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Long-term Safety and Dosing of OnabotulinumtoxinA: A Prospective, Observational Study

Published online by Cambridge University Press:  01 July 2019

Theodore Wein*
Affiliation:
Division of Neurology, McGill University, Montreal, QC, Canada
Mandar Jog
Affiliation:
Department of Clinical Neurological Sciences, London Health Sciences Centre, London, ON, Canada
Meetu Bhogal
Affiliation:
Allergan plc., Markham, ON, Canada
Sonja Dhani
Affiliation:
Allergan plc., Markham, ON, Canada
Robert Miller
Affiliation:
Department of Diagnostic Radiology, Division of Cardiology, Dalhousie University, Halifax, NS, Canada
Farooq Ismail
Affiliation:
Westpark Healthcare Centre, Toronto, ON, Canada
Richard Beauchamp
Affiliation:
Children's and Women's Health Centre of B.C., and Department of Orthopedic Surgery, University of BC, Vancouver, BC, Canada
Grace Trentin
Affiliation:
Allergan plc., Markham, ON, Canada
*
Correspondence to: Theodore Wein, McGill University Health Centre, Department of Neurology and Neurosurgery, L7 312 Montreal General Hospital, 1650 Cedar Ave, Montreal, QC H3G 1A4 Canada. Email: twein@videotron.ca
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Abstract:

Background:

Although therapeutic treatments are intended to help alleviate symptoms associated with disease, safety must be carefully considered and monitored to confirm continued positive benefit/risk balance. The objective of MOBILITY was to study the long-term safety of onabotulinumtoxinA for treatment of various therapeutic indications.

Methods:

A prospective, multicenter, observational, Phase IV Canadian study in patients treated with onabotulinumtoxinA for a therapeutic indication. Dosing was determined by the participating physician. Adverse events (AEs) were recorded throughout the study.

Results:

Patients (n = 1372) with adult focal spasticity, blepharospasm, cerebral palsy, cervical dystonia, hemifacial spasm, hyperhidrosis, or “other” diagnoses were enrolled into the safety cohort. Eighty-three patients (6%) reported 209 AEs; 44 AEs in 24 patients (2%) were considered treatment-related AEs. Seventy-two serious AEs were reported by 38 patients (3%); 10 serious AEs in 5 patients (0.4%) were considered treatment related. Most commonly reported treatment-related AEs were muscular weakness (n = 7/44) and dysphagia (n = 6/44).

Conclusions:

In patients with follow-up for up to six treatments with onabotulinumtoxinA, treatment-related AEs were reported in <2% of the safety population over the course of nearly 5 years. Our findings from MOBILITY provide further evidence that onabotulinumtoxinA treatment is safe for long-term use across a variety of therapeutic indications.

Résumé:

Dosage et sécurité à long terme de l’onabotulinumtoxinA : une étude prospective et observationnelle. Contexte : Bien que les traitements thérapeutiques soient destinés à soulager les symptômes associés à une maladie, il importe d’examiner avec grand soin leur sécurité et d’en assurer un suivi afin de maintenir un rapport bénéfice/risque qui soit positif. L’objectif de MOBILITY a donc été d’étudier la sécurité à long terme de l’onabotulinumtoxinA dans le traitement de plusieurs indications thérapeutiques. Méthodes : Nous avons ainsi fait appel à une étude canadienne prospective et observationnelle menée dans plusieurs centres de santé. Dans cette étude de phase IV, des patients ont été traités avec l’onabotulinumtoxinA en vertu d’indications thérapeutiques. Ce sont des médecins participants qui en avaient déterminé le dosage. De plus, tout événement indésirable a été noté en cours d’étude. Résultats : Au total 1372 patients ont été inclus dans cette cohorte (n = 1372). Ces patients étaient atteints des troubles suivants : spasticité focale chez l’adulte, blépharospasme, infirmité motrice cérébrale, dystonie cervicale, spasmes hémifaciaux, hyperhidrose, etc. On a signalé chez 83 patients, soit 6 % d’entre eux, des événements indésirables. On a aussi estimé que 44 événements indésirables ayant affecté 24 patients (2 %) étaient reliés au traitement proprement dit. Ajoutons que 38 patients (3 %) ont signalé avoir été victimes d’événements indésirables et que 10 événements indésirables ont été reliés au traitement chez 5 patients (0,4 %). Enfin, les événements indésirables les plus communément signalés ont été la faiblesse musculaire (n = 7/44) et la dysphagie (n = 6/44). Conclusions : Dans le cas de patients ayant bénéficié de six traitements ou moins avec l’onabotulinumtoxinA, des événements indésirables ont été signalés chez < 2 % d’entre eux au cours des presque cinq prochaines années. Tirés de MOBILITY, nos résultats apportent une preuve additionnelle que les traitements avec l’onabotulinumtoxinA sont à long terme sécuritaires dans le cas de nombreuses indications thérapeutiques.

