Abstract
Objective
The aim of this study was to determine the efficacy of sustained-release fampridine (4-aminopyridine) in veterans with multiple sclerosis (MS) with limited ambulatory ability, and its impact on motor function in an outpatient setting.
Design
Retrospective.
Setting
Tertiary referral center [Veterans Affairs (VA) Medical Center].
Participants
Veterans; 20 MS patients were prescribed dalfampridine (10 mg twice daily) due to their difficulty with walking based on patient and caregiver report and clinician impression of change in the ability to ambulate based on prior 10-meter (10M) and 2-minute walk tests (2MWTs).
Intervention
Not applicable.
Main Outcome Measures
The primary outcome measures were mean changes in walking speed (10M walk test), walking distance (2MWT), and Total Functional Independence Measure (TFIM). Improvement of >20 % in walking speed was indicated as a clinically meaningful change.
Results
Treatment with dalfampridine resulted in significant improvement in walking speed and endurance (p < 0.05). Walking speed increased by 33 % and walking endurance by 31 %, representing clinically meaningful improvement. This change was not influenced by change in muscle tone. This improvement in mobility was associated with a clinically significant change in motor function. Adverse effects, including insomnia, dizziness, and headache, were experienced by five patients who discontinued the medication after a minimum of 4 weeks.
Conclusion
Treatment with dalfampridine resulted in clinically relevant improvements in walking speed and endurance in MS patients with limited ambulation and helped improve their motor function.
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1 Introduction
Gait disturbance is reported by many patients with multiple sclerosis (MS) as a major primary symptom [1] and occurs in 50 % of cases [2]. It presents early in the course of the disease [3] and is perceived as a major health issue by patients with MS [4]. It is a limiting factor with progression of the disease [1]. This gait disturbance is caused by muscle weakness and spasticity from pyramidal tract lesions, ataxia from cerebellar lesions, sensory disturbance due to dorsal column lesions, and vestibular and visual dysfunction, or a combination of these symptoms [5]. It impacts upon their activities of daily living and emotional state, and thus decreases their quality of life and health state [6]. Recommended treatment options specific to gait disturbance have mainly been physical therapy measures such as exercises for strengthening affected muscles, reducing spasticity, use of ankle–foot braces, and rolling walkers. None of the current immunomodulatory therapies have any effect on improving gait disturbance. Thus, gait disturbance is an important outcome measure in the treatment and rehabilitation of patients with MS.
Fampridine (4-aminopyridine) is a voltage-dependent potassium channel-blocker [7, 8] found to restore action potential conduction in poorly myelinated central nerve fibers [9] and also affects synaptic transmission and neuronal excitability [10]. Several clinical trials have shown fampridine use has been associated with clinical improvement in MS patients [11–14]. The adverse effects of fampridine are confusion, seizure disorder, and balance disorders [15, 16]. These adverse effects are directly related to its dosing and plasma concentration [17, 18]. Recently, two phase III studies showed sustained-release oral fampridine (dalfampridine), a long-acting form with similar physiological action, improved walking ability in 35–43 % of MS patients with ambulatory difficulty compared with 8–9 % for placebo. In the treated group, the improvement in walking speed was 25 % during the treatment period [19, 20]. Dalfampridine is nowadays considered the standard of care for MS patients with ambulatory difficulty.
The objective of the present study was to replicate these findings in veterans with MS in an outpatient setting (real-world environment) and its impacts on their motor function.
2 Methods
2.1 Study Population and Procedures
This study was approved by the Institutional Review Board of the University of Oklahoma and the Veterans Affairs Medical Center Research and Development Committee. Retrospective chart review was conducted for MS patients (n = 20) regularly followed in an outpatient MS clinic who were prescribed dalfampridine (10 mg twice daily). The inclusion criteria were difficulty with walking based on (i) the patient and caregiver report; and (ii) clinician’s impression of change in ambulation based on prior 10-meter (10M) and 2-minute walk tests (2MWT). Exclusion criteria included (i) renal impairment (creatinine clearance <50 mL/min); (ii) prior or current history of seizure disorder; and (iii) presence of disease instability as evidenced by recent MS relapse and/or change in immunomodulatory therapy. Patients were non-Hispanic White (85 %) males (100 %), aged 33–72 years (55.3 ± 10.8; mean ± SD) (see Table 1).
