Multiple Sclerosis Clinical Trial
Official title:
Factors That Influence Compliance With Disease-Modifying Therapy in Multiple Sclerosis
The purpose of this study is to evaluate the coorelation between patient factors, health care provider factors, drug factors and compliance in patients with relapsing forms of multiple sclerosis (RMS) treated with Disease Modifying Agents (DMA). We hypothesize that a number of factors influence compliance with DMA's.
While compliance rates with interferons and glatiramer acetate treatment have been high when
assessed in the context of controlled clinical trials, we have observed substantially less
consistent rates of drug administration in general practice. Correspondingly, the magnitude
of drug efficacy achieved on clinical and surrogate markers of disease activity in the
latter patient group may be compromised compared to patients participating in controlled
clinical trials. Further, in many circumstances, the perception of breakthrough disease
simply constitutes treatment noncompliance.
The National Multiple Sclerosis Society reports only 50% of all MS patients and 60% with
relapsing remitting MS are taking disease modifying agents in the U.S. (Zwibel 2003) A
number of studies have investigated this challenging issue. When glatiramer acetate therapy
was specifically evaluated, the investigators found several factors to be associated with
compliance. They discovered adherence to be higher with the patient perception of physician
support of the medication prescribed, patient sense of control, higher levels of hope and no
previous use of other disease modifying therapy (Fraser, Hadjimichael, and Vollmer 2001).
Another study by Hadjimichael and Vollmer (1999) surveyed patients for reasons that
medications were discontinued. Disease progression, lack of improvement and side effects
were some of the reasons reported by patients for stopping disease-modifying therapy.
Depression is another factor found to impact adherence. Mohr, Goodkin, Likosky, Gatto,
Baumann and Rudick (1997) saw increased rates of compliance with Interferon beta-1b therapy
in multiple sclerosis with the treatment of underlying depression. The study showed that
patients with increased depression were more likely to discontinue therapy. This link of
depression has also been demonstrated with noncompliance with antihypertensive medications.
(Wang,Bohn, Harooni et al. 2002) In another study, Mohr (2001) saw patient’s experienced
level of anxiety with their injections was related to adherence.
We hypothesize that a number of factors influence compliance with DMA’s, these include:
1. Patient factors
1. Perceived quality of life
2. Empowerment, sense of control & hope
3. Support structure (family, faith, injection assistance, etc.)
4. Depression
5. Fatigue
6. Cognitive problems
7. Perception of drug efficacy (benefit over costs)
2. Physician (HCP support) factors
1. Patient’s perception of MD support
2. Relationship with MD
3. Access to nurses and other HCP support functions
4. Services provided by physician/clinical practice (i.e. academic, community-based,
or MS clinic)
5. Adequate education on MS, establishing reasonable expectations concerning the
benefit derived from therapy,
3. Drug factors
1. complexity of drug administration
2. drug associated side effects/tolerability
3. Perceived MS symptom control
4. Insurance coverage of the injection
5. Concomitant medications
Once the factors that contribute to noncompliance to DMA therapies are identified,
healthcare professionals can evaluate how they can be impacted. The healthcare team can work
towards addressing those barriers where there is a possibility for change, to help improve
patient outcomes.
The primary objective of this study is to evaluate the correlation between patient factors,
HCP support factors, drug factors, and compliance in patients with relapsing forms of
multiple sclerosis (RMS) treated with Disease Modifying Agents (DMA).
The secondary objectives of the study are to determine differences in patient compliance
between patients treated by academic centers/MS specialists and community neurology centers;
and to determine the factors that impact this difference.
Patients are asked to sign (electronic agreement) a consent to participate in this
confidential study when they initially log-on to the study website. Patients are assigned a
unique identification number when they log into the internet for the first time to complete
the study survey. By using this assigned number, health information will be protected for
each individual. Patient names will be used only for purposes of check distribution and
participation in following studies if the patient consents. If a patient drops out of the
study, TNS Healthcare will contact the patient to find out the reason. The treating
physician does not know who elected to participate in the study.
Study Design- This is a multicenter, retrospective trial administered through patient
surveys. We are utilizing the validated MS quality of life 54 (MSQOL-54), the Beck’s Fast
Screen for medical patients, the Hope Herth Index, and a patient self-reported drug
compliance survey. The participating neurologists were asked to give patients with relapsing
forms of MS flyers describing the study. The flyers direct patients to the designated study
website to complete the confidential survey by internet. As described below, patients log-on
to the website a total of 3 times during the study period, Baseline (time 0), Month 1 (Time
1) and Month 2 (Time 2). Patients log on with a unique identification number rather than
names to ensure that confidentiality is maintained throughout the study.
The goal is to have an equal number of patients treated with the four different DMA’s,
AVONEX, Rebif, Copaxone, and Betaseron. The sample is to include at least 150-200 patients
from each of the MS Centers and 15-20 patients from each of the community sites, for a total
of approximately 1040 patients. Power analysis was performed assuming a 15% critical effect
value. The sample size was calculated to provide 80% power to detect the critical effect
value at a confidence interval of 95%. Response rates are estimated to be 60% for the first
wave and 75% for the second wave of questionnaires.
;
Observational Model: Defined Population, Time Perspective: Cross-Sectional
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