Clinical characteristics.

Biotin-thiamine-responsive basal ganglia disease (BTBGD) may present in early infancy, childhood, or adulthood. Early-infantile BTBGD presents before age three months with vomiting, feeding difficulties, encephalopathy, hypotonia, seizures, and respiratory failure. Classic BTBGD presents between ages three and ten years with recurrent subacute encephalopathy manifesting as confusion, seizures, ataxia, supranuclear facial palsy, external ophthalmoplegia, and/or dysphagia that, if left untreated, can eventually lead to coma and even death. Dystonia and cogwheel rigidity are nearly always present; hyperreflexia, ankle clonus, and Babinski responses are common. Hemiparesis or quadriparesis may be seen. Episodes are often triggered by febrile illness or mild trauma or stress. Simple partial or generalized seizures are easily controlled with anti-seizure medication. Adult Wernicke-like encephalopathy BTBGD, described in three individuals to date, presents after age ten years with acute onset of status epilepticus, ataxia, nystagmus, diplopia, and ophthalmoplegia.

Prompt administration of biotin and thiamine early in the disease course results in partial or complete improvement within days in classic and adult BTBGD; however, most infants with early-infantile BTBGD have a poor outcome.

Diagnosis/testing.

The diagnosis of BTBGD is established in a proband with biallelic pathogenic variants in SLC19A3 identified by molecular genetic testing.

Management.

Targeted therapies: Biotin (5-10 mg/kg/day) and thiamine (up to 40 mg/kg/day with a maximum of 1,500 mg daily) are given orally as early in the disease course as possible and are continued lifelong. During acute decompensations thiamine may be increased to double the regular dose and given intravenously. Disease manifestations typically resolve within days in classic and adult BTBGD.

Supportive care: Acute encephalopathic episodes may require care in an ICU to manage seizures and increased intracranial pressure; thiamine may be increased to double the regular dose and given intravenously. Anti-seizure medication is used to control seizures. Treatment of dystonia is symptomatic and includes administration of trihexyphenidyl or levodopa. Rehabilitation, physical therapy, occupational therapy, and speech therapy as needed and adaptation of educational programs to meet individual needs. Education of the family regarding the importance of lifelong adherence to medical therapy.

Surveillance: At each visit, review neurologic status and assess developmental progress, educational needs, social support, and need for care coordination.

Agents/circumstances to avoid: Avoid use of sodium valproate to treat epilepsy. Use of ACTH to treat epileptic spasms can induce status dystonicus.

Evaluation of relatives at risk: It is appropriate to clarify the genetic status of apparently asymptomatic older and younger sibs of an affected individual to identify as early as possible those who would benefit from prompt initiation of treatment with biotin and thiamine and information about agents/circumstances to avoid.

Pregnancy management: Affected women should continue thiamine and biotin during pregnancy.

Genetic counseling.

BTBGD is inherited in an autosomal recessive manner. If both parents are known to be heterozygous for an SLC19A3 pathogenic variant, each sib of an affected individual has at conception a 25% chance of being affected, a 50% chance of being an asymptomatic carrier, and a 25% chance of being unaffected and not a carrier. Once the SLC19A3 pathogenic variants have been identified in an affected family member, carrier testing for at-risk family members and prenatal/preimplantation genetic testing for BTBGD are possible.

Suggestive Findings

BTBGD should be suspected in probands with the following clinical, laboratory, and imaging findings (by phenotype) and family history.

Establishing the Diagnosis

The diagnosis of BTBGD is established in a proband with suggestive findings and biallelic pathogenic (or likely pathogenic) variants in SLC19A3 identified by molecular genetic testing (see Table 1).

Note: (1) Per ACMG/AMP variant interpretation guidelines, the terms "pathogenic variant" and "likely pathogenic variant" are synonymous in a clinical setting, meaning that both are considered diagnostic and can be used for clinical decision making [Richards et al 2015]. Reference to "pathogenic variants" in this GeneReview is understood to include likely pathogenic variants. (2) Identification of biallelic SLC19A3 variants of uncertain significance (or of one known SLC19A3 pathogenic variant and one SLC19A3 variant of uncertain significance) does not establish or rule out the diagnosis.

