Next Article in Journal
Verbal Fluency in Metabolic Syndrome
Previous Article in Journal
Thick Mucus in ALS: A Mixed-Method Study on Associated Factors and Its Impact on Quality of Life of Patients and Caregivers
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
Brain Sciences
Volume 12
Issue 2
10.3390/brainsci12020254
brainsci-logo
Submit to this Journal Review for this Journal Propose a Special Issue
Article Menu

Article Menu

share Share announcement Help format_quote Cite question_answer Discuss in SciProfiles thumb_up
...
Endorse textsms
...
Comment
first_page
settings
Order Article Reprints
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Article

Effectiveness of ACTH in Patients with Infantile Spasms

by
Justyna Paprocka
1,*,
Jakub Malkiewicz
2,
Veronica Palazzo-Michalska
3,
Barbara Nowacka
3,
Mikołaj Kuźniak
3 and
Ilona Kopyta
1
1
Department of Pediatric Neurology, Faculty of Medical Sciences in Katowice, Medical University of Silesia, 40-752 Katowice, Poland
2
Department of Neurology, Faculty of Medical Sciences in Katowice, Medical University of Silesia, 40-752 Katowice, Poland
3
Students’ Scientific Society, Department of Pediatric Neurology, Faculty of Medical Sciences in Katowice, Medical University of Silesia, 40-752 Katowice, Poland
*
Author to whom correspondence should be addressed.
Brain Sci. 2022, 12(2), 254; https://doi.org/10.3390/brainsci12020254
Submission received: 13 December 2021 / Revised: 4 February 2022 / Accepted: 7 February 2022 / Published: 11 February 2022
(This article belongs to the Section Neuropharmacology and Neuropathology)
Versions Notes

Abstract

:
(1) Background: West syndrome is a severe, refractory, epileptic syndrome that usually appears in infancy or early childhood. ACTH is one of the more effective drugs for treating this condition. (2) Aim of the study and methods: The objective of our study was to examine short-term efficacy (during treatment schedule) and long-term outcome of intramuscular 0.02 mg/kg/day ACTH (tetracosactide) depot, used concomitantly with other antiepileptic drugs (AEDs) in patients with infantile spasms who did not achieve seizure cessation or relapse when taking only the AEDs. The drug efficacy was evaluated in retrospective and prospective analyses of 50 patients diagnosed with infantile spasms. (3) Results: Complete cessation of spasms was achieved in 42 cases (84%). EEG improvement was seen in 41 (82%) patients who responded to ACTH therapy. Information on the clinical course of 28 patients was obtained duringlong-term follow-up. In 17 (60.7%) cases, seizures were still present. Normal or near-normal development was observed in 11 out of 28 children (39%). ACTH used concomitantly with other AEDis a highly effective treatment with acceptable side effects. (4) Conclusion: Randomized controlled clinical trialswith long-term follow-up are needed to compare the effectiveness of ACTH in polytherapy and monotherapy. Dyskinesias as a potential side effect observed in our study group should be investigated in the following studies.

1. Introduction

Infantile spasms (IS) is a challenging epileptic syndrome to treat. Its incidence is approximately from 1:4000 to 1:6000 live births [1], constituting 13–14.5% of all cases of infantile epilepsies [2]. It can also be called infantile epileptic encephalopathy since the continuous, disorganized, and arrhythmic electrical activity of neuronal networks may influence brain maturation, cause arrest or regression of previously gained functions, or make infant milestones impossible to achieve [2]. Infantile spasms consist of three features: epileptic spasms, developmental arrest or regression, and hypsarrhythmia—an interictal EEG pattern. However, not all of them must be present. Hypsarrhythmia together with epileptic spasms in clusters are obligatory features to diagnose West syndrome (WS), according to the West Delphi Proposal, but some studies use the terms West syndrome and infantile spasms as synonyms. Neurodevelopmental arrest or regression before the onset of spasms is not required for the diagnosis of WS by the aforementioned Proposal [3]. This epileptic disorder occurs most frequently within 12 months of life, with a peak between 4 and 7 months. However, cases with later onset have been reported [4].
Epileptic spasms are brief contractions (flexions, extensions, or mixed) of the neck, trunk, and upper and lower limbs or head nodding, occurring in clusters, frequently on awakening. They last about 1–2 s and are followed by a tonic phase lasting up to 10 s [3,5]. Their origin is either focal, generalized, or both; thus, they can have a symmetrical or asymmetrical form. Subtle spasms may also occur in the course of this condition. They are easily overlooked and take the form of yawning, gasping, eye deviation, facial grimacing, or focal motor activity. They are associated with hypsarrhythmia [3]. Although the definition of hypsarrhythmia has not been established by the West Delphi Proposal [3], some authors define it as an interictal EEG pattern, which is characterized by continuous, asynchronic, disorganized background of high-amplitude, slow waves and coexisting multifocal spikes, polyspikes, sharp waves, and spike-waves [6]. Hypsarrhythmia is not always present in patients suffering from infantile spasms, and it can be modified/atypical depending on the stage of brain development and physiologic situations, such as sleep/wakefulness, treatment with AED, and etiology [6].
Classifications regarding etiology have been established, including the 1989 International League Against Epilepsy division into two subgroups: symptomatic and cryptogenic [7]. The first one means that etiology is known, or previous signs of brain damage, such as psychomotor retardation, neurologic signs, radiologic signs, or other types of seizures, have been present. The latter one means that signs of previous brain damage have been absent, and etiology has not been identified during medical examinations [7]. Many studies prove that cryptogenic patients have a better response to ACTH treatment, and their neurodevelopmental outcome is also more favorable [5,8,9,10,11,12]. Nowadays, according to the ILAE 2017 classification, etiologies are more precisely divided into structural, infectious, genetic, metabolic, immune, and unknown [13].
ACTH, vigabatrin, and corticosteroids are effective and commonly used in infantile spasms [4,14]. There are also some limited data about other non-standard treatment options, such as topiramate, levetiracetam, zonisamide, sodium valproate, benzodiazepines, pyridoxine, and dietary treatments, which seem to be especially promising for topiramate and ketogenic diet [4,14,15]. On the other hand, using non-standard therapies as a first-line treatment was associated with worse response rate [16,17]. There is also evidence that shorter lead time to effective treatment results in better developmental outcome [9,11].
The aim of the study was to assess the short-term efficacy (during treatment schedule) and long-term outcome of intramuscular 0.02 mg/kg/day ACTH (tetracosactide) depot, used concomitantly with other antiepileptic drugs in patients with infantile spasms who did not achieve seizure cessation or relapse when taking only the AEDs.

2. Materials and Methods

2.1. Patient’s Characteristics

Fifty children (29 male, 21 female) diagnosed with infantile spasms were included in the study. The age at the onset of epileptic spasms varied between 1 and 11 months, while the mean was 5.2 ± 2.2 months. The age at the onset of ACTH therapy was 8.6 (6–9) months. According to the ILAE classification, 41 (82%) patients could be classified as symptomatic. A detailed presentation of patients with known etiology is shown in Table 1. Other types of seizures prior to the onset of epileptic spasms were present in 17 (34%) patients, and developmental delay was observed during hospitalization in 45 children (90%, the first developmental evaluations were performed at onset in hypsarrhythmic state), microcephaly in 13 (26%), and dysmorphic features in 17 (34%). The family history was relevant in the case of 10 (20%) patients. Ten (20%) patients were born preterm. Abnormalities in MRI were present in 35 cases (70%).

