Your search keyword '"Thiamine Deficiency genetics"' showing total 64 results

1. Causal relationships of familial hypercholesterolemia with the risk of multiple vitamin deficiencies: a Mendelian randomization study.

Author

Zhang C, Wei G, Zhou H, and Liu L

Subjects

Humans, Proprotein Convertase 9 genetics, Receptors, LDL genetics, Avitaminosis epidemiology, Avitaminosis genetics, Avitaminosis complications, Polymorphism, Single Nucleotide, Female, Male, Risk Factors, Apolipoproteins E genetics, Vitamin D Deficiency complications, Vitamin D Deficiency genetics, Vitamin D Deficiency epidemiology, Thiamine Deficiency epidemiology, Thiamine Deficiency genetics, Mendelian Randomization Analysis, Hyperlipoproteinemia Type II genetics, Hyperlipoproteinemia Type II complications, Hyperlipoproteinemia Type II epidemiology, Hyperlipoproteinemia Type II blood

Abstract

Background: The causal relationship between familial hypercholesterolemia (FH) and various vitamin deficiencies has not yet been elucidated. Therefore, this study investigated the cause-and-effect relationship between FH and the risk of multiple vitamin deficiencies in humans., Methods: Mendelian randomization (MR) analysis was performed by extracting six datasets for FH, FH with ischemic heart disease (IHD), and vitamin deficiency (vitamin A, thiamine, other B-group vitamins, and vitamin D) from the FinnGen study, covering a total of 329,115; 316,290; 354,932; 354,949; 355,411 and 355,238 individuals, respectively., Results: FH was suggestively associated with higher odds of thiamine deficiency [inverse variance weighted odds ratio (OR IVW ) 95% confidence interval (CI): 1.62 (1.03, 2.55), P = 0.036] and vitamin D deficiencies [OR IVW CI: 1.35 (1.04, 1.75), P = 0.024], low-density lipoprotein receptor ( LDLR ) rs112898275 variant, rs11591147 and rs499883 in proprotein convertase subtilisin/kexin 9 ( PCSK9 ), rs9644862 in cyclin-dependent kinase inhibitor 2 B antisense RNA1 ( CDKN2B-AS1 ), and rs142834163 in dedicator of cytokinesis 6 ( DOCK6 ) and rs115478735 in ABO blood group ( ABO ) strongly influenced the risk of thiamine deficiency, while the rs7412 variant in apolipoprotein E ( APOE ) mostly influenced the risk of vitamin D deficiency. FH with IHD was suggestively associated with higher odds of vitamin D deficiency (OR IVW, weighted median [WM][95%CI]: 1.31 [1.05, 1.64]; 1.47 [1.10, 1.97]) ( P = 0.018; 0.010) without any single significant SNPs observed., Conclusion: FH was positively associated with increased risks of thiamine and vitamin D deficiencies, revealing a prospective and unfortunate complication of FH., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Zhang, Wei, Zhou and Liu.)

Published

2024

2. Clinical profile and thiamine transporter gene (SLC19A2 and SLC19A3) variations in infants with thiamine-responsive pulmonary hypertension and acute respiratory infection.

Author

Shenoy S, Deekshit VK, Rao SS, Ashwini PS, and Shenoy RD

Subjects

Humans, Female, Infant, Male, India epidemiology, Prospective Studies, Breast Feeding, Acute Disease, Infant, Newborn, Membrane Transport Proteins genetics, Hypertension, Pulmonary genetics, Thiamine therapeutic use, Respiratory Tract Infections genetics, Thiamine Deficiency genetics

Abstract

Maternal thiamine deficiency is prevalent in low- and middle-income countries. Thiamine-responsive pulmonary hypertension (TRPHTN) in exclusively breastfed infants is reported in India. Thiamine transporter gene (ThTR) variations have not been studied. This study compared the presentation of exclusively breastfed infants with respiratory distress diagnosed as TRPHTN or acute respiratory infection (ARI). We investigated pathogenic variations in the SLC19A2 and SLC19A3 ThTr genes in a representative sample. Observational study. Tertiary care pediatric unit of a teaching hospital in southern India. Data collection was prospective. We included exclusively breastfed infants between 1 and 6 months of age with respiratory distress. Infants with PHTN in echocardiography and lactic acidosis (LA) received thiamine. TRPHTN was diagnosed based on response within 72 h. Infants with fever, chest findings, and positive microbiology were managed as ARI. The ThTr genes were sequenced and analyzed. Chi-square and stratified analysis were done to determine TRPHTN risk. Forty infants with TRPHTN and 42 with ARI were included. The median pulmonary arterial pressure in the TRPHTN group was 51.5 mmHg. Mild PHTN was seen in 65%, moderate in 22.5%, and severe in 12.5%. Cardiac failure (P < .001), stridor and aphonia (P < .001), encephalopathy (P = .024), LA (P < .001), and PHTN (P <.001) facilitated the diagnosis. The adjusted risk was 17.3 (95% confidence interval 7.8-38.3; P <.001). The ThTR sequencing showed wild-type genotypes. TRPHTN has a distinct, identifiable presentation. Lactate and pulmonary pressure estimations are useful investigations in thiamine deficiency endemic areas. We could not demonstrate a genetic variation that determines susceptibility., (© The Author(s) [2024]. Published by Oxford University Press. All rights reserved. For permissions, please email: journals.permissions@oup.com.)

Published

2024

3. SLC19A1 Genetic Variation Leads to Altered Thiamine Diphosphate Transport: Implications for the Risk of Developing Wernicke-Korsakoff's Syndrome.

Author

O'Brien NL, Quadri G, Lightley I, Sharp SI, Guerrini I, Smith I, Heydtmann M, Morgan MY, Thomson AD, Bass NJ, McHugh PC, and McQuillin A

Subjects

Ethanol, Folic Acid, Genetic Variation genetics, HEK293 Cells, Humans, Thiamine, Thiamine Pyrophosphate metabolism, Alcoholism complications, Korsakoff Syndrome complications, Reduced Folate Carrier Protein genetics, Thiamine Deficiency genetics

Abstract

Aims: Wernicke-Korsakoff syndrome (WKS) is commonly associated with chronic alcohol misuse, a condition known to have multiple detrimental effects on thiamine metabolism. This study was conducted to identify genetic variants that may contribute to the development of WKS in individuals with alcohol dependence syndrome through alteration of thiamine transport into cells., Methods: Exome sequencing data from a panel of genes related to alcohol metabolism and thiamine pathways were analysed in a discovery cohort of 29 individuals with WKS to identify possible genetic risk variants associated with its development. Variant frequencies in this discovery cohort were compared with European frequencies in the Genome Aggregation Database browser, and those present at significantly higher frequencies were genotyped in an additional cohort of 87 alcohol-dependent cases with WKS and 197 alcohol-dependent cognitively intact controls., Results: Thirty non-synonymous variants were identified in the discovery cohort and, after filtering, 23 were taken forward and genotyped in the case-control cohort. Of these SLC19A1:rs1051266:G was nominally associated with WKS. SLC19A1 encodes the reduced folate carrier, a major transporter for physiological folate in plasma; rs1051266 is reported to impact folate transport. Thiamine pyrophosphate (TPP) efflux was significantly decreased in HEK293 cells, stably transfected with rs1051266:G, under thiamine deficient conditions when compared with the efflux from cells transfected with rs1051266:A (P = 5.7 × 10-11)., Conclusion: This study provides evidence for the role of genetic variation in the SLC19A1 gene, which may contribute to the development of WKS in vivo through modulation of TPP transport in cells., (© The Author(s) 2022. Medical Council on Alcohol and Oxford University Press. All rights reserved.)

Published

2022

4. Diabetes Out-of-the-Box: Diabetes Mellitus and Impairment in Hearing and Vision.

Author

Gruber N and Pinhas-Hamiel O

Subjects

Deafness, Hearing, Humans, Mitochondrial Diseases, Thiamine, Anemia, Megaloblastic complications, Anemia, Megaloblastic diagnosis, Anemia, Megaloblastic genetics, Diabetes Mellitus diagnosis, Diabetes Mellitus genetics, Diabetes Mellitus, Type 2 complications, Diabetes Mellitus, Type 2 diagnosis, Diabetes Mellitus, Type 2 genetics, Hearing Loss, Sensorineural complications, Hearing Loss, Sensorineural diagnosis, Hearing Loss, Sensorineural genetics, Thiamine Deficiency complications, Thiamine Deficiency genetics

Abstract

Purposeof Review: This review aims to provide an update on the etiologies of diabetes that are due to genetic disorders and that co-occur with impaired hearing or vision and to compare them. The potential mechanisms, including novel treatments, will be detailed., Recent Findings: Wolfram syndrome, Kearns-Sayre syndrome, thiamine-responsive megaloblastic anemia, and maternally inherited diabetes and deafness are genetic disorders characterized by diabetes, impaired hearing, and vision. They differ in mode of inheritance, age at presentation, and the involvement of other organs; they are often misdiagnosed as type 1 or type 2 diabetes. Suspicion of a genetic diabetes syndrome should be raised when pancreatic autoantibodies are negative, other organs are involved, and family history includes diabetes. Correct diagnosis of the various syndromes is important for tailoring the most advanced treatment, preventing disease progression, and enabling proper genetic counseling., (© 2022. The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2022

5. Identification and functional analysis of novel SLC25A19 variants causing thiamine metabolism dysfunction syndrome 4.

Author

Chen Y, Fang B, Hu X, Guo R, Guo J, Fang K, Ni J, Li W, Qian S, and Hao C

Subjects

Humans, Membrane Transport Proteins genetics, Mutation genetics, Phenotype, Thiamine, Brain Diseases, Mitochondrial Membrane Transport Proteins genetics, Thiamine Deficiency genetics

Abstract

Background: Thiamine metabolism dysfunction syndrome 4 (THMD4, OMIM #613710) is an autosomal recessive inherited disease caused by the deficiency of SLC25A19 that encodes the mitochondrial thiamine pyrophosphate (TPP) transporter. This disorder is characterized by bilateral striatal degradation and progressive polyneuropathy with the onset of fever of unknown origin. The limited number of reported cases and lack of functional annotation of related gene variants continue to limit diagnosis., Results: We report three cases of encephalopathy from two unrelated pedigrees with basal ganglia signal changes after fever of unknown origin. To distinguish this from other types of encephalopathy, such as acute necrotizing encephalopathy, exome sequencing was performed, and four novel heterozygous variations, namely, c.169G>A (p.Ala57Thr), c.383C>T (p.Ala128Val), c.76G>A (p.Gly26Arg), and c.745T>A (p.Phe249Ile), were identified in SLC25A19. All variants were confirmed using Sanger sequencing. To determine the pathogenicity of these variants, functional studies were performed. We found that mitochondrial TPP levels were significantly decreased in the presence of SLC25A19 variants, indicating that TPP transport activities of mutated SLC25A19 proteins were impaired. Thus, combining clinical phenotype, genetic analysis, and functional studies, these variants were deemed as likely pathogenic., Conclusions: Exome sequencing analysis enables molecular diagnosis as well as provides potential etiology. Further studies will enable the elucidation of SLC25A19 protein function. Our investigation supplied key molecular evidence for the precise diagnosis of and clinical decision-making for a rare disease., (© 2021. The Author(s).)

