Updated on 2024/10/01

Information

 

写真a

 
CHONG PIN FEE
 
Organization
Kyushu University Hospital Comprehensive Maternity and Perinatal Care Center Assistant Professor
School of Medicine Department of Medicine(Joint Appointment)
Title
Assistant Professor
Tel
0926425421
External link

Degree

  • M.D., Ph.D.

Research Interests・Research Keywords

  • Research theme:Pediatric neuroinflammatory disease

    Keyword:myelitis, encephalitis

    Research period: 2023.4 - 2024.4

Papers

  • Dural arteriovenous fistulae in a 6-year-old girl with trisomy 21 and congenital heart disease

    Ishikura, T; Sonoda, Y; Kajiwara, K; Chong, PF; Kanemasa, H; Motomura, Y; Kaku, N; Hirata, Y; Nagata, H; Yamamura, K; Arimura, K; Nakamizo, A; Sakai, Y; Ohga, S

    CLINICAL NEUROLOGY AND NEUROSURGERY   246   108540   2024.11   ISSN:0303-8467 eISSN:1872-6968

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    Language:English   Publisher:Clinical Neurology and Neurosurgery  

    Dural arteriovenous fistula (DAVF) represents a pathological group of intracranial shunts arising from the dural artery to venous sinus and veins. Childhood-onset DAVF is generally considered to be poor in prognosis, whereas only limited information is available for the onset and long-term outcomes. We herein report a Japanese girl with trisomy 21, large ventricular septal defects, and pulmonary vein stenosis, for which a transcatheter stent had been placed after birth. At age 6 years, she developed bacterial meningitis due to S. pneumoniae, leading to the diagnosis of venous sinus thrombosis and multiple intracranial shunts. Cerebral angiography identified multiple shunts arising from the middle meningeal arteries to the superior sagittal sinus and a concurrent reflux to cortical vein. Endovascular embolization successfully occluded the shunts without neurovascular complications over 24 months. This report first demonstrates the favorable outcome of DAVF in a pediatric patient with trisomy 21 after the catheter intervention. For children at a risk for intracranial thrombosis, preemptive neurovascular evaluation and transcatheter intervention provide a chance of early diagnosis of DAVF to improve their survival and neurologic outcome.

    DOI: 10.1016/j.clineuro.2024.108540

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  • Exploring unsolved cases of lissencephaly spectrum: integrating exome and genome sequencing for higher diagnostic yield

    Furukawa, S; Kato, M; Ishiyama, A; Kumada, T; Yoshida, T; Takeshita, E; Chong, PF; Yamanouchi, H; Kotake, Y; Kyoda, T; Nomura, T; Miyata, Y; Nakashima, M; Saitsu, H

    JOURNAL OF HUMAN GENETICS   2024.8   ISSN:1434-5161 eISSN:1435-232X

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    Language:English   Publisher:Journal of Human Genetics  

    Lissencephaly is a rare brain malformation characterized by abnormal neuronal migration during cortical development. In this study, we performed a comprehensive genetic analysis using next-generation sequencing in 12 unsolved Japanese lissencephaly patients, in whom PAFAH1B1, DCX, TUBA1A, and ARX variants were excluded using the Sanger method. Exome sequencing (ES) was conducted on these 12 patients, identifying pathogenic variants in CEP85L, DYNC1H1, LAMC3, and DCX in four patients. Next, we performed genome sequencing (GS) on eight unsolved patients, and structural variants in PAFAH1B1, including an inversion and microdeletions involving several exons, were detected in three patients. Notably, these microdeletions in PAFAH1B1 could not to be detected by copy number variation (CNV) detection tools based on the depth of coverage methods using ES data. The density of repeat sequences, including Alu sequences or segmental duplications, which increase the susceptibility to structural variations, is very high in some lissencephaly spectrum genes (PAFAH1B1, TUBA1A, DYNC1H1). These missing CNVs were due to the limitations of detecting repeat sequences in ES-based CNV detection tools. Our study suggests that a combined approach integrating ES with GS can contribute to a higher diagnostic yield and a better understanding of the genetic landscape of the lissencephaly spectrum.