2.2. Study Pattern

This study was conducted by a retrospective and prospective analysis of patients hospitalized in the Department of Pediatric Neurology of the Medical University of Silesia in Katowice diagnosed with infantile spasms who were admitted between March 2009 and September 2017. Table 2 shows the onset of epilepsy depending on presence or absence of hypsarrhythmia. Patients who were not treated with ACTH were excluded from the study. ACTH was not the first-line treatment in this population and was used concomitantly with other antiepileptic drugs. AEDs taken by the participants of the study during and before the onset of tetracosactide therapy were noted. Tetracosactide was used at a dose of 0.02 mg/kg/d for two weeks and tapered to zero over the next 4 or 6 weeks—the exact treatment schedule is presented in Section 3 (Table 3). Patients with treatment lasting 6 weeks had the same schedule without the last 2 weeks with one dose per week. The time of ACTH administration was shortened to 5 weeks in one patient because she was qualified for the neurosurgical operation of hypothalamic hamartoma.
Video EEG was taken in all patients. Video EEG and EEG were performed at two-week intervals and after the end of ACTH treatment. Improvement of EEG recording in patients with hypsarrhythmia meant its withdrawal and, in other cases, reduction of paroxysmal changes and their amplitude and the dominance of slow theta and delta waves.
As far as the causes of epilepsy are concerned, patients were categorized according to the 2017 ILAE classification as structural, genetic, infectious, metabolic, immune, and unknown. Some patients could be classified into more than one category. The primary clinical outcome was cessation of spasms, defined as the lack of observed seizures until the 14th day of ACTH treatment, and a seizure-free interval during hospitalization. Patients who achieved cessation of epileptic spasms did not have seizures for 28 consecutive days or more from the last witnessed seizure.

2.3. Statistical Analyses

Continuous variables were expressed as the mean ± standard deviation or median (lower quartile-upper quartile), when distribution was not normal. Shapiro–Wilk test and Q-Q plots were used to test normality. Categorical variables were presented as numbers and percentages using Open Office (Apache Open Office 4.1.2 Copyright 2015 The Apache Software Foundation). Continuous data were compared by means of the Mann–Whitney U test. To compare the categorical variables in the short- and long-term outcome, the chi-square test with Yates’s correction and Fisher’s exact probability test were used, respectively. The data were compared using Statistica 12 (Tulusa, OK, USA). Statistical significance was defined as p < 0.05.

2.4. Treatment Schedule

All patients took at least one AED prior to tetracosactide, and they did not achieve cessation of spasms or had recurrence of epileptic spasms when they started ACTH therapy. The time from diagnosis of epilepsy to administration of the first AED was longer than 30 days in 7 symptomatic patients. The average time lag between the onset of epileptic spasms and the beginning of ACTH therapy was 1.5 (1–3) months. ACTH was used with many other AEDs as add-on therapy. The median number of drugs used prior to tetracosactide was 3.66 ± 1.85 (Table 4). Some patients were undergoing discontinuation of other AEDs when they started ACTH therapy. The following drugs were used during the first two weeks of ACTH therapy:valproate in 41 (82%) patients, vigabatrin in 36 patients, levetiracetam in 9 patients, clobazam in 8 patients, clonazepam in4 patients, phenobarbital in 2 patients, lamotrigine in 2 patients, and topiramate in 2 patients. The mean number of drugs used during ACTH treatment was 2.06.
Twenty-five (50%) patients used the two most common drugs—both vigabatrin and valproic acid at the same time. During the whole period of ACTH therapy, the children were hospitalized.

3. Results

Complete cessation of spasms was achieved in 42 cases out of 50 children (84%) withcombined antiepileptic therapy (ACTH and AEDs). Among children who responded to ACTH, 20 were with hypsarrhythmia. EEG improvement was seen in 41 (82%) patients. Improvement of EEG recording in patiets with hypsarrhytmia meant its withdrawal and, in other cases, reduction of paroxysmal changes and their amplitude and the dominance of slow theta and delta waves. A substantial reduction (75%) in the frequency of seizures was present in five patients (10%). Two of them were seizure-free after 2 weeks of treatment but had recurrence of seizures during a tapering-off period. In patients with genetic etiology, therapy was effective in 5/8 (62.5%) patients. The treatment failed in one patient with tuberous sclerosis (TSC), one with a mitochondrial disease, and one with microdeletion 2q24.4. Efficacy in patients with structural etiology other than TSC was 17/20 (85%). In this group, the treatment was effective in 10/11 patients (91%) with HIE, 5/7 (72%) with cerebral malformations, one patient with two possible causes of epilepsy, and one patient with postinfectious changes. In patients with unknown etiology, the therapy was effective in 20 patients (91%), including all patients who could be classified as cryptogenic according to the previous ILAE classification. A total of 80.5% of patients previously classified as symptomatic had cessation of spasms. The differences between cryptogenic and symptomatic patients in the chi-square test were not statistically significant (p = 0.345) (using of terms symptomatic and cryptogenic, although not recommended by ILAE, allow for better comparison with previous study). There were also no statistically significant differences between the children with known and unknown etiology (p = 0.427). Gender did not have any influence on cessation of seizures (p = 0.501).

3.1. Adverse Events during ACTH Treatment

There was no case of death during ACTH therapy. The most common adverse events during treatment and taper were infections (respiratory tract, urinary system, gastrointestinal), N = 26 (52%). Most of them were mild and did not have an impact on the epilepsy treatment. Antibiotics were used in 19 (38%) patients. In six (12%) patients, stereotyped dyskinesia (usually of the facial region: oral buccal) was observed. These movement disorders stopped gradually within a month of discontinuation of ACTH treatment. Arterial hypertension was present in five (10%) patients. Hypertension had been diagnosed by cardiologist, who made the decision of temporary use of blood pressure-lowering drugs. In all patients, the blood pressure values returned to normal after completion of the steroid therapy.
Hypokalemia was noted in four (8%) patients.

3.2. Follow-Up

Information on the clinical course of 28 patients was obtained during phone follow-up. The study was conducted between June and September 2017. We focused on the presence or absence of seizures (not only IS), drug therapy, and development.
The average follow-up was 37 ± 24.4 months. Table 5 shows the duration of follow-up.
In 17 (60.7%) cases, seizures were still present. Among patients without seizures, six children were classified as cryptogenic, and five children (23%) were recognized as symptomatic (three children were diagnosed with mitochondrial encephalopathy, one with neurofibromatosis type 1, and one with microdeletion 2q24.4). There was not any significant difference related to gender (p = 1.0).
Twenty-seven children (97%) were still on anti-epileptic therapy. Most commonly used were valproate, vigabatrin, and levetiracetam in 20, 14, and 12 patients, respectively. Moreover, in 18 cases, valproate was in combination with other drugs: in 10 children, vigabatrin; in 8 cases, levetiracetam; in 3 cases, clobazam; in 3 cases, clonazepam; in 2 children, topiramate; and in 1 case, lacosamide.
Normal or near-normal development was observed in 11 out of 28 children (39%).The clinical outcomes of all 28 cases and the comparison of symptomatic and cryptogenic patients are shown in Table 6.