Published

2021

6. The Effects of Genetic Mutations and Drugs on the Activity of the Thiamine Transporter, SLC19A2.

Author

Enogieru OJ, Koleske ML, Vora B, Ngo H, Yee SW, Chatad D, Sirota M, and Giacomini KM

Subjects

Adult, Anemia, Megaloblastic blood, Anemia, Megaloblastic chemically induced, Cell Membrane metabolism, Diabetes Mellitus blood, Diabetes Mellitus chemically induced, Drug Interactions, Erythromycin pharmacokinetics, Female, Genetic Variation, HEK293 Cells, Hearing Loss, Sensorineural blood, Hearing Loss, Sensorineural chemically induced, Humans, Loss of Function Mutation, Male, Membrane Transport Proteins metabolism, Thiamine Deficiency blood, Thiamine Deficiency chemically induced, Thiamine Deficiency genetics, Thiamine Pyrophosphate blood, Thiamine Pyrophosphate metabolism, Anemia, Megaloblastic genetics, Diabetes Mellitus genetics, Erythromycin adverse effects, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics, Thiamine Deficiency congenital, Thiamine Pyrophosphate antagonists & inhibitors

Abstract

A rare cause of megaloblastic anemia (MA) is thiamine-responsive megaloblastic anemia (TRMA), a genetic disorder caused by mutations in SLC19A2 (encoding THTR1), a thiamine transporter. The study objectives were to (1) functionally characterize selected TRMA-associated SLC19A2 variants and (2) determine whether current prescription drugs associated with drug-induced MA (DIMA) may act via inhibition of SLC19A2. Functional characterization of selected SLC19A2 variants was performed by confocal microscopy and isotopic uptake studies of [3H]-thiamine in HEK293 cells. Sixty-three drugs associated with DIMA were screened for SLC19A2 inhibition in isotopic uptake studies. Three previously uncharacterized SLC19A2 variants identified in TRMA patients exhibited disrupted localization to the plasma membrane along with near-complete loss-of-function. Ten of 63 drugs inhibited SLC19A2-mediated thiamine transport ≥ 50% at screening concentrations; however, with the exception of erythromycin, none was predicted to inhibit SLC19A2 at clinically relevant unbound plasma concentrations. Data from electronic health records revealed reduced levels of thiamine pyrophosphate (TPP) in patients prescribed erythromycin, consistent with inhibition of SLC19A2-mediated thiamine transport. Here, we confirmed the role of three SLC19A2 variants in TRMA pathology. Additionally, we report that inhibition of SLC19A2 is a potential, but uncommon mechanism for DIMA.

Published

2021

7. Novel p.P298L SURF1 mutation in thiamine deficient Leigh syndrome patients compromises cytochrome c oxidase activity.

Author

Mani S, Chandak GR, Singh KK, Singh R, and Rao SN

Subjects

Animals, COS Cells, Child, Chlorocebus aethiops, Electron Transport Complex IV metabolism, Genetic Predisposition to Disease, Humans, India, Leigh Disease complications, Leigh Disease metabolism, Membrane Proteins metabolism, Mitochondrial Proteins metabolism, Thiamine Deficiency metabolism, Leigh Disease genetics, Membrane Proteins genetics, Mitochondrial Proteins genetics, Polymorphism, Single Nucleotide, Thiamine Deficiency genetics

Abstract

SURF1 is a nuclear gene and encodes for an important assembly factor for cytochrome c oxidase enzyme. A number of mutations in SURF1 gene render cytochrome c oxidase deficiency, a major causative factor for Leigh syndrome. We screened all the 9 exons and exon-intron boundaries of SURF1 gene in 165 Indian Leigh syndrome patients who were thiamine responsive too. Consequently, we identified several novel and reported nucleotide variations in this gene. The nucleotide changes were analysed by using different in-silico tools for predicting their pathogenicity. Based upon the predictions, we further validated the analyzed functional significance of p.N249D and p.P298L mutations in SURF1 protein using COS-7 cells. Though, both the mutations did not affect the localization of SURF1protein into the mitochondria. But, interestingly the novel mutation p.P298L was reported to significantly compromise the COX activity in these cells., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier B.V. and Mitochondria Research Society. All rights reserved.)

Published

2020

8. Functional analysis of the third identified SLC25A19 mutation causative for the thiamine metabolism dysfunction syndrome 4.

Author

Bottega R, Perrone MD, Vecchiato K, Taddio A, Sabui S, Pecile V, Said HM, and Faletra F

Subjects

Adolescent, Brain Diseases genetics, Brain Diseases physiopathology, Humans, Male, Microcephaly physiopathology, Mitochondrial Membrane Transport Proteins chemistry, Mutation, Protein Conformation, RNA, Messenger genetics, Thiamine genetics, Thiamine metabolism, Thiamine Deficiency physiopathology, Genetic Predisposition to Disease, Microcephaly genetics, Mitochondrial Membrane Transport Proteins genetics, Thiamine Deficiency genetics

Abstract

Thiamine metabolism dysfunction syndrome-4 (THMD4) includes episodic encephalopathy, often associated with a febrile illness, causing transient neurologic dysfunction and a slowly progressive axonal polyneuropathy. Until now only two mutations (G125S and S194P) have been reported in the SLC25A19 gene as causative for this disease and a third mutation (G177A) as related to the Amish lethal microcephaly. In this work, we describe the clinical and molecular features of a patient carrying a novel mutation (c.576G>C; Q192H) on SLC25A19 gene. Functional studies on this mutation were performed explaining the pathogenetic role of c.576G>C in affecting the translational efficiency and/or stability of hMTPPT protein instead of the mRNA expression. These findings support the pathogenetic role of Q192H (c.576G>C) mutation on SLC25A19 gene. Moreover, despite in other patients the thiamine supplementation leaded to a substantial improvement of peripheral neuropathy, our patient did not show a clinical improvement.

Published

2019

9. Genetic heterogeneity of mitochondrial genome in thiamine deficient Leigh syndrome patients.

Author

Mani S, Rao SN, and Kranthi Kumar MV

Subjects

Biopsy, Child, DNA, Mitochondrial genetics, Humans, Leigh Disease complications, Leigh Disease pathology, Mitochondria, Muscle metabolism, Mitochondria, Muscle pathology, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Thiamine Deficiency complications, Thiamine Deficiency pathology, Genetic Heterogeneity, Genome, Mitochondrial, Leigh Disease genetics, Thiamine Deficiency genetics

Abstract

In our previously published study, we cared for 165 thiamine deficient Leigh syndrome (LS) patients who presented in acute life threatening conditions with severe neurological abnormalities. However the molecular basis for this atypical phenotype was not explored. This study is an effort to undermine the possible molecular defects in mitochondria of those patients and put-forth an explanation towards this clinical presentation. Protein coding genes of mitochondrial (mt) DNA were sequenced in total 165 LS patients and 94 age matched controls. To understand their pathogenic significance, nucleotide variations were also studied using various in-silico tools. Histochemical and electron microscopic analysis was also done in tissue samples obtained from 23 patients. We observed a very high level of genetic heterogeneity across the mt DNA of all these patients. In the concordance of published literature we also observed a large number of variations in ND5 gene (hot spot for LS). We also observed a total 13 nucleotide variations across COX genes, which is otherwise not common in LS. As per in-silico analysis, many of these variations were suggested to be pathogenic. Histochemical and electron microscopic studies also suggested the defects in the mitochondria of these patients. As these patients were thiamine deficient, hence we propose that genetic defects and thiamine deficiency may together severely affect the ATP levelof these patients, leading to acute and life threatening clinical presentation. Present study has opened up many avenues for further research towards understanding the genetic basis and possible role of thiamine deficiency in LS patients., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

10. TRMA syndrome with a severe phenotype, cerebral infarction, and novel compound heterozygous SLC19A2 mutation: a case report.

Author

Li X, Cheng Q, Ding Y, Li Q, Yao R, Wang J, and Wang X

Subjects

Adult, Anemia, Megaloblastic drug therapy, Anemia, Megaloblastic pathology, Arrhythmias, Cardiac etiology, Atrophy, Brain pathology, Child, DNA Mutational Analysis, Diabetes Mellitus drug therapy, Diabetes Mellitus pathology, Diabetes Mellitus, Type 1 etiology, Dwarfism etiology, Female, Hearing Loss, Bilateral etiology, Hearing Loss, Sensorineural drug therapy, Hearing Loss, Sensorineural pathology, Heterozygote, High-Throughput Nucleotide Sequencing, Humans, Male, Phenotype, Thiamine therapeutic use, Thiamine Deficiency drug therapy, Thiamine Deficiency genetics, Thiamine Deficiency pathology, Ventricular Premature Complexes etiology, Anemia, Megaloblastic genetics, Cerebral Infarction etiology, Diabetes Mellitus genetics, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics, Thiamine Deficiency congenital

Abstract

Background: Thiamine-responsive megaloblastic anemia (TRMA) is a rare autosomal recessive inherited disease characterized by the clinical triad of megaloblastic anemia, sensorineural deafness, and diabetes mellitus. To date, only 100 cases of TRMA have been reported in the world., Case Presentation: Here, we describe a six-year-old boy with diabetes mellitus, anemia, and deafness. Additionally, he presented with thrombocytopenia, leukopenia, horizontal nystagmus, hepatomegaly, short stature, ventricular premature beat (VPB), and cerebral infarction. DNA sequencing revealed a novel compound heterozygous mutation in the SLC19A2 gene: (1) a duplication c.405dupA, p.Ala136Serfs*3 (heterozygous) and (2) a nucleotide deletion c.903delG p.Trp301Cysfs*13 (heterozygous). The patient was diagnosed with a typical TRMA., Conclusion: Novel mutations in the SLC19A2 gene have been identified, expanding the mutation spectrum of the SLC19A2 gene. For the first time, VPB and cerebral infarction have been identified in patients with TRMA syndrome, providing a new understanding of the phenotype.

Published

2019

11. Whole exome sequencing identifies a new mutation in the SLC19A2 gene leading to thiamine-responsive megaloblastic anemia in an Egyptian family.

Author

Amr K, Pawlikowska P, Aoufouchi S, Rosselli F, and El-Kamah G

Subjects

Anemia, Megaloblastic metabolism, Child, Consanguinity, Egypt, Family, Humans, Male, Membrane Transport Proteins metabolism, Mutation, Pedigree, Thiamine Deficiency genetics, Exome Sequencing methods, Anemia, Megaloblastic genetics, Diabetes Mellitus genetics, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics, Thiamine Deficiency congenital

Abstract

Background: The Solute Carrier Family 19 Member 2 (SLC19A2, OMIM *603941) encodes the thiamine transporter 1 (THTR-1) that brings thiamine (Vitamin B1) into cells. THTR-1 is the only thiamine transporter expressed in bone marrow, cochlear, and pancreatic beta cells. THTR-1 loss-of-function leads to the rare recessive genetic disease Thiamine-Responsive Megaloblastic Anemia (TRMA, OMIM #249270)., Methods: In vitro stimulated blood lymphocytes were used for cytogenetics and the isolation of genomic DNA used to perform whole exome sequencing (WES). To validate identified mutations, direct Sanger sequencing was performed following PCR amplification., Results: A 6-year-old male born from a consanguineous couple presenting bone marrow failure and microcephaly was referred to our clinic for disease diagnosis. The patient presented a normal karyotype and no chromosomal fragility in response to DNA damage. WES analysis led to the identification of a new pathogenic variant in the SLC19A2 gene (c.596C>G, pSer199Ter) allowing to identify the young boy as a TRMA patient., Conclusion: Our analysis extend the number of inactivating mutations in SLC19A2 leading to TRMA that could guide future prenatal diagnosis for the family and follow-up for patients., (© 2019 CNRS. Molecular Genetics & Genomic Medicine published by Wiley Periodicals, Inc.)

Published

2019

12. Genetic defects of thiamine transport and metabolism: A review of clinical phenotypes, genetics, and functional studies.

Author

Marcé-Grau A, Martí-Sánchez L, Baide-Mairena H, Ortigoza-Escobar JD, and Pérez-Dueñas B

Subjects

Anemia, Megaloblastic, Biological Transport, Biomarkers blood, Biomarkers cerebrospinal fluid, Diabetes Mellitus, Hearing Loss, Sensorineural, Humans, Leigh Disease, Membrane Transport Proteins genetics, Membrane Transport Proteins metabolism, Mutation, Phenotype, Thiamine cerebrospinal fluid, Thiamine therapeutic use, Thiamine Deficiency congenital, Thiamine Deficiency drug therapy, Thiamine Pyrophosphate metabolism, Membrane Transport Proteins deficiency, Thiamine metabolism, Thiamine Deficiency genetics

Abstract

Thiamine is a crucial cofactor involved in the maintenance of carbohydrate metabolism and participates in multiple cellular metabolic processes within the cytosol, mitochondria, and peroxisomes. Currently, four genetic defects have been described causing impairment of thiamine transport and metabolism: SLC19A2 dysfunction leads to diabetes mellitus, megaloblastic anemia and sensory-neural hearing loss, whereas SLC19A3, SLC25A19, and TPK1-related disorders result in recurrent encephalopathy, basal ganglia necrosis, generalized dystonia, severe disability, and early death. In order to achieve early diagnosis and treatment, biomarkers play an important role. SLC19A3 patients present a profound decrease of free-thiamine in cerebrospinal fluid (CSF) and fibroblasts. TPK1 patients show decreased concentrations of thiamine pyrophosphate in blood and muscle. Thiamine supplementation has been shown to improve diabetes and anemia control in Rogers' syndrome patients due to SLC19A2 deficiency. In a significant number of patients with SLC19A3, thiamine improves clinical outcome and survival, and prevents further metabolic crisis. In SLC25A19 and TPK1 defects, thiamine has also led to clinical stabilization in single cases. Moreover, thiamine supplementation leads to normal concentrations of free-thiamine in the CSF of SLC19A3 patients. Herein, we present a literature review of the current knowledge of the disease including related clinical phenotypes, treatment approaches, update of pathogenic variants, as well as in vitro and in vivo functional models that provide pathogenic evidence and propose mechanisms for thiamine deficiency in humans., (© 2019 SSIEM.)