    DOI: 10.1038/s10038-024-01283-0

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  • Long-read sequencing identifies an SVA_D retrotransposon insertion deep within the intron of <i>ATP7A</i> as a novel cause of occipital horn syndrome

    Yano, N; Chong, PF; Kojima, KK; Miyoshi, T; Luqmen-Fatah, A; Kimura, Y; Kora, K; Kayaki, T; Maizuru, K; Hayashi, T; Yokoyama, A; Ajiro, M; Hagiwara, M; Kondo, T; Kira, R; Takita, J; Yoshida, T

    JOURNAL OF MEDICAL GENETICS   61 ( 10 )   950 - 958   2024.7   ISSN:0022-2593 eISSN:1468-6244

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    Language:English   Publisher:Journal of Medical Genetics  

    Background: SINE-VNTR-Alu (SVA) retrotransposons move from one genomic location to another in a 'copy-and-paste' manner. They continue to move actively and cause monogenic diseases through various mechanisms. Currently, disease-causing SVA retrotransposons are classified into human-specific young SVA_E or SVA_F subfamilies. In this study, we identified an evolutionarily old SVA_D retrotransposon as a novel cause of occipital horn syndrome (OHS). OHS is an X-linked, copper metabolism disorder caused by dysfunction of the copper transporter, ATP7A. Methods: We investigated a 16-year-old boy with OHS whose pathogenic variant could not be detected via routine molecular genetic analyses. Results: A 2.8 kb insertion was detected deep within the intron of the patient's ATP7A gene. This insertion caused aberrant mRNA splicing activated by a new donor splice site located within it. Long-read circular consensus sequencing enabled us to accurately read the entire insertion sequence, which contained highly repetitive and GC-rich segments. Consequently, the insertion was identified as an SVA_D retrotransposon. Antisense oligonucleotides (AOs) targeting the new splice site restored the expression of normal transcripts and functional ATP7A proteins. AO treatment alleviated excessive accumulation of copper in patient fibroblasts in a dose-dependent manner. Pedigree analysis revealed that the retrotransposon had moved into the OHS-causing position two generations ago. Conclusion: This is the first report of a human monogenic disease caused by the SVA_D retrotransposon. The fact that the evolutionarily old SVA_D is still actively transposed, leading to increased copy numbers may make a notable impact on rare genetic disease research.

    DOI: 10.1136/jmg-2024-110056

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  • Rapid and long-lasting efficacy of high-dose ambroxol therapy for neuronopathic Gaucher disease: A case report and literature review

    Higashi, K; Sonoda, Y; Kaku, N; Fujii, F; Yamashita, F; Lee, S; Tocan, V; Ebihara, G; Matsuoka, W; Tetsuhara, K; Sonoda, M; Chong, PF; Mushimoto, Y; Kojima-Ishii, K; Ishimura, M; Koga, Y; Fukuta, A; Tsuchihashi, NA; Kikuchi, Y; Karashima, T; Sawada, T; Hotta, T; Yoshimitsu, M; Terazono, H; Tajiri, T; Nakagawa, T; Sakai, Y; Nakamura, K; Ohga, S

    MOLECULAR GENETICS & GENOMIC MEDICINE   12 ( 4 )   e2427   2024.4   ISSN:2324-9269

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    Language:English   Publisher:Molecular Genetics and Genomic Medicine  

    Gaucher disease (GD) is a lysosomal storage disorder caused by a deficiency in the GBA1-encoded enzyme, β-glucocerebrosidase. Enzyme replacement therapy is ineffective for neuronopathic Gaucher disease (nGD). High-dose ambroxol has been administered as an alternative treatment for a group of patients with nGD. However, little is known about the clinical indication and the long-term outcome of patients after ambroxol therapy. We herein report a case of a female patient who presented with a progressive disease of GD type 2 from 11 months of age and had the pathogenic variants of p.L483P (formerly defined as p.L444P) and p.R502H (p.R463H) in GBA1. A combined treatment of imiglucerase with ambroxol started improving the patient's motor activity in 1 week, while it kept the long-lasting effect of preventing the deteriorating phenotype for 30 months. A literature review identified 40 patients with nGD, who had received high-dose ambroxol therapy. More than 65% of these patients favorably responded to the molecular chaperone therapy, irrespective of p.L483P homozygous, heterozygous or the other genotypes. These results highlight the long-lasting effect of ambroxol-based chaperone therapy for patients with an expanding spectrum of mutations in GBA1.