4. Discussion

The mechanism of action of ACTH is still unknown. Treatment with ACTH may reduce neuronal excitability by lowering the production and release of CRH and by directly affecting limbic neurons via melanocortin specific receptors, mainly MC1R and MC3R [1,2,3,4,5,6,7,8,9,10,11,12]. Randomized, controlled hormonal-treatment trials in West syndrome/epileptic spasms are shown in Table 7.
In this study, we present high short-term efficacy of ACTH used concomitantly with other AEDs in a group of patients with IS who did not achieve cessation of seizures or relapsed when taking other AEDs. Monitored adverse events were common (especially infections) but acceptable, and they did not require ACTH discontinuation. Dyskinesia occurred in six (12%) patients. In follow-up, effects were better in cryptogenic patients.
Adverse events in randomized, controlled trials, in which at least one group used hormonal treatment, and were published after 2010 are listed in Table 7.
Using ACTH in polytherapy is an interesting approach, and some studies suggest that it can be more effective than monotherapy in infantile spasms treatment [18,19,20]. A randomized, multicenter, open-label trial provided evidence that hormonal therapy (tetracosactide, prednisolone) and vigabatrin are more effective than hormonal therapy alone during four weeks of observation [18]. A randomized, open-label study from China also suggested that ACTH in polytherapy with MgSO4 has a better effect than ACTH monotherapy in 24 weeks of follow-up [19]. Prospective study at Severance Children’s Hospital also demonstrated the potential of a treatment protocol using polytherapy(vigabatrin and prednisolone) for West syndrome [20]. Other studies also showed that initial polytherapy with ACTH and other AED or topiramate followed by low-dose ACTH are effective and well-tolerated options in IS [21,22,23]; however, it is worth noting that the randomized, open-label, controlled trial denied the effectiveness of combination of hormonal therapy(prednisone) and moderate dose of to piramate [24].
In our study, short-term efficacy seems to be high in comparison with the results from randomized studies from the last ten years (Table 6) [18,19,24,25,26,27,28,29,30,31,32,33,34].
The number of patients with cessation of IS in our study is very similar to the groups using hormonal treatments in combination with other drugs [18,19,20,35]. Relatively good short-term efficacy of the add-on ACTH polytherapy in our study might be associated with cumulative effects of different drugs suggested by the previously mentioned studies, especially vigabatrin, which was taken by most patients [18,19,20,35]. Valproate was also commonly used in our study and might have had an important role in the reached outcome, but there are limited data about its efficacy in IS [14,36]. In addition, clobazam used in our study might be a potentially effective adjunctive drug for West syndrome [37]. It is worth mentioning that similar results were reached in some old studies in the case of high-dose ACTH monotherapy and combination of low-dose ACTH and pyridoxine [23,38]. According to some authors, increasing the dose of ACTH does not necessarily result in better seizures control [39].
However, on the other hand, we would not favor polytherapy because of the risk of serious adverse effects (e.g., potential hepatotoxicity in infancy). There is also no proven evidence of effectiveness of polyteraphy in infantile spasms. Based on observation, we would like to stress that it is worthwhile to start ACTH even after refractory spasms and relapses and even after a long delay.
Monitored adverse events reported in this study were relatively mild, and they did not require discontinuation of treatment (Table 8).
Table
Table 7. Randomized, controlled hormonal-treatment trials published after 2010.
Table 7. Randomized, controlled hormonal-treatment trials published after 2010.
StudyTherapyNo.
of Patients		EtiologyCessation of
Seizures Rate (%)
Zou 2010 [19]ACTH 25 U/d and MgSO4 0.25 g/kg/d
3 weeks		19Cryp. 3 (16%)
Symp. 16 (84%)		1st week, 42%
2nd week, 53%
4th week, 63%
8th week, 79%
12th week, 74%
24th week, 63%
ACTH 25 U/d
3 weeks		19Cryp. 2 (11%)
Symp. 17 (89%)		1st week 5%
2nd week 21%
4th week 42%
8th week 53%
12th week, 47%
24th week, 53%
Chellamuthu et al., 2014 [28]Oral prednisolone 2 mg/kg/d32Known, 27 (84%)
Unknown, 5 (16%)		14 days, 25%
Oral prednisolone 4 mg/kg/d31Known 26 (84%)
Unknown 5 (16%)		14 days, 51.6%
Wanigasinghe 2015 [29]
Wanigashingasighe
2017 [30]		Corticotropin 0.5–0.75 mg (40 IU)/2 d
2 weeks and taper		49Known 68%
Unknown 24%
Incomplete evaluation 7%		14 days, 37%
42 days, 41%
3 months, 39%
6 months, 45%
12 months 41%
Oral prednisolone
40–60 mg/d
2 weeks and taper		4814 days, 58%
42 days, 67%
3 months, 65%
6 months, 58%
12 months, 56%
O’Callaghan et al., 2017 [18]
O’Callaghan et al., 2018 [31]		Prednisolone 40–60 mg/d or tetracosactide 0.5–0.75 mg (40 IU)/2 d
2 weeks and taper
Vigabatrin 50–150 mg/kg/d
3 months and taper		186Known, 219 (58%)
Unknown, 158 (42%)		14 days 89%
42 days, 72%
At age 18–19 months, 70%
Prednisolone 40–60 mg/d or tetracosactide 0.5–0.75 mg (40 IU)/d
2 weeks and taper		19114 days 69%
42 days, 57%
At age 18–19 months, 71%
Kunnanayaka V. 2018 [32]Prednisolone 4 mg/kg/d32Known, 27 (84%)
Unknown, 5 (16%)		14 days 37.5%
1 month, 25%
Prednisolone 4 mg/kg/d and 30 mg/kg/d pyridoxine30Known, 26 (86%)
Unknown, 4 (14%)		14 days, 37%
1 month, 33%
ZhaoshiYi
et al., 2019 [24]		Prednisone 4 × 10 mg/d a39Known 25 (64.1%)
Unknown 14 (35.9%)		14 days 71.8%
120 days 61.5%
Prednisone 4 × 10 mg/ a and TPM gradually titrated from 1 mg to 5 mg in 14 day/kg/d b38Known 23 (60.5%)
Unknown 15 (39.5%)		14 days 76.3%
120 days 50.0%
Angappan et al., 2019 [33]Tetracosactide 30–60 IU/d, the dose increasing every 2–3 days by 10 IU and taper15Structural 12 (80%)
Non-structural 3 (10%)		2 weeks till 6 weeks 40%
Oral zonisamide 4–25 mg/kg/day15Structural 100%2 weeks till 6 weeks 27%
Gowda et al., 2019 [34]ACTH 100 IU/body surface area/d18Symp 14 (77.77%)
Idiop 1 (5.55%)
Cryp. 3 (16.66%)		14 days 50%
28 days 61.11%
PRDL 4 mg/kg/d for 2 weeks, then tapered over 3–4 weeks)16Symp 13 (81.25%)
Idiop 0 (0%)
Cryp. 3 (18.75%)		14 days 33.33%
28 days 40%
Dressler et al., 2019 [25]ACTH 150 IU/m2 for 2 weeks and taper16Known 11 (69%)
Unknown 5 (31%)		24 month 44%
Ketogenic diet16Known 7 (44%)
Unknown 8 (66%)		24 month 38%
Fayyazzi et al., 2020 [26]ACTH 0.1 mg/d16Known 25 (78%)
Structural 17 (53%)
Unknown 7 (22%)		c
ACTH 0.25 mg/d d16c
Imannezhad et al., 2020 [27]ACTH 5 × 2–3 IU/kg/d (max: 100 IU)25N.A.14 days 69.2%
Prednisolone 8 mg/kg/d (max: 60 mg) e2614 days 76%
a If spasm still occurred on day 7, the dose was changed; it reached 15 mg once and was kept at this level for the next 14 days, four times each day. Whether the spasms hadstopped or not, after these 14 days, the dose of prednisone was decreased every week until completing a 49-day or 56-day course (e.g., 40 mg one time a day for a week or 30 mg one time a day for a week, 20 mg one time a day for a week, 10 mg one time a day for a week, 5 mg one time a day for a week, and finally, 5 mg every two days for a week). b Additionally, the combination therapy group used TPM at an initial dose of 1 mg/kg/day twice a day, then gradually increased it to 3 mg/kg/day on day 7 and 5 mg/kg /day on day 14. c No further medications were needed at the end of the therapeutic protocol since symptoms, such as convulsions and spasm, were fully controlled in 18.7% of patients. Apart from ACTH, another medicine was given to 5.37% of patients to fully control the convulsions. Using another drug helped 25% of patients with controlling, to some extent, theoccurring convulsions and spasms. The mentioned symptoms were resistant to treatment in 3.9% of patients despite concomitant treatment with ACTH and several other drugs. There was no significant change in any of the four levels defined for controlling spasms and convulsions. d The method of ACTH administration: 1st week, one time a day; 2nd week, once every second day; 3rd week, two times a week; 4th week, one weekly; and 5th to 8th week, once every two weeks. Increase daily dose if the patient was not responsive after two weeks; 14 days of therapy, and then, the dose was tapered off over the remaining two weeks. e A dose of 8 mg/kg/day of prednisolone (max: 60 mg) was administrated to patients who belonged to the corticosteroid group. It was used for three weeks, divided into three doses. Later, the dose was decreased in responders. Two weeks later, non-responders were given 2–3 U/kg/day of ACTH (max: 100 U) for five days. If the patients did not show signs of improvement within two weeks of treatment, they were planned to receive intramuscular biologic ACTH immediately after the failure of corticosteroid therapy. The patients received five daily doses of 2–3 IU/kg of ACTH (max: 100 IU), and the treatment was then changed to the oral corticosteroid. In the second group (25 patients), patients first received five daily doses of 2–3 IU/kg of ACTH.
Table
Table 8. Adverse events in randomized, controlled trials, in which at least one group used hormonal treatment, and were published after 2010, which were found in bases PubMed, Google Scholar, and Embase. Studies about including patients without IS are not presented in the table.
Table 8. Adverse events in randomized, controlled trials, in which at least one group used hormonal treatment, and were published after 2010, which were found in bases PubMed, Google Scholar, and Embase. Studies about including patients without IS are not presented in the table.