Molecular genetic testing approaches can include a combination of gene-targeted testing (single-gene testing, multigene panel) and comprehensive genomic testing (exome sequencing, genome sequencing). Gene-targeted testing requires that the clinician determine which gene(s) are likely involved (see Option 1), whereas comprehensive genomic testing does not (see Option 2).

Clinical Description

Biotin-thiamine-responsive basal ganglia disease (BTBGD), resulting from the inability of thiamine to cross the blood-brain barrier, comprises three age-related phenotypes: early-infantile BTBGD (presenting by age 3 months), classic (childhood) BTBGD (ages 3-10 years), and adult Wernicke-like encephalopathy BTBGD (age >10 years). To date, more than 169 individuals have been identified with biallelic pathogenic variants in SLC19A3 [Wang et al 2021]. The following descriptions of the phenotypic features associated with BTBGD is based on this report.

Early-infantile BTBGD is characterized by poor feeding, vomiting, acute encephalopathy, and severe lactic acidosis. One child had exaggerated eye opening and paroxysmal tonic downgaze [Maney et al 2023]. Four infants had atypical infantile spasms [Yamada et al 2010]. Most children in this group have had poor outcome or even death (even after supplementation with biotin and thiamine). Of note, the child reported by Maney et al [2023] showed partial response to vitamin supplementation.

Classic BTBGD usually presents between ages three and ten years; however, exceptions include onset in one infant at age one month [Pérez-Dueñas et al 2013, Kobayashi et al 2022] and one adult at age 20 years [Debs et al 2010].

Most commonly, classic BTBGD is characterized by recurrent acute/subacute onset of encephalopathy, often triggered by febrile illness, mild trauma, or stress, manifesting as confusion, seizures, ataxia, dystonia, supranuclear facial palsy, external ophthalmoplegia, and/or dysphagia. The encephalopathy may be associated with raised intracranial pressure.

Dystonia and cogwheel rigidity are nearly always present. Hyperreflexia, ankle clonus, and Babinski responses are common. Hemiparesis or quadriparesis may be seen.

Seizures are mainly simple partial or generalized and are easily controlled with anti-seizure medication. Infantile spasms also occur [Yamada et al 2010].

Administration of biotin and thiamine early in the disease course results in complete clinical improvement within days (see Management, Targeted Therapies). Lifelong treatment is required. Treatment initiated later in the disease course or lack of treatment may result in death or chronic neurologic sequelae including dystonia, quadriparesis, epilepsy, and/or mild intellectual disability.

Adult Wernicke-like encephalopathy BTBGD is characterized by acute onset of status epilepticus, ataxia, nystagmus, diplopia, and ophthalmoplegia in the second decade of life [Kono et al 2009].

Affected individuals show dramatic response to high doses of thiamine (see Management, Targeted Therapies).

Prevalence

Biotin-thiamine-responsive basal ganglia disease (BTBGD) is pan ethnic.

Of note, homozygosity for the Saudi Arabian founder variant c.1264A>G (p.Thr422Ala) accounts for 52% (76/146) of BTBGD in that population (see Table 6).

The carrier frequency of the SLC19A3 c.1264A>G (p.Thr422Ala) pathogenic variant in the Saudi Arabian population is 1:500 [Alfadhel et al 2019].

Genotype-Phenotype Correlations

Although genotype-phenotype correlations remain unclear, the following have been observed:

• Biallelic SLC19A3 pathogenic variants predicted to cause loss of function are more likely to be associated with early-infantile BTBGD.
• Compound heterozygosity for one SLC19A3 missense pathogenic variant and one predicted loss-of-function variant has been associated with classic BTBGD.
• Homozygosity for the founder Saudi Arabian pathogenic variant c.1264A>G (p.Thr422Ala) is associated with classic BTBGD and, in some individuals, mitochondrial DNA depletion [Felhi et al 2023].