Type
Original Article
Copyright
© 2019 The Canadian Journal of Neurological Sciences Inc. 

Background

OnabotulinumtoxinA (BOTOX®) is a purified neurotoxin that acts by blocking presynaptic acetylcholine release, leading to localized reduction of muscle contractions.Reference Aoki1 This unique mechanism of action led to the investigation of therapeutic uses with the toxin, starting with treatment for strabismus.Reference Schantz and Johnson2, Reference Jankovic3 Since then, the broad applicability of onabotulinumtoxinA has been widely recognized and studied and has been used for over 25 years for many therapeutic indications.Reference Jankovic3 More recently, data has illustrated the ability of onabotulinumtoxinA to act not only on efferent pathways but also on afferent pathways, leading to a decrease in pain responses.Reference Aoki and Francis4, Reference Burstein, Zhang, Levy, Aoki and Brin5 In Canada, onabotulinumtoxinA is currently approved for nine therapeutic indications including, but not limited to, blepharospasm, strabismus, cervical dystonia (CD), focal spasticity including the treatment of upper limb spasticity associated with stroke, dynamic equinus foot deformity due to spasticity in pediatric cerebral palsy (CP), and primary hyperhidrosis of the axillae.6 Treatment paradigms with onabotulinumtoxinA vary greatly as recommendations on dose, dilution, and guidance techniques are specific to each indication. In addition to variability in recommended treatment paradigms, it is also known that treatment with onabotulinumtoxinA is individualized and often further varied in real-world clinical practice depending on disease presentation and desired outcomes. Although the highest recommended total adult dose of onabotulinumtoxinA in Canada is 360 U and in the USA is 400 U within a three-month period, reports have shown that doses exceeding this recommendation have been used in actual clinical practice.7, 8 Therefore, it is very important to continue to monitor the safety profile of onabotulinumtoxinA in real-world use.Reference Nuanthaisong, Abraham and Goldman9 Here we report on the safety and treatment parameters during a long-term, multicenter, observational trial, MOBILITY® (NCT00535935), using onabotulinumtoxinA for a variety of therapeutic indications in real-world clinical practice in Canada.

Methods

Study Design and Population

MOBILITY® was a prospective, multicenter, observational Phase IV study conducted in Canada. Patients were enrolled into the study between October 2007 and July 2012 if treatment with onabotulinumtoxinA was determined to be medically necessary. Patients who were new to onabotulinumtoxinA treatment (naive) or those receiving ongoing treatments (maintenance) prior to study entry were included. Patients were consecutively approached, firstly to only the naive patients and then those on maintenance. Participants in the study were men and women ≥14 years of age with no contraindications to use onabotulinumtoxinA and not participating in any onabotulinumtoxinA clinical trial. The safety cohort included all patients who were enrolled in the study and received at least one onabotulinumtoxinA treatment for their condition during the study.

Baseline clinical characteristics and demographics were collected at the initial visit. Safety and tolerability were monitored throughout the study period. Patients received their first onabotulinumtoxinA treatment at the baseline visit and were considered to have completed the study if they completed at least five subsequent treatments (six treatments total). Each participating physician was responsible for managing their own patient’s condition (i.e., starting, stopping, or changing treatment) and for scheduling subsequent treatment visits, as treatments and treatment schedules were not stipulated in the study protocol. All data were collected on standardized case report forms and entered into an electronic database.