StudyTherapy 1Therapy 2
Adverse EventsNo (%)Adverse EventsNo (%)
Zou 2010 [19]ACTH 25 U/d and MgSO4 0.25 g/kg/d
3 weeks
(19) *		ACTH 25 U/d
3 weeks
(19) *
Pyrexia3 (15.8)Pyrexia3 (15.8)
Upper respiratory tract infection3 (15.8)Upper respiratory tract infection3 (15.8)
Diarrhea2 (10.5)Diarrhea2 (10.5)
Anorexia1 (5.3)Anorexia1 (5.3)
Vomiting0 (0)Vomiting1 (5.3)
Hypertension2 (10.5)Hypertension0 (0)
Insomnia2 (10.5)Insomnia0 (0)
Irritability2 (10.5)Irritability0 (0)
Decreased heart rate, prolonged PR interval1 (5.3)Decreased heart rate, prolonged PR interval0 (0)
Chellamuth et al., 2014 [28]Oral prednisolone 2 mg/kg/d
(32) *		Oral prednisolone 4 mg/kg/d
(31) *
Weight gain4 (12.5)Weight gain9 (29)
Hypertension1 (3.12)Hypertension0 (0)
Cushingoid facies7 (22.6)Cushingoid facies13 (41.9)
Infections6 (18.7)Infections9 (29)
Irritability3 (9.4)Irritability2 (6.5)
Increased appetite2 (6.3)Increased appetite4 (12.9)
Glycosuria0 (0)Glycosuria0 (0)
Others2 (6.3)Others1 (3)
Wanigasinghe 2015 [29]
Wanigassighe 2017 [30]		Oral prednisolone
40–60 mg/d
2 weeks and taper
(48) *		Tetracosactide
0.5–0.75 mg (40 IU)/2 d
2 weeks and taper
(49) *
Increased appetite28 (73.7)Increased appetite19 (43.2)
Weight gain19 (50)Weight gain14 (31.8)
Frequent crying spells16 (42.1)Frequent crying spells11 (25)
Drowsiness4 (10.5)Drowsiness7 (15.9)
Cushingoid features8 (21.1)Cushingoid features9 (20.5)
Insomnia3 (7.9)Insomnia2 (4.5)
Lethargy2 (5.3)Lethargy2 (4.5)
Reduction in social behavior2 (5.3)Reduction in social behavior1 (2.3)
Abdominal distension8 (21.1)Abdominal distension0 (0)
Hypertension1 (2.6)Hypertension1 (2.3)
Increased susceptibility to infection0 (0)Increased susceptibility to infection1 (2.3)
Irritability8 (21.1)Irritability5 (11.4)
Nausea1 (2.6)Nausea1 (2.3)
Vomiting2 (5.3)Vomiting1 (2.3)
Diarrhea2 (5.3)Diarrhea3 (6.8)
Dyspepsia2 (5.3)Dyspepsia2 (4.5)
Electrolyte imbalances2 (5.3)Electrolyte imbalances0 (0)
O’Callaghan et al., 2017 [18]
O’Callaghan et al., 2018 [31]		Prednisolone 40–60 mg/d or
tetracosactide 0.5–0.75 mg (40 IU)/d
2 weeks and taper
(191) *		Prednisolone 40–60 mg/d or
tetracosactide 0.5–0.75 mg (40 IU)/2 d
2 weeks and taper
Vigabatrin 50–150 mg/kg/d
3 months and taper
(186) *
Allergic rash or
anaphylaxis		1 (1)Allergic rash or
anaphylaxis		0 (0)
Drowsiness3 (2)Drowsiness45 (24)
Endocrine or metabolic disturbance2 (1)Endocrine or metabolic disturbance1 (1)
Fluid or
electrolyte disturbance		23 (12)Fluid or
electrolyte disturbance		12 (6)
Gastrointestinal upset26 (14)Gastrointestinal upset23 (12)
Hypertonia9 (5)Hypertonia3 (2)
Hypotonia8 (4)Hypotonia7 (4)
Immunosuppression3 (2)Immunosuppression3 (2)
Increased appetite51 (27)Increased appetite35 (19)
Infection19 (10)Infection14 (8)
Irritability75 (39)Irritability61 (33)
Neuropsychiatric (disturbed sleep)35 (18)Neuropsychiatric (disturbed sleep)29 (16)
Varicella zoster (chicken pox)4 (2)Varicella zoster (chicken pox)2 (1)
Weight gain34 (18)Weight gain24 (13)
Abnormal eye movements0 (0)Abnormal eye movements1 (1)
Blood disorder (high platelet count)0 (0)Blood disorder (high platelet count)1 (1)
Bradycardia0 (0)Bradycardia1 (1)
Abnormal breathing pattern1 (1)Abnormal breathing pattern0 (0)
High MRI signal in basal ganglia1 (1)High MRI signal in basal ganglia2 (1)
Hypoxia1 (1)Hypoxia0 (0)
Movement disorder2 (1)Movement disorder14 (8)
Not focusing (vision)0 (0)Not focusing (vision)1 (1)
Obstructive cardiac hypertrophy1 (1)Obstructive cardiac hypertrophy0 (0)
Pallor1 (1)Pallor0 (0)
Squinting1 (1)Squinting0 (0)
Sweating1 (1)Sweating1 (1)
Tachypnoea1 (1)Tachypnoea0 (0)
Kunnanayaka V 2018 [32]Prednisolone 4 mg/kg/d
(32) *		Prednisolone 4 mg/kg/d and 30 mg/kg/d pyridoxine
(30) *
Increased appetite25 (78)Increased appetite24 (75)
Irritability19 (59)Irritability12 (40)
Excessive daytime sleepiness21 (66)Excessive daytime sleepiness20 (67)
Cushingoid facies5 (16)Cushingoid facies4 (13)
Oral ulcers4 (13)Oral ulcers6 (20)
Weight gain5 (16)Weight gain4 (13)
ZhaoshiYi et al., 2019 [24]Prednisone 4 × 10 mg/d
(39) *		Prednisone 4 × 10 mg/and TPM gradually titrated from 1 mg to 5 mg in 14 day/kg/d
(38) *
Cushing’s symptoms34 (87.2%)Cushing’s symptoms32 (84.2)
Increased appetite35 (89.7)Increased appetite29 (76.3)
Irritability18 (46.2)Irritability12 (31.6)
Drowsiness8 (20.5)Drowsiness7 (18.4)
Intercurrent infection11 (28.2)Intercurrent infection12 (31.6)
Hypertension1 (2.6)Hypertension0 (0.0)
Sleep disturbance9 (23.1)Sleep disturbance7 (18.4)
Angappan et al., 2019 [33]Tetracosactide 30–60 IU/d, the dose increasing every 2–3 days by 10 IU and taper
(15) *		Oral zonisamide 4–25 mg/kg/day
(15) *
Hypertension14 (93.3)Lethargy8
Weight gain5 (33.3)Irritability5 (33.3)
Cushingoid faces3 (20)Gastroenteritis2 (13.3)
Irritability3 (20)Dryness of skin and mouth1 (6.7)
Infection2 (13.3)Loss of appetite1 (6.7)
Hyperpigmentation1 (6.7)Metabolic acidosis1 (6.7)
Gowda et al., 2019 [34]ACTH 100 IU/body surface area/d
(18) *		PRDL 4 mg/kg/d for 2 weeks, then tapered over 3–4 weeks)
(16) *
Side effects in general3 (16.6)Side effects in general3 (20)
Dressler et al., 2019 [25]ACTH 150 IU/m2 a 2 weeks and taper
(48) *		Ketogenic diet
(53) *
Adverse effects overall45 (94)Adverse effects overall42 (79)
Needing acute intervention45 (94)Needing acute intervention16 (30)
Hypertonia41 (85)High triglycerides16 (30)
Potassium (intravenous)19 (40)Obstipation14
Cushing syndrome17 (35)Ketones > 5 mmol L−113
Cardiac hypertrophy16 (33)Solid food refusal9
Leukocytosis16 (33)Liquids (intravenous)7
Infections14 (29)Infections6 (11)
Hyperexcitability12 (25)Diarrhea6 (11)
Acne12 (25)High cholesterol5 (9)
Weight gain11 (23)Growth deficit5 (9)
Drowsiness8 (17)Cholecystolithiasis5 (9)
Edema8 (17)Tiredness at start3 (6)
--Hypoglycemia3 (6)
--Carnitine deficiency3 (6)
--Weight loss3 (6)
--Refusal of KD liquids3 (6)
--Weight gain1 (2)
Fayyazzi et al., 2020 [26]ACTH 0.1 mg/d
(16) *		ACTH 0.25 mg/d
(16) *
N.AN.AN.AN.A
Imannezhad et al. 2020 [27]ACTH 5× 2-3IU/kg/d(max: 100 IU)
(25) *		Prednisolone 8 mg/kg/d(max: 60 mg)
(26) *
N.AN.AN.AN.A
* Number of patient
Dyskinesia is a newly reported side effect of hormonal treatment. In this study, six (12%) patients had a dyskinesia similar to that previously reported [40,41]. Many patients in this study took vigabatrin, and movement disorders might be also potentially associated with vigabatrin [42,43]. In ICISS, the group treated with the combination of hormonal therapy and vigabatrin had higher rate of movement disorders than the group taking hormonal therapy alone [18]. In ten investigated patients enrolled in ICISS, eight of them had movement disorders after initiation of vigabatrin, but they resolved after vigabatrin withdrawal only in two patients. Seven of them also took hormonal treatment during the onset of the movement disorders [42]. Due to the ICISS report, mentioned movement disorders were not linked to vigabatrin, and they were likely caused by an underlying neurological disease [18].
In our study, the number of patients with a developmental delay and seizures in a long-term perspective was significantly lower in cryptogenic patients, which is consistent with previous studies [8,9,10,11,12,31]. In total, 39% of them were seizure free, and among them, all were cryptogenic patients (100%), and 22.7% were symptomatic patients. This result resembles long-term outcome in other studies; however, some treatment options used in the studies presented in the Table 6 resulted in better long-term outcome, which can be caused by differences in methodology and time of observation [11,19,25,26,27,29,30,33,34,44]. Cryptogenic patients seem to have slightly better and symptomatic slightly worse seizure outcome than patients from UKISS and the observational multicenter Belgian study by Mert et al. [10,11,12]. Development was normal or near normal in 39% of patients—83% cryptogenic and 27% symptomatic patients. According to the meta-analysis and systematic review published in 2015, 54.3% of cryptogenic and 12.5% of symptomatic patients with IS had normal or near-normal developmental outcome [9]. In the context of these data, the developmental outcome in our study seems to be good. On the other hand, there is a possibility that assessment of development was stricter in other studies. Shorter time to treatment results in better developmental outcome, especially in cryptogenic patients [8,9,31,45]. Good developmental outcome among cryptogenic patients in our study might be also associated with short lead time to treatment in this group of patients.
It should be mentioned that according to the latest meta-analysis, high-dose prednisolone is not inferior to adrenocorticotrophic hormone [46,47]; indeed, ACTH is less cost-effective, defined as probability of clinical spasm resolution 14 days after treatment initiation, than oral prednisolone (in the United States) [48].
Our study has some weakness and limitations. The first is a partially retrospective character. Others are an inaccessibility of almost half of patients for follow-up and differences in time of follow-up for particular patients. The follow-up method, phone interview, might be less accurate than direct clinical assessment. The study did not assess some ACTH adverse events. This study is not a clinical trial but only a description of experience from our clinic. There was not a control group, so it does not allow for making an accurate comparison for different used drugs or approaches in infantile spasms treatment; it only assesses effectiveness of the add-on ACTH therapy in this group of patients.

