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January 15, 2013; 80 (3) Article

Biotin-responsive basal ganglia disease revisited

Clinical, radiologic, and genetic findings

Brahim Tabarki, Shatha Al-Shafi, Saad Al-Shahwan, Zeeshan Azmat, Amel Al-Hashem, Nawal Al-Adwani, Nabil Biary, Mohamed Al-Zawahmah, Sonia Khan, Giulio Zuccoli
First published December 26, 2012, DOI: https://doi.org/10.1212/WNL.0b013e31827deb4c
Brahim Tabarki
From the Divisions of Pediatric Neurology (B.T., S. Al-Shafi, S. Al-Shahwan) and Genetics (A.A.-H.), Department of Pediatrics; Department of Radiology (Z.A., N.A-A.); Department of Neurosciences (N.B., M.A.-Z., S.K.), Riyadh Military Hospital, Kingdom of Saudi Arabia; and Department of Radiology (G.Z.), Children's Hospital of Pittsburgh of UPMC, Pittsburgh, PA.
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Shatha Al-Shafi
From the Divisions of Pediatric Neurology (B.T., S. Al-Shafi, S. Al-Shahwan) and Genetics (A.A.-H.), Department of Pediatrics; Department of Radiology (Z.A., N.A-A.); Department of Neurosciences (N.B., M.A.-Z., S.K.), Riyadh Military Hospital, Kingdom of Saudi Arabia; and Department of Radiology (G.Z.), Children's Hospital of Pittsburgh of UPMC, Pittsburgh, PA.
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Saad Al-Shahwan
From the Divisions of Pediatric Neurology (B.T., S. Al-Shafi, S. Al-Shahwan) and Genetics (A.A.-H.), Department of Pediatrics; Department of Radiology (Z.A., N.A-A.); Department of Neurosciences (N.B., M.A.-Z., S.K.), Riyadh Military Hospital, Kingdom of Saudi Arabia; and Department of Radiology (G.Z.), Children's Hospital of Pittsburgh of UPMC, Pittsburgh, PA.
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Zeeshan Azmat
From the Divisions of Pediatric Neurology (B.T., S. Al-Shafi, S. Al-Shahwan) and Genetics (A.A.-H.), Department of Pediatrics; Department of Radiology (Z.A., N.A-A.); Department of Neurosciences (N.B., M.A.-Z., S.K.), Riyadh Military Hospital, Kingdom of Saudi Arabia; and Department of Radiology (G.Z.), Children's Hospital of Pittsburgh of UPMC, Pittsburgh, PA.
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Amel Al-Hashem
From the Divisions of Pediatric Neurology (B.T., S. Al-Shafi, S. Al-Shahwan) and Genetics (A.A.-H.), Department of Pediatrics; Department of Radiology (Z.A., N.A-A.); Department of Neurosciences (N.B., M.A.-Z., S.K.), Riyadh Military Hospital, Kingdom of Saudi Arabia; and Department of Radiology (G.Z.), Children's Hospital of Pittsburgh of UPMC, Pittsburgh, PA.
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Nawal Al-Adwani
From the Divisions of Pediatric Neurology (B.T., S. Al-Shafi, S. Al-Shahwan) and Genetics (A.A.-H.), Department of Pediatrics; Department of Radiology (Z.A., N.A-A.); Department of Neurosciences (N.B., M.A.-Z., S.K.), Riyadh Military Hospital, Kingdom of Saudi Arabia; and Department of Radiology (G.Z.), Children's Hospital of Pittsburgh of UPMC, Pittsburgh, PA.
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Nabil Biary
From the Divisions of Pediatric Neurology (B.T., S. Al-Shafi, S. Al-Shahwan) and Genetics (A.A.-H.), Department of Pediatrics; Department of Radiology (Z.A., N.A-A.); Department of Neurosciences (N.B., M.A.-Z., S.K.), Riyadh Military Hospital, Kingdom of Saudi Arabia; and Department of Radiology (G.Z.), Children's Hospital of Pittsburgh of UPMC, Pittsburgh, PA.
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Mohamed Al-Zawahmah
From the Divisions of Pediatric Neurology (B.T., S. Al-Shafi, S. Al-Shahwan) and Genetics (A.A.-H.), Department of Pediatrics; Department of Radiology (Z.A., N.A-A.); Department of Neurosciences (N.B., M.A.-Z., S.K.), Riyadh Military Hospital, Kingdom of Saudi Arabia; and Department of Radiology (G.Z.), Children's Hospital of Pittsburgh of UPMC, Pittsburgh, PA.
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Sonia Khan
From the Divisions of Pediatric Neurology (B.T., S. Al-Shafi, S. Al-Shahwan) and Genetics (A.A.-H.), Department of Pediatrics; Department of Radiology (Z.A., N.A-A.); Department of Neurosciences (N.B., M.A.-Z., S.K.), Riyadh Military Hospital, Kingdom of Saudi Arabia; and Department of Radiology (G.Z.), Children's Hospital of Pittsburgh of UPMC, Pittsburgh, PA.
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Giulio Zuccoli
From the Divisions of Pediatric Neurology (B.T., S. Al-Shafi, S. Al-Shahwan) and Genetics (A.A.-H.), Department of Pediatrics; Department of Radiology (Z.A., N.A-A.); Department of Neurosciences (N.B., M.A.-Z., S.K.), Riyadh Military Hospital, Kingdom of Saudi Arabia; and Department of Radiology (G.Z.), Children's Hospital of Pittsburgh of UPMC, Pittsburgh, PA.
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Citation
Biotin-responsive basal ganglia disease revisited
Clinical, radiologic, and genetic findings
Brahim Tabarki, Shatha Al-Shafi, Saad Al-Shahwan, Zeeshan Azmat, Amel Al-Hashem, Nawal Al-Adwani, Nabil Biary, Mohamed Al-Zawahmah, Sonia Khan, Giulio Zuccoli
Neurology Jan 2013, 80 (3) 261-267; DOI: 10.1212/WNL.0b013e31827deb4c