MOBILITY® was conducted in accordance with the principles of the Declaration of Helsinki and Good Clinical Practice, and the study protocol was approved by an independent ethics committee at each participating site. All patients were required to provide written informed consent prior to enrollment in the study.

Study Measures

Demographics and clinical characteristics were captured at the baseline visit. Adverse events (AEs) were documented at each subsequent treatment visit throughout the study. An AE was defined as any untoward medical occurrence that was temporally associated with onabotulinumtoxinA, regardless of causality. A serious AE (SAE) was defined as an AE that resulted in death, immediate risk of death (“life-threatening”), required or prolonged an existing hospitalization, persistent or significant disability, or was a congenital anomaly/birth defect. Physicians were required to report any SAE that occurred from the point that informed consent was obtained until 4 weeks after a patient ended study participation. Physicians were also required to report the degree to which an AE was related to onabotulinumtoxinA expressed as definite, probable, possible, unlikely, or unrelated. Additional treatment information, including dosing and injection frequency information, was collected following each treatment session.

Statistical Analyses

Patient demographics and onabotulinumtoxinA treatment information were summarized using descriptive statistics. The frequency and percent of all AEs were reported for the safety population, which included all patients who were enrolled in the study and received at least one onabotulinumtoxinA treatment during the study. Treatment-related AEs (TRAEs) include those reported by the investigator as possible, probable, highly probable, and related. Adverse events considered unrelated include those reported as unlikely and unrelated. MedDRA version 15.1 was used to summarize AEs by system organ class and preferred term.10 The analyses presented here were calculated using SAS® software, version 9.2 (SAS Institute Inc., Cary, NC, USA). There were no hypothesis testing or P-value calculations; however, 95% confidence intervals were provided around estimates of differences. As this project was exploratory in nature, no formal sample size calculations were carried out.

Results

Demographics

A total of 1372 patients were enrolled into the study across 46 participating centers in Canada. All enrolled patients were included in the safety cohort. The majority of patients (n = 866/1372, 63%) were on maintenance onabotulinumtoxinA treatment upon study entry and had received between 1 and 90 treatments of onabotulinumtoxinA prior to entering the study (Table 1). Adult movement disorders (encompassing CD, blepharospasm, and hemifacial spasm [HFS], n = 455/1372) and adult focal spasticity (AFS, n = 452/1372) were the most commonly enrolled diagnoses (both 33%), and cerebral palsy (CP) was the least common (n = 27/1372, 2%). Due to differences in the management of adult versus pediatric CP, adult CP patients were included in the AFS cohort while the CP cohort consisted of pediatric patients between 14 and 18 years old. A total of 150 enrolled patients were grouped under “other” diagnoses, which was mainly comprised of patients diagnosed with focal dystonia, headache, tremor, and pain. Of the 1372 enrolled patients, 519 (38%) completed the five required subsequent visits as indicated in the study protocol, 149 (11%) exited the study with less than the five subsequent visits, and 704 (51%) discontinued the study. Of the patients who discontinued, the proportions of naive (n = 336/704, 48%) and maintenance (n = 368/704, 52%) patients were comparable. The majority of the patients who discontinued the study were due to reasons reported as “other” (n = 363/704, 52%), lost to follow-up (n = 195/704, 28%), and patient withdrawing consent (n = 92/704, 13%). Study discontinuations grouped under “other” included study site closure, investigator study discontinuation, limited availability of resources (i.e., clinic nurse) at the participating clinic, or subject follow-up visits not carried out. Only 6 out of 704 of the discontinued patients (0.9%) were due to AEs, comprising 2 (0.6%) naive and 4 (1.1%) maintenance patients. Among the six patients, only two discontinued the study due to a TRAE (facial paresis/eyelid ptosis and dysphagia).Those who discontinued due to lack of drug efficacy only accounted for 4% (n = 31/704) of the discontinued patient population. Reasons for study discontinuation were similar between naive and maintenance patients and between indications. Patient demographics exhibited some variability across indications, consistent with the range of therapeutic indications treated in this study. The oldest patient population consisted of those who were diagnosed with HFS, whereas the youngest population was of patients with CP (Table 1). Consistent with the youngest population, CP patients reported the lowest weight, height, and body mass index at baseline compared to other indications. However, gender and race distributions were generally comparable between indications with the majority of patients being female (n = 881/1372, 64%) and Caucasian (n = 1253/1372, 91%). Within the maintenance population, HFS, CD, and blepharospasm patients received the most number of onabotulinumtoxinA treatments prior to study entry (1–90 treatments), whereas patients with AFS, CP, and hyperhidrosis received the fewest (1–32 treatments).