5. Conclusions

ACTH used concomitantly with other AED is a highly effective treatment with acceptable side effects. In accordance with other studies, the long-term outcome was better throughout cryptogenic patients. Randomized, controlled, clinical trials with long-term follow-up are needed to compare effectiveness of ACTH in polytherapy and monotherapy. Dyskinesias as a potential side effect observed in our study group should be investigated in future studies.

Author Contributions

Conceptualization, J.P.; methodology, J.P.; J.M.; V.P.-M.; B.N.; M.K.; software, J.P.; J.M.; V.P.-M.; B.N.; M.K.; validation, J.P.; J.M.; V.P.-M.; B.N.; M.K.; formal analysis, J.P.; J.M.; V.P.-M.; B.N.; M.K.; investigation, J.P.; J.M.; V.P.-M.; B.N.; M.K.; resources, J.P.; J.M.; V.P.-M.; B.N.; M.K.; data curation, J.P.; J.M.; V.P.-M.; B.N.; M.K.; writing—original draft preparation, J.P.; J.M.; V.P.-M.; B.N.; M.K.; writing—review and editing, J.P.; J.M.; V.P.-M.; B.N.; M.K.; visualization, J.P.; J.M.; V.P.-M.; B.N.; M.K.; supervision, J.P.; I.K.; project administration, J.P.; funding acquisition, J.P. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

The study was conducted according to the guidelines of the Declaration of Helsinki.

