
in women undergoing PTNS or MT for OAB/UUI. Recruitment is being conducted at MedStar
Washington Hospital Center, MedStar Franklin Square, Indiana University, University of Texas
Southwestern, University of Louisville and the University of Oklahoma. Potential subjects are
adult women presenting to a urogynecology clinic for symptoms of overactive bladder such as
urgency and UUI. Eligible subjects must report urinary urgency or urge incontinence and be
recommended for treatment with medical therapy (with anticholinergic or beta agonist) or PTNS
by the treating physician. Potential subjects are approached by their treating physician in
the context of a private clinical visit regarding enrollment. Women who enroll are asked to
complete the validated OAB-q, FSFI, Beck Depression Inventory and a visual analog pain scale
prior to therapy and then again after twelve weeks of therapy. These forms may be completed
in person on paper or via the online RedCap database. Demographic data including age,
comorbidities and menopausal status are extracted from the medical record.
The primary endpoint of the study is improvement in overall FSFI score which is hypothesized
to be greater in the PTNS group. Sample size calculations were conducted using
http://clincalc.com/stats/samplesize.aspx with the primary endpoint of FSFI assessed as a
continuous variable. Group sample sizes of 63 per group (total 126 patients) will be
necessary to detect a clinically relevant difference of 5 points in FSFI assuming standard
deviation of 10 and achieve a power of 80%, alpha=0.05. By incorporating a 10% loss to
follow-up rate, the plan is to to recruit 70 patients per group, with a total of 140
patients. Because approximately 45% of patients with OAB will have FSD as determined by an
FSFI score below 26.5, the study may include up to 312 patients in the study. A planned
interim analysis will be conducted comparing patients receiving anticholinergics and those
receiving beta agonists. This will be conducted once 63 patients receiving anticholinergics
and 63 receiving beta agonists have completed the study. This will address Aim 3. A
Mann-Whitney U test will be used to compare FSFI between patients receiving anticholinergics
and beta agonists.
Data Collection and Transmission:
Potential subjects will be approached by their treating physician in the context of a private
clinical visit regarding enrollment in the study. After discussion of the risks and benefits
and obtaining written informed consent, each subject will be assigned a participant
identification number (ID). Those patients who express interest but are unable to sign
consent in the context of an office visit due to time constraints will be contacted via
telephone to complete the consent process; once consent is obtained these patients will have
the option of completing paper questionnaires which will be mailed to them or online
questionnaires which they will receive through a secured email link. Treating physicians and
investigators will monitor patients at clinic visits. Case report forms will be generated for
each subject and completed by the investigator or study coordinator at each site, these will
then be entered by the investigator or study coordinator into a password protected REDCap
database with each patient identified only by ID. Patients will be asked to complete
questionnaires in the setting of clinic visits to minimize mailings and their potential for
privacy breach. Mailing of questionnaires will only be used if patients are unable to return
to clinic for follow up; forms may also be returned via fax or secure email. Patients may
also complete questionnaires online directly in the REDCap database. Patients will be
encouraged to complete forms in REDCap to minimize the potential for transcription error and
breach of privacy. For those patients who cannot mail the forms or access them online, they
may be completed via phone with an investigator or study coordinator. Original case report
forms and questionnaires will be securely maintained on site in a locked file cabinet within
a locked office. MedStar Washington Hospital Center will be the Data Collecting Center (DCC).
Copies of the case report forms and questionnaires will be forwarded by courier or fax to the
DCC with participant ID number visible and personal information obscured. The following
interim data will be monitored via review of the database at scheduled six-month intervals by
the PI: accrual rate, patient adherence, adverse events and accuracy and completeness of the
data.
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