Table 1: Patient characteristics stratified by indication and treatment history

AFS = adult focal spasticity; BMI = body mass index; CD = cervical dystonia; CI = confidence interval; CP = cerebral palsy; Diff = difference; HFS = hemifacial spasm; HH = hyperhidrosis; maint = maintenance; NA = not applicable; SD = standard deviation.

a Unless otherwise indicated.

b Difference calculated for naive minus maintenance groups, for means.

c Includes the following that were each ≤5% of the population: Aboriginal, Arab/West Asian, Black, Chinese, Filipino, Japanese, Korean, Latin American, South Asian, Southeast Asian, and/or those categorized as “other,” except for the CP cohort where South Asian accounted for 9% (n = 2) of the maintenance population.

d Number of onabotulinumtoxinA injections received prior to entering the study; maintenance patients only.

The mean (standard deviation) and median doses of onabotulinumtoxinA were 221 U (148). Naive patients generally received lower doses when compared to maintenance, and doses varied widely by indication. For example, CD naive patients received a mean (SD) dose of 173 U (71), whereas maintenance patients received a mean (SD) dose of 248 U (102) (Table 1). Patients who presented with AFS received the highest average (SD) doses (naive: 285 U [147], maintenance: 350 U [149]) during the study, whereas HFS patients received the lowest average (SD) doses (naive: 32.6 U [14.8], maintenance: 42.2 U [27.6]). Dosing remained consistent throughout the study within each indication for treatment naive (Figure 1A) and maintenance (Figure 1B) patients.

Figure 1: Mean administered dose of onabotulinumtoxinA at each treatment visit for (A) naive and (B) maintenance patients. Note: Plot for cerebral palsy cohort not presented due to low patient number; plot for “other” diagnoses not included due to heterogeneity of indications. AFS = adult focal spasticity, CD = cervical dystonia, HFS = hemifacial spasm, SV = subsequent visit, LTV = last treatment visit.

Safety

A total of 209 AEs were reported in 83 patients (83/1372, 6%) in the overall safety cohort (Table 2). Of the 209 AEs, 72 were serious AEs reported in 38 patients (38/1372, 3%). The majority of reported AEs (143/209, 68%) were determined to be unrelated to treatment by the participating investigator. The causalities for 22 reported AEs (22/209, 11%) were not determined or were not reported. Forty-four AEs (44/209, 21%) in 24 patients were reported as TRAEs, of which 10 AEs in 5 patients were reported as being a serious TRAE. Of the 24 patients who reported TRAEs, only 2 (2/24, 8%) patients, representing only 0.15% of the entire safety cohort, discontinued the study (facial paresis/eyelid ptosis and dysphagia).

Table 2: Characteristics of all reported adverse events by indication and treatment history

AE = adverse event; AFS = adult focal spasticity; BMI = body mass index; CD = cervical dystonia; CI = confidence interval; CP = cerebral palsy; Diff = difference; HFS = hemifacial spasm; HH = hyperhidrosis; maint = maintenance.

No AEs were reported in the CP population. Treatment-related AEs include those reported as “related,” “highly probable,” “probable,” and “possible” by the investigator; treatment-unrelated AEs include those reported as “Not related” and “unlikely” by the investigator.

a Each patient is only counted once for each AE category.

b Total number of of AEs reported across all patients. Each patient may be counted more than once.

