Clinical Heterogeneity of Atypical Pantothenate Kinase-Associated Neurodegeneration in Koreans
Article information
Abstract
Objective
Neurodegeneration with brain iron accumulation (NBIA) represents a group of inherited movement disorders characterized by iron accumulation in the basal ganglia. Recent advances have included the identification of new causative genes and highlighted the wide phenotypic variation between and within the specific NBIA subtypes. This study aimed to investigate the current status of NBIA in Korea.
Methods
We collected genetically confirmed NBIA patients from twelve nationwide referral hospitals and from a review of the literature. We conducted a study to describe the phenotypic and genotypic characteristics of Korean adults with atypical pantothenate kinase-associated neurodegeneration (PKAN).
Results
Four subtypes of NBIA including PKAN (n = 30), PLA2G6-related neurodegeneration (n = 2), beta-propeller protein-associated neurodegeneration (n = 1), and aceruloplasminemia (n = 1) have been identified in the Korean population. The clinical features of fifteen adults with atypical PKAN included early focal limb dystonia, parkinsonism-predominant feature, oromandibular dystonia, and isolated freezing of gait (FOG). Patients with a higher age of onset tended to present with parkinsonism and FOG. The p.R440P and p.D378G mutations are two major mutations that represent approximately 50% of the mutated alleles. Although there were no specific genotype-phenotype correlations, most patients carrying the p.D378G mutation had a late-onset, atypical form of PKAN.
Conclusions
We found considerable phenotypic heterogeneity in Korean adults with atypical PKAN. The age of onset may influence the presentation of extrapyramidal symptoms.
Neurodegeneration with brain iron accumulation (NBIA) represents a group of inherited disorders characterized by iron deposition in the brain, and NBIA exhibits the clinical features of movement disorders [1]. Over the last decade, several causative genes, directly involved in iron homeostasis, mitochondrial function, lipid metabolism, and autophagic activity, have been identified including FTL, CP, PANK2, PLA2G6, C19orf12, COASY, FA2H, WDR45, and ATP13A2 [2]. Of the known causes of NBIA, the most common cause of NBIA is pantothenate kinase-associated neurodegeneration (PKAN) due to mutations in the PANK2 gene, followed by PLA2G6-related neurodegeneration (PLAN) due to mutations in the PLA2G6 gene [1,3]. The diagnosis of NBIA is made by combining clinical features and magnetic resonance imaging evidence of iron accumulation in the brain [3].
NBIA patients commonly exhibit mixed extrapyramidal and pyramidal features [1,4]. However, the clinical spectrum ranges from global neurodevelopmental delay in infancy to dystonia-parkinsonism in adulthood, with wide phenotypic variability within the specific NBIA subtypes [1,3,5]. In PKAN, the classic form is characterized by early childhood onset with rapid progression [1,6]. The atypical variant presents in the second or third decade of life with less severe and slow-progressive extrapyramidal and pyramidal signs [1,6]. Cognitive impairment and neuropsychiatric symptoms may be prominent [1,6]. Similar age-dependent presentations have also been recognized in PLAN [1,3,4]. Adult-onset NBIA may also mimic the clinical presentations of other neurodegenerative diseases, making the diagnosis challenging [4].
To date, reports on the clinical and genetic profile of Korean patients with NBIA have been restricted to single cases or case series that were lacking in detailed data [7-18]. To investigate the current status of NBIA in Korea, we collected NBIA data from twelve nationwide referral hospitals and from a review of the literature. We also conducted a study to describe the phenotypic and genotypic characteristics of Korean adults with atypical PKAN.
MATERIALS & METHODS
This study was approved by the Ethical Committee of the Pusan National University Yangsan Hospital. We recruited thirty-four Korean patients with genetically determined NBIA using a structural survey and a literature review of published case reports. A nationwide survey was organized by the Korean Movement Disorders Society. For PKAN, nine new cases and twenty-one previously published cases from twenty-eight families were collected. Among these cases, sixteen patients were classified as having an atypical disease according to the criteria of Hayflick et al. [6]. Three pediatric patients who had typical clinical features of PKAN and the eye-of-the-tiger sign carried only one heterozygous missense mutation that was detected by direct sequencing of the PANK2 gene. Two siblings with PLAN and one patient with beta-propeller protein-associated neurodegeneration (BPAN) were recently described in the literature [16,18]. One unpublished case of aceruloplasminemia, a 60-year-old female presenting with dystonia, chorea, and dementia, was included in the present study.