Data collected from the charts of the 20 patients included demographic information, MS characterization, and initial and follow-up scores for the following: Medical Research Council (MRC) lower extremity muscle strength (LEMMT), Total Functional Independence Measure (TFIM), Modified Ashworth Scale (MAS), 10M walk time, and 2MWT distance. Consistent with Veterans Affairs (VA) guidelines for veterans on dalfampridine, response to treatment, compliance, adverse effects, and withdrawals were assessed at 4, 3, 6, and 12 months following treatment initiation. All data were prospectively recorded in the computerized patient record system as part of patient care by a clinician who was unaware of the study hypothesis.
2.2 Primary Outcome Measures
The 10M and 2MWT were administered to the MS patients to assess general walking speed and capacity [21, 22]. The 10M walk test measures walking speed (in seconds) of the patient over a set distance. The patient was instructed to walk at usual speed using whatever aid was needed as in everyday life. This test was selected as it is simple and quick to administer, inexpensive, and is easily generalizable to community walking [21]. It has been found to be a reliable, valid, and sensitive measure [23–25]. The limitation of the 10M walk test is that the quality of gait is not assessed and a ceiling effect is apparent at normal walking speed (1.2–1.4 m/s) [26].
The 2MWT, commonly used to measure walking capacity or endurance in persons with cardiac and pulmonary disease, assessed endurance in these patients. The patient was instructed to cover as much ground as possible in 2 min walking at a comfortable speed using ambulation aids as used in their everyday life. Rest periods were allowed during the evaluation. The distance (in feet) covered was measured using a Trumeter Mini-Measure Distance-Measuring Wheel, a device that accurately measures up to 10,000 feet. The 2-minute timed walk test is a valid, reliable, and sensitive measure that is easy to administer [22, 27]. The limiting factors for the 2-minute timed walk test are pain, mood, and cardiovascular fitness, which can influence the result [28].
The MAS was administered to measure spasticity [29]. It is widely used, easy to administer, and has good validity but limited reliability [30–32]. Research has shown that disability tends to be more related to weakness than spasticity [33]. Therefore, the association between ambulatory gains and spasticity changes were examined.
MRC scale graded the lower extremity muscle strength (LEMMT). It is a widely used ordinal measure of power, with 0 = no movement to 5 = normal movement. It has established validity and reliability [34]. The major limitation of MRC grading is that the scale neither considers the range of motion (ROM) for which a movement can be performed nor defines the strength of resistance against which a movement can be performed [35].
The TFIM assessed MS-related disability. The TFIM is a reliable [36] and valid [37] functional assessment instrument that is widely used in many rehabilitation settings [38] to measure the degree of disability [39]. The TFIM has 18 items; each item is scored on an ordinal scale ranging from 1 (‘total assist’: patient performs <25 % of task) to 7 (‘complete independence’). The resulting score indicates the level of assistance needed to achieve independence and ranges from 18 (totally dependent) to 126 (independent). Thus, increased disability is reflected in lower TFIM scores.
2.3 Statistical Analysis
All data analyses for this paper were generated using SAS software, Version 9.2 of the SAS System for Windows (SAS Institute Inc., Cary, NC, USA). The significance level for all statistical tests was set a priori at p < 0.05. Paired t tests were used to compare the pre-treatment and 12-month follow-up assessments of spasticity, walking speed, walking capacity, and TFIM. Improvement of >20 % in walking speed was used to detect clinically meaningful change. Pearson correlation coefficients were examined to describe the relationship between 10M and 2MWT at initial evaluation and 12-month follow-up, as well as between changes in spasticity and ambulation. A ‘responder status’ was defined based on faster walking speed for three of the four visits during the treatment period [19]. The difference in the proportion of responders between the continuation and discontinuation group was analyzed using the Chi-square test.