Among the safety cohort (n = 1372), 13 patients (0.9%) who were naive to onabotulinumtoxinA treatment reported 24/44 TRAEs, whereas 11 (0.8%) maintenance patients had 20/44 TRAEs, as determined by the investigator. The most commonly reported TRAEs across indications were muscular weakness (n = 8/1372, 0.6%) and dysphagia (n = 6/1372, 0.4%). The majority of TRAEs were reported in patients presenting with “other” indications (Table 3). A total of six patients (0.4%) categorized as “other” diagnoses reported 13/44 TRAEs, as assessed by the investigator. Of these six “other” patients, with a diagnosis of focal dystonia (n = 3), headache (n = 1), pain (n = 1), and tremor (n = 1), three commonly reported muscular weakness as an AE. No AEs were reported in the CP cohort. There was one TRAE (herpes zoster in an AFS patient) that was considered to be related to the injection procedure. A total of 14 deaths were reported in the safety cohort, and none were considered treatment related by the investigator. There were no pregnancies or abortions reported during the study.

Table 3: Listing of all treatment-related adverse events by indication as reported by the investigator

AFS = adult focal spasticity; CD = cervical dystonia; CP = cerebral palsy; HFS = hemifacial spasm; HH = hyperhidrosis; maint = maintenance.

No treatment-related AEs were reported in the CP population. Treatment-related AEs include those reported as “related,” “highly probable,” “probable,” and “possible” by the investigator.

a Patients counted once for each listed AE when multiple occurrences were reported. One patient with AFS reported two muscular weakness AEs, and one patient with blepharospasm reported two dysphonia adverse events; however, each was only counted once here.

Although the majority of patients (n = 888/1372, 65%) received a baseline dose of ≥200 U, the frequency of TRAEs was highest in patients administered ≤199 U at baseline (Figure 2). There was no statistically significant association between the incidence of TRAEs and the dose of onabotulinumtoxinA at baseline (Mantel Haenszel Chi-square test, P = 0.0237; Figure 2). When compared across age groups, incidence of TRAEs tended to increase with increasing age; there was a statistically significant association between the incidence of TRAEs and the patient’s age group (Mantel Haenszel Chi-square test, P = 0.002; Figure 3).

Figure 2: Percent of patients who reported treatment-related adverse events by dose administered at baseline. *Mantel Haenzel Chi-square test for association between treatment-related adverse events and onabotulinumtoxinA dose at baseline.

Figure 3: Percent of patients who reported treatment-related adverse events by age at baseline. *Mantel Haenzel Chi-square test for association between treatment-related adverse events and patient’s age group.

Adult Focal Spasticity

Of 452 AFS patients, 17 patients reported 33 AEs (17/452, 4%), of which 8 AEs in four patients (4/452, 0.9%) were considered TRAEs by the investigator. No single AE was reported by more than one AFS patient. The reported TRAEs were equally distributed between naive and maintenance patients, and no apparent trends were observed with regard to treatment pattern. Two patients who received injections of onabotulinumtoxinA 400 U and 500 U, which included injections in the hand, experienced TRAEs of weakness and stiffness in the hand and finger and swelling and pain in the hand that was suggestive of complex regional pain syndrome, respectively.

AFS patients did not report any serious TRAEs. Out of a total of 14 deaths, nine were reported in the AFS cohort, of which four with known etiology were determined to be unrelated to treatment by the investigator (progression of multiple sclerosis, malignant neoplasm, sudden cardiac death, and complications from cardiomegaly/diabetes/pulmonary edema). The cause of death for 4/9 of the fatalities was not specified by the investigators, although for 3 of these patients the investigators did report that the deaths were either not (2 patients), or were unlikely to be (1 patient), related to the study treatment. For the remaining patient (a 71-year-old male), no information on relation to treatment was reported. No serious bleeding events were reported. There were no discontinuations due to TRAEs.

Pediatric Cerebral Palsy

There were no reported AEs in the 27 patients with diagnosed CP who received onabotulinumtoxinA treatments in the study.

Movement Disorders

Of the 455 patients with blepharospasm (n = 83), CD (n = 250), or HFS (n = 122), a total of 136 AEs were reported by 46 (10%; Table 2). Within the blepharospasm and HFS cohorts (n = 205), where facial muscles were injected, seven patients (3.4%) reported a total of 10 TRAEs. Each TRAE was reported by only one patient. There were no major trends in reported TRAEs with respect to treatment history or treatment characteristics.