We collected detailed clinical data on fifteen adult PKAN patients from fourteen unrelated families. Genomic DNA from all patients was sequenced for PANK2 mutations. For the numbering of the mutations, all published and unpublished cases were adjusted by comparison with the wild-type nucleotide and amino acid sequences (GenBank ID: NM_153638.2, NP_705902.2). For analysis of the clinical and genetic data, the medical records of five new patients from 4 referral hospitals were reviewed. We also attempted to contact the authors of the publications to update the clinical information, and we obtained additional follow-up data from six published cases [8,12-15]. We analyzed the following clinical information: age at onset of the disease, age at diagnosis, age at the last evaluation, presenting symptoms, and clinical characteristics at the last evaluation including dystonia, tremor, parkinsonism, gait/posture, pyramidal signs, bulbar symptoms, cognitive/behavioral changes, results of ophthalmologic examinations, peripheral blood smears, neuroimaging findings, mutations in the PANK2 gene, response to treatment, and disease course. Fourteen pediatric patients with typical PKAN were excluded from this clinical data analysis because of insufficient clinical or genetic information. Instead, we gathered genetic data from ten unrelated pediatric PKAN patients carrying two mutated alleles to investigate the differences in the mutation frequencies between the classic and atypical forms.
RESULTS
The clinical, neuroimaging and molecular results from fifteen patients (thirteen males and two females with the atypical form of PKAN) are summarized in Table 1 and Supplementary Table 1 (in the online-only Data Supplement). The mean age at onset was 31.1 ± 11.8 years (range 15–52 years), and the mean disease duration was 13.8 ± 9.7 years (range 1–34 years). Patients 7 (P7) and 8 (P8) were siblings. Five patients declared that they had at least 1 family member who was affected with similar symptoms. The remaining patients were presumed to be sporadic cases. The presenting symptoms were as follows: difficulty in writing or handling objects in ten patients (hand dystonia in six patients and hand tremor in four patients), gait disturbance in four patients [dystonic gait in two patients, dystonic gait with freezing in one patient, and isolated freezing of gait (FOG) in one patient], speech changes in three patients (monotonous speech, dysphonia, and dysarthria), and oromandibular dystonia (OMD) in one patient (jaw-opening). Two patients presented with a rapid onset, OMD and painful dystonia (P2 and P7).
At the last evaluation, the predominant neurological features were dystonia and parkinsonism (eight patients with dystonia without parkinsonism, four patients with parkinsonism and dystonia, and two patients with parkinsonism without dystonia). Dystonia most commonly involved the limbs (n = 12), often affecting the craniocervical musculature including blepharospasm, cervical dystonia, and OMD (n = 8). Early focal limb dystonia progressed to involve other limbs. Axial involvement, with retrocollis or truncal tilting, was not prominent in most of the patients. Gait and balance problems were very common (n = 12), unsteadiness and freezing were reported in six and three patients, respectively. Although some patients needed to use canes for walking, none of them completely lost the ability to walk. Speech disturbances, including dysarthria, palilalia and hypophonia, were frequent (n = 10) and presented from the early stage in three patients. Dysarthria was accompanied by dysphagia or drooling in four patients. Tremors (n = 9) were usually postural in nature and presented as dystonic tremors. Rest tremors were observed in two patients; one of them presented with parkinsonism (P13), and the other had unilateral leg tremors (P12). Corticospinal tract signs (spasticity, hyperreflexia and extensor plantar reflexes) were rarely described.
Other features including pigmentary retinopathy, acanthocytosis [19], and seizure were not mentioned in the medical records. Psychiatric symptoms with cognitive decline were not prominent in most patients. Cognitive impairment was evident in two young siblings (P7 and P8). The results of neuropsychological tests revealed mild mental retardation. The older brother showed psychiatric signs of obsessive-compulsive disorder and attention-deficit and hyperactivity disorder. Two patients who underwent neuropsychological testing had mild frontal dysfunction (P10 and P15). Three patients over 50 years of age presented with subjective memory complaints; however, neuropsychological tests were not performed.
All had the eye-of-the-tiger sign on T2-weighted images. Marked hyperintensities on T1-weighted images in bilateral anteromedial globus pallidi were reported in two patients (P5 and P10). Susceptibility-weighted imaging dramatically revealed the evidence of iron deposition restricted to the globus pallidus and substantia nigra (Figure 1). Dopamine transporter imaging with N-{3-[(18)F]fluoropropyl}-2-carbomethoxy-3-(4-iodophenyl) nortropane positron emission tomography studies in two patients with parkinsonism (P13) and gait freezing (P15) revealed no striatal dopamine depletion. No perfusion defect was observed in one patient (P3).
