Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT03149809 |
| Other study ID # |
N2293-I |
| Secondary ID |
|
| Status |
Completed |
| Phase |
Phase 3
|
| First received |
|
| Last updated |
|
| Start date |
March 1, 2018 |
| Est. completion date |
September 8, 2023 |
Study information
| Verified date |
October 2023 |
| Source |
VA Office of Research and Development |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The impact of urinary symptoms in Parkinson disease (PD) extends beyond worsened well-being.
Urinary symptoms common in PD, especially incontinence and nocturia, are major risk factors
for falls likely due to the combination of urinary urgency and impaired mobility (and falls
are a leading cause of mortality in PD), for spouse/caregiver stress due to decreased
mutuality in the relationship, and for institutionalization, largely due to increased
disability. Additionally, most medications currently recommended for urinary symptoms in PD
are anticholinergic and have the potential to worsen the progressive cognitive and autonomic
burdens of the disease. Veterans with PD are also more likely to rely solely on VA for their
health care than Veterans without PD. Thus, optimizing the care of urinary symptoms for
Veterans with PD becomes imperative, particularly for VA. Using a non-inferiority design,
this proposal seeks to demonstrate the comparative effectiveness of pelvic floor muscle
exercise-based behavioral therapy versus drug therapy to treat urinary symptoms in PD.
Description:
The number of persons with Parkinson Disease (PD) in the United States is expected to double
by 2030 as the population ages. Importantly, this increase in the prevalence of PD will have
greater impact within the Department of Veterans Affairs (VA) because the Veteran population
is older than the general population and Veterans with PD are more likely than those without
PD to rely solely on VA for their health care. While PD is often characterized by the motor
symptoms of the disease (tremor, bradykinesia, rigidity), non-motor symptoms such as urinary
symptoms correlate more closely with impaired well-being as the disease progresses. However,
the impact of urinary symptoms in PD extends beyond worsened well-being. The urinary symptoms
of overactive bladder (OAB), including urgency, frequency, and nocturia, with or without
urinary incontinence, are the most common urinary symptoms of PD. OAB symptoms are associated
with falls (a cause of increased mortality in PD), with spouse/caregiver stress, and,
ultimately with institutionalization, thus it is critical that we optimize the care of
urinary symptoms for Veterans with PD.
Several studies suggest abnormal central nervous system processing of sensory input from
bladder afferent nerves contributes to OAB symptoms in PD, possibly because of delayed
recognition of bladder fullness. This mirrors findings in non-PD populations with OAB. In the
non-PD OAB population, pelvic floor muscle contractions diminish bladder muscle contraction
and recent evidence demonstrates that behavioral training with pelvic floor muscle exercises
improves the cortical integration of bladder afferent signals. Pelvic floor muscle
exercise-based behavioral therapy for OAB symptoms requires individuals to learn a motor
skill and implement an adaptive behavioral strategy to delay the need to void. Because of its
effectiveness compared to drug therapy, pelvic floor muscle exercise-based behavioral therapy
is recommended first-line in men and women with OAB who do not have PD. However, the most
recent clinical guidelines for the treatment of urinary symptoms in PD recommend treatment
with anticholinergic drugs. While some anticholinergic drugs are effective in reducing
symptoms of OAB, it is important to note that there is a glaring lack of an empirical
evidence base to promote these drugs in the setting of PD given that they add to the
anticholinergic burden of antiparkinsonian therapy, and may worsen the cognitive and
autonomic burdens of the illness. Therefore, randomized controlled trials (RCTs) are needed
to optimize treatment paradigms for urinary symptoms in PD.
The investigators propose a three-site, RCT conducted at the Atlanta (lead site), Birmingham
and Richmond VA's to establish non-inferiority of pelvic floor muscle exercise-based
behavioral therapy compared to drug therapy for OAB symptoms in adults with PD. Groups will
be stratified by OAB symptom severity, PD motor symptom severity, gender, and site. The
investigators will randomize 90 participants in order to complete the study in 80
participants, assuming 85% power and a non-inferiority margin for the OAB symptom score of
15% at 12-weeks. The primary outcome measure will be urinary symptom severity as measured by
the International Consultation on Incontinence Questionnaire (ICIQ)-OAB symptom score
collected at 3 time points during the study: baseline, 6 weeks, and 12 weeks. The
investigators' benchmark for successful treatment will be a 2 point reduction in the ICIQ-OAB
symptom score, which corresponds with perceived benefit in preliminary studies of behavioral
therapy treatment for OAB symptoms in PD. To evaluate the primary efficacy outcome, the
investigators will utilize a random effects mixed model and adjust for baseline OAB symptom
score severity. Additionally, in order to better understand central control mechanisms of
bladder function, the investigators will determine if domain-specific cognitive function
impacts the response to exercise-based behavioral therapy or drug therapy for urinary
symptoms. At baseline and 12 weeks, randomized participants will undergo a brief
neuropsychological battery. Understanding how domain-specific cognitive function impacts
response to treatment may inform new targets for rehabilitation therapy.