Published

2019

13. 50 Years Ago in The Journal of Pediatrics: Thiamine-Responsive Megaloblastic Anemia.

Author

Mullikin D and Grimes AB

Subjects

Anemia, Megaloblastic history, Child, Diabetes Mellitus history, Female, Hearing Loss, Sensorineural history, History, 20th Century, Humans, Membrane Transport Proteins, Mutation, Thiamine Deficiency genetics, Thiamine Deficiency history, Anemia, Megaloblastic genetics, Diabetes Mellitus genetics, Hearing Loss, Sensorineural genetics, Thiamine Deficiency congenital

Published

2019

14. Identification of two novel TPK1 gene mutations in a Chinese patient with thiamine pyrophosphokinase deficiency undergoing whole exome sequencing.

Author

Zhu L, Wu R, Ye Z, Gu R, Wang Y, Hou Y, Feng Z, and Ma X

Subjects

Brain diagnostic imaging, Humans, Infant, Newborn, Male, Thiamine Deficiency diagnostic imaging, Exome Sequencing, Mutation, Thiamin Pyrophosphokinase genetics, Thiamine Deficiency genetics

Abstract

Background The mutations of thiamine pyrophosphokinase-1 (TPK1) gene have been frequently studied in some patients with thiamine metabolism dysfunction syndrome-5 (THMD5), while TPK1 mutations in Chinese patients have been investigated by only homozygous. A search of the literature on the mutations in the Chinese population currently published revealed that no reports of compound heterozygous mutations were reported. Here, we report a Chinese patient with compound heterozygous TPK1 mutations who underwent magnetic resonance imaging (MRI), whole exome sequencing (WES), molecular diagnosis, bioinformatics analysis, and three-dimensional (3D) protein structure analysis. Case presentation A Chinese boy was born after an uneventful pregnancy to non-consanguineous and healthy parents. On the sixth day after his birth, the lactate level of the patient was between 8.6 mmol/L and 14.59 mmol/L in plasma (the normal level is in the range of 0.5-2.2 mmol/L). Lactate was reduced to the normal level after rehydration, acid correction, expansion, and other treatments. After 4 months, the patient presented with an acute, 3-h-long, non-induced convulsions, and was admitted to our hospital for weakness, decreased oral intake, and lethargy. Results achieved by electroencephalography (EEG), cerebrospinal fluid, and other biochemical findings were normal. A visible hemorrhagic lesion was also observed in the brain. Seizures increased significantly during infection, which was accompanied by higher lactic acid levels. MRI of the brain showed an obvious signal shadow, in which bilateral frontal and temporal parietal subarachnoid cavities were widened, and more abnormal signals were observed; therefore, further consideration of hypoxic-ischemic encephalopathy and genetic metabolic disease was taken into account. Conclusions The results of WES revealed that the patient was associated with compound heterozygous mutations NM&#95;022445.3:c.[263G>A]; [226A>G] of TPK1. His parents were non-consanguineous; while his father was found to be a heterozygous carrier with the mutation c.[263G>A], his mother was identified as a heterozygous carrier with the mutation c.[226A>G]. The results indicated that the patient had a compound heterozygous TPK1 mutation, and this is the first reported case in China.

Published

2019

15. Telomere shortening in alcohol dependence: Roles of alcohol and acetaldehyde.

Author

Yamaki N, Matsushita S, Hara S, Yokoyama A, Hishimoto A, and Higuchi S

Subjects

Aged, Aldehyde Dehydrogenase, Mitochondrial genetics, Humans, Japan, Male, Middle Aged, Acetaldehyde adverse effects, Aging, Premature chemically induced, Aging, Premature etiology, Aging, Premature genetics, Alcoholism complications, Alcoholism genetics, Ethanol adverse effects, Telomere Shortening drug effects, Telomere Shortening genetics, Thiamine Deficiency chemically induced, Thiamine Deficiency genetics

Abstract

Heavy drinking leads to premature aging and precipitates the onset of age-related diseases. Acetaldehyde (AcH), a toxic metabolite of ethanol, has been implicated in various types of cancer. However, whether alcohol accelerates biological aging at a cellular level is controversial and the mechanism involved is unclear. We addressed these questions by measuring telomere length (TL) in peripheral blood leukocytes of Japanese patients with alcohol dependence (AD) and examined the association between TL, genetic variants of alcohol dehydrogenase (ADH)1B and aldehyde dehydrogenase (ALDH)2, and other clinical characteristics. A total of 134 male AD patients and 121 age- and sex-matched healthy controls were evaluated. All patients received endoscopic screening for cancer of the upper aerodigestive tract (UADT). TL was almost 50% shorter in AD patients relative to controls. There were no significant differences in TL between AD patients with and without UADT cancer, and no associations between ADH1B and ALDH2 genotypes and TL. AD patients with thiamine (vitamin B1) deficiency at admission had significantly shorter TL than those with normal thiamine status. Although the exact mechanism underlying the shorter TL in AD patients remain unclear, our findings suggest that alcohol rather than AcH is associated with telomere shortening in AD, which may be accelerated by thiamine deficiency. Future studies should also focus on the association between telomere shortening and TD in the context of oxidative stress., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2019

16. A novel mutation in the SLC19A2 gene in a Turkish male with thiamine-responsive megaloblastic anemia syndrome.

Author

Odaman-Al I, Gezdirici A, Yıldız M, Ersoy G, Aydoğan G, Şalcıoğlu Z, Tahtakesen TN, Önal H, and Küçükemre-Aydın B

Subjects

Anemia, Megaloblastic metabolism, Child, Preschool, DNA Mutational Analysis, Diabetes Mellitus metabolism, Hearing Loss, Sensorineural metabolism, Humans, Male, Membrane Transport Proteins metabolism, Thiamine Deficiency genetics, Thiamine Deficiency metabolism, Turkey, Anemia, Megaloblastic genetics, DNA genetics, Diabetes Mellitus genetics, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics, Mutation, Thiamine Deficiency congenital

Abstract

Odaman-Al I, Gezdirici A, Yıldız M, Ersoy G, Aydoğan G, Şalcıoğlu Z, Tahtakesen TN, Önal H, Küçükemre-Aydın B. A novel mutation in the SLC19A2 gene in a Turkish male with thiamine-responsive megaloblastic anemia syndrome. Turk J Pediatr 2019; 61: 257-260. Thiamine-responsive megaloblastic anemia (TRMA) is a very rare syndrome characterized by the triad of early onset megaloblastic anemia, sensorineural deafness and diabetes mellitus. Here we report, a 5-year-old boy who presented with transfusion dependent anemia and diabetes mellitus and was diagnosed with TRMA. Besides reporting a novel mutation of the causative gene SLC19A2, we wanted to emphasize this syndrome in the aspect of coexistence of insulin dependent diabetes, transfusion dependent anemia and thrombocytopenia.

Published

2019

17. A novel mutation in the SLC19A2 gene in a Turkish male with thiamine-responsive megaloblastic anemia syndrome.

Author

Odaman-Al I, Gezdirici A, Yıldız M, Ersoy G, Aydoğan G, Şalcıoğlu Z, Tahtakesen TN, Önal H, and Küçükemre-Aydın B

Subjects

Anemia, Megaloblastic epidemiology, Anemia, Megaloblastic metabolism, Child, Preschool, DNA Mutational Analysis, Diabetes Mellitus epidemiology, Diabetes Mellitus metabolism, Female, Hearing Loss, Sensorineural epidemiology, Hearing Loss, Sensorineural metabolism, Humans, Male, Membrane Transport Proteins metabolism, Thiamine Deficiency epidemiology, Thiamine Deficiency genetics, Thiamine Deficiency metabolism, Turkey epidemiology, Anemia, Megaloblastic genetics, DNA genetics, Diabetes Mellitus genetics, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics, Mutation, Thiamine Deficiency congenital

Abstract

Odaman-Al I, Gezdirici A, Yıldız M, Ersoy G, Aydoğan G, Şalcıoğlu Z, Tahtakesen TN, Önal H, Küçükemre-Aydın B. A novel mutation in the SLC19A2 gene in a Turkish male with thiamine-responsive megaloblastic anemia syndrome. Turk J Pediatr 2019; 61: 257-260. Thiamine-responsive megaloblastic anemia (TRMA) is a very rare syndrome characterized by the triad of early onset megaloblastic anemia, sensorineural deafness and diabetes mellitus. Here we report, a 5-year-old boy who presented with transfusion dependent anemia and diabetes mellitus and was diagnosed with TRMA. Besides reporting a novel mutation of the causative gene SLC19A2, we wanted to emphasize this syndrome in the aspect of coexistence of insulin dependent diabetes, transfusion dependent anemia and thrombocytopenia.

Published

2019

18. Pancytopenia in an adult patient with thiamine-responsive megaloblastic anaemia.

Author

Moulin V, Grandoni F, Castioni J, and Lu H

Subjects

Administration, Oral, Adult, Anemia, Megaloblastic diagnosis, Anemia, Megaloblastic drug therapy, Anemia, Megaloblastic genetics, Diabetes Mellitus drug therapy, Diabetes Mellitus genetics, Female, Hearing Loss, Sensorineural complications, Hearing Loss, Sensorineural drug therapy, Hearing Loss, Sensorineural genetics, Humans, Infusions, Parenteral, Mutation, Pancytopenia drug therapy, Rare Diseases, Thiamine administration & dosage, Thiamine metabolism, Thiamine therapeutic use, Thiamine Deficiency complications, Thiamine Deficiency diagnosis, Thiamine Deficiency drug therapy, Thiamine Deficiency genetics, Treatment Outcome, Vitamin B Complex therapeutic use, Anemia, Megaloblastic complications, Diabetes Mellitus diagnosis, Hearing Loss, Sensorineural diagnosis, Pancytopenia etiology, Thiamine Deficiency congenital

Abstract

Thiamine-responsive megaloblastic anaemia (TRMA) is a syndrome associated with megaloblastic anaemia, diabetes mellitus and sensorineural deafness, due to mutations in the SLC19A2 gene, which codes for a thiamine carrier protein. Oral thiamine supplementation is the main treatment. We report the case of a 25-year-old woman known for TRMA, who presented with pancytopenia (haemoglobin 7.6 g/dL, leucocytes 2.9×10 9 /L, thrombocytes 6×10 9 /L) revealed by dyspnoea. Investigations excluded coagulopathy, a recent viral infection, vitamin and iron deficiencies, and a malignant process. We later found out that thiamine treatment had been discontinued 5 weeks before, due to prescription error. Parenteral thiamine administration resulted in the recovery of haematopoiesis within 3 weeks. Pancytopenia is uncommon in patients with TRMA. Pre-existing medullary impairment caused by the patient's daily antipsychotic medications or the natural course of the syndrome may explain the severity of the laboratory findings in our patient., Competing Interests: Competing interests: None declared., (© BMJ Publishing Group Ltd (unless otherwise stated in the text of the article) 2018. All rights reserved. No commercial use is permitted unless otherwise expressly granted.)