There were no overt responses to conventional drugs used for the control of dystonia, tremor, or parkinsonism, although partial improvements were reported. In two patients with FOG as the main clinical feature, FOG showed dramatic responses to medications [7,17]. One patient (P9) dramatically improved with trihexyphenidyl, and the other patient (P15) dramatically improved with methylphenidate. Three patients (P4, P7, and P10) underwent bilateral globus pallidus pars interna (GPi) deep brain stimulation (DBS). All patients showed some improvements in the clinical rating scales of dystonia and disability (Supplementary Table 1 in the online-only Data Supplement). The patient with rapid exacerbation of painful dystonic spasms immediately underwent bilateral GPi-DBS (P7). His axial and limb dystonia showed sustained improvement for up to 5 years after DBS. However, he developed intractable jaw-opening OMD which severely interfered with speech and mastication. In two other patients (P4 and P10), disabling hand dystonia responded to DBS. Their functional improvement continued for 3-year follow-up period. However, in one patient (P4, previously published), the effect disappeared four year after DBS.
We identified 18 different mutations in 24 Korean families with PKAN. Mutations were found in both PANK2 alleles and included missense mutations (37/48 alleles), frameshift mutations (8/48 alleles), nonsense mutations (1/48 alleles), and deletions (4/48 alleles) (Table 2). Most of the patients had compound heterozygous mutations. In two atypical cases, one was homozygous (P12), and the other had two different missense mutations and one frameshift mutation (P13). An intragenic deletion ranging from exons 2 to 4 (c.629-?_1412+ ?del) was found in a pediatric patient [15]. The most frequent mutations identified were p.D378G (10/28 alleles) and p.R440P (8/28 alleles) in Korean adults with atypical PKAN (Table 2: atypical). Within the atypical group, there were no specific genotype-phenotype correlations. Five patients who were all compound heterozygotes for these two mutations (p. D378G and p.R440P) showed variable clinical manifestations, including dystonia without parkinsonism (n = 2), dystonia with parkinsonism (n = 1), parkinsonism-predominant (n = 1), and isolated FOG (n = 1). Two siblings (P7 and P8) presented with different spreading patterns of dystonia, although they had a similar age at onset in the second decade. The older brother, initially, developed twisting postures in his right hand, whereas his younger brother had dystonia starting in the legs.
In pediatric patients with typical PKAN, the most prevalent mutation was the p.R440P mutation (9/20 alleles), followed by the p.I501N mutation (3/20 alleles) (Table 2: classic). Eight published cases initially presented with gait disturbance and generalized dystonia before 10 years of age. Half of them had lost ambulation within 3 years of onset [15]. Three newly enrolled patients had dystonic opisthotonus and tip-toe gait. Two possibly pathogenic novel variants were identified (c.1676C > G, p.A559G and c.1257del, p.F419fs). One adolescence patient with atypical presentation had two compound heterozygous mutations (c.1351C > T, p.R451X and c.1607A > G, p.Y536C) [15]. The allele frequencies of protein-truncating mutations were not different between the two groups (Table 2).
DISCUSSION
Among the ten forms of NBIA, four subtypes of NBIA including PKAN, PLAN, BPAN, and aceruloplasminemia have been identified in the Korean population. PKAN was the most common cause of NBIA. The characteristic eye-of-the-tiger sign of PKAN may aid in diagnosing this disorder [1,6]. The other forms of NBIA were rare and were reported only in single cases [16,18]. However, it may still be too early to determine the frequency and distribution of these disorders in the Korean population. Increasing clinician awareness will improve early recognition and diagnosis of various types of NBIA.
All fifteen patients analyzed in this study could be classified as having atypical PKAN on the basis of late onset and slow progression [1,6]. Patients with long-lasting movement disorders exhibited similar functional disabilities regardless of the disease duration and no significant functional declines during the past several years. None of them completely lose their ability to ambulate even after a disease duration of 20 years or more. This observation is most likely related to the specific pattern of disease progression of atypical PKAN. The rate of decline tends to be steeper after the onset of symptoms, followed by a relatively stable period of slower progression [1,20].
In addition to the age at onset and disease duration, other atypical features in our patients included early focal limb dystonia, tremor, parkinsonism, changes in speech patterns, OMD, and FOG. Early dystonia frequently involved a unilateral hand with manifestation of writer’s cramp or action-induced dystonia. Most of them slowly progressed to involve other limbs and, less commonly, craniocervical regions. This initial distribution of dystonia is different from that of patients with the classic form that predominantly affects the lower limbs. Dystonic opisthotonus, a hallmark of early-onset typical PKAN [21], was rare in our series. The presentation and progression of dystonia tends to differ between ethnic groups. As demonstrated by a previous report, OMD was less common than in Caucasians [20,22]. In a recent prospective study, half of the patients developed dystonic opisthotonus within five years after onset [20]. This disease course was more progressive than that observed in our patients.