    DOI: 10.1002/mgg3.2427

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  • High-Titer Anti-ZSCAN1 Antibodies in a Toddler Clinically Diagnosed with Apparent Rapid-Onset Obesity with Hypothalamic Dysfunction, Hypoventilation, and Autonomic Dysregulation Syndrome

    Tocan, V; Nakamura-Utsunomiya, A; Sonoda, Y; Matsuoka, W; Mizuguchi, S; Muto, Y; Hijioka, T; Nogami, M; Sasaoka, D; Nagamatsu, F; Oba, U; Kawakubo, N; Hamada, H; Mushimoto, Y; Chong, PF; Kaku, N; Koga, Y; Sakai, Y; Oda, Y; Tajiri, T; Ohga, S

    INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES   25 ( 5 )   2024.3   ISSN:1661-6596 eISSN:1422-0067

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    Language:English   Publisher:International Journal of Molecular Sciences  

    Severe obesity in young children prompts for a differential diagnosis that includes syndromic conditions. Rapid-Onset Obesity with Hypothalamic Dysfunction, Hypoventilation, and Autonomic Dysregulation (ROHHAD) syndrome is a potentially fatal disorder characterized by rapid-onset obesity associated with hypoventilation, neural crest tumors, and endocrine and behavioral abnormalities. The etiology of ROHHAD syndrome remains to be established, but recent research has been focusing on autoimmunity. We report on a 2-year-old girl with rapid-onset obesity during the first year of life who progressed to hypoventilation and encephalitis in less than four months since the start of accelerated weight gain. The patient had a high titer of anti-ZSCAN1 antibodies (348; reference range < 40), and the increased values did not decline after acute phase treatment. Other encephalitis-related antibodies, such as the anti-NDMA antibody, were not detected. The rapid progression from obesity onset to central hypoventilation with encephalitis warns about the severe consequences of early-onset ROHHAD syndrome. These data indicate that serial measurements of anti-ZSCAN1 antibodies might be useful for the diagnosis and estimation of disease severity. Further research is needed to determine whether it can predict the clinical course of ROHHAD syndrome and whether there is any difference in antibody production between patients with and without tumors.

    DOI: 10.3390/ijms25052820

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  • The Etiology and Outcome of Area Postrema Syndrome in Childhood: Two Cases and a Literature Review

    Tomari, Y; Igata, Y; Chong, PF; Kajiwara, K; Hatai, E; Sonoda, Y; Oba, U; Kaku, N; Koga, Y; Sakai, Y; Ohga, S

    PEDIATRIC NEUROLOGY   152   11 - 15   2024.3   ISSN:0887-8994 eISSN:1873-5150

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    Language:English   Publisher:Pediatric Neurology  

    Background: Area postrema syndrome (APS), a rare childhood condition, manifests as intractable nausea and hiccups. APS has high diagnostic significance in neuromyelitis optica syndrome spectrum disorders (NMOSD) and can be the initial presentation of other critical diseases, including brainstem glioma. Methods: We described two representative cases of unrelated Japanese patients with APS. An etiologic evaluation, including a detailed intracranial neuroradiological examination and autoantibodies assessment, was performed. We also reviewed the literature focusing on the prognosis of pediatric APS symptoms. Results: A 14-year-old girl with aquaporin-4 antibody-positive NMOSD showed a good prognosis with immunotherapy, whereas another nine-year-old girl with irresectable medullary low-grade glioma had persistent symptoms for more than 10 years. All reported children aged >12 years were diagnosed with NMOSD, and patients aged <13 years showed heterogeneous etiologies. Conclusions: Distinctive time courses and neuroimaging features were key clinical findings for the diagnostic and therapeutic processes in these patients. This literature review highlights the wide spectrum and prognosis of pediatric-onset APS.