Published

2018

19. Pharmacogenomics in diabetes: outcomes of thiamine therapy in TRMA syndrome.

Author

Habeb AM, Flanagan SE, Zulali MA, Abdullah MA, Pomahačová R, Boyadzhiev V, Colindres LE, Godoy GV, Vasanthi T, Al Saif R, Setoodeh A, Haghighi A, Haghighi A, Shaalan Y, Hattersley AT, Ellard S, and De Franco E

Subjects

Alleles, Child, Preschool, Cohort Studies, Female, Genetic Testing, Genotype, Humans, Infant, Male, Membrane Transport Proteins genetics, Mutation, Phenotype, Surveys and Questionnaires, Thiamine Deficiency drug therapy, Thiamine Deficiency genetics, Anemia, Megaloblastic drug therapy, Anemia, Megaloblastic genetics, Diabetes Mellitus drug therapy, Diabetes Mellitus genetics, Hearing Loss, Sensorineural drug therapy, Hearing Loss, Sensorineural genetics, Pharmacogenetics, Thiamine therapeutic use, Thiamine Deficiency congenital

Abstract

Aims/hypothesis: Diabetes is one of the cardinal features of thiamine-responsive megaloblastic anaemia (TRMA) syndrome. Current knowledge of this rare monogenic diabetes subtype is limited. We investigated the genotype, phenotype and response to thiamine (vitamin B 1 ) in a cohort of individuals with TRMA-related diabetes., Methods: We studied 32 individuals with biallelic SLC19A2 mutations identified by Sanger or next generation sequencing. Clinical details were collected through a follow-up questionnaire., Results: We identified 24 different mutations, of which nine are novel. The onset of the first TRMA symptom ranged from birth to 4 years (median 6 months [interquartile range, IQR 3-24]) and median age at diabetes onset was 10 months (IQR 5-27). At presentation, three individuals had isolated diabetes and 12 had asymptomatic hyperglycaemia. Follow-up data was available for 15 individuals treated with thiamine for a median 4.7 years (IQR 3-10). Four patients were able to stop insulin and seven achieved better glycaemic control on lower insulin doses. These 11 patients were significantly younger at diabetes diagnosis (p = 0.042), at genetic testing (p = 0.01) and when starting thiamine (p = 0.007) compared with the rest of the cohort. All patients treated with thiamine became transfusion-independent and adolescents achieved normal puberty. There were no additional benefits of thiamine doses >150 mg/day and no reported side effects up to 300 mg/day., Conclusions/interpretation: In TRMA syndrome, diabetes can be asymptomatic and present before the appearance of other features. Prompt recognition is essential as early treatment with thiamine can result in improved glycaemic control, with some individuals becoming insulin-independent., Data Availability: SLC19A2 mutation details have been deposited in the Decipher database ( https://decipher.sanger.ac.uk/ ).

Published

2018

20. Organic cation transporter 1 (OCT1) modulates multiple cardiometabolic traits through effects on hepatic thiamine content.

Author

Liang X, Yee SW, Chien HC, Chen EC, Luo Q, Zou L, Piao M, Mifune A, Chen L, Calvert ME, King S, Norheim F, Abad J, Krauss RM, and Giacomini KM

Subjects

Animals, Blood Glucose metabolism, Cholesterol, HDL blood, Cholesterol, LDL blood, Diabetes Mellitus, Experimental metabolism, Diabetes Mellitus, Experimental pathology, Diabetes Mellitus, Type 2 metabolism, Diabetes Mellitus, Type 2 pathology, Fatty Acids metabolism, Gene Expression Regulation, Gluconeogenesis genetics, Humans, Ketone Oxidoreductases genetics, Ketone Oxidoreductases metabolism, Lipid Metabolism genetics, Liver metabolism, Liver pathology, Mice, Mice, Knockout, Obesity metabolism, Obesity pathology, Octamer Transcription Factor-1 deficiency, Signal Transduction, Thiamine Deficiency metabolism, Thiamine Deficiency pathology, Triglycerides blood, Diabetes Mellitus, Experimental genetics, Diabetes Mellitus, Type 2 genetics, Longevity genetics, Obesity genetics, Octamer Transcription Factor-1 genetics, Thiamine metabolism, Thiamine Deficiency genetics

Abstract

A constellation of metabolic disorders, including obesity, dysregulated lipids, and elevations in blood glucose levels, has been associated with cardiovascular disease and diabetes. Analysis of data from recently published genome-wide association studies (GWAS) demonstrated that reduced-function polymorphisms in the organic cation transporter, OCT1 (SLC22A1), are significantly associated with higher total cholesterol, low-density lipoprotein (LDL) cholesterol, and triglyceride (TG) levels and an increased risk for type 2 diabetes mellitus, yet the mechanism linking OCT1 to these metabolic traits remains puzzling. Here, we show that OCT1, widely characterized as a drug transporter, plays a key role in modulating hepatic glucose and lipid metabolism, potentially by mediating thiamine (vitamin B1) uptake and hence its levels in the liver. Deletion of Oct1 in mice resulted in reduced activity of thiamine-dependent enzymes, including pyruvate dehydrogenase (PDH), which disrupted the hepatic glucose-fatty acid cycle and shifted the source of energy production from glucose to fatty acids, leading to a reduction in glucose utilization, increased gluconeogenesis, and altered lipid metabolism. In turn, these effects resulted in increased total body adiposity and systemic levels of glucose and lipids. Importantly, wild-type mice on thiamine deficient diets (TDs) exhibited impaired glucose metabolism that phenocopied Oct1 deficient mice. Collectively, our study reveals a critical role of hepatic thiamine deficiency through OCT1 deficiency in promoting the metabolic inflexibility that leads to the pathogenesis of cardiometabolic disease.

Published

2018

21. [Defect of thiamine transport and activation and related disease].

Author

Xian X and Lin F

Subjects

Anemia, Megaloblastic genetics, Anemia, Megaloblastic metabolism, Biological Transport genetics, Diabetes Mellitus genetics, Diabetes Mellitus metabolism, Hearing Loss, Sensorineural genetics, Hearing Loss, Sensorineural metabolism, Humans, Membrane Transport Proteins metabolism, Thiamine Deficiency congenital, Thiamine Deficiency genetics, Thiamine Deficiency metabolism, Membrane Transport Proteins genetics, Mutation, Thiamine metabolism, Thiamine Pyrophosphate metabolism

Abstract

Thiamine, also known as vitamin B1, is an important vitamin for the body. The activated form of thiamine pyrophosphate is involved in cell metabolism as an important co-enzyme. Defects of thiamine transport and activation may cause lack of thiamine and affection of cell metabolism, leading a variety of diseases. This review has summarized defects of thiamine transport and activation and related diseases.

Published

2018

22. Thiamin.

Author

Lonsdale D

Subjects

Diet, Genetic Predisposition to Disease, Humans, Stress, Physiological, Thiamine Deficiency epidemiology, Thiamine Deficiency etiology, Thiamine Deficiency genetics, Vitamins administration & dosage, Vitamins pharmacology, Thiamine administration & dosage, Thiamine pharmacology, Thiamine Deficiency prevention & control

Abstract

Starting with a brief history of beriberi and the discovery that thiamin deficiency is its cause, the symptoms and signs are reviewed. None are pathognomonic. The disease has a low mortality and a long morbidity. The appearance of the patient can be deceptive, often being mistaken for psychosomatic disease in the early stages. The chemistry of thiamin and the laboratory methodology for depicting its deficiency are outlined. The diseases associated with thiamin deficiency, apart from malnutrition, include a number of genetically determined conditions where mutations, either in the cofactor relationship or a transporter, provide the etiology. It is emphasized that such mutations are often epigenetically responsive to megadoses of thiamin or one of its derivatives. The use of thiamin in clinical practice requires a high index of suspicion on the part of the clinician since it has a part to play in eating disorders, diabetes, neurodegenerative disease, and cancer. A high rate of critical illness and postsurgery thiamin deficiency have been reported, particularly those associated with gastrointestinal bypass. Emphasis is placed on thiamin deficiency as a major cause of asymmetric dysautonomia, because of the high degree of sensitivity to thiamin deficiency in the brainstem, cerebellum, and hypothalamus. The relationship of thiamin with regional pain syndrome, eosinophilic esophagitis, its analgesic capacity, and its preventive use in obstetrics is raised as a potential issue. The role of thiamin in SIDS and autism is outlined. It is emphasized that megadose thiamin is being used as a drug, either in stimulating the damaged cofactor/enzyme combination, or mitochondria., (© 2018 Elsevier Inc. All rights reserved.)

Published

2018

23. A Novel Mutation of SLC19A2 in a Chinese Zhuang Ethnic Family with Thiamine-Responsive Megaloblastic Anemia.

Author

Xian X, Liao L, Shu W, Li H, Qin Y, Yan J, Luo J, and Lin FQ

Subjects

Anemia, Megaloblastic ethnology, Anemia, Megaloblastic metabolism, Anemia, Megaloblastic pathology, Asian People, China ethnology, Diabetes Mellitus ethnology, Diabetes Mellitus metabolism, Diabetes Mellitus pathology, Female, Hearing Loss, Sensorineural ethnology, Hearing Loss, Sensorineural metabolism, Hearing Loss, Sensorineural pathology, Humans, Infant, Male, Membrane Transport Proteins chemistry, Membrane Transport Proteins metabolism, Thiamine Deficiency ethnology, Thiamine Deficiency genetics, Thiamine Deficiency metabolism, Thiamine Deficiency pathology, Anemia, Megaloblastic genetics, Diabetes Mellitus genetics, Exons, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics, Mutation, Thiamine Deficiency congenital

Abstract

Background/aims: Thiamine-responsive megaloblastic anemia syndrome is a rare autosomal recessive disorder resulting from mutations in SLC19A2, and is mainly characterized by megaloblastic anemia, diabetes, and progressive sensorineural hearing loss., Methods: We study a Chinese Zhuang ethnicity family with thiamine-responsive megaloblastic anemia. The proband of the study presented with anemia and diabetes, similar to his late brother, as well as visual impairment. All clinical manifestations were corrected with thiamine (30 mg/d) supplementation for 1-3 months, except for visual impairment, which was irreversible. The presence of mutations in all exons and the flanking sequences of the SLC19A2 gene were analyzed in this family based on the proband's and his brother's clinical data. Computer analysis and prediction of the protein conformation of mutant THTR-1. The relative concentration of thiamine pyrophosphate in the proband's whole blood before and after initiation of thiamine supplement was measured by high performance liquid chromatography (HPLC)., Results: Gene sequencing showed a homozygous mutation in exon 6 of the SLC19A2 gene (c.1409insT) in the proband. His parents and sister were diagnosed as heterozygous carriers of the c.1409insT mutation. Computer simulation showed that the mutations caused a change in protein conformation. HPLC results suggested that the relative concentration of thiamine pyrophosphate in the proband's whole blood after thiamine supplement was significantly different (P=0.016) from that at baseline., Conclusions: This novel homozygous mutation (c.1409insT) caused the onset of thiamine-responsive megaloblastic anemia in the proband., (© 2018 The Author(s). Published by S. Karger AG, Basel.)

Published

2018

24. First 2 cases with thiamine-responsive megaloblastic anemia in the Czech Republic, a rare form of monogenic diabetes mellitus: a novel mutation in the thiamine transporter SLC19A2 gene-intron 1 mutation c.204+2T>G.