Evaluations Following Initial Diagnosis

To establish the extent of disease and needs in an individual diagnosed with BTBGD, the evaluations summarized in Table 3 (if not performed as part of the evaluation that led to the diagnosis) are recommended.

Treatment of Manifestations

Surveillance

To monitor existing manifestations, the individual's response to supportive care, and the emergence of new manifestations, the evaluations summarized in Table 5 are recommended at each visit.

Agents/Circumstances to Avoid

Use of sodium valproate for treatment of epilepsy should be avoided.

Use of adrenocorticotropic hormone (ACTH) for epileptic spasms in individuals with BTBGD can induce status dystonicus [Hoshino & Kanemura 2022].

Evaluation of Relatives at Risk

It is appropriate to clarify the genetic status of apparently asymptomatic older and younger at-risk sibs of an affected individual to identify as early as possible those who would benefit from prompt initiation of treatment with biotin and thiamine and avoidance of use of sodium valproate (for treatment of epilepsy) or ACTH (for treatment of infantile spasms).

See Genetic Counseling for issues related to testing of at-risk relatives for genetic counseling purposes.

Pregnancy Management

Affected women should continue biotin and thiamine therapy during pregnancy. No information regarding risk to the fetus of an affected mother is available.

Therapies Under Investigation

Search ClinicalTrials.gov in the US and EU Clinical Trials Register in Europe for access to information on clinical studies for a wide range of diseases and conditions. Note: There may not be clinical trials for this disorder.

Mode of Inheritance

Biotin-thiamine-responsive basal ganglia disease (BTBGD) is inherited in an autosomal recessive manner.

Risk to Family Members

Parents of a proband

• The parents of an affected individual are presumed to be heterozygous for an SLC19A3 pathogenic variant.
• Molecular genetic testing is recommended for the parents of a proband to confirm that both parents are heterozygous for an SLC19A3 pathogenic variant and to allow reliable recurrence risk assessment.
• If a pathogenic variant is detected in only one parent and parental identity testing has confirmed biological maternity and paternity, it is possible that one of the pathogenic variants identified in the proband occurred as a de novo event in the proband or as a postzygotic de novo event in a mosaic parent [Jónsson et al 2017, Maney et al 2023]. If the proband appears to have homozygous pathogenic variants (i.e., the same two pathogenic variants), additional possibilities to consider include:
  • A single- or multiexon deletion in the proband that was not detected by sequence analysis and that resulted in the artifactual appearance of homozygosity;
  • Uniparental isodisomy for the parental chromosome with the pathogenic variant that resulted in homozygosity for the pathogenic variant in the proband.
• Heterozygotes (carriers) are asymptomatic and are not at risk of developing the disorder.

Sibs of a proband

• If both parents are known to be heterozygous for an SLC19A3 pathogenic variant, each sib of an affected individual has at conception a 25% chance of being affected, a 50% chance of being an asymptomatic carrier, and a 25% chance of being unaffected and not a carrier.
• Heterozygotes (carriers) are asymptomatic and are not at risk of developing the disorder.

Offspring of a proband. Unless an affected individual's reproductive partner also has BTBGD or is a carrier (see Related Genetic Counseling Issues, Family planning), offspring will be obligate heterozygotes (carriers) for a pathogenic variant in SLC19A3.

Other family members. Each sib of the proband's parents is at a 50% risk of being a carrier of a pathogenic variant in SLC19A3.

Carrier Detection

Carrier testing for at-risk relatives requires prior identification of the SLC19A3 pathogenic variants in the family.

Related Genetic Counseling Issues

See Management, Evaluation of Relatives at Risk for information on evaluating at-risk sibs for the purpose of early diagnosis and treatment.