    DOI: 10.1016/j.pediatrneurol.2023.12.010

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  • Clinical characteristics of SARS-CoV-2-associated encephalopathy in children: Nationwide epidemiological study

    Kasai M., Sakuma H., Abe Y., Kuki I., Maegaki Y., Murayama K., Murofushi Y., Nagase H., Nishiyama M., Okumura A., Sakai Y., Tada H., Mizuguchi M., Takanashi J.i., Akamine S., Chong P.F., Ema T., Enomoto S., Fukatsu R., Hanaoka Y., Igarashi A., Ikeda T., Ishida K., Ishikawa N., Itamura S., Iwayama H., Kawata N., Kawano G., Kikuchi K., Kobayashi O., Kondo H., Korematsu S., Matsuoka T., Minamisawa Y., Mitani O., Mizuma K., Mori T., Morichi S., Moriyama Y., Motobayashi M., Motoi H., Muramatsu K., Nakamura K., Nakazawa T., Negishi Y., Nishizawa Y., Okada H., Okanari K., Oki K., Okumura Y., Omata T., Saeki S., Sano F., Sano K., Sato T., Shiihara T., Shimoda K., Suzuki M., Tanaka R., Tokorodani C., Uematsu M., Yamada H., Yamamoto N., Yamamoto T., Yokoyama H.

    Journal of the Neurological Sciences   457   2024.2   ISSN:0022510X

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    Publisher:Journal of the Neurological Sciences  

    Objective: Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) sometimes triggers acute encephalopathy as a serious neurological complication in children. We previously reported the clinico-radiological findings of SARS-CoV-2-associated encephalopathy. The advent of the SARS-CoV-2 omicron variant led to a marked increase in pediatric patients with coronavirus disease 2019 (COVID-19); however, epidemiological changes with acute encephalopathy according to the emergence of SARS-CoV-2 have not yet been documented. Therefore, the present study investigated epidemiological differences in SARS-CoV-2-associated encephalopathy during the BA.1/BA.2 and BA.5 predominant periods and also between SARS-CoV-2-associated and non-SARS-CoV-2-associated encephalopathy. Methods: We conducted a nationwide survey of SARS-CoV-2-associated encephalopathy in Japanese children between June and November 2022. We compared the present results during the BA.5 predominant period and previous findings during the BA.1/BA.2 predominant period. We also compared the clinico-radiological syndromes of encephalopathy between SARS-CoV-2-associated and non-SARS-CoV-2-associated encephalopathy. Results: Although many patients with SARS-CoV-2-associated encephalopathy in the BA.5 predominant period had seizures as their initial symptoms, no significant differences were observed in the clinical features. Patients with SARS-CoV-2-associated encephalopathy had worse outcomes than those with non-SARS-CoV-2-associated encephalopathy (p-value = 0.003). Among 103 patients with SARS-CoV-2-associated encephalopathy, 14 (13.6%) had severe types of acute encephalopathy, namely, encephalopathy with acute fulminant cerebral edema (AFCE) and hemorrhagic shock and encephalopathy syndrome (HSES). Also, 28 (27.2%) patients with SARS-CoV-2-associated encephalopathy had poor outcome: severe neurological sequelae or death. Ninety-five patients (92.2%) were not vaccinated against SARS-CoV-2. Conclusions: In SARS-CoV-2-associated encephalopathy, high percentages of AFCE and HSES can result in poor outcomes.

    DOI: 10.1016/j.jns.2024.122867

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  • Progressive myoclonic epilepsy as an expanding phenotype of NGLY1-associated congenital deglycosylation disorder: A case report and review of the literature

    Sonoda, Y; Fujita, A; Torio, M; Mukaino, T; Sakata, A; Matsukura, M; Yonemoto, K; Hatae, K; Ichimiya, Y; Chong, PF; Ochiai, M; Wada, Y; Kadoya, M; Okamoto, N; Murakami, Y; Suzuki, T; Isobe, N; Shigeto, H; Matsumoto, N; Sakai, Y; Ohga, S

    EUROPEAN JOURNAL OF MEDICAL GENETICS   67   104895   2024.2   ISSN:1769-7212 eISSN:1878-0849

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    Language:English   Publisher:European Journal of Medical Genetics  