Author

Pomahačová R, Zamboryová J, Sýkora J, Paterová P, Fiklík K, Votava T, Černá Z, Jehlička P, Lád V, Šubrt I, Dort J, and Dortová E

Subjects

Child, Preschool, Czech Republic, Female, Humans, Infant, Mutation, Thiamine Deficiency genetics, Anemia, Megaloblastic genetics, Diabetes Mellitus genetics, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics, Thiamine Deficiency congenital

Abstract

Thiamine-responsive megaloblastic anemia (TRMA) is a rare autosomal recessive disorder caused by mutations in the SLC19A2 gene. To date at least 43 mutations have been reported for the gene encoding a plasma membrane thiamine transporter protein (THTR-1). TRMA has been reported in less than 80 cases worldwide. Here, we illustrate 2 female patients with TRMA first diagnosed in the Czech Republic and in central Europe being confirmed by sequencing of the THTR-1 gene SLC19A2. Both subjects are compound heterozygotes with 3 different mutations in the SLC19A2 gene. In case 2, the SLC19A2 intron 1 mutation c.204+2T>G has never been reported before. TRMA subjects are at risk of diabetic ketoacidosis during intercurrent disease and arrythmias. Thiamine supplementation has prevented hematological disorders over a few years in both pediatric subjects, and improved glycaemic control of diabetes mellitus. Patient 1 was suffering from hearing loss and rod-cone dystrophy at the time of diagnosis, however, she was unresponsive to thiamine substitution. Our patient 2 developed the hearing loss despite the early thiamine substitution, however no visual disorder had developed. The novel mutation described here extends the list of SLC19A2 mutations causing TRMA., (© 2016 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2017

25. Thiamine antagonists trigger p53-dependent apoptosis in differentiated SH-SY5Y cells.

Author

Chornyy S, Parkhomenko Y, and Chorna N

Subjects

Cell Differentiation, Cell Line, Tumor, Energy Metabolism, Gene Expression Regulation, Neoplastic, Gene Regulatory Networks, Humans, Neurons metabolism, Oxidative Stress, Protein Binding, Signal Transduction, Thiamine Deficiency genetics, Thiamine Deficiency metabolism, Tumor Suppressor Protein p53 metabolism, Apoptosis drug effects, Apoptosis genetics, Thiamine antagonists & inhibitors, Tumor Suppressor Protein p53 genetics

Abstract

Accumulating evidences suggest that p53 is a key coordinator of cellular events triggered by oxidative stress often associated with the impairment in thiamine metabolism and its functions. However, there are limited data regarding the pursuant feedback between p53 transactivation and thiamine homeostasis. Impairment in thiamine metabolism can be induced experimentally via interference with the thiamine uptake and/or inhibition of the thiamin pyrophosphate-dependent enzymes using thiamine antagonists - amprolium (AM), oxythiamine (OT) or pyrithiamine (PT). We found that exposure of neuronally differentiated SH-SY5Y cells to AM, OT and PT triggered upregulation of p53 gene expression, post-translational modification of p53 via phosphorylation and activation of p53 DNA-binding activity. Phosphorylation of p53 at Ser20 was equally efficient in upregulation of thiamine transporter 1 (THTR1) by all antagonists. However, induction of the expressions of the pyruvate dehydrogenase E1 component subunit beta (PDHB) and oxoglutarate dehydrogenase (OGDH) required dual phosphorylation of p53 at Ser9 and Ser20, seen in cells treated with PT and OT. Moreover, pretreatment of the cells with a decoy oligonucleotide carrying wild-type p53-response element markedly attenuated OT-induced THTR1, PDHB and OGDH gene expression suggesting an important role of p53 in transactivation of these genes. Finally, analysis of gene and metabolic networks showed that OT triggers cell apoptosis through the p53-dependent intrinsic pathway.

Published

2017

26. Thiamine deficiency in childhood with attention to genetic causes: Survival and outcome predictors.

Author

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, and Pérez-Dueñas B

Subjects

Adolescent, Age of Onset, Child, Child, Preschool, Female, Humans, Infant, Membrane Transport Proteins genetics, Mitochondrial Membrane Transport Proteins, Mutation, Prognosis, Survival Rate, Thiamine Deficiency mortality, Young Adult, Thiamine Deficiency genetics

Abstract

Primary and secondary conditions leading to thiamine deficiency have overlapping features in children, presenting with acute episodes of encephalopathy, bilateral symmetric brain lesions, and high excretion of organic acids that are specific of thiamine-dependent mitochondrial enzymes, mainly lactate, alpha-ketoglutarate, and branched chain keto-acids. Undiagnosed and untreated thiamine deficiencies are often fatal or lead to severe sequelae. Herein, we describe the clinical and genetic characterization of 79 patients with inherited thiamine defects causing encephalopathy in childhood, identifying outcome predictors in patients with pathogenic SLC19A3 variants, the most common genetic etiology. We propose diagnostic criteria that will aid clinicians to establish a faster and accurate diagnosis so that early vitamin supplementation is considered. Ann Neurol 2017;82:317-330., (© 2017 American Neurological Association.)

Published

2017

27. Monogenic diabetes syndromes: Locus-specific databases for Alström, Wolfram, and Thiamine-responsive megaloblastic anemia.

Author

Astuti D, Sabir A, Fulton P, Zatyka M, Williams D, Hardy C, Milan G, Favaretto F, Yu-Wai-Man P, Rohayem J, López de Heredia M, Hershey T, Tranebjaerg L, Chen JH, Chaussenot A, Nunes V, Marshall B, McAfferty S, Tillmann V, Maffei P, Paquis-Flucklinger V, Geberhiwot T, Mlynarski W, Parkinson K, Picard V, Bueno GE, Dias R, Arnold A, Richens C, Paisey R, Urano F, Semple R, Sinnott R, and Barrett TG

Subjects

Adolescent, Adult, Child, Child, Preschool, Exons, Family Health, Female, Genetic Association Studies, Genetic Variation, Genotype, Homozygote, Humans, Male, Phenotype, Prognosis, Sensitivity and Specificity, Thiamine Deficiency genetics, Young Adult, Anemia, Megaloblastic genetics, Databases, Genetic, Diabetes Mellitus genetics, Hearing Loss, Sensorineural genetics, Thiamine Deficiency congenital, Wolfram Syndrome genetics

Abstract

We developed a variant database for diabetes syndrome genes, using the Leiden Open Variation Database platform, containing observed phenotypes matched to the genetic variations. We populated it with 628 published disease-associated variants (December 2016) for: WFS1 (n = 309), CISD2 (n = 3), ALMS1 (n = 268), and SLC19A2 (n = 48) for Wolfram type 1, Wolfram type 2, Alström, and Thiamine-responsive megaloblastic anemia syndromes, respectively; and included 23 previously unpublished novel germline variants in WFS1 and 17 variants in ALMS1. We then investigated genotype-phenotype relations for the WFS1 gene. The presence of biallelic loss-of-function variants predicted Wolfram syndrome defined by insulin-dependent diabetes and optic atrophy, with a sensitivity of 79% (95% CI 75%-83%) and specificity of 92% (83%-97%). The presence of minor loss-of-function variants in WFS1 predicted isolated diabetes, isolated deafness, or isolated congenital cataracts without development of the full syndrome (sensitivity 100% [93%-100%]; specificity 78% [73%-82%]). The ability to provide a prognostic prediction based on genotype will lead to improvements in patient care and counseling. The development of the database as a repository for monogenic diabetes gene variants will allow prognostic predictions for other diabetes syndromes as next-generation sequencing expands the repertoire of genotypes and phenotypes. The database is publicly available online at https://lovd.euro-wabb.org., (© 2017 The Authors. **Human Mutation published by Wiley Periodicals, Inc.)

Published

2017

28. Infantile-onset thiamine responsive megaloblastic anemia syndrome with SLC19A2 mutation: a case report.

Author

Katipoğlu N, Karapinar TH, Demir K, Aydin Köker S, Nalbantoğlu Ö, Ay Y, Korkmaz HA, Oymak Y, Yıldız M, Tunç S, Hazan F, Vergin C, and Ozkan B

Subjects

Female, Humans, Infant, Thiamine Deficiency genetics, Anemia, Megaloblastic genetics, Diabetes Mellitus genetics, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics, Mutation, Thiamine Deficiency congenital

Abstract

Background: Thiamine-responsive megaloblastic anemia syndrome (TRMA), also known as Rogers syndrome, is characterized by megaloblastic anemia, sensorineural hearing loss, and diabetes mellitus. Disturbances of the thiamine transport into the cells results from homozygous or compound heterozygous mutations in the SLC19A2 gene., Case Presentation: We report a girl which presented with sensorineural deafness treated with a hearing prosthesis, insulin requiring diabetes, macrocytic anemia, treated with thiamine (100 mg/day). Hemoglobin level improved to 12.1 g/dl after dose of thiamine therapy increased up to 200 mg/day., Conclusion: Patients with TRMA must be evaluated for megaloblastic anemia, sensorineural hearing loss, and diabetes mellitus. They must be followed for response of hematologic and diabetic after thiamine therapy. It should be kept in mind that dose of thiamine therapy may be increased according to the clinical response. Genetic counseling should be given.

Published

2017

29. Novel nonsense mutation (p.Ile411Metfs*12) in the SLC19A2 gene causing Thiamine Responsive Megaloblastic Anemia in an Indian patient.

Author

Manimaran P, Subramanian VS, Karthi S, Gandhimathi K, Varalakshmi P, Ganesh R, Rathinavel A, Said HM, and Ashokkumar B

Subjects

Anemia, Megaloblastic diagnosis, Child, Preschool, Diabetes Mellitus diagnosis, Female, Genotype, Hearing Loss, Sensorineural diagnosis, Humans, India, Thiamine Deficiency diagnosis, Thiamine Deficiency genetics, Anemia, Megaloblastic genetics, Codon, Nonsense genetics, Diabetes Mellitus genetics, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics, Thiamine Deficiency congenital

Abstract

Thiamine-responsive megaloblastic anemia (TRMA), an autosomal recessive disorder, is caused by mutations in SLC19A2 gene encodes a high affinity thiamine transporter (THTR-1). The occurrence of TRMA is diagnosed by megaloblastic anemia, diabetes mellitus, and sensorineural deafness. Here, we report a female TRMA patient of Indian descent born to 4th degree consanguineous parents presented with retinitis pigmentosa and vision impairment, who had a novel homozygous mutation (c.1232delT/ter422; p.Ile411Metfs*12) in 5th exon of SLC19A2 gene that causes premature termination of hTHTR-1. PROSITE analysis predicted to abrogate GPCRs family-1 signature motif in the variant by this mutation c.1232delT/ter422, suggesting uncharacteristic rhodopsin function leading to cause RP clinically. Thiamine transport activity by the clinical variant was severely inhibited than wild-type THTR-1. Confocal imaging had shown that the variant p.I411Mfs*12 is targeted to the cell membrane and showed no discrepancy in membrane expression than wild-type. Our findings are the first report, to the best of our knowledge, on this novel nonsense mutation of hTHTR-1 causing TRMA in an Indian patient through functionally impaired thiamine transporter activity., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2016

30. Thiamine Deprivation Produces a Liver ATP Deficit and Metabolic and Genomic Effects in Mice: Findings Are Parallel to Those of Biotin Deficiency and Have Implications for Energy Disorders.

Author

Hernandez-Vazquez AJ, Garcia-Sanchez JA, Moreno-Arriola E, Salvador-Adriano A, Ortega-Cuellar D, and Velazquez-Arellano A

Subjects

Adenosine Triphosphate deficiency, Animals, Gene-Environment Interaction, Genome drug effects, Gluconeogenesis drug effects, Gluconeogenesis genetics, Liver drug effects, Male, Metabolic Diseases genetics, Metabolic Diseases metabolism, Mice, Mice, Inbred C57BL, Thiamine pharmacology, Adenosine Triphosphate metabolism, Biotinidase Deficiency genetics, Biotinidase Deficiency metabolism, Energy Metabolism drug effects, Energy Metabolism genetics, Liver metabolism, Metabolic Diseases etiology, Thiamine Deficiency genetics, Thiamine Deficiency metabolism

Abstract

Thiamine is one of several essential cofactors for ATP generation. Its deficiency, like in beriberi and in the Wernicke-Korsakoff syndrome, has been studied for many decades. However, its mechanism of action is still not completely understood at the cellular and molecular levels. Since it acts as a coenzyme for dehydrogenases of pyruvate, branched-chain keto acids, and ketoglutarate, its nutritional privation is partly a phenocopy of inborn errors of metabolism, among them maple syrup urine disease. In the present paper, we report metabolic and genomic findings in mice deprived of thiamine. They are similar to the ones we have previously found in biotin deficiency, another ATP generation cofactor. Here we show that thiamine deficiency substantially reduced the energy state in the liver and activated the energy sensor AMP-activated kinase. With this vitamin deficiency, several metabolic parameters changed: blood glucose was diminished and serum lactate was increased, but insulin, triglycerides, and cholesterol, as well as liver glycogen, were reduced. These results indicate a severe change in the energy status of the whole organism. Our findings were associated with modified hepatic levels of the mRNAs of several carbon metabolism genes: a reduction of transcripts for liver glucokinase and fatty acid synthase and augmentation of those for carnitine palmitoyl transferase 1 and phosphoenolpyruvate carboxykinase as markers for glycolysis, fatty acid synthesis, beta-oxidation, and gluconeogenesis, respectively. Glucose tolerance was initially increased, suggesting augmented insulin sensitivity, as we had found in biotin deficiency; however, in the case of thiamine, it was diminished from the 3rd week on, when the deficient animals became undernourished, and paralleled the changes in AKT and mTOR, 2 main proteins in the insulin signaling pathway. Since many of the metabolic and gene expression effects on mice deprived of thiamine are similar to those in biotin deficiency, it may be that they result from a more general impairment of oxidative phosphorylation due to a shortage of ATP generation cofactors. These findings may be relevant to energy-related disorders, among them several inborn errors of metabolism, as well as common energy disorders like obesity, diabetes, and neurodegenerative illnesses., (© 2017 S. Karger AG, Basel.)