Family planning

• The optimal time for determination of genetic risk and discussion of the availability of prenatal/preimplantation genetic testing is before pregnancy.
• It is appropriate to offer genetic counseling (including discussion of potential risks to offspring and reproductive options) to young adults who are affected, are carriers, or are at risk of being carriers.
• Carrier testing should be considered for the reproductive partners of individuals affected with BTBGD and individuals known to be carriers of BTBGD, particularly if consanguinity is likely and/or if both partners are of the same ancestry. An SLC19A3 founder variant has been identified in the Saudi Arabian population (see Table 6).

Prenatal Testing and Preimplantation Genetic Testing

Once the SLC19A3 pathogenic variants have been identified in an affected family member, prenatal and preimplantation genetic testing for BTBGD are possible.

Differences in perspective may exist among medical professionals and within families regarding the use of prenatal and preimplantation genetic testing. While use of prenatal and preimplantation genetic testing is a personal decision, discussion of these issues may be helpful.

Molecular Pathogenesis

SLC19A3 encodes thiamine transporter 2 (ThTr-2). A second gene, SLC19A2, encodes thiamine transporter 1 (ThTr-1). Thiamine enters the cytosol by either ThTr-1 or ThTr-2 and is converted into thiamine pyrophosphate (TPP, the active form) by thiamine pyrophosphokinase 1 (TPK1).

Thiamine pyrophosphate is:

• An essential cofactor for transketolase in the cytoplasm;
• Transported into mitochondria, where it binds to pyruvate dehydrogenase and stimulates conversion of pyruvate to acetyl-coenzyme A;
• A cofactor for alpha-ketoglutarate and branched-chain alpha-ketoacid dehydrogenase, entering the tricarboxylic acid cycle for energy production and biosynthesis.

Mechanism of disease causation. Biotin-thiamine-responsive basal ganglia disease (BTBGD) results from loss of ThTr-2 function.

Revision History

• 9 January 2025 (bp) Comprehensive update posted live
• 16 April 2020 (ha) Comprehensive update posted live
• 21 November 2013 (me) Review posted live
• 28 May 2013 (aah) Original submission