Informed Consent Statement

Informed consent was obtained from all subjects involved in the study.

Data Availability Statement

The data analyzed during the current study are available from the corresponding author on reasonable request.

Conflicts of Interest

The authors declare no conflict of interest.

References

  1. Fois, A. Infantile spasms: Review of the literature and personal experience. Ital. J. Pediatr. 2010, 36, 15. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  2. Wilmshurst, J.M.; Gaillard, W.D.; Vinayan, K.P.; Tsuchida, T.N.; Plouin, P.; Van Bogaert, P.; Carrizosa, J.; Elia, M.; Craiu, D.; Jovic, N.J.; et al. Summary of recommendations for the management of infantile seizures: Task Force Report for the ILAE Commission of Pediatrics. Epilepsia 2015, 56, 1185–1197. [Google Scholar] [CrossRef] [PubMed]
  3. Lux, A.L.; Osborne, J.P. A proposal for case definitions and outcome measures in studies of infantile spasms and West syndrome: Consensus statement of the West Delphi Group. Epilepsia 2004, 45, 1416–1428. [Google Scholar] [CrossRef] [PubMed]
  4. Wilmshurst, J.M.; Ibekwe, R.C.; O’Callaghan, F.J.K. Epileptic spasms—175 years on: Trying to teach an old dog new tricks. Seizure 2017, 44, 81–86. [Google Scholar] [CrossRef] [Green Version]
  5. Wheless, J.W.; Gibson, P.A.; Rosbeck, K.L.; Hardin, M.; O’Dell, C.; Whittemore, V.; Pellock, J.M. Infantile spasms (West syndrome): Update and resources for pediatricians and providers to share with parents. BMC Pediatr. 2012, 12, 108. [Google Scholar] [CrossRef] [Green Version]
  6. Rudzka-Dybała, M.; Szczepanik, E.; Terczyńska, I. Patterns of the EEG records in children with West Syndrome. Przegl. Lek. 2015, 72, 694–696. [Google Scholar]
  7. Proposal for Revised Classification of Epilepsies and Epileptic Syndromes. Epilepsia 1989, 30, 389–399. [CrossRef]
  8. Lux, A.L.; Edwards, S.W.; Hancock, E.; Johnson, A.L.; Kennedy, C.R.; Newton, R.W.; O’Callaghan, F.J.K.; Verity, C.M.; Osborne, J.P. The United Kingdom Infantile Spasms Study (UKISS) comparing hormone treatment with vigabatrin on developmental and epilepsy outcomes to age 14 months: A multicentre randomised trial. Lancet Neurol. 2005, 4, 712–717. [Google Scholar] [CrossRef]
  9. Widjaja, E.; Go, C.; McCoy, B.; Snead, O.C. Neurodevelopmental outcome of infantile spasms: A systematic review and meta-analysis. Epilepsy Res. 2015, 109, 155–162. [Google Scholar] [CrossRef]
  10. Gul Mert, G.; Herguner, M.O.; Incecik, F.; Altunbasak, S.; Sahan, D.; Unal, I. Risk factors affecting prognosis in infantile spasm. Int. J. Neurosci. 2017, 127, 1012–1018. [Google Scholar] [CrossRef]
  11. Darke, K.; Edwards, S.W.; Hancock, E.; Johnson, A.L.; Kennedy, C.R.; Lux, A.L.; Newton, R.W.; O’Callaghan, F.J.K.; Verity, C.M.; Osborne, J.P. Developmental and epilepsy outcomes at age 4 years in the UKISS trial comparing hormonal treatments to vigabatrin for infantile spasms: A multi-centre randomised trial. Arch. Dis. Child. 2010, 95, 382–386. [Google Scholar] [CrossRef] [PubMed]
  12. Lagae, L.; Verhelst, H.; Ceulemans, B.; De Meirleir, L.; Nassogne, M.C.; De Borchgrave, V.; D’Hooghe, M.; Foulon, M.; Van Bogaert, P. Treatment and long term outcome in West syndrome: The clinical reality. A multicentre follow up study. Seizure 2010, 19, 159–164. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  13. Scheffer, I.E.; Berkovic, S.; Capovilla, G.; Connolly, M.B.; French, J.; Guilhoto, L.; Hirsch, E.; Jain, S.; Mathern, G.W.; Moshé, S.L.; et al. ILAE classification of the epilepsies: Position paper of the ILAE Commission for Classification and Terminology. Epilepsia 2017, 58, 512–521. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  14. Song, J.M.; Hahn, J.; Kim, S.H.; Chang, M.J. Efficacy of treatments for infantile spasms: A systematic review. Clin. Neuropharmacol. 2017, 40, 63–84. [Google Scholar] [CrossRef]
  15. Iyer, A.; Appleton, R. Improving Outcomes in Infantile Spasms: Role of Pharmacotherapy. Pediatr. Drugs 2016, 18, 357–366. [Google Scholar] [CrossRef]
  16. Knupp, K.G.; Coryell, J.; Nickels, K.C.; Ryan, N.; Leister, E.; Loddenkemper, T.; Grinspan, Z.; Hartman, A.L.; Kossoff, E.H.; Gaillard, W.D.; et al. Response to treatment in a prospective national infantile spasms cohort. Ann. Neurol. 2016, 79, 475–484. [Google Scholar] [CrossRef] [Green Version]
  17. Demarest, S.T.; Shellhaas, R.A.; Gaillard, W.D.; Keator, C.; Nickels, K.C.; Hussain, S.A.; Loddenkemper, T.; Patel, A.D.; Saneto, R.P.; Wirrell, E.; et al. The impact of hypsarrhythmia on infantile spasms treatment response: Observational cohort study from the National Infantile Spasms Consortium. Epilepsia 2017, 58, 2098–2103. [Google Scholar] [CrossRef]
  18. O’Callaghan, F.J.K.; Edwards, S.W.; Alber, F.D.; Hancock, E.; Johnson, A.L.; Kennedy, C.R.; Likeman, M.; Lux, A.L.; Mackay, M.; Mallick, A.A.; et al. Safety and effectiveness of hormonal treatment versus hormonal treatment with vigabatrin for infantile spasms (ICISS): A randomised, multicentre, open-label trial. Lancet Neurol. 2017, 16, 33–42. [Google Scholar] [CrossRef] [Green Version]
  19. Zou, L.P.; Wang, X.; Dong, C.H.; Chen, C.H.; Zhao, W.; Zhao, R.Y. Three-week combination treatment with ACTH + magnesium sulfate versus ACTH monotherapy for infantile spasms: A 24-week, randomized, open-label, follow-up study in China. Clin. Ther. 2010, 32, 692–700. [Google Scholar] [CrossRef]
  20. Ko, A.; Youn, S.E.; Chung, H.J.; Kim, S.H.; Lee, J.S.; Kim, H.D.; Kang, H.C. Vigabatrin and high-dose prednisolone therapy for patients with West syndrome. Epilepsy Res. 2018, 145, 127–133. [Google Scholar] [CrossRef]