The parkinsonism-predominant phenotype was also the characteristic subgroup of our patients. They initially presented with hand tremor, even with a resting component, and were clinically indistinguishable from patients with degenerative parkinsonism. The results of normal striatal binding with dopamine transporter imaging are consistent with previous reports [23]. Moreover, a neuropathological study identified only minimal loss of neuromelanin in the substantia nigra, while the central pallidum and substantia nigra pars reticulata were mainly involved [24]. Two major extrapyramidal symptoms of PKAN, dystonia and parkinsonism, showed age-dependency, as previously reported [1,25]. Patients with parkinsonism tended to have a later age of onset than patients in the dystonia-predominant group, while adolescent patients or patients in early adulthood demonstrated more dystonia than parkinsonism. In addition, though the number of cases was limited, dystonic patients with late-adult onset tended to have less craniocervical involvement at initial presentation. The age of onset may influence the presentation of extrapyramidal symptoms in the atypical form of PKAN.
Contrary to previous reports [5,6,26], neuropsychiatric symptoms and cognitive impairment were uncommon and were not prominent in our series. This discrepancy can be explained by ethnicity-related differences. A previous comparative analysis noted a lower prevalence of these symptoms in Asians than in Caucasians [22]. Epidemiological surveys showed lower prevalence rates of mental disorders in Asians [27]. However, other confounding factors should be considered. Standardized assessment measures revealed that age of onset was associated with intellectual and adaptive functioning [28]. A younger age at onset of the disease was associated with a greater degree of cognitive impairment [1]. Neuropsychiatric symptoms can be early presenting signs of adolescence [1]. Patients enrolled in this study were much older than those of previous reports [5,6,22,26]. Most of them revealed stable preserved cognition and behavior except for two siblings with an age of onset in the mid-teenage years. Patients who survive into middle or old age should not be assumed to have a progressive dementia [29]. However, they may be underdiagnosed due to insufficient evaluation. Further systematic assessment is warranted to determine the ethnic differences in cognitive and psychiatric symptoms.
The p.R440P and p.D378G mutations are two major mutations representing approximately 50% of the mutated alleles. Most of the mutations were different from those reported in Caucasians [6,22,26]. The common mutations (p.G521R and p.T528M) found in Caucasians have not been found in any Korean PKAN patients so far. The p.D378G mutation is also a frequent mutation in Chinese individuals and most likely represents a hotspot in PKAN patients from Eastern Asia [22,30]. The p.R440P mutation may be a founder genotype in the Korean population [15]. This mutation was associated with both classic and atypical phenotypes [15]. Notably, most patients carrying the p.D378G mutation had a late-onset, atypical form of PKAN [30]. Previous studies have shown that the locations of the missense mutations correlated with the residual activity of pantothenate kinase and the age of onset [26,31]. The enzymatic activity of the p.D378G mutation should be determined to confirm the association of this mutation with the atypical clinical phenotype. It has been shown that two null mutations result in a loss of enzyme activity and lead to early-onset classic disease [6,26]. However, no Korean pediatric patients with classic PKAN had two predicted loss-of-function alleles. Other genetic modifiers and environmental factors may also be involved.
Dystonia and parkinsonism showed limited responses to medications. The preservation of nigrostriatal dopaminergic integrity can be associated with limited benefits of dopaminergic drugs. Isolated FOG with drug responsiveness is the most striking presenting feature in our series, although the exact mechanism remains uncertain [7,17]. GPi-DBS performed in three patients was shown to be partially effective for relieving dystonic symptoms. The patients exhibited a sustained positive response to GPi-DBS for a 3- to 5-year follow-up period. Previous studies have demonstrated the efficacy of bilateral GPi-DBD for the treatment of dystonia in patients with PKAN, although the effect was not as great as the benefit reported in patients with primary generalized dystonia [15,32]. However, most reports are limited by short periods of observation. Additional follow-up data in this study add to the evidence supporting the long-term benefit [33].
In this study, we attempted a more detailed analysis of clinical manifestations in Korean adults with atypical PKAN, and we found considerable phenotypic heterogeneity. Some characteristic symptoms of the atypical form tended to show an age-dependent presentation. However, the present study is limited because every detail of the clinical severities could not be obtained as our data were gathered retrospectively from medical records and from a review of literatures. Clinical rating scales primarily focused on PKAN or well-structured registries should be used for the clearer delineation of the severity and natural history of this disease [1].
Supplementary Materials
The online-only Data Supplement is available with this article at http://dx.doi.org/10.14802/jmd.15058.
Notes
Conflicts of Interest
The authors have no financial conflicts of interest.
Acknowledgements
This research was supported by the Basic Science Research Program through the National Research Foundation of Korea (NRF) funded by the Ministry of Education, Science and Technology (2014R1A1A2059252) and by the Pusan National University Yangsan Hospital (2015).