Literature Cited

• Aldosari AN. Efficacy of high thiamine dosage in treating patients with biotin thiamine responsive basal ganglia disease: a two case reports. Int J Neurosci. 2024. Epub ahead of print. [PubMed: 38709666]
• Alfadhel M, Almuntashri M, Jadah RH, Bashiri FA, Al Rifai MT, Al Shalaan H, Al Balwi M, Al Rumayan A, Eyaid W, Al-Twaijri W. Biotin-responsive basal ganglia disease should be renamed biotin-thiamine-responsive basal ganglia disease: a retrospective review of the clinical, radiological and molecular findings of 18 new cases. Orphanet J Rare Dis. 2013;8:83. [PMC free article: PMC3691666] [PubMed: 23742248]
• Alfadhel M, Umair M, Almuzzaini B, Alsaif S, AlMohaimeed SA, Almashary MA, Alharbi W, Alayyar L, Alasiri A, Ballow M, AlAbdulrahman A, Alaujan M, Nashabat M, Al-Odaib A, Altwaijri W, Al-Rumayyan A, Alrifai MT, Alfares A, AlBalwi M, Tabarki B. Targeted SLC19A3 gene sequencing of 3000 Saudi newborn: a pilot study toward newborn screening. Ann Clin Transl Neurol. 2019;6:2097-103. [PMC free article: PMC6801173] [PubMed: 31557427]
• Debs R, Depienne C, Rastetter A, Bellanger A, Degos B, Galanaud D, Keren B, Lyon-Caen O, Brice A, Sedel F. Biotin-responsive basal ganglia disease in ethnic Europeans with novel SLC19A3 mutations. Arch Neurol. 2010;67:126-30. [PubMed: 20065143]
• Değerliyurt A, Gündüz M, Ceylaner S, Ünal Ö, Ünal S. Neonatal form of biotin-thiamine-responsive basal ganglia disease. Clues to diagnosis. Turk J Pediatr. 2019;61:261-6. [PubMed: 31951338]
• Felhi R, Sfaihi L, Charif M, Frikha F, Aoiadni N, Kamoun T, Lenaers G, Fakhfakh F. Vitamin B1 deficiency leads to high oxidative stress and mtDNA depletion caused by SLC19A3 mutation in consanguineous family with Leigh syndrome. Metab Brain Dis. 2023;38:2489-97. [PubMed: 37642897]
• Flønes I, Sztromwasser P, Haugarvoll K, Dölle C, Lykouri M, Schwarzlmüller T, Jonassen I, Miletic H, Johansson S, Knappskog PM, Bindoff LA, Tzoulis C. Novel SLC19A3 promoter deletion and allelic silencing in biotin-thiamine-responsive basal ganglia encephalopathy. PLoS One. 2016;11:e0149055. [PMC free article: PMC4749299] [PubMed: 26863430]
• Hoshino H, Kanemura H. ACTH for epileptic spasms in Leigh syndrome with SLC19A3 mutation can induce status dystonicus. Epileptic Disord. 2022;24:171-5. [PubMed: 34789446]
• Huang H, Jiang H, Yang M, Gao Y, Cao L. Case report: biotin-thiamine-responsive basal ganglia disease with severe subdural hematoma on magnetic resonance imaging. Int J Neurosci. 2024;134:184-92. [PubMed: 35775132]
• Jónsson H, Sulem P, Kehr B, Kristmundsdottir S, Zink F, Hjartarson E, Hardarson MT, Hjorleifsson KE, Eggertsson HP, Gudjonsson SA, Ward LD, Arnadottir GA, Helgason EA, Helgason H, Gylfason A, Jonasdottir A, Jonasdottir A, Rafnar T, Frigge M, Stacey SN, Th Magnusson O, Thorsteinsdottir U, Masson G, Kong A, Halldorsson BV, Helgason A, Gudbjartsson DF, Stefansson K. Parental influence on human germline de novo mutations in 1,548 trios from Iceland. Nature. 2017;549:519-22. [PubMed: 28959963]
• Kelsch RD, Nolan DA, Krishnan A. Unusual case of biotin-thiamine responsive encephalopathy without basal ganglia involvement. Pediatr Radiol. 2021;51:485-8. [PubMed: 33000323]
• Kobayashi M, Suzuki Y, Nodera M, Matsunaga A, Kohda M, Okazaki Y, Murayama K, Yamagata T, Osaka H. A Japanese patient with neonatal biotin-responsive basal ganglia disease. Hum Genome Var. 2022;9:35. [PMC free article: PMC9522647] [PubMed: 36175418]
• Kono S, Miyajima H, Yoshida K, Togawa A, Shirakawa K, Suzuki H. Mutations in a thiamine-transporter gene and Wernicke's-like encephalopathy. N Engl J Med. 2009;360:1792-4. [PubMed: 19387023]