    Introduction: NGLY1-associated congenital disorder of deglycosylation (CDDG1: OMIM #615273) is a rare autosomal recessive disorder caused by a functional impairment of endoplasmic reticulum in degradation of glycoproteins. Neurocognitive dysfunctions have been documented in patients with CDDG1; however, deteriorating phenotypes of affected individuals remain elusive. Case presentation: A Japanese boy with delayed psychomotor development showed ataxic movements from age 5 years and myoclonic seizures from age 12 years. Appetite loss, motor and cognitive decline became evident at age 12 years. Electrophysiological studies identified paroxysmal discharges on myoclonic seizure and a giant somatosensory evoked potential. Perampanel was effective for controlling myoclonic seizures. Exome sequencing revealed that the patient carried compound heterozygous variants in NGLY1, NM_018297.4: c.857G > A and c.-17_12del, which were inherited from mother and father, respectively. A literature review confirmed that myoclonic seizures were observed in 28.5% of patients with epilepsy. No other patients had progressive myoclonic epilepsy or cognitive decline in association with loss-of-function variations in NGLY1. Conclusion: Our data provides evidence that a group of patients with CDDG1 manifest slowly progressive myoclonic epilepsy and cognitive decline during the long-term clinical course.

    DOI: 10.1016/j.ejmg.2023.104895

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  • Persistent intracranial hyper-inflammation in ruptured cerebral aneurysm after COVID-19: case report and review of the literature

    Chong, PF; Higashi, K; Matsuoka, W; Arimura, K; Sangatsuda, Y; Iwaki, K; Sonoda, Y; Ichimiya, Y; Kamori, A; Kawakami, A; Mizuguchi, S; Kaku, N; Sakai, Y; Ohga, S

    BMC NEUROLOGY   24 ( 1 )   17   2024.1   eISSN:1471-2377

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    Language:English   Publisher:BMC Neurology  

    Background: The systemic manifestations of coronavirus disease 2019 (COVID-19) include hyperinflammatory reactions in various organs. Recent studies showed evidence for the frequent involvement of central nervous system in affected patients; however, little is known about clinical features of cerebrovascular diseases in childhood-onset COVID-19. Case presentation: A 10-year-old boy recovered from SARS-CoV-2 infection without complication. On 14 days after infection, he presented with loss of consciousness. A head computed tomography detected a ruptured cerebral aneurysm at the left posterior cerebral artery accompanying subarachnoid hemorrhage (SAH). Immediate surgical intervention did not rescue the patient, resulting in the demise 7 days after admission. Serological and genetic tests excluded the diagnosis of vasculitis and connective tissue disorders. Retrospective analysis showed markedly higher levels of interleukin (IL)-1β, IL-6 and IL-8 in the cerebrospinal fluid than the serum sample concurrently obtained. A review of literature indicated that adult patients with COVID-19 have a risk for the later development of SAH during the convalescent phase of COVID-19. Conclusions: SAH is a severe complication of COVID-19 in children and adults who have asymptomatic cerebrovascular aneurysms. The markedly high levels of cytokines detected in the cerebrospinal fluid suggested that intracranial hyperinflammatory condition might be one of the possible mechanisms involved in the rupture of a preexisting cerebrovascular aneurysms.

    DOI: 10.1186/s12883-023-03493-z

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  • Diagnostic MR imaging features of hypomyelination of early myelinating structures: A case report

    Abe, T; Yamashita, K; Kikuchi, K; Hatai, E; Fujii, F; Chong, PF; Sakai, Y; Saitsu, H; Inoue, K; Togao, O; Ishigami, K

    NEURORADIOLOGY JOURNAL   19714009231224419   2023.12   ISSN:1971-4009 eISSN:2385-1996

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    Language:English   Publisher:Neuroradiology Journal  

    Hypomyelination of early myelinating structures (HEMS) has recently been defined as a new genetic disorder accompanied by clinical and MR imaging characteristics. However, no studies have focused on diffusion-weighted imaging (DWI) findings of HEMS. We would like to propose a “sheep sign,” which is formed by DWI hyperintensity in the medial medullary lamina along with alternating high-low-high (HLH) intensity stripes in the posterior limb of the internal capsule. We believe the presence of the “sheep sign” on DWI in combination with alternating HLH intensity stripes may be a valuable tool for diagnosing HEMS.