One serious AE (dysphagia) possibly related to treatment was reported in one maintenance dystonia patient with Meige’s syndrome. The patient received six intramuscular treatments of onabotulinumtoxinA between 147.5 U and 150 U for the maintenance indication, including for blepharospasm and spasmodic dysphonia (the latter being outside of the MOBILITY study; Table 4). One death due to small bowel obstruction in a patient with facial nerve disorder was reported as not related to treatment by the investigator.

Table 4: Characteristics of investigator-reported, treatment-related adverse events

NA = not applicable; NR = not reported.

a Patients counted once for each listed AE when multiple occurrences were reported; patient 2 (AFS) reported two muscular weakness AEs, and patient 6 (blepharospasm) reported two dysphonia adverse events; however, each was only counted once here. An arbitrary patient number is used to identify patients experiencing ≥1 AE.

b Number of injections received prior to and including date of event onset.

c Range of all doses administered prior to and including date of event onset.

d Range of all dilutions used prior to and including date of event onset; calculated as volume of diluent added in mL per 100 units of onabotulinumtoxinA dose administered.

e Symptoms indicated as ongoing at the last treatment visit/end of study.

f Patient treated for Meige’s syndrome, including blepharospasm and spasmodic dysphonia (onabotulinumtoxinA into each thyroarytenoid muscle for spasmodic dysphonia outside of the MOBILITY study).

g Resolved with sequelae.

h Patient treated with onabotulinumtoxinA for pain.

i Patient treated with onabotulinumtoxinA for focal dystonia.

j Patient treated with onabotulinumtoxinA for headache.

k Patient treated with onabotulinumtoxinA for tremor.

In the CD group (n = 250), a total of 95 AEs were reported by 33 (13%) patients (Table 2). In six (2.4%) patients, 12 (13%) of the 95 AEs reported were considered TRAEs by the investigator. More than one TRAE could be reported by a patient, and the most commonly reported TRAEs in the CD group were dysphagia (n = 4/250, 2%) and muscular weakness (n = 3/250, 1%). There did not appear to be any correlation between TRAEs and treatment history or treatment characteristics. A total of eight serious TRAEs were reported in three patients (1%). All patients who reported serious TRAEs were on maintenance onabotulinumtoxinA treatment. One patient with a serious TRAE (dysphagia) subsequently discontinued the study. Two fatal cases were reported, due to bowel infarction and metastases to lung, and both were considered unrelated to treatment.

Hyperhidrosis

Of the 288 patients in the hyperhidrosis cohort, 1 patient (<1%) treated for facial sweating reported a total of three AEs (eyelid ptosis, worsening hyperhidrosis, and facial paresis). The mild facial paresis and eyelid ptosis were the only AEs considered treatment related and appeared to be local effects, likely related to the location of the injection. Both are well-known temporary side effects of this treatment. This patient withdrew from the study.

Other Diagnoses

By definition, in this study patients categorized under “other” diagnoses (n = 150) as classified by investigators presented with focal dystonia, headache, pain, tics, tremors, or multiple indications. These patients reported a total of 33 AEs in 14 out of 150 patients (9%) (Table 2). Of the 33 AEs reported, 13 AEs in 6 out of 150 patients (4%) were reported as TRAEs by the investigator. Muscular weakness was the most commonly reported TRAE (7/44, 17%), which was reported by three patients in the maintenance cohort (Table 3). There did not appear to be any major trend in TRAEs with regard to treatment history or treatment characteristics. One serious TRAE (dysphagia) was reported in one patient who had presented with focal dystonia. Two deaths were reported as unrelated to treatment. One death, due to myocardial infarction, was reported in one patient who had been treated with onabotulinumtoxinA for pain. The second death, due to Parkinson’s disease, was reported in a patient who had been treated for oromandibular dystonia.

Discussion

The purpose of MOBILITY was to examine the long-term safety of onabotulinumtoxinA following multiple treatments across multiple therapeutic indications. MOBILITY is the longest study to date (approximately 5 years) to investigate the safety of onabotulinumtoxinA across multiple therapeutic indications by reporting the incidence rate of AEs in relation to the treatment.

Data were collected from patients who received between one and six treatments of onabotulinumtoxinA. Overall, onabotulinumtoxinA treatment was safe and well tolerated, with few discontinuations due to AEs (n = 6/704, 0.9%) and no new safety signals.