Secondary analyses were conducted comparing initial and 12-month follow-up scores on the 10M, 2MWT, and MAS according to MS type (relapsing-remitting, RR; secondary-progressive, SP; or primary-progressive, PP), MS severity (mild: Expanded Disability Status Scale [EDSS] score ≤4.0, or moderate-to-severe: EDSS ≥4.5), and duration of dalfampridine use (discontinued after a minimum of 4 weeks or continued 12-months use) using repeated measures of analysis of variance (MS type) and paired t tests. These analyses were not included in the primary analyses because of the low sample sizes after dividing the sample into groups.
3 Results
The mean age of MS onset was 35.2 years (SD 11.9) and mean duration of MS condition was 23.5 years (SD 14.5). The most common type of MS was RR (55 %) followed by SP (30 %) and PP (15 %) types. The initial mean MAS, 10M, 2MWT, and LEMMT test scores across the entire sample were 0.5 ± 0.7, 28.4 ± 18.7 s, 155.4 ± 94.5 feet, and 3.9 ± 0.9 (2–5), respectively. The mean initial EDSS and TFIM scale scores were 5.5 ± 1.9, and 83.7 ± 13.3, respectively. Thus, patients with MS were moderately functionally impaired with little muscle tone (spasticity).
Table 2 presents the change in the 10M and 2MWT, and MAS, LEMMT, and TFIM scores. Data were missing for several patients; therefore, values are only presented for those with data at both timepoints. Significant improvement was observed for walking speed (p = 0.008), and walking distance (p = 0.03), but not for spasticity (p = 0.10) and lower extremity muscle strength (p = 1.0). The change in 10M represented a 33 % improvement in walking speed, exceeding the minimally important clinical difference of 20 %, and endurance improved by 31 %. While the MAS score doubled, the score still fell in the range representing no change in muscle tone. Likewise, there was no change in the LEMMT score. The correlations between MAS change and change in walking speed and endurance did not achieve significance (p > 0.05). This improvement in ambulatory ability was mirrored by an improvement in motor function (p = 0.07); however, it did not achieve statistical significance.
The correlation between walking speed (10M) and walking distance (2MWT) was examined for scores obtained on initial evaluation and at 12-month follow-up (Fig. 1). The correlation at baseline was not significant r = −0.38, p = 0.22 (n = 12). However, at 12-months, there was a significant inverse relationship between walking speed and walking distance, r = −0.88, p < 0.0001 (n = 13), indicating that the faster walkers were also able to walk further distances.
The number of patients who met the responder criterion was 6/12 (50 %) in the continuation group compared with 2/8 (25 %) in the discontinuation group (p = 0.37). There was no difference in change in leg strength at 12 months between responders and non-responders (−0.2 ± 1.0 vs. 0.1 ± 1.1; mean ± SD; p = 0.63).
3.1 Secondary Analyses
No significant differences were observed in change at 12 months for 10M, 2MWT, or MAS according to MS type (see Appendix 1, electronic supplementary material [ESM]) or MS severity (see Appendix 2, ESM) [all p > 0.05]. However, SP and PP MS patients had the fastest walking speed and had more endurance compared with the RR MS patients when on dalfampridine. Similarly, moderate to severely disabled MS patients had the fastest walking speed and had more endurance compared with the mildly disabled MS patients when on dalfampridine. Although no significant differences were observed in change at 12 months for 10M, 2MWT, and MAS scores according to the duration for which dalfampridine was taken (p > 0.5) (see Appendix 3, ESM), it did show that veterans who took dalfampridine for a minimum of 4 weeks were able to maintain faster walking speed and endurance at 12 months when compared with those who continued taking their medication for 12 months.
