Biotin-Thiamine Responsive Encephalopathy: Report of an Egyptian Family with a Novel SLC19A3 Mutation and Review of the Literature

Savasta, Salvatore; Bassanese, Francesco; Buschini, Chiara; Foiadelli, Thomas; Trabatti, Chiara; Efthymiou, Stéphanie; Salpietro, Vincenzo; Houlden, Henry; Simoncelli, Annamaria; Marseglia, Gian Luigi

doi:10.1055/s-0038-1676603

Cited by 9 publications

(11 citation statements)

References 40 publications

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“…The clinical pictures in patients with infantile phenotypes were almost the same, all manifesting an acute devastating course during early months of life, with feeding difficulties, inconsolable crying or lethargy, loss of milestones. Respiratory failure and hypotonia were more common in patients of this group ( Yamada et al, 2010 ; Perez-Duenas et al, 2013 ; Gerards et al, 2013 ; Kevelam et al, 2013 ; Sremba et al, 2014 ; Ygberg et al, 2016 ; Alfadhel, 2017 ; Algahtani et al, 2017 ; Pronicki et al, 2017 ; Savasta et al, 2019 ). Wernicke’s-like encephalopathy was only described in two Japanese patients ( Kono et al, 2009 ).…”

Section: Discussionmentioning

confidence: 77%

“…Including our study, a total of 159 patients were diagnosed with THMD2 in 40 reports ( Ozand et al, 1998 ; Adhisivam et al, 2007 ; El-Hajj et al, 2008 ; Bindu et al, 2009 ; Kono et al, 2009 ; Debs et al, 2010 ; Yamada et al, 2010 ; Serrano et al, 2012 ; Alfadhel et al, 2013 ; Fassone et al, 2013 ; Gerards et al, 2013 ; Kevelam et al, 2013 ; Perez-Duenas et al, 2013 ; Tabarki et al, 2013a , b , 2015 ; Distelmaier et al, 2014 ; Haack et al, 2014 ; Kassem et al, 2014 ; Ortigoza-Escobar et al, 2014 , 2016 , 2017 ; Schanzer et al, 2014 ; Sremba et al, 2014 ; Kohrogi et al, 2015 ; Aljabri et al, 2016 ; Bin Saeedan and Dogar, 2016 ; Bubshait et al, 2016 ; Flones et al, 2016 ; Schwarting et al, 2016 ; Ygberg et al, 2016 ; Alfadhel, 2017 ; Algahtani et al, 2017 ; Eichler et al, 2017 ; Pronicki et al, 2017 ; Whitford et al, 2017 ; Gowda et al, 2018 ; Tonduti et al, 2018 ; Savasta et al, 2019 ; Li et al, 2020 ). Thirteen patients were excluded, including 9 patients without genetic results and 4 patients without clinical information.…”

Section: Resultsmentioning

confidence: 99%

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Report of the Largest Chinese Cohort With SLC19A3 Gene Defect and Literature Review

Wang

Han

et al. 2021

Front. Genet.

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Thiamine metabolism dysfunction syndrome 2 (THMD2) is a rare metabolic disorder caused by SLC19A3 mutations, inherited in autosomal recessive pattern. As a treatable disease, early diagnosis and therapy with vitamin supplementation is important to improve the prognosis. So far, the reported cases were mainly from Saudi Arab regions, and presented with relatively simple clinical course because of the hot spot mutation (T422A). Rare Chinese cases were described until now. In this study, we investigated 18 Chinese THMD2 patients with variable phenotypes, and identified 23 novel SLC19A3 mutations, which expanded the genetic and clinical spectrum of the disorder. Meanwhile, we reviewed all 146 reported patients from different countries. Approximately 2/3 of patients presented with classical BTBGD, while 1/3 of patients manifested as much earlier onset and poor prognosis, including infantile Leigh-like syndrome, infantile spasms, neonatal lactic acidosis and infantile BTBGD. Literature review showed that elevated lactate in blood and CSF, as well as abnormal OXPHOS activities of muscle or skin usually correlated with infantile phenotypes, which indicated poor outcome. Brainstem involvement on MRI was more common in deceased cases. Thiamine supplementation is indispensable in the treatment of THMD2, whereas combination of biotin and thiamine is not superior to thiamine alone. But biotin supplementation does work in some patients. Genotypic-phenotypic correlation remains unclear which needs further investigation, and biallelic truncated mutations usually led to more severe phenotype.

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Section: Discussionmentioning

confidence: 77%

Section: Resultsmentioning

confidence: 99%

Report of the Largest Chinese Cohort With SLC19A3 Gene Defect and Literature Review

Wang

Han

et al. 2021

Front. Genet.

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“…It is a pan ethnic disease with most cases diagnosed in Saudi Arab. 2 Affected patients usually present in childhood, with average age of diagnosis 8 years; however, patients have been diagnosed as late as age 33 years. 3 Clinical characterization consists of three different stages with variable combinations of encephalopathy, seizures, coma, and death.…”

Section: Introductionmentioning

confidence: 99%

Biotin–Thiamine Responsive Basal Ganglia Disease Presented as Intractable Seizure in a 1-Month-Old Infant

Verlani

Agarwal

Singh

et al. 2020

Journal of Pediatric Neurology

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Biotin–thiamine responsive basal ganglia disease is a neurometabolic disorder, seen in children presenting with encephalopathy, seizures, and positive family history. The disease is diagnosed based on typical magnetic resonance imaging (MRI) findings and whole exome sequencing but may be initially misdiagnosed as a mitochondrial encephalopathy or an inborn error of metabolism (IEM). We describe the case of an infant who presented with uncontrolled seizures and encephalopathy, responding to high doses of thiamine and biotin. Life-long supplementation of biotin (2–10 mg/kg/day) and thiamine (200–300 mg/day) improves the symptomatology and prevents relapse. Outcomes of the disease are heterogeneous, ranging in scope from complete remission to severe neurological sequelae.

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“…A fourth shortcoming is that no discussion was hold about the possibility that all the lesions seen on MRI were multi-locular stroke-like lesions (SLLs). 4 Since at least the supra-tentorial lesion were hyperintense on DWI and also the infra-tentorial lesions were described as DWI hyperintense, we should know if corresponding ADC maps were hyperintense, isointense, or hypointense. Knowing if a cytotoxic or vasogenic edema was present is crucial as therapy may be different from that applied in this case.…”

mentioning

confidence: 99%

“…Such poor prognosis is especially common in patients with early neonatal Leighlike syndrome and the early infantile-onset form of BTBGD, as in our patient, even when treated with biotin and thiamine. 2,3 The fact that these patients show neurodevelopmental problems in various degrees despite early treatment 4,5 indicates that it may be too late to prevent permanent brain damage even when treatment is started at the time of the first symptoms. 6…”

mentioning

confidence: 99%

Are homozygous SLC19A3 deletions non-responsive to thiamine/biotin?

Finsterer¹

2020

Turk J Pediatr

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Biotin-Thiamine Responsive Encephalopathy: Report of an Egyptian Family with a Novel SLC19A3 Mutation and Review of the Literature

Cited by 9 publications

References 40 publications

Report of the Largest Chinese Cohort With SLC19A3 Gene Defect and Literature Review

Report of the Largest Chinese Cohort With SLC19A3 Gene Defect and Literature Review

Biotin–Thiamine Responsive Basal Ganglia Disease Presented as Intractable Seizure in a 1-Month-Old Infant

Are homozygous SLC19A3 deletions non-responsive to thiamine/biotin?

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