    DOI: 10.1177/19714009231224419

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  • Heterogeneity and mitochondrial vulnerability configurate the divergent immunoreactivity of human induced microglia-like cells

    Yonemoto, K; Fujii, F; Taira, R; Ohgidani, M; Eguchi, K; Okuzono, S; Ichimiya, Y; Sonoda, Y; Chong, PF; Goto, H; Kanemasa, H; Motomura, Y; Ishimura, M; Koga, Y; Tsujimura, K; Hashiguchi, T; Torisu, H; Kira, R; Kato, TA; Sakai, Y; Ohga, S

    CLINICAL IMMUNOLOGY   255   109756   2023.10   ISSN:1521-6616 eISSN:1521-7035

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    Language:English   Publisher:Clinical Immunology  

    Microglia play versatile roles in progression of and protection against neuroinflammatory diseases. Little is known, however, about the mechanisms underlying the diverse reactivity of microglia to inflammatory conditions. We investigated how human induced microglia-like (iMG) cells respond to innate immune ligands. Quantitative PCR showed that poly-I:C and lipopolysaccharide (LPS) activated the expression of IL1B and TNF. Immunoreactivity of iMG did not differ between controls (n = 11) and patients with neuroinflammatory diseases (n = 24). Flow cytometry revealed that CD14high cells expressed interleukin (IL) -1β after LPS treatment. Immunoblotting showed that poly-I:C and LPS differentially activated inflammatory pathways but commonly induced mitochondrial instability and the expression of pyruvate kinase isoform M2 (PKM2). Furthermore, a potent stimulator of PKM2 (DASA-58) alleviated IL-1β production after LPS treatment. These data indicate that heterogeneous cell populations and mitochondrial stability underlie the divergent immunoreactivity of human iMG in environments.

    DOI: 10.1016/j.clim.2023.109756

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  • Critical vitamin deficiencies in autism spectrum disorder: Reversible and irreversible outcomes

    Chong, PF; Torio, M; Fujii, F; Hirata, Y; Matsuoka, W; Sonoda, Y; Ichimiya, Y; Yada, Y; Kaku, N; Ishimura, M; Sasazuki, M; Koga, Y; Sanefuji, M; Sakai, Y; Ohga, S

    EUROPEAN JOURNAL OF CLINICAL NUTRITION   76 ( 11 )   1618 - 1621   2022.11   ISSN:0954-3007 eISSN:1476-5640

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    Language:English   Publisher:European Journal of Clinical Nutrition  

    Vitamin deficiencies are an emerging concern in the management of children with autism spectrum disorder (ASD). Particular attention is required for recognizing the variable signs caused by unbalanced food intakes. We herein report two patients with multiple vitamin deficiencies who needed critical care showing different prognoses. Patient 1 with ‘Shoshin’ beriberi presenting with cardiac arrest had thiamine deficiency developed severe neurological sequelae despite rapid vitamin supplementation. Patient 2, who had leg pain and a limping gait, showed a rapid recovery with intravenous infusion and tube feeding after being diagnosed with scurvy. A literature search revealed several children with ASD with critically ill thiamine deficiency, but few reports documented a life-threatening condition in the form of cardiac arrest at the onset. Considering the high observation rate of food selectivity in children with ASD, early intervention is required to prevent the exacerbation of vitamin deficiencies to severe neurological disabilities.

    DOI: 10.1038/s41430-022-01170-x

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  • Genotype-phenotype correlation in six patients with interstitial deletions spanning 13q31

    Muramatsu M., Shimojima-Yamamoto K., Chong P.F., Kira R., Okamoto N., Yamamoto T.

    No To Hattatsu   54 ( 5 )   317 - 322   2022   ISSN:00290831

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    Publisher:No To Hattatsu  

    Objective:Since the gene responsible for neurodevelopmental delay observed in patients with chromosomal microdeletions involving the 13q31 region has never been identified, we aimed to narrow the candidate genes. Methods:Analysis of genomic copy number variations was performed as a part of the diagnostic workflow for six patients with neurodevelopmental disorders. Detailed clinical information was collected for each patient carrying a 13q31 deletion. Then, genotype-phenotype correlation analysis was carried out. Results:Genotype-phenotypic correlation analysis excluded regions that were not considered disease-related and focused on the shortest region overlapped between three patients (chr13:75691448_83625667). Among the genes included in this region, MYCBP2 showed a pLI score of “1”, suggesting haploinsufficiency intolerance, and was therefore considered as one of the possible candidate genes for neurodevelopmental delay. Conclusions:There is little information on chromosomal microdeletions involving the 13q31 region, and more information should be accumulated to understand better the genomic contribution of this region.