Published

2016

31. Thiamine Deficiency-Mediated Brain Mitochondrial Pathology in Alaskan Huskies with Mutation in SLC19A3.1.

Author

Vernau K, Napoli E, Wong S, Ross-Inta C, Cameron J, Bannasch D, Bollen A, Dickinson P, and Giulivi C

Subjects

Animals, Brain ultrastructure, DNA, Mitochondrial genetics, Dogs, Mitochondria genetics, Models, Molecular, Nervous System Diseases etiology, Thiamine metabolism, Brain pathology, Membrane Transport Proteins genetics, Mitochondria pathology, Mutation genetics, Thiamine Deficiency genetics, Thiamine Deficiency pathology, Thiamine Deficiency veterinary

Abstract

Alaskan Husky encephalopathy (AHE(1) ) is a fatal brain disease associated with a mutation in SLC19A3.1 (c.624insTTGC, c.625C>A). This gene encodes for a thiamine transporter 2 with a predominately (CNS) central nervous system distribution. Considering that brain is particularly vulnerable to thiamine deficiency because of its reliance on thiamine pyrophosphate (TPP)-dependent metabolic pathways involved in energy metabolism and neurotransmitter synthesis, we characterized the impact of this mutation on thiamine status, brain bioenergetics and the contribution of oxidative stress to this phenotype. In silico modeling of the mutated transporter indicated a significant loss of alpha-helices resulting in a more open protein structure suggesting an impaired thiamine transport ability. The cerebral cortex and thalamus of affected dogs were severely deficient in TPP-dependent enzymes accompanied by decreases in mitochondrial mass and oxidative phosphorylation (OXPHOS) capacity, and increases in oxidative stress. These results along with the behavioral and pathological findings indicate that the phenotype associated with AHE is consistent with a brain-specific thiamine deficiency, leading to brain mitochondrial dysfunction and increased oxidative stress. While some of the biochemical deficits, neurobehavior and affected brain areas in AHE were shared by Wernicke's and Korsakoff's syndromes, several differences were noted likely arising from a tissue-specific vs. that from a whole-body thiamine deficiency., (© 2014 International Society of Neuropathology.)

Published

2015

32. Thiamine responsive megaloblastic anemia syndrome: a novel homozygous SLC19A2 gene mutation identified.

Author

Mikstiene V, Songailiene J, Byckova J, Rutkauskiene G, Jasinskiene E, Verkauskiene R, Lesinskas E, and Utkus A

Subjects

Base Sequence, Child, Preschool, Homozygote, Humans, Lithuania, Male, Molecular Sequence Data, Sequence Analysis, DNA, Thiamine Deficiency drug therapy, Thiamine Deficiency genetics, Treatment Outcome, Anemia, Megaloblastic drug therapy, Anemia, Megaloblastic genetics, Diabetes Mellitus drug therapy, Diabetes Mellitus genetics, Hearing Loss, Sensorineural drug therapy, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics, Mutation, Missense genetics, Thiamine therapeutic use, Thiamine Deficiency congenital

Abstract

Thiamine responsive megaloblastic anemia syndrome (TRMAS) is a rare autosomal recessive disorder especially in countries where consanguinity is uncommon. Three main features are characteristic of the disease - megaloblastic anemia, early onset deafness, and non-type I diabetes. TRMAS is a Mendelian disorder; a gene SLC19A2 coding high affinity thiamine transporter mediating vitamin B1 uptake through cell membrane has been identified. We present the first patient with TRMAS in Lithuania - a 3-year-old boy born to a non-consanguineous family with a novel homozygous SLC19A2 gene mutation. The patient had insulin dependent diabetes (onset 11 months), respiratory illness (onset 11 months), bilateral profound hearing loss (onset at 7 months, verified at 20 months), refractory anemia (onset 2 years), and decreased vision acuity and photophobia (onset 2.5 years). The psychomotor abilities developed according to age. Phenotypic evaluation did not reveal any dysmorphic features. The clinical diagnosis of TRMAS was suspected and daily supplementation with thiamine 100 mg was started. The condition of the patient markedly improved several days after the initiation of treatment. The results of SLC19A2 gene molecular testing confirmed the clinical diagnosis - novel homozygous c.[205G>T], p.[(Val69Phe)] mutation changing conserved amino acid residue or even interfering the mRNA splicing. Clinical heterogeneity, diverse dynamics, and wide spectrum of symptoms are aggravating factors in the diagnosis. The possibility of treatment demands early recognition of disorder to facilitate the improvement of the patient's condition., (© 2015 Wiley Periodicals, Inc.)

Published

2015

33. Spatial cognitive deficits in an animal model of Wernicke-Korsakoff syndrome are related to changes in thalamic VDAC protein concentrations.

Author

Bueno KO, de Souza Resende L, Ribeiro AF, Dos Santos DM, Gonçalves EC, Vigil FA, de Oliveira Silva IF, Ferreira LF, de Castro Pimenta AM, and Ribeiro AM

Subjects

Animals, Disease Models, Animal, Korsakoff Syndrome genetics, Male, Proteomics methods, Rats, Wistar, Space Perception, Thiamine Deficiency genetics, Cognition Disorders metabolism, Korsakoff Syndrome metabolism, Learning physiology, Thalamus metabolism, Voltage-Dependent Anion Channels metabolism

Abstract

Proteomic profiles of the thalamus and the correlation between the rats' performance on a spatial learning task and differential protein expression were assessed in the thiamine deficiency (TD) rat model of Wernicke-Korsakoff syndrome. Two-dimensional gel-electrophoresis detected 320 spots and a significant increase or decrease in seven proteins. Four proteins were correlated to rat behavioral performance in the Morris Water Maze. One of the four proteins was identified by mass spectrometry as Voltage-Dependent Anion Channels (VDACs). The association of VDAC is evident in trials in which the rats' performance was worst, in which the VDAC protein was reduced, as confirmed by Western blot. No difference was observed on the mRNA of Vdac genes, indicating that the decreased VDAC expression may be related to a post-transcriptional process. The results show that TD neurodegeneration involves changes in thalamic proteins and suggest that VDAC protein activity might play an important role in an initial stage of the spatial learning process., (Copyright © 2015 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2015

34. Defects of thiamine transport and metabolism.

Author

Brown G

Subjects

Animals, Biological Transport genetics, Humans, Maple Syrup Urine Disease genetics, Maple Syrup Urine Disease metabolism, Membrane Transport Proteins metabolism, Pyruvate Dehydrogenase Complex Deficiency Disease genetics, Pyruvate Dehydrogenase Complex Deficiency Disease metabolism, Thiamin Pyrophosphokinase deficiency, Thiamin Pyrophosphokinase genetics, Thiamine Deficiency metabolism, Membrane Transport Proteins genetics, Thiamine metabolism, Thiamine Deficiency genetics

Abstract

Thiamine, in the form of thiamine pyrophosphate, is a cofactor for a number of enzymes which play important roles in energy metabolism. Although dietary thiamine deficiency states have long been recognised, it is only relatively recently that inherited defects in thiamine uptake, activation and the attachment of the active cofactor to target enzymes have been described, and the underlying genetic defects identified. Thiamine is transported into cells by two carriers, THTR1 and THTR2, and deficiency of these results in thiamine-responsive megaloblastic anaemia and biotin-responsive basal ganglia disease respectively. Defective synthesis of thiamine pyrophosphate has been found in a small number of patients with episodic ataxia, delayed development and dystonia, while impaired transport of thiamine pyrophosphate into the mitochondrion is associated with Amish lethal microcephaly in most cases. In addition to defects in thiamine uptake and metabolism, patients with pyruvate dehydrogenase deficiency and maple syrup urine disease have been described who have a significant clinical and/or biochemical response to thiamine supplementation. In these patients, an intrinsic structural defect in the target enzymes reduces binding of the cofactor and this can be overcome at high concentrations. In most cases, the clinical and biochemical abnormalities in these conditions are relatively non-specific, and the range of recognised presentations is increasing rapidly at present as new patients are identified, often by genome sequencing. These conditions highlight the value of a trial of thiamine supplementation in patients whose clinical presentation falls within the spectrum of documented cases.

Published

2014

35. Thiamine deficiency: the importance of recognition and prompt management.

Author

Crook MA and Sriram K

Subjects

Humans, Male, Beriberi genetics, Membrane Transport Proteins genetics, Mutation, Thiamine genetics, Thiamine Deficiency genetics

Published

2014

36. Analysis of thiamine transporter genes in sporadic beriberi.

Author

Bravatà V, Minafra L, Callari G, Gelfi C, and Edoardo Grimaldi LM

Subjects

Adult, Alcoholism, Beriberi etiology, Humans, Male, Mitochondrial Membrane Transport Proteins, Thiamine Deficiency complications, Beriberi genetics, Membrane Transport Proteins genetics, Mutation, Thiamine genetics, Thiamine Deficiency genetics

Abstract

Objective: Thiamine or vitamin B1 deficiency diminishes thiamine-dependent enzymatic activity, alters mitochondrial function, impairs oxidative metabolism, and causes selective neuronal death. We analyzed for the first time, the role of all known mutations within three specific thiamine carrier genes, SLC19 A2, SLC19 A3, and SLC25 A19, in a patient with atrophic beriberi, a multiorgan nutritional disease caused by thiamine deficiency., Methods: A 44-year-old male alcoholic patient from Morocco developed massive bilateral leg edema, a subacute sensorimotor neuropathy, and incontinence. Despite normal vitamin B1 serum levels, his clinical picture was rapidly reverted by high-dose intramuscular thiamine treatment, suggesting a possible genetic resistance. We used polymerase chain reaction followed by amplicon sequencing to study all the known thiamine-related gene mutations identified within the Human Gene Mutation Database., Results: Thirty-seven mutations were tested: 29 in SLC19 A2, 6 in SLC19 A3, and 2 in SLC25 A19. Mutational analyses showed a wild-type genotype for all sequences investigated., Conclusion: This is the first genetic study in beriberi disease. We did not detect any known mutation in any of the three genes in a sporadic dry beriberi patient. We cannot exclude a role for other known or unknown mutations, in the same genes or in other thiamine-associated genes, in the occurrence of this nutritional neuropathy., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

37. Neuropathology of alcoholism.

Author

Sutherland GT, Sheedy D, and Kril JJ

Subjects

Alcoholism genetics, Alcoholism metabolism, Animals, Brain metabolism, Humans, Thiamine Deficiency genetics, Thiamine Deficiency metabolism, Thiamine Deficiency pathology, Wernicke Encephalopathy genetics, Wernicke Encephalopathy metabolism, Wernicke Encephalopathy pathology, Alcoholism pathology, Brain pathology

Abstract

Chronic alcohol consumption results in structural changes to the brain. In alcoholics without coexisting thiamine deficiency or liver disease this is largely restricted to a loss of white-matter volume. When it occurs, neuronal loss is limited in anatomic distribution and only detected with quantitative techniques. This relative paucity of neurodegeneration is reflected in studies of gene and protein expression in postmortem brain where findings are subtle and discordant between studies. In alcoholics with coexisting pathologies, neuronal loss is more marked and affects a wider range of anatomic regions, especially subcortical nuclei. Although this more widespread damage may reflect a more severe drinking history, there is evidence linking thiamine deficiency and the consequences of liver disease to the pathogenesis of alcohol-related brain damage. Furthermore, a range of other factors, such as cigarette smoking and mood disorders, that are common in alcoholics, have the potential to influence studies of brain pathology and should be considered in further studies of the neuropathology of alcoholism., (© 2014 Elsevier B.V. All rights reserved.)

Published

2014

38. The role of thiamine in cancer: possible genetic and cellular signaling mechanisms.

Author

Lu'o'ng KV and Nguyễn LT

Subjects

Cyclooxygenase 2 genetics, Humans, Neoplasms pathology, Prostaglandins metabolism, Reduced Folate Carrier Protein metabolism, Signal Transduction, Thiamine genetics, Thiamine Deficiency genetics, Thiamine Deficiency pathology, Transketolase genetics, Transketolase metabolism, Neoplasms blood, Neoplasms genetics, Thiamine blood, Thiamine pharmacokinetics

Abstract

The relationship between supplemental vitamins and various types of cancer has been the focus of recent investigation, and supplemental vitamins have been reported to modulate cancer rates. A significant association has been demonstrated between cancer and low levels of thiamine in the serum. Genetic studies have helped identify a number of factors that link thiamine to cancer, including the solute carrier transporter (SLC19) gene, transketolase, transcription factor p53, poly(ADP-ribose) polymerase-1 gene, and the reduced form of nicotinamide adenine dinucleotide phosphate. Thiamine supplementation may contribute to a high rate of tumor cell survival, proliferation and chemotherapy resistance. Thiamine has also been implicated in cancer through its effects on matrix metalloproteinases, prostaglandins, cyclooxygenase-2, reactive oxygen species, and nitric oxide synthase. However, some studies have suggested that thiamine may exhibit some antitumor effects. The role of thiamine in cancer is controversial. However, thiamine deficiency may occur in patients with cancer and cause serious disorders, including Wernicke's encephalopathy, that require parenteral thiamine supplementation. A very high dose of thiamine produces a growth-inhibitory effect in cancer. Therefore, further investigations of thiamine in cancer are needed to clarify this relationship.

Published

2013

39. Reversible lactic acidosis in a newborn with thiamine transporter-2 deficiency.

Author

Pérez-Dueñas B, Serrano M, Rebollo M, Muchart J, Gargallo E, Dupuits C, and Artuch R

Subjects

Acidosis, Lactic drug therapy, Biotin administration & dosage, Blood Chemical Analysis, Carnitine administration & dosage, Diagnosis, Differential, Drug Therapy, Combination, Follow-Up Studies, Gene Expression Regulation, Humans, Infant, Newborn, Magnetic Resonance Imaging methods, Male, Membrane Transport Proteins genetics, Mutation, Risk Assessment, Thiamine administration & dosage, Thiamine Deficiency diagnosis, Thiamine Deficiency drug therapy, Treatment Outcome, Acidosis, Lactic diagnosis, Membrane Transport Proteins deficiency, Thiamine Deficiency genetics, Wernicke Encephalopathy diagnosis

Abstract

Thiamine transporter-2 deficiency is a recessive disease caused by mutations in the SLC19A3 gene. Patients manifest acute episodes of encephalopathy; symmetric lesions in the cortex, basal ganglia, thalami or periaqueductal gray matter, and a dramatic response to biotin or thiamine. We report a 30-day-old patient with mutations in the SLC19A3 gene who presented with acute encephalopathy and increased level of lactate in the blood (8.6 mmol/L) and cerebrospinal fluid (7.12 mmol/L), a high excretion of α-ketoglutarate in the urine, and increased concentrations of the branched-chain amino acids leucine and isoleucine in the plasma. MRI detected bilateral and symmetric cortico-subcortical lesions involving the perirolandic area, bilateral putamina, and medial thalami. Some lesions showed low apparent diffusion coefficient values suggesting an acute evolution; others had high values likely to be subacute or chronic, most likely related to the perinatal period. After treatment with thiamine and biotin, irritability and opisthotonus disappeared, and the patient recovered consciousness. Biochemical disturbances also disappeared within 48 hours. After discontinuing biotin, the patient remained stable for 6 months on thiamine supplementation (20 mg/kg/day). The examination revealed subtle signs of neurologic sequelae, and MRI showed necrotic changes and volume loss in some affected areas. Our observations suggest that patients with thiamine transporter 2 deficiency may be vulnerable to metabolic decompensation during the perinatal period, when energy demands are high. Thiamine defects should be excluded in newborns and infants with lactic acidosis because prognosis largely depends on the time from diagnosis to thiamine supplementation.

Published

2013

40. The evolution and treatment of Korsakoff's syndrome: out of sight, out of mind?

Author

Thomson AD, Guerrini I, and Marshall EJ

Subjects

Alcoholism pathology, Animals, Brain pathology, Disease Models, Animal, Humans, Korsakoff Syndrome complications, Korsakoff Syndrome etiology, Korsakoff Syndrome genetics, Thiamine Deficiency complications, Thiamine Deficiency genetics, Wernicke Encephalopathy complications, Wernicke Encephalopathy etiology, Wernicke Encephalopathy genetics, Korsakoff Syndrome therapy, Wernicke Encephalopathy therapy

Abstract

Wernicke's Encephalopathy is an acute neuro-psychiatric condition caused by an insufficient supply of thiamine (Vitamin B1) to the brain. If undiagnosed or inadequately treated, it is likely to proceed to Korsakoff's Syndrome. Wernicke's Encephalopathy can result from dietary deficiency alone and this form is usually successfully treated, with little chance of Korsakoff's Syndrome supervening. On the other hand, thiamine deficiency associated with alcohol misuse/dependence may require up to 1 gram of thiamine IV in the first 24 hours to be treated successfully. The reasons for this difference in treatment will be discussed. Thiamine diphosphate acts as a co-factor for a number of thiamine-dependent enzymes. Thiamine deficiency leads to a reduction in the activity of these enzymes, and this leads to alterations in mitochondrial activity, impairment of oxidative metabolism, decreased energy status and eventually selective neuronal death. The damage caused by the combination of thiamine deficiency and alcohol metabolism probably interferes with adequate thiamine transport at a number of sites in the body, including the blood-brain barrier, as well as causing damage to the apoenzymes which then require higher concentrations of thiamine to work normally. The accumulated damage is likely to render the use of oral thiamine therapeutically inadequate since the body is unable to produce high enough concentrations of thiamine in the blood to traverse the blood-brain barrier. Some individuals are probably genetically predisposed to develop Wernicke's. Long before individuals with alcohol misuse or dependence develop Wernicke's Encephalopathy the neurons and other cells of the body are functioning sub-optimally because of the inadequate supply of thiamine and the neurotoxic effect of alcohol. This relative deficiency initiates a series of pathological changes which accumulate and further interfere with the supply of thiamine and its utilisation at a time when the requirements are increased. The best treatment for Korsakoff's Syndrome is timely recognition of Wernicke's Encephalopathy and appropriate intervention and prevention.

Published

2012

41. Glucose-induced down regulation of thiamine transporters in the kidney proximal tubular epithelium produces thiamine insufficiency in diabetes.

Author

Larkin JR, Zhang F, Godfrey L, Molostvov G, Zehnder D, Rabbani N, and Thornalley PJ

Subjects

Animals, Cells, Cultured, Diabetes Mellitus metabolism, Diabetes Mellitus pathology, Diabetic Nephropathies genetics, Diabetic Nephropathies metabolism, Diabetic Nephropathies pathology, Down-Regulation drug effects, Down-Regulation genetics, Epithelium metabolism, Epithelium pathology, Humans, Kidney Tubules, Proximal pathology, Male, Membrane Transport Proteins genetics, Rats, Rats, Sprague-Dawley, Thiamine Deficiency metabolism, Thiamine Deficiency pathology, Diabetes Mellitus genetics, Glucose pharmacology, Kidney Tubules, Proximal metabolism, Membrane Transport Proteins metabolism, Thiamine metabolism, Thiamine Deficiency genetics

Abstract

Increased renal clearance of thiamine (vitamin B(1)) occurs in experimental and clinical diabetes producing thiamine insufficiency mediated by impaired tubular re-uptake and linked to the development of diabetic nephropathy. We studied the mechanism of impaired renal re-uptake of thiamine in diabetes. Expression of thiamine transporter proteins THTR-1 and THTR-2 in normal human kidney sections examined by immunohistochemistry showed intense polarised staining of the apical, luminal membranes in proximal tubules for THTR-1 and THTR-2 of the cortex and uniform, diffuse staining throughout cells of the collecting duct for THTR-1 and THTR-2 of the medulla. Human primary proximal tubule epithelial cells were incubated with low and high glucose concentration, 5 and 26 mmol/l, respectively. In high glucose concentration there was decreased expression of THTR-1 and THTR-2 (transporter mRNA: -76% and -53% respectively, p<0.001; transporter protein -77% and -83% respectively, p<0.05), concomitant with decreased expression of transcription factor specificity protein-1. High glucose concentration also produced a 37% decrease in apical to basolateral transport of thiamine transport across cell monolayers. Intensification of glycemic control corrected increased fractional excretion of thiamine in experimental diabetes. We conclude that glucose-induced decreased expression of thiamine transporters in the tubular epithelium may mediate renal mishandling of thiamine in diabetes. This is a novel mechanism of thiamine insufficiency linked to diabetic nephropathy.

Published

2012

42. Loss of the glutamate transporter splice-variant GLT-1b in inferior colliculus and its prevention by ceftriaxone in thiamine deficiency.

Author

Jhala SS, Wang D, and Hazell AS

Subjects

Animals, Ceftriaxone pharmacology, Cells, Cultured, Excitatory Amino Acid Transporter 2 genetics, Inferior Colliculi drug effects, Male, Protein Isoforms deficiency, Protein Isoforms genetics, Rats, Rats, Sprague-Dawley, Thiamine Deficiency genetics, Ceftriaxone therapeutic use, Excitatory Amino Acid Transporter 2 deficiency, Inferior Colliculi metabolism, Thiamine Deficiency metabolism, Thiamine Deficiency prevention & control

Abstract

Downregulation of astrocytic glutamate transporters is a feature of thiamine deficiency (TD), the underlying cause of Wernicke's encephalopathy, and plays a major role in its pathophysiology. Recent investigations suggest that ceftriaxone, a β-lactam antibiotic, stimulates GLT-1 expression and confers neuroprotection against ischemic and motor neuron degeneration. Thus, ceftriaxone treatment may be a protective strategy against excitotoxic conditions. In the present study, we examined the effects of ceftriaxone on the glutamate transporter splice-variant GLT-1b in rats with TD and in cultured astrocytes under TD conditions. Our results indicate that ceftriaxone protects against loss of GLT-1b levels in the inferior colliculus during TD, but with no significant effect in the thalamus and frontal cortex by immunoblotting and immunohistochemistry. Ceftriaxone also normalized the loss of GLT-1b in astrocyte cultures under conditions of TD. These results suggest that ceftriaxone has the ability to increase GLT-1b levels in astrocytes during TD, and may be an important pharmacological strategy for the treatment of excitotoxicity in this disorder., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

43. Effect of chronic alcohol feeding on physiological and molecular parameters of renal thiamin transport.

Author

Subramanian VS, Subramanya SB, Tsukamoto H, and Said HM

Subjects

Animals, Biological Transport, Cell Polarity, Down-Regulation, Epithelial Cells metabolism, Homeostasis, Kidney metabolism, Male, Membrane Transport Proteins genetics, Microvilli metabolism, RNA, Heterogeneous Nuclear metabolism, RNA, Messenger metabolism, Rats, Rats, Wistar, Thiamin Pyrophosphokinase metabolism, Thiamine Deficiency etiology, Thiamine Deficiency genetics, Time Factors, Transcription, Genetic, Alcohol Drinking adverse effects, Central Nervous System Depressants toxicity, Epithelial Cells drug effects, Ethanol toxicity, Kidney drug effects, Membrane Transport Proteins metabolism, Thiamine metabolism, Thiamine Deficiency metabolism

Abstract

The renal thiamin reabsorption process plays an important role in regulating thiamin body homeostasis and involves both thiamin transporters-1 and -2 (THTR1 and THTR2). Chronic alcohol use is associated with thiamin deficiency. Although a variety of factors contribute to the development of this deficiency, effects of chronic alcohol use on renal thiamin transport have not been thoroughly examined. We addressed this issue by examining the effect of chronic alcohol feeding of rats with liquid diet on physiological and molecular parameters of renal thiamin transport. Chronic alcohol feeding caused a significant inhibition in carrier-mediated thiamin transport across the renal brush-border membrane and was evident as early as 2 wk after initiation of alcohol feeding. Similarly, thiamin transport across the renal basolateral membrane was significantly inhibited by chronic alcohol feeding. The inhibition in renal thiamin transport was associated with a marked decrease in the level of expression of THTR1 and -2 proteins, mRNAs, and heterogeneous nuclear RNAs. Chronic alcohol feeding also caused a significant reduction in the level of expression of thiamin pyrophosphokinase but not that of the mitochondrial thiamin pyrophosphate transporter. These studies show that chronic alcohol feeding inhibits the entry and exit of thiamin in the polarized renal epithelial cells and that the effect is, at least in part, mediated at the transcriptional level. These findings also suggest that chronic alcohol feeding interferes with the normal homeostasis of thiamin in renal epithelial cells.

Published

2010

44. Unraveling the pathophysiology of alcohol-induced thiamin deficiency.

Author

Kiela PR

Subjects

Animals, Biological Transport, Down-Regulation, Epithelial Cells drug effects, Epithelial Cells metabolism, Homeostasis, Humans, Kidney metabolism, Membrane Transport Proteins genetics, Rats, Thiamine Deficiency genetics, Thiamine Deficiency metabolism, Thiamine Deficiency physiopathology, Transcription, Genetic, Alcohol Drinking adverse effects, Central Nervous System Depressants toxicity, Ethanol toxicity, Kidney drug effects, Membrane Transport Proteins metabolism, Thiamine metabolism, Thiamine Deficiency etiology

Published

2010

45. Molecular genetics of alcohol-related brain damage.

Author

Guerrini I, Thomson AD, and Gurling HM

Subjects

Alcoholism genetics, Alcoholism pathology, Animals, Brain Damage, Chronic pathology, Carrier Proteins genetics, Carrier Proteins metabolism, Humans, Thiamine Deficiency genetics, Thiamine Deficiency psychology, Brain Damage, Chronic genetics, Ethanol toxicity

Abstract

Aims: In the scientific literature it has been repeatedly hypothesized that there is a heritable susceptibility to thiamine deficiency comparable to other hereditary metabolic disorders. The aim of this paper is to review the most recent knowledge on the genetic susceptibility to the development of alcohol-related Wernicke-Korsakoff syndrome (WKS)., Methods: A literature review was carried out looking at the molecular genetics studies performed in alcohol-dependent patients affected by WKS., Results: A genetic component in the pathogenesis of WKS has been postulated since the late seventies. Since then, very few genetic studies have been carried out on candidate genes such as thiamine-dependent enzymes, alcohol-metabolizing enzymes and GABA receptors. The findings are controversial and not conclusive. Several authors reported the important role of the thiamine transporters in the pathogenesis of the thiamine deficiency disorders. Our findings on SLC19A2 and SLC19A3 suggest a potential role of these two genes in the pathophysiology of alcohol-related thiamine deficiency but further studies need to be carried out., Conclusions: The WKS may be a very complex, multifactorial disorder where the interaction of multiple genes and environment plays an important role in the pathogenesis. However, it is still plausible that megaphenic gene effects are responsible for WKS susceptibility and the thiamine transport genes are good candidates for having such a role. Further genetic studies are definitely needed to investigate the association with candidate genes or linkage with hot spot areas.

Published

2009

46. Targeting and intracellular trafficking of clinically relevant hTHTR1 mutations in human cell lines.

Author

Subramanian VS, Marchant JS, and Said HM

Subjects

Anemia, Megaloblastic genetics, Cell Line, Cytoplasm metabolism, DNA Mutational Analysis, Deafness genetics, Deafness metabolism, Diabetes Mellitus genetics, Diabetes Mellitus metabolism, Flow Cytometry, Humans, Microscopy, Confocal, Protein Transport, Reverse Transcriptase Polymerase Chain Reaction, Thiamine Deficiency genetics, Thiamine Deficiency metabolism, Transfection methods, Anemia, Megaloblastic metabolism, Membrane Transport Proteins genetics, Membrane Transport Proteins metabolism, Point Mutation, Thiamine metabolism

Abstract

The micronutrient thiamine is required for normal growth and development of human tissues, and is accumulated into cells through the activity of plasma membrane thiamine transporters, e.g. hTHTR1 (human thiamine transporter 1). Recent genetic evidence has linked mutations in hTHTR1 with the manifestation of TRMA (thiamine-responsive megaloblastic anaemia), a condition also associated with diabetes mellitus, sensorineural deafness and retinal disorders. To examine how mutations in hTHTR1 impair thiamine accumulation, we have investigated the targeting and functional properties of several different hTHTR1 mutants in human cell lines derived from epithelia relevant to thiamine absorption or tissues implicated in TRMA pathology. These constructs encompassed two newly identified point mutations (P51L and T158R) and two truncations of hTHTR1 identical with those found in TRMA kindreds (W358X and Delta383fs). Our results reveal a spectrum of mutant phenotypes, underlining that TRMA can result from decreased thiamine transport activity underpinned by changes in hTHTR1 expression levels, cellular targeting and/or protein transport activity.

Published

2007

47. Thiamine deficiency caused by thiamine antagonists triggers upregulation of apoptosis inducing factor gene expression and leads to caspase 3-mediated apoptosis in neuronally differentiated rat PC-12 cells.

Author

Chornyy S, Parkhomenko J, and Chorna N

Subjects

Active Transport, Cell Nucleus drug effects, Amprolium pharmacology, Animals, Annexin A5 metabolism, Apoptosis drug effects, Cell Differentiation drug effects, Cell Membrane drug effects, Cell Membrane metabolism, Nerve Growth Factor pharmacology, Neurons cytology, Neurons drug effects, Oxythiamine pharmacology, PC12 Cells, Protein Binding drug effects, Pyrithiamine pharmacology, Rats, Thiamine Deficiency pathology, Up-Regulation, Apoptosis physiology, Apoptosis Inducing Factor genetics, Caspase 3 metabolism, Neurons metabolism, Thiamine antagonists & inhibitors, Thiamine Deficiency genetics, Thiamine Deficiency metabolism

Abstract

Recent evidence suggests that alterations in oxidative metabolism induced by thiamine deficiency lead to neuronal cell death. However, the molecular mechanisms underlying this process are still under extensive investigation. Here, we report that rat pheochromocytoma PC-12 cells differentiated in the presence of NGF into neurons undergo apoptosis due to thiamine deficiency caused by antagonists of thiamine - amprolium, pyrithiamine and oxythiamine. Confocal laser scanning fluorescence microscopy revealed that annexin V binds to PC-12 cells in presence of thiamine antagonists after 72 h incubation. Results also show that thiamine antagonists trigger upregulation of gene expression of mitochondrial-derived apoptosis inducing factor, DNA fragmentation, cleavage of caspase 3 and translocation of active product to the nucleus. We therefore propose that apoptosis induced by amprolium, pyrithiamine or oxythiamine occurs via the mitochondria-dependent caspase 3-mediated signaling pathway. In addition, our data indicate that pyrithiamine and oxythiamine are more potent inducers of apoptosis than amprolium.

Published

2007

48. A theoretical argument for inherited thiamine insensitivity as one possible biological cause of familial alcoholism.

Author

Manzardo AM and Penick EC

Subjects

Animals, Cerebellum physiopathology, Dopamine physiology, Humans, Nutritional Physiological Phenomena, Thiamine Deficiency genetics, Alcoholism genetics, Alcoholism physiopathology, Thiamine physiology

Abstract

Thiamine deficiency has been specifically linked to the development of Wernicke-Korsakoff syndrome (WK)--a degenerative brain disorder that is typically associated with alcoholic drinking. Alcoholism-related thiamine deficiency is a major cause of WK. However, an inherited abnormality in thiamine utilization has been identified in some WK patients that may predispose heavy drinkers to this severe neurological syndrome. Individuals who possess this variant require more thiamine throughout their lives to prevent them from experiencing thiamine deficiency. Recent prospective studies have implicated early childhood nutritional and environmental influences in the etiology of alcoholism in adults. These studies have suggested that developmental abnormalities involving brain white matter growth might precipitate the later development of alcoholism possibly by altering the emerging reward-related brain systems. Brain white matter growth is highly sensitive to nutritional deficiency (including thiamine deficiency) and oxidative injury, especially during the perinatal period. The proposed model of familial alcoholism hypothesizes that an inherited insensitivity to thiamine can precipitate brain abnormalities very early in life that will greatly increase the risk of developing alcoholism in adulthood. This paper offers a heuristic model of a possible mechanism by which both inherited and environmental factors related to thiamine utilization might coaggregate to cause alcoholism.

Published

2006

49. Thiamine-responsive megaloblastic anaemia syndrome: long-term follow-up and mutation analysis of seven families.

Author

Ricketts CJ, Minton JA, Samuel J, Ariyawansa I, Wales JK, Lo IF, and Barrett TG

Subjects

Adolescent, Adult, Child, Child, Preschool, DNA Mutational Analysis, Deafness etiology, Diabetes Mellitus drug therapy, Diabetes Mellitus etiology, Female, Follow-Up Studies, Humans, India ethnology, Male, Mutation, Missense, Pedigree, Syndrome, Thiamine therapeutic use, Thiamine Deficiency complications, Anemia, Megaloblastic etiology, Membrane Transport Proteins genetics, Thiamine Deficiency genetics

Abstract

Aim: Thiamine-responsive megaloblastic anaemia syndrome (TRMA) is the association of diabetes mellitus, anaemia and deafness, due to mutations in SLC19A2, encoding a thiamine transporter protein. This is a unique monogenic form of vitamin-dependent diabetes for which there is limited long-term data. We aimed to study genotype-phenotype relationships and long-term follow-up in our cohort., Methods: We have studied 13 patients from seven families and have follow-up data for a median of 9 y (2-30 y)., Results: All patients originated from Kashmir or Punjab, and presented with non-immune, insulin-deficient diabetes mellitus, sensorineural deafness and a variable anaemia in the first 5 y of life, the anaemia progressing to megaloblastic and sideroblastic changes in the bone marrow. The anaemia and diabetes mellitus responded to oral thiamine hydrochloride 25 mg/d, but during puberty thiamine supplements became ineffective, and almost all patients require insulin therapy and regular blood transfusions in adulthood. All patients are homozygous for mutations in the SLC19A2 gene. We have identified a novel missense mutation (T158R) that was excluded in 100 control alleles., Conclusion: Diabetes in this syndrome is due to an insulin insufficiency that initially responds to thiamine supplements; however, most patients become fully insulin dependent after puberty. A mutation screening strategy is feasible and likely to identify mutations in almost all cases.

Published

2006

50. Adaptive regulation of intestinal thiamin uptake: molecular mechanism using wild-type and transgenic mice carrying hTHTR-1 and -2 promoters.

Author

Reidling JC and Said HM

Subjects

Absorption, Adaptation, Physiological, Animals, Humans, Mice, Mice, Transgenic, Promoter Regions, Genetic, Thiamine Deficiency genetics, Up-Regulation, Intestines physiology, Membrane Transport Proteins genetics, Membrane Transport Proteins pharmacology, Thiamine pharmacokinetics, Thiamine Deficiency physiopathology

Abstract

Thiamin participates in metabolic pathways contributing to normal cellular functions, growth, and development. The molecular mechanism of the human intestinal thiamin absorption process involves the thiamin transporters-1 (hTHTR-1) and -2 (hTHTR-2), products of the SLC19A2 and SLC19A3 genes. Little is known about adaptive regulation of the intestinal thiamin uptake process or the molecular mechanism(s) involved during thiamin deficiency. In these studies, we addressed these issues using wild-type mice and transgenic animals carrying the promoters of the hTHTR-1 and -2. We show that, in thiamin deficiency, a significant and specific upregulation in intestinal carrier-mediated thiamin uptake occurs and that this increase is associated with an induction in protein and mRNA levels of mTHTR-2 but not mTHTR-1; in addition, an increase in the activity of the SLC19A3, but not the SLC19A2, promoter was observed in the intestine of transgenic mice. Similar findings were detected in the kidney; however, expression of both thiamin transporters and activity of both human promoters were upregulated in this organ in thiamin deficiency. We also examined the effect of thiamin deficiency on the level of expression of mTHTR-1 and mTHTR-2 messages and activity of the human promoters in the heart and brain of transgenic mice and found an increase in mTHTR-1 mRNA and a rise in activity of the SLC19A2 promoter in thiamin-deficient mice. These results show that the intestinal and renal thiamin uptake processes are adaptively upregulated during dietary thiamin deficiency, that expression of mTHTR-1 and mTHTR-2 is regulated in a tissue-specific manner, and that this upregulation is mediated via transcriptional regulatory mechanism(s).

Published

2005