Very Long-Term Utilization and Safety

Patients on maintenance onabotulinumtoxinA treatment had received as many as 90 treatments (mean [SD] = 11 [13]) for over 22 years prior to entering the study and showed no notable differences in the number of TRAEs reported when compared to the naive population, indicating no increased safety risk with chronic use. Earlier reports of long-term safety have agreed with this finding and have even indicated that the incidence of AEs at times decreases with increased treatment duration.Reference Albavera-Hernandez, Rodriguez and Idrovo11, Reference Brashear12 This, of course, is an important observation as these indications are chronic conditions requiring repeat treatments with onabotulinumtoxinA over the long term.

Dosing and Safety

The mean dose administered was 221 U (median, 200 U) of onabotulinumtoxinA, which is reflective of real-world clinical practice (Figure 2). A total of 280 patients were treated with >360 U of onabotulinumtoxinA during the study, and there did not appear to be any correlation between high doses and an increased incidence of TRAEs; indeed, there was no statistically significant association between dose of onabotulinumtoxinA at baseline and the incidence of TRAEs. Overall, from the safety population of 1372 patients, the majority of TRAEs were reported by patients who had received <360 U (within a 3-month period) with only two patients reporting TRAEs following administration of high doses of onabotulinumtoxinA (400 U and 500 U).

In addition to examining the correlation between dose and incidence of AEs, the relationship of age and AEs was explored, as onabotulinumtoxinA is indicated for a variety of diseases spanning a wide range of age groups. The data show an overall trend of increasing incidence of AEs with increasing age. This finding is not unexpected as older patients often suffer from additional comorbidities and associated AEs.Reference Wolff, Starfield and Anderson13

The most commonly reported TRAE in this study was muscular weakness (n = 8/1372, 0.6%) which is consistent with previously published findings, the adverse reactions outlined in the product label, and the known mechanism of action of onaboutlinumtoxinA.Reference Burstein, Zhang, Levy, Aoki and Brin5, 6, Reference Albavera-Hernandez, Rodriguez and Idrovo11, Reference Brashear12, Reference Defazio, Abbruzzese and Girlanda14Reference Russo, Crotty, Miller, Murchland, Flett and Haan17 The reports of muscular weakness are to be expected as onabotulinumtoxinA acts by locally reducing acetylcholine release at neuromuscular junctions. A single incidence was reported as a TRAE considered related to the injection procedure rather than the therapeutic treatment itself. The reported TRAE was herpes zoster in one AFS patient, where symptoms were likely exacerbated by the injection procedure.Reference Gadient, Smith and Ryan18

In addition to the impact of the disease condition on AEs, there is significant heterogeneity in patients with neurological disorders that may also influence incidence of AEs.

Limited safety data are available from long-term, prospective, observational studies with onabotulinumtoxinA. Overall, results from MOBILITY are comparable to existing published reports from studies with similar designs and with the product label.6, Reference Misra, Ehler, Zakine, Maisonobe and Simonetta-Moreau19, Reference Muller, Cugy and Ducerf20

Limitations

Although our study was able to capture long-term safety information across a number of indications in real-world clinical practice, several limitations should be noted. Overall, a large proportion of patients in the safety cohort discontinued the study (n = 704/1372, 51%) for various reasons including “other” (363/704, 52%), comprising mostly study site closure, investigator study discontinuations, or limited availability of resources (i.e., clinic nurse) at the participating clinic; lost to follow-up (195/704, 28%); and patient withdrawal of consent (92/704, 13%). Study discontinuations grouped under “other” were primarily due to study site closure, possibly limiting the generalizability of the findings as data are biased toward those patients who remained in the study. Investigators were required to monitor and report all AEs based on their clinical assessment; however, there was no formalized direct questioning for AEs nor was there any required laboratory testing as may be more typical in a controlled clinical trial. This may mean that all details regarding an AE may not have been captured, including data pertaining to disease severity and comorbidities, which may have helped to further characterize and understand the reported AEs. In addition, reports on concomitant medications were only captured for the condition in which they were being treated with onabotulinumtoxinA; therefore, not all concomitant medication information was captured. Furthermore, information regarding physician experience with administering onabotulinumtoxinA may have been helpful in determining whether there was any correlation to the reported AEs. Similarly, information regarding the specific muscles injected would have been helpful to classify AEs as local or due to the distal spread of the toxin.