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Abstract

Objective: To investigate the clinical, genetic, and neuroradiologic data of biotin-responsive basal ganglia disease (BBGD) and clarify the disease spectrum.

Methods: We first investigated all patients attending our Division of Pediatric Neurology with a genetically proven diagnosis of BBGD between 2009 and 2011. All patients underwent a detailed medical history and clinical examination, extensive laboratory investigations including genetic tests, and brain MRI. Finally, we conducted a systematic review of the literature.

Results: We enrolled 10 patients meeting the diagnostic criteria for BBGD, and analyzed the data on 14 patients from 4 previous reports. The BBGD occurred predominantly in preschool/school-aged patients in the Saudi population, but it was also observed in other ethnic groups. The typical clinical picture consisted of recurrent subacute encephalopathy leading to coma, seizures, and extrapyramidal manifestations. The brain MRI typically showed symmetric and bilateral lesions in the caudate nucleus and putamen, infra- and supratentorial brain cortex, and in the brainstem. Vasogenic edema characterized the acute crises as demonstrated by diffusion-weighted imaging/apparent diffusion coefficient MRI. Atrophy and gliosis in the affected regions were observed in patients with chronic disease. Early treatment with a combination of biotin and thiamine resulted in clinical and neuroradiologic improvement. Death and neurologic sequelae including dystonia, mental retardation, and epilepsy were observed in those who were not treated or were treated late.

Conclusion: BBGD is an underdiagnosed pan-ethnic treatable condition. Clinicians caring for patients with unexplained encephalopathy and neuroimaging showing vasogenic edema in the bilateral putamen and caudate nuclei, infra- and supratentorial cortex, and brainstem should consider this disorder early in the hospital course because a therapeutic trial with biotin and thiamine can be lifesaving.

Glossary

BBGD=
biotin-responsive basal ganglia disease;
hTHTR2=
human thiamine transporter 2;
WE=
Wernicke encephalopathy

Footnotes

  • Go to Neurology.org for full disclosures. Funding information and disclosures deemed relevant by the authors, if any, are provided at the end of the article.

  • Supplemental data at www.neurology.org

  • Received May 9, 2012.
  • Accepted August 27, 2012.
  • © 2012 American Academy of Neurology
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