  21. Jia, F.Y.; Jiang, H.Y.; Du, L.; Li, N.; Sun, J.; Niu, C.B. An effective initial polytherapy for children with West syndrome. Neural Regen. Res. 2013, 8, 1623–1630. [Google Scholar] [CrossRef] [PubMed]
  22. Zhu, X.; Chen, O.; Zhang, D.; Jin, R.; Li, F.; Wang, Y.; Sun, R. A prospective study on the treatment of infantile spasms with first-line topiramate followed by low-dose ACTH. Epilepsy Res. 2011, 93, 149–154. [Google Scholar] [CrossRef] [PubMed]
  23. Takuma, Y.; Seki, T. Combination therapy of infantile spasms with high-dose pyridoxal phosphate and low-dose corticotropin. J. Child Neurol. 1996, 11, 35–40. [Google Scholar] [CrossRef] [PubMed]
  24. Yi, Z.; Wu, H.; Yu, X.; Zha, J.; Chen, H.; Chen, Y.; Zhong, J. High-dose prednisone therapy for infantile spasms and late-onset epileptic spasms in China: The addition of topiramate provides no benefit. Seizure 2019, 71, 174–178. [Google Scholar] [CrossRef]
  25. Dressler, A.; Benninger, F.; Trimmel-Schwahofer, P.; Gröppel, G.; Porsche, B.; Abraham, K.; Mühlebner, A.; Samueli, S.; Male, C.; Feucht, M. Efficacy and tolerability of the ketogenic diet versus high-dose adrenocorticotropic hormone for infantile spasms: A single-center parallel-cohort randomized controlled trial. Epilepsia 2019, 60, 441–451. [Google Scholar] [CrossRef]
  26. Fayyazi, A.; Eslamian, R.; Khajeh, A.; Dehghani, M. Comparison of the effect of high and low doses of adrenocorticotropic hormone (Acth) in the management of infantile spasms. Iran. J. Child Neurol. 2020, 14, 17–25. [Google Scholar] [CrossRef]
  27. Imannezhad, S.; Akhondian, J.; Ashrafzadeh, F.; Toosi, M.B.; Hahemi, N.; Emadzadeh, M.; Akhondian, M.R. A Single-center Randomized Clinical Trial Comparing the Treatment Efficacy of High Dose Oral Prednisolone with Intramuscular Adrenocorticotropic Hormone in Patients with Infantile Spasm. Int. J. Pediatr. 2020, 8, 12157–12163. [Google Scholar] [CrossRef]
  28. Chellamuthu, P.; Sharma, S.; Jain, P.; Kaushik, J.S.; Seth, A.; Aneja, S. High dose (4 mg/kg/day) versus usual dose (2 mg/kg/day) oral prednisolone for treatment of infantile spasms: An open-label, randomized controlled trial. Epilepsy Res. 2014, 108, 1378–1384. [Google Scholar] [CrossRef]
  29. Wanigasinghe, J.; Arambepola, C.; Sri Ranganathan, S.; Sumanasena, S.; Attanapola, G. Randomized, single-blind, parallel clinical trial on efficacy of oral prednisolone versus intramuscular corticotropin on immediate and continued spasm control in west syndrome. Pediatr. Neurol. 2015, 53, 193–199. [Google Scholar] [CrossRef]
  30. Wanigasinghe, J.; Arambepola, C.; Ranganathan, S.S.; Sumanasena, S. Randomized, Single-Blind, Parallel Clinical Trial on Efficacy of Oral Prednisolone Versus Intramuscular Corticotropin: A 12-Month Assessment of Spasm Control in West Syndrome. Pediatr. Neurol. 2017, 76, 14–19. [Google Scholar] [CrossRef] [Green Version]
  31. O’Callaghan, F.J.K.; Edwards, S.W.; Alber, F.D.; Cortina Borja, M.; Hancock, E.; Johnson, A.L.; Kennedy, C.; Likeman, M.; Lux, A.L.; Mackay, M.T.; et al. Vigabatrin with hormonal treatment versus hormonal treatment alone (ICISS) for infantile spasms: 18-month outcomes of an open-label, randomised controlled trial. Lancet Child Adolesc. Health 2018, 2, 715–725. [Google Scholar] [CrossRef] [Green Version]
  32. Kunnanayaka, V.; Jain, P.; Sharma, S.; Seth, A.; Aneja, S. Addition of pyridoxine to prednisolone in the treatment of infantile spasms: A pilot, randomized controlled trial. Neurol. India 2018, 66, 385–390. [Google Scholar] [CrossRef] [PubMed]
  33. Angappan, D.; Sahu, J.K.; Malhi, P.; Singhi, P. Safety, tolerability, and effectiveness of oral zonisamide therapy in comparison with intramuscular adrenocorticotropic hormone therapy in infants with West syndrome. Eur. J. Paediatr. Neurol. 2019, 23, 136–142. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  34. Gowda, V.K.; Narayanaswamy, V.; Shivappa, S.K.; Benakappa, N.; Benakappa, A. Corticotrophin-ACTH in Comparison to Prednisolone in West Syndrome—A Randomized Study. Indian J. Pediatr. 2019, 86, 165–170. [Google Scholar] [CrossRef]
  35. Knupp, K.G.; Leister, E.; Coryell, J.; Nickels, K.C.; Ryan, N.; Juarez-Colunga, E.; Gaillard, W.D.; Mytinger, J.R.; Berg, A.T.; Millichap, J.; et al. Response to second treatment after initial failed treatment in a multicenter prospective infantile spasms cohort. Epilepsia 2016, 57, 1834–1842. [Google Scholar] [CrossRef]
  36. Pavone, P.; Polizzi, A.; Marino, S.D.; Corsello, G.; Falsaperla, R.; Marino, S.; Ruggieri, M. West syndrome: A comprehensive review. Neurol. Sci. 2020, 41, 3547–3562. [Google Scholar] [CrossRef]
  37. Hahn, J.; Lee, H.; Kang, H.C.; Lee, J.S.; Kim, H.D.; Kim, S.H.; Chang, M.J. Clobazam as an adjunctive treatment for infantile spasms. Epilepsy Behav. 2019, 95, 161–165. [Google Scholar] [CrossRef]
  38. Baram, T.Z.; Mitchell, W.G.; Tournay, A.; Snead, O.C.; Hanson, R.A.; Horton, E.J. High-dose corticotropin (ACTH) versus prednisone for infantile spasms: A prospective, randomized, blinded study. Pediatrics 1996, 97, 375–379. [Google Scholar] [CrossRef]
  39. Ito, M.; Okuno, T.; Fujii, T.; Mutoh, K.; Oguro, K.; Shiraishi, H.; Shirasaka, Y.; Mikawa, H. ACTH therapy in infantile spasms: Relationship between dose of ACTH and initial effect or long-term prognosis. Pediatr. Neurol. 1990, 6, 240–244. [Google Scholar] [CrossRef]
  40. Sukhudyan, B.G.; Dimova, P.S.; Capuano, A.; Vigevano, F. Dyskinesia as a new adverse effect of hormonal treatment in West syndrome. Epileptic Disord. 2014, 16, 5–12. [Google Scholar] [CrossRef]
  41. Arita, J.H.; Vale, T.C.; Pedroso, J.L.; Faria, E.C.; Arita, F.N.; Masruha, M.R.; Barsottini, O.G.P. ACTH-induced dyskinesia in a child with West syndrome (infantile spasms). Park. Relat. Disord. 2016, 24, 145–146. [Google Scholar] [CrossRef] [PubMed]