    DOI: 10.11251/ojjscn.54.317

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  • Clinical and electrophysiological features of acute flaccid myelitis: A national cohort study Reviewed International journal

    Chong, P. F. @Torisu, H. @Yasumoto, S. @Okumura, A. @Mori, H. @Sato, T. @Kimura, J. Ohga, S. @Tanaka-Taya, K. Kira, R.

    Clin Neurophysiol   2021.7

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    DOI: 10.1016/j.clinph.2021.07.013

  • Acute flaccid myelitis: cause, diagnosis, and management Reviewed International journal

    @Murphy, O. C. @Messacar, K. @Benson, L. @Bove, R. @Carpenter, J. L. @Crawford, T. @Dean, J. @DeBiasi, R. @Desai, J. @Elrick, M. J. @Farias-Moeller, R. @Gombolay, G. Y. @Greenberg, B. @Harmelink, M. @Hong, S. @Hopkins, S. E. @Oleszek, J. @Otten, C. @Sadowsky, C. L. @Schreiner, T. L. @Thakur, K. T. @Van Haren, K. @Carballo, C. M. Chong, P. F. @Fall, A. @Gowda, V. K. @Helfferich, J. @Kira, R. @Lim, M. @Lopez, E. L. @Wells, E. M. @Yeh, E. A. @Pardo, C. A.

    Lancet   2020.12

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    DOI: 10.1016/s0140-6736(20)32723-9

  • Clinical Features of Acute Flaccid Myelitis Temporally Associated With an Enterovirus D68 Outbreak: Results of a Nationwide Survey of Acute Flaccid Paralysis in Japan, August-December 2015 Reviewed International journal

    Chong, P. F. @Kira, R. @Mori, H. @Okumura, A. @Torisu, H. @Yasumoto, S. @Shimizu, H. @Fujimoto, T. @Hanaoka, N. @Kusunoki, S. @Takahashi, T. @Oishi, K. @Tanaka-Taya, K.

    Clin Infect Dis   2017.10

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    Language:English   Publishing type:Research paper (scientific journal)  

    DOI: 10.1093/cid/cix860

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Professional Memberships

  • 日本小児科学会

  • 日本小児神経学会

  • 日本てんかん学会

Research Projects

  • 発達期の欠神てんかんと注意欠如・多動性障害の関連の解明~定量的脳波・遺伝子解析~

    Grant number:22K07893  2022.4 - 2026.3

    科学研究費助成事業  基盤研究(C)

    園田 有里, 實藤 雅文, 吉良 龍太郎, Chong Pin・Fee

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    Grant type:Scientific research funding

    小児欠神てんかん(CAE)は、4-8歳に好発するてんかんであり、脳波検査では特徴的な3Hz棘徐波複合を呈する。CAEには、高率に注意欠如・多動症(ADHD)を合併するが、その成因は明らかでない。申請者はCAEの診断時の脳波を定量的に解析する方法を確立した。本研究では、CAE・ADHDを合併する小児が示す脳波の特徴を明らかにし、両疾患に関与する遺伝的要因の有無を検証する。CAEとADHD発症の重複メカニズムを明らかにすることで、小児てんかん全般に合併する発達障害の発生機序を研究するプラットフォームを提供するとともに、ADHDを合併するCAEに対する転帰予測の支援と障害予後の改善を目的とする。

    CiNii Research

  • 小児脳炎における疫学調査および自己抗体の網羅的解析

    Grant number:19K10613  2019.4 - 2024.3

    科学研究費助成事業  基盤研究(C)

    Chong Pin・Fee, 酒井 康成

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    Grant type:Scientific research funding

    本研究の概要は、福岡県を中心とした九州内の小児医療機関の多施設、前向きコホート研究を基盤とした小児脳炎の疫学調査である。感染性脳炎、自己免疫性脳炎、中枢脱髄性疾患の割合、発症頻度を始め、異なる病態ごと脳炎の予後の相違等を明らかにするために行う研究である。

    CiNii Research

Class subject

  • 臨床医学Ⅳ-②

    2024.4 - 2024.9   First semester

  • 臨床医学群(神経)

    2023.10 - 2024.3   Second semester