cblE type of homocystinuria due to methionine synthase reductase deficiency: functional correction by minigene expression
Jazyk angličtina Země Spojené státy americké Médium print
Typ dokumentu časopisecké články, práce podpořená grantem
PubMed
15714522
DOI
10.1002/humu.20131
Knihovny.cz E-zdroje
- MeSH
- 5-methyltetrahydrofoláthomocystein-S-methyltransferasa nedostatek MeSH
- běloši genetika MeSH
- betain terapeutické užití MeSH
- bodová mutace MeSH
- ferredoxin-NADP-reduktasa nedostatek genetika MeSH
- fibroblasty enzymologie patologie MeSH
- genetická terapie * MeSH
- haplotypy genetika MeSH
- homocystein krev MeSH
- homocystinurie krev klasifikace farmakoterapie enzymologie genetika patologie terapie MeSH
- hydroxokobalamin terapeutické užití MeSH
- kyselina listová terapeutické užití MeSH
- lidé MeSH
- missense mutace MeSH
- mozek patologie MeSH
- mutační analýza DNA MeSH
- nesmyslný kodon MeSH
- polymerázová řetězová reakce MeSH
- polymorfismus délky restrikčních fragmentů MeSH
- polymorfismus genetický MeSH
- rekombinantní fúzní proteiny fyziologie MeSH
- sekvenční delece MeSH
- substituce aminokyselin MeSH
- syntetické geny MeSH
- testy genetické komplementace MeSH
- transfekce MeSH
- transformované buněčné linie enzymologie patologie MeSH
- Check Tag
- lidé MeSH
- Publikační typ
- časopisecké články MeSH
- práce podpořená grantem MeSH
- Názvy látek
- 5-methyltetrahydrofoláthomocystein-S-methyltransferasa MeSH
- betain MeSH
- ferredoxin-NADP-reduktasa MeSH
- homocystein MeSH
- hydroxokobalamin MeSH
- kyselina listová MeSH
- methionine synthase reductase MeSH Prohlížeč
- nesmyslný kodon MeSH
- rekombinantní fúzní proteiny MeSH
The cblE type of homocystinuria is a rare autosomal recessive disorder caused by impaired reductive activation of methionine synthase. Although earlier biochemical studies proposed that the methionine synthase enzyme might be activated by two different reducing systems, mutations were reported in only the methionine synthase reductase gene (MTRR) in cblE patients. The pathogenicity of MTRR mutations, however, has not yet been tested functionally. We report on nine patients of European origin affected by the cblE type of homocystinuria. They presented between 2 weeks and 3 years of age (median age 4 weeks) with anemia, which was macrocytic in only three patients, and with neurological involvement in all but two cases. Bone marrow examination performed in seven patients showed megaloblastic changes in all but one of them. All patients exhibited moderate to severe hyperhomocysteinemia (median plasma total homocysteine [Hcy] 92 mumol/L, range 44-169), while clearly reduced methionine was observed only in four cases. Pathogenic mutations were identified in both parental alleles of the MTRR gene in all patients. Five known (c.903+469T>C, c.1361C>T, c.1459G>A, c.1557-4_1557+3del7, and c.1622_1623dupTA) and three novel mutations (c.7A>T, c.1573C>T, and c.1953-6_1953-2del5) were detected. Importantly, transfection of fibroblasts of cblE patients with a wild-type MTRR minigene expression construct resulted in a significant approximately four-fold increase of methionine synthesis, indicating correction of the enzyme defect. Our study shows a link between a milder predominantly hematological presentation and homozygosity for the c.1361C>T mutation, but no other obvious genotype-phenotype correlation. The identification of mutations in the MTRR gene, together with restoration of methionine synthesis following MTRR minigene expression in cblE cells confirms that this disease is caused by defects in the MTRR gene.
Hum Mutat. 2005 Dec;26(6):590 PubMed
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