• Lail G, Blaser S, Inbar-Feigenberg M. An unusually mild case of biotin-thiamine-responsive basal ganglia disease. Mol Genet Metab Rep. 2023;37:101004. [PMC free article: PMC10694770] [PubMed: 38053933]
• Maney K, Pizoli C, Russ JB. Child neurology: infantile biotin thiamine responsive basal ganglia disease: case report and brief review. Neurology. 2023;100:836-9. [PMC free article: PMC10136005] [PubMed: 36657988]
• McCormick EM, Zolkipli-Cunningham Z, Falk MJ. Mitochondrial disease genetics update: recent insights into the molecular diagnosis and expanding phenotype of primary mitochondrial disease. Curr Opin Pediatr. 2018;30:714-24. [PMC free article: PMC6467265] [PubMed: 30199403]
• Oommen AT, Polavarapu K, Christopher R, Netravathi M. biotin-responsive basal ganglia disease: treatable metabolic disorder with SLC19A3 mutation presenting as rapidly progressive dementia. Neurol India. 2022;70:733-36. [PubMed: 35532649]
• Ortigoza-Escobar JD, Alfadhel M, Molero-Luis M, Darin N, Spiegel R, de Coo IF, Gerards M, Taylor RW, Artuch R, Nashabat M, Rodríguez-Pombo P, Tabarki B, Pérez-Dueñas B; Thiamine Deficiency Study Group. Thiamine deficiency in childhood with attention to genetic causes: Survival and outcome predictors. Ann Neurol. 2017;82:317-30. [PubMed: 28856750]
• Ortigoza-Escobar JD, Molero-Luis M, Arias A, Oyarzabal A, Darín N, Serrano M, Garcia-Cazorla A, Tondo M, Hernández M, Garcia-Villoria J, Casado M, Gort L, Mayr JA, Rodríguez-Pombo P, Ribes A, Artuch R, Pérez-Dueñas B. Free-thiamine is a potential biomarker of thiamine transporter-2 deficiency: a treatable cause of Leigh syndrome. Brain. 2016;139:31-8. [PubMed: 26657515]
• Ozand PT, Gascon GG, Al Essa M, Joshi S, Al Jishi E, Bakheet S, Al Watban J, Al-Kawi MZ, Dabbagh O. Biotin-responsive basal ganglia disease: a novel entity. Brain. 1998;121:1267-79. [PubMed: 9679779]
• Pérez-Dueñas B, Serrano M, Rebollo M, Muchart J, Gargallo E, Dupuits C, Artuch R. Reversible lactic acidosis in a newborn with thiamine transporter-2 deficiency. Pediatrics. 2013;131:e1670-5. [PubMed: 23589815]
• Ramsay J, Morton J, Norris M, Kanungo S. Organic acid disorders. Ann Transl Med. 2018;6:472. [PMC free article: PMC6331355] [PubMed: 30740403]
• Richards S, Aziz N, Bale S, Bick D, Das S, Gastier-Foster J, Grody WW, Hegde M, Lyon E, Spector E, Voelkerding K, Rehm HL, et al Standards and guidelines for the interpretation of sequence variants: a joint consensus recommendation of the American College of Medical Genetics and Genomics and the Association for Molecular Pathology. Genet Med. 2015;17:405-24. [PMC free article: PMC4544753] [PubMed: 25741868]
• Stenson PD, Mort M, Ball EV, Chapman M, Evans K, Azevedo L, Hayden M, Heywood S, Millar DS, Phillips AD, Cooper DN. The Human Gene Mutation Database (HGMD®): optimizing its use in a clinical diagnostic or research setting. Hum Genet. 2020;139:1197-207. [PMC free article: PMC7497289] [PubMed: 32596782]
• Tabarki B, Al-Shafi S, Al-Shahwan S, Azmat S, Al-Hashem A, Al-Adwani, Biary N, Al-Zawahmah M, Khan S, Zuccoli G. Biotin-responsive basal ganglia disease revisited: clinical, neuroradiological, and genetic findings. Neurology. 2013;80:261-7. [PubMed: 23269594]
• Yamada K, Miura K, Hara K, Suzuki M, Nakanishi K, Kumagai T, Ishihara N, Yamada Y, Kuwano R, Tsuji S, Wakamatsu N. A wide spectrum of clinical and brain MRI findings in patients with SLC19A3 mutations. BMC Med Genet. 2010;11:171. [PMC free article: PMC3022826] [PubMed: 21176162]
• Wang J, Wang J, Han X, Liu Z, Ma Y, Chen G, Zhang H, Sun D, Xu R, Liu Y, Zhang Y, Wen Y, Bao X, Chen Q, Fang F. Report of the largest Chinese cohort with SLC19A3 gene defect and literature review. Front Genet. 2021;12:683255. [PMC free article: PMC8281341] [PubMed: 34276785]