  42. Fong, C.Y.; Osborne, J.P.; Edwards, S.W.; Hemingway, C.; Hancock, E.; Johnson, A.L.; Kennedy, C.R.; Kneen, R.; Likeman, M.; Lux, A.L.; et al. An investigation into the relationship between vigabatrin, movement disorders, and brain magnetic resonance imaging abnormalities in children with infantile spasms. Dev. Med. Child Neurol. 2013, 55, 862–867. [Google Scholar] [CrossRef] [PubMed]
  43. Schonstedt, V.; Stecher, X.; Venegas, V.; Silva, C. Vigabatrin-induced MRI changes associated with extrapyramidal symptoms in a child with infantile spasms. Neuroradiol. J. 2015, 28, 515–518. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  44. Lux, A.L.; Edwards, S.W.; Hancock, E.; Johnson, A.L.; Kennedy, C.R.; Newton, R.W.; O’Callaghan, F.J.K.; Verity, C.M.; Osborne, J.P. The United Kingdom Infantile Spasms Study comparing vigabatrin with prednisolone or tetracosactide at 14 days: A multicentre, randomised controlled trial. Lancet 2004, 364, 1773–1778. [Google Scholar] [CrossRef]
  45. O’Callaghan, F.J.K.; Lux, A.L.; Darke, K.; Edwards, S.W.; Hancock, E.; Johnson, A.L.; Kennedy, C.R.; Newton, R.W.; Verity, C.M.; Osborne, J.P. The effect of lead time to treatment and of age of onset on developmental outcome at 4 years in infantile spasms: Evidence from the United Kingdom Infantile Spasms Study. Epilepsia 2011, 52, 1359–1364. [Google Scholar] [CrossRef]
  46. Chang, Y.H.; Chen, C.; Chen, S.H.; Shen, Y.C.; Kuo, Y.T. Effectiveness of corticosteroids versus adrenocorticotropic hormone for infantile spasms: A systematic review and meta-analysis. Ann. Clin. Transl. Neurol. 2019, 6, 2270–2281. [Google Scholar] [CrossRef]
  47. Li, S.; Zhong, X.; Hong, S.; Li, T.; Jiang, L. Prednisolone/prednisone as adrenocorticotropic hormone alternative for infantile spasms: A meta-analysis of randomized controlled trials. Dev. Med. Child Neurol. 2020, 62, 575–580. [Google Scholar] [CrossRef]
  48. Sánchez Fernández, I.; Amengual-Gual, M.; Gaínza-Lein, M.; Barcia Aguilar, C.; Bergin, A.M.; Yuskaitis, C.J.; Harini, C. Cost-effectiveness of adrenocorticotropic hormone versus oral steroids for infantile spasms. Epilepsia 2021, 62, 347–357. [Google Scholar] [CrossRef]
Table
Table 1. Epilepsy etiology.
Table 1. Epilepsy etiology.
Etiology
StructuralGeneticMetabolic
-
15 (50%) hypoxic-ischemic encephalopathy
-
8 (16%) cerebral malformation
-
1 (2%) hypothalamic hamartoma and cerebral malformation
-
1 (2%) postinfectious changes
-
4 (8%) tuberous sclerosis
-
2 (4%) CDKL5 mutation
-
1 (2%) neurofibromatosis type, 1
-
1 (2%) microdeletion 2q24.4
-
1 (2%) SPTAN mutation
-
1 (2%) CHD2 mutation
-
1 (2%) ARX1 mutation
-
1 (2%) STXBP1 mutation
-
3 (6%) mitochondrial diseases
-
1 (2%) nonketotic hyperglycinemia
Table
Table 2. Epilepsy onset: 2 days–11 months.
Table 2. Epilepsy onset: 2 days–11 months.
Mean Age of the Patients at the First Seizures (months)
Patients with hypsarrhythmia5.5 SD = 2.3
Patients without hypsarrhythmia3.3 SD = 2.0
Study group4.6 SD = 2.1
Table
Table 3. Schedule of treatment shows frequency of 0.02 mg/kg/d ACTH administration in particular weeks of treatment.
Table 3. Schedule of treatment shows frequency of 0.02 mg/kg/d ACTH administration in particular weeks of treatment.
Weeks of TreatmentFrequency of Administration
1–2Every day
3–4Every second day
5–62 times in a week
7–8Once in a week
Table
Table 4. Antiepileptic drugs used before the onset of ACTH.
Table 4. Antiepileptic drugs used before the onset of ACTH.
Antiepileptic DrugsPatients with
Hypsarrhythmia		Patients without HypsarrhythmiaStudy Group
VigabatrinN = 22 (92%)N = 14 (82%)N = 36 (88%)
Valproic acidN = 22 (92%)N = 15 (88%)N = 37 (90%)
LevetiracetamN = 5 (21%)N = 9 (52%)N = 14 (34%)
ClobazamN = 5 (21%)N = 8 (47%)N = 13 (31%)
PhenobarbitalN = 3 (13%)N = 6 (35%)N = 9 (22%)
ClonazepamN = 3 (13%)N = 3 (18%)N = 6 (15%)
CarbamazepineN = 0N = 3 (18%)N = 3 (7%)
LamotrigineN = 1 (4%)N = 2 (12%)N = 3 (7%)
PhenytoinN = 0N = 2 (12%)N = 2 (5%)
TopiramateN = 2 (8%)N = 1 (6%)N = 2 (5%)
AcetazolamideN = 1 (4%)N = 1 (6%)N = 1 (2%)
NitrazepamN = 0N = 1 (6%)N = 1 (2%)
Table
Table 5. Duration of follow-up.
Table 5. Duration of follow-up.
Length of Follow-Up Study
(Months)		<1313–2425–3637–4849–6061–72>72
Number of patients (%)5 (18)4 (14)7 (25)3 (11)2 (7)3 (11)4 (14)
Table
Table 6. Differences in follow-up between cryptogenic and symptomatic patients.
Table 6. Differences in follow-up between cryptogenic and symptomatic patients.
Cryptogenic
Patients (%)		Symptomatic
Patients (%)		p-Value
Seizures 0.001
absent6 (100)5 (23)
present:017 (77)
more than 2 per month011 (50)
less than 2 per month06 (27)
AED 0.078
absent01 (5)
monotherapy2 (33)2 (9)
2 drugs4 (67)9 (39)
3 or more010 (43)
Mean1.7 SD = 0.52.4 SD = 1.0
Development: 0.022
unfavorable1 (17)16 (73)
favorable5 (83)6 (27)
Publisher’s Note: MDPI stays neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Share and Cite

MDPI and ACS Style

Paprocka, J.; Malkiewicz, J.; Palazzo-Michalska, V.; Nowacka, B.; Kuźniak, M.; Kopyta, I. Effectiveness of ACTH in Patients with Infantile Spasms. Brain Sci. 2022, 12, 254. https://doi.org/10.3390/brainsci12020254

AMA Style

Paprocka J, Malkiewicz J, Palazzo-Michalska V, Nowacka B, Kuźniak M, Kopyta I. Effectiveness of ACTH in Patients with Infantile Spasms. Brain Sciences. 2022; 12(2):254. https://doi.org/10.3390/brainsci12020254

Chicago/Turabian Style

Paprocka, Justyna, Jakub Malkiewicz, Veronica Palazzo-Michalska, Barbara Nowacka, Mikołaj Kuźniak, and Ilona Kopyta. 2022. "Effectiveness of ACTH in Patients with Infantile Spasms" Brain Sciences 12, no. 2: 254. https://doi.org/10.3390/brainsci12020254

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop