INTRODUCTION
Neuroacanthocytosis is a rare movement disorder characterized by progressive muscle weakness and atrophy, progressive cognitive loss, chorea, and acanthocytosis (1). Acanthocytes, abnormal thorny red blood cells (RBC), are one of the biological hallmarks of neuroacanthocytosis syndromes (NA) that is a group of rare hereditary neurodegenerative disorders (2). Neuroacanthocytosis syndromes are exceptionally rare with an estimated prevalence of less than 1 to 5 per 1 000 000 inhabitants for each disorder. The core NA syndromes include autosomal recessive chorea-acanthocytosis and X-linked McLeod syndrome which have a Huntington’s disease-like phenotype consisting of a choreatic movement disorder, psychiatric manifestations and cognitive decline, and additional multi-system features including myopathy and axonal neuropathy. Additionally there are several genetically defined disorders in which acanthocytosis is occasionally seen, such as pantothenate kinase-associated neurodegeneration (PKAN) and Huntington disease-like 2 (HDL2) (2).Fluor 18 -2-fluoro-2-deoxyglucose (18F-FDG-PET) positron emission tomography (PET) and technetium 99m -d, l-hexamethyl-propylene amine oxime (99mTc-HMPAO) brain single photon emission computed tomography (SPECT) have been increasingly used for the detection of neurologic disorders, such as dementia, epilepsy, and movement disorders. In this article, we report two patients with neuroacanthocytosis syndromes with the imaging features of brain metabolism by PET and brain perfusion by SPECT. In addition brain PET and brain SPECT findings of patients with neuroacanthocytosis syndromes were reviewed.
Patient 1
A 29-year-old male patient who had a 2-year history of dysarthria, dysphasia, lip biting and chorea of the trunk and limbs was previously admitted to psychiatry clinics, and was referred to our department for evaluation of neurologic pathologies. His gestation, delivery, and early developmental milestones were unremarkable. The neurological examination revealed a complex hyperkinetic disorder including generalized chorea, orofacial dyskinesias, dysarthria with slurred speech, dysphonia, and minimal dysdiadochokinesia. The gait was bizarre due to both choreatic and dystonic components. Further neurological, general and psychiatric examinations were normal. The patient’s serum creatine kinase (CK) level was 1585 U/L (Normal range: 20-200 U/L), myoglobulin was 198.3 ng/ml (Normal range: 0-110 ng/ml), and serum coeruloplasmin, copper, serum lipoprotein electrophoresis, and vitamin E levels were within normal limits. Peripheral blood smear showed 3-5% acanthocytosis. His EEG showed right temporal paroxysmal activity, and the patient’s needle electromyography and nerve conduction velocities were unremarkable. Cardiac examination and echocardiography were also normal. The patient’s magnetic resonance imaging (MRI) of the brain which was performed in 1.5 Tesla MR system with axial T1-weighted, T2-weighted, axial proton density, axial fluid attenuation inversion recovery (FLAIR) and axial and coronal gadolinium-enhanced T1-weighted images was normal (Figure 1).On the 18F-FDG-PET images of the patient, no 18F-FDG uptake was observed visually in both caudate nuclei. There was minimal 18F-FDG uptake in both lentiform nuclei. The activity uptake of the left lentiform nucleus was less than that of the right side (Figure 2). In the quantitative analysis, hypometabolic areas were identified in the left caudate nucleus, left lentiform nucleus, right caudate nucleus and left lentiform nucleus. The standard deviations from the mean of asymptomatic control group of NeuroQ were -5.4108, - 3.4497, -3.2298 and -1.6914, respectively (Figure 3).
Patient 2
A 35-year-old male patient, whose cousin was suffering from similar complaints such as involuntary movements, lip biting, feeding difficulties, involuntary vocalizations, and left sided choreatic movement with dystonic component was admitted to our hospital. His gestation, delivery, and early developmental milestones were unremarkable until age 30. The neurological examination revealed a complex hyperkinetic disorder including left sided chorea, orofacial dyskinesias, dysarthria with slurred speech, dysphonia, sudden flexion and extension movements of the left arm, dysdiadochokinesia, dystonia, and vocalizations with different noises such as snoring, snorting, nonsense words, and the syllable “hap”. Hyperkinetic movements were more prominent on the left part of the body. Reflexes were absent and muscle tonus was reduced. Further neurological examinations were normal but cardiac examination and echocardiography revealed global akinesia and left ventricular myocardial bands. Psychiatric examination showed cognitive impairment, depression, and self-neglect. The patient’s CK level was 502 U/L, serum ceruloplasmin, copper, serum lipoprotein electrophoresis, vitamin E levels were within normal limits. Peripheral blood smear showed 1-3% acanthocytosis. His EEG, needle electromyography and nerve conduction velocities were unremarkable.The patient’s MRI of the brain which was performed in 1.5 Tesla MR system with axial T1-weighted, T2-weighted, axial proton density, FLAIR and axial and coronal gadolinium-enhanced T1-weighted images showed irregularity of bilateral caudate, putamen and globus pallidus nuclei (Figure 4). 99mTc-HMPAO SPECT showed hypoperfusion in the right lentiform nucleus (Figure 5).Both patients’ genetic consultations were also performed but genetic analyses for the definite diagnosis of neuroacanthocytosis syndromes could not be performed. The patients were put on tetrabenazine treatment with the diagnosis of neuroacanthocytosis syndromes and showed minimal clinical improvement.
Literature Review and Discussion
The terms “neuroacanthocytosis syndromes+PET” and “neuroacanthocytosis syndromes+SPECT”, “neuroacanthocytosis+PET”, “neuroacanthocytosis+SPECT”, “chorea-acanthocytosis+PET”, “chorea-acanthocytosis+SPECT”, “McLeod Syndrome+PET”, and “McLeod Syndrome+SPECT” were searched in the US National Library of Medicine National Institutes of Health-Pubmed. After examining the all results, a total of 11 manuscripts were evaluated (3,4,5,6,7,8,9,10,11,12,13). [tbl:4995]Table 1[/tbl] summarizes the articles according to the number and diagnosis of cases, technique used by nuclear medicine clinics, as well as the results of PET and/or SPECT scans.Regional brain glucose metabolism in neuroacanthocytosis was first described by Dubinsky et al. (3), and his patients’ MRI were normal similar to one of our patients presented herein (case 1). The visual interpretation of the cerebral MRI was reported to be normal in a patient with McLeod syndrome with cerebral involvement by Jung et al. However, visual interpretation of the PET scans, and analysis of region-of-interest values that provided z-scores of less than 2 were also reported to be normal in their patient (12). In case 1, clinical signs and symptoms of cerebral involvement were more prominent and 18F-FDG-PET scan showed no FDG in the caudate nuclei. Therefore, utilization of different neuroimaging techniques would be helpful to detect disease involvement, especially in asymptomatic cases.A study by Müller-Vahl et al. evaluated glucose metabolism of monozygotic twins with chorea-acanthocytosis, and global glucose metabolic rates were found normal in both twins. However, glucose uptake was relatively reduced in the striatum of both patients. The clusters of relative decrease in uptake were significantly different between twins, and they concluded that this result would be attributed to other environmental factors rather than genetic factors (9).99mTc HMPAO SPECT showed hypoperfusion in the right lentiform nucleus in case 2. Bilateral striatal hypometabolism in 18F-FDG-PET, and hypoperfusion in 99mTc HMPAO SPECT was also previously reported in a case of chorea-acanthocytosis (10). Müler-Vahl et al. reported reduced striatal dopamine transporter binding on the right side, in one of the twins by 123I-2-b-carbomethoxy-3-b-(4-iodophenyl)-tropane (123I-b-CIT) single photon emission computed tomography 123IBZM-SPECT (123IBZM-SPECT) scans (9). We think these different results can be explained by the wide spectrum of neuroacanthocytosis syndromes and different techniques used by nuclear medicine clinics.Combined positron-emission tomography and MRI studies may improve diagnostic accuracy in patients with neuroacanthocytosis syndromes. Peppard et al. reported two patients with parkinsonism and neuroacanthocytosis whose 18F-FDG PET scans showed nigrostriatal deficit. They also reported that these two patients responded well to dopaminomimetic therapy (4). As neuroacanthocytosis syndromes can present with variable symptoms, use of different neuroimaging techniques may be helpful in both confirming the diagnosis and deciding on symptomatic treatment.Sydenham chorea is one of the most common causes of choreatic diseases that shows striatal hypermetabolism on PET-CT images (14). In our cases, the ratio of acanthocytosis was fewer than 5%, and although they had some clinical clues to diagnosis, the differential diagnosis of choreatic movement disorders characterized by basal ganglia hypermetabolism such as autoimmune causes or Sydenham chorea could be achieved by the information gained from both PET and SPECT examinations.In summary, nuclear medicine techniques used for evaluating brain activity in patients with chorea-neuroacantocytosis syndromes include SPECT studies using 123I-IMP, 123I-IBZM, 99mTc-ECD HMPAO SPECT, and PET studies by 18F-FDG PET and PET with oxygen-15 steady state technique. Reduced striatal metabolism is the most common finding in 18F-FDG PET studies. In addition, Saiki et al. also reported hypometabolism of the frontal cortex in patients with chorea-acanthocytosis (7). Reduced striatal dopamine D2-receptor binding is the common finding in all SPECT studies. When all case reports are assessed together; it is difficult to claim existence of a strong correlation between clinical signs and PET and/or SPECT findings. Further case reports and studies would be helpful to understand the clinical utility of PET and/or SPECT in patients with neuroacanthocytosis syndromes.