Beyond local effects, the distant spread of the toxin is a concern when evaluating the safety of onabotulinumtoxinA treatment. Reports have suggested that botulinum toxin treatment has the potential to spread beyond the local injection site, causing symptoms consistent with botulism.Reference Bakheit, Ward and McLellan21Reference Tugnoli, Eleopra, Quatrale, Capone, Sensi and Gastaldo23 These concerns have been raised by the EMA, FDA, and Health Canada, prompting the inclusion of a warning in product labeling to acknowledge the risk of the effect of the distal spread of toxin.2426 Although the concern is recognized, data regarding the specific muscles injected were not collected in this study, and therefore, we were not able to report whether AEs were possibly due to local or distant spread of the toxin.

Conclusion

In patients with follow-up for up to six treatments, TRAEs were reported in <2% of the safety population over the course of nearly 5 years. Overall, our findings suggest that treatment with onabotulinumtoxinA is safe for long-term use across a variety of therapeutic indications.

Acknowledgements

This study was sponsored by Allergan, Inc. The authors thank Merlin Njoya of McKesson for statistical support; Amy Kuang, PhD, of Allergan plc for writing and editorial support for this manuscript; and Aleksej Zuzek, PhD, of Allergan plc (Irvine, CA) for his critical review of an earlier draft of this manuscript.

Statement of Authorship

All authors met the ICMJE authorship criteria. Neither honoraria nor payments were made for authorship. Conceptualized and designed the study: MB, TW. Designed the data collection instruments: MB. Carried out the initial analysis: MB, TW. Coordinated and supervised data collection: MB, GT, RB, TW. Reviewed and revised the manuscript: TW, MJ, MB, SD, RM, FI, RB, GT. Approved the final manuscript as submitted: TW, MJ, MB, SD, RM, FI, RB, GT.

Conflicts of Interest

TW has received research funds from Allergan plc, has been a member of an advisory board, steering committee, and mentoring program for Allergan plc, and has been a member of advisory boards for Ipsen and Merz. MJ has participated in speaking engagements and advisory boards with Allergan, Merz, Novartis, Abbvie, and Teva and has received research grants from CIHR, AMOSO, MITACS, and NCE. MB is an employee of Allergan. SD was formerly a full-time employee of Allergan plc during the conduct, analysis, and publication of this study. RM has been a member of a scientific advisory committee for Allergan and has been a speaker/consultant for Merz. FI has received honoraria and research funds from Allergan plc and Merz Pharma Canada. RB has no conflicts of interest to declare. GT was a former employee of Allergan plc.

Footnotes

Present address: Sonja Dhani, Purdue Pharma (Canada), Pickering, ON, Canada; Grace Trentin, Akcea Therapeutics Canada, Ottawa, ON, Canada

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Figure 0

Table 1: Patient characteristics stratified by indication and treatment history

Figure 1

Figure 1: Mean administered dose of onabotulinumtoxinA at each treatment visit for (A) naive and (B) maintenance patients. Note: Plot for cerebral palsy cohort not presented due to low patient number; plot for “other” diagnoses not included due to heterogeneity of indications. AFS = adult focal spasticity, CD = cervical dystonia, HFS = hemifacial spasm, SV = subsequent visit, LTV = last treatment visit.

Figure 2

Table 2: Characteristics of all reported adverse events by indication and treatment history

Figure 3

Table 3: Listing of all treatment-related adverse events by indication as reported by the investigator

Figure 4

Figure 2: Percent of patients who reported treatment-related adverse events by dose administered at baseline. *Mantel Haenzel Chi-square test for association between treatment-related adverse events and onabotulinumtoxinA dose at baseline.

Figure 5

Figure 3: Percent of patients who reported treatment-related adverse events by age at baseline. *Mantel Haenzel Chi-square test for association between treatment-related adverse events and patient’s age group.

Figure 6

Table 4: Characteristics of investigator-reported, treatment-related adverse events