4 Discussion
Results of this study in MS patients who were on stable immunomodulatory therapy confirm the beneficial effect of dalfampridine in the treatment of veterans with MS and ambulatory dysfunction [16, 19], but also expands upon the findings of Goodman et al. [19, 20] by demonstrating the following: (i) improved ambulation persists when dalfampridine is taken over an extended time period (12 months); (ii) the change in ambulation speed and endurance is both clinically relevant and significant; (iii) the changes in ambulation were not influenced by change in muscle tone (spasticity), or improvement in muscle strength in the legs; and (iv) this improvement in ambulation was associated with an improvement in motor function.
In terms of the major outcome measures of walking speed and endurance, walking speed improved by 33 % with a simultaneous increase in endurance (the distance ambulated) by 31 % for the whole group. Studies by Goodman et al. [19, 20] showed the average change from baseline in walking speed in the fampridine-treated group was 25 %, which is similar to our study results, and this change was maintained during the 12-month treatment period. This improvement in walking speed translated into improved endurance, resulting in them becoming community ambulators [40, 41]. The improvements in walking speed exceed ≥20 %, which is considered to represent clinically relevant change [42–44].
While the small sample sizes limit the power and generalizability of the analyses, the current study also demonstrated that, of the MS types, PP and SP made the most gains in ambulation compared with the RR group. This was not unusual given that the PP and SP groups were slow in ambulation to begin with and ambulated shorter distances (more impaired). Similar changes were observed for the more impaired patients (moderate to severe impairment) when compared with mildly impaired patients. Both sets of patients who continued taking the medication and those who discontinued after a minimum of 4 weeks use were able to maintain their improved walking speed and endurance at 12-month follow-up. This improvement in ambulatory ability translated into improved motor function. The change in TFIM score was 18 points. A TFIM change of ~20 points is considered a minimally clinically significant change [45]. This implied that patients who were now able to ambulate more were now more able to self-care and thus less dependent on their caregivers.
The present study also revealed a negative correlation between walking speed and endurance on initial evaluation and 12-month follow-up, with slower walking patients also ambulating shorter distances. However, this association was statistically significant at 12-month follow-up only. This finding suggests that the results of the two ambulation tests are better aligned at the follow-up assessment.
Eight patients (40 %) discontinued dalfampridine use after 4 weeks. Three patients did so volitionally due to perceived lack of benefit, while in five patients this was due to adverse effects which included insomnia in two patients, and weakness, dizziness, and headache in one patient each.
The limitations of this study include (i) the small sample size; (ii) the sample comprised of veterans who were all White men; (iii) it was a single institution study; and (iv) retrospective analysis with missing data may bias the findings of this study. However, the strength of this study lies in the longitudinal follow-up for 12 months with 100 % adherence to intake in 60 % (12/20) of the patient population studied.
5 Conclusion
Ambulation is crucial for patients with MS. This study provides evidence that treatment with dalfampridine in veterans with MS with ambulatory dysfunction produces clinically meaningful improvement in walking speed and endurance in the absence of meaningful change in muscle tone. This improvement in ambulation was associated with improved motor functioning.
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Author contributions
Study concept and design was undertaken by Meheroz H. Rabadi; acquisition of data was carried out by Kimberly Kreymborg and Meheroz H. Rabadi; analysis and interpretation of data was conducted by Meheroz H. Rabadi and Andrea S. Vincent; drafting of the manuscript was undertaken by Meheroz H. Rabadi, Kimberly Kreymborg and Andrea S. Vincent; critical revision of the manuscript for important intellectual content was undertaken by Meheroz H. Rabadi and Andrea S. Vincent; statistical analysis was conducted by Andrea S. Vincent; and study supervision was carried out by Meheroz H. Rabadi.
Conflicts of interest
Meheroz H. Rabadi, Kimberly Kreymborg and Andrea S. Vincent declare no conflicts of interest.
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Rabadi, M.H., Kreymborg, K. & Vincent, A.S. Sustained-Release Fampridine (4-Aminopyridine) in Multiple Sclerosis: Efficacy and Impact on Motor Function. Drugs R D 13, 175–181 (2013). https://doi.org/10.1007/s40268-013-0020-x
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DOI: https://doi.org/10.1007/s40268-013-0020-x