Literature DB >> 15714522

cblE type of homocystinuria due to methionine synthase reductase deficiency: functional correction by minigene expression.

Petra Zavadáková1, Brian Fowler, Terttu Suormala, Zorka Novotna, Peter Mueller, Julia B Hennermann, Jirí Zeman, M Antonia Vilaseca, Laura Vilarinho, Sven Gutsche, Ekkehard Wilichowski, Gerd Horneff, Viktor Kozich.   

Abstract

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. (c) 2005 Wiley-Liss, Inc.

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Year:  2005        PMID: 15714522     DOI: 10.1002/humu.20131

Source DB:  PubMed          Journal:  Hum Mutat        ISSN: 1059-7794            Impact factor:   4.878


  14 in total

1.  cblE-Type Homocystinuria Presenting with Features of Haemolytic-Uremic Syndrome in the Newborn Period.

Authors:  Daniel Palanca; Angels Garcia-Cazorla; Jessica Ortiz; Cristina Jou; Victoria Cusí; Mariona Suñol; Teresa Toll; Belén Perez; Aida Ormazabal; Brian Fowler; Rafael Artuch
Journal:  JIMD Rep       Date:  2012-07-21

2.  A Fast Multiple-Kernel Method With Applications to Detect Gene-Environment Interaction.

Authors:  Rachel Marceau; Wenbin Lu; Shannon Holloway; Michèle M Sale; Bradford B Worrall; Stephen R Williams; Fang-Chi Hsu; Jung-Ying Tzeng
Journal:  Genet Epidemiol       Date:  2015-07-03       Impact factor: 2.135

3.  Clinical onset and course, response to treatment and outcome in 24 patients with the cblE or cblG remethylation defect complemented by genetic and in vitro enzyme study data.

Authors:  M Huemer; C Bürer; P Ješina; V Kožich; M A Landolt; T Suormala; B Fowler; P Augoustides-Savvopoulou; E Blair; K Brennerova; A Broomfield; L De Meirleir; G Gökcay; J Hennermann; P Jardine; J Koch; S Lorenzl; A S Lotz-Havla; J Noss; R Parini; H Peters; B Plecko; F J Ramos; A Schlune; K Tsiakas; M Zerjav Tansek; M R Baumgartner
Journal:  J Inherit Metab Dis       Date:  2014-12-20       Impact factor: 4.982

Review 4.  Genetic disorders of vitamin B₁₂ metabolism: eight complementation groups--eight genes.

Authors:  D Sean Froese; Roy A Gravel
Journal:  Expert Rev Mol Med       Date:  2010-11-29       Impact factor: 5.600

5.  Metabolic derangement of methionine and folate metabolism in mice deficient in methionine synthase reductase.

Authors:  C Lee Elmore; Xuchu Wu; Daniel Leclerc; Erica D Watson; Teodoro Bottiglieri; Natalia I Krupenko; Sergey A Krupenko; James C Cross; Rima Rozen; Roy A Gravel; Rowena G Matthews
Journal:  Mol Genet Metab       Date:  2007-03-21       Impact factor: 4.797

6.  Sulfur Metabolism Under Stress.

Authors:  Colin G Miller; Edward E Schmidt
Journal:  Antioxid Redox Signal       Date:  2020-08-14       Impact factor: 8.401

7.  Outcomes of four patients with homocysteine remethylation disorders detected by newborn screening.

Authors:  Derek Wong; Silvia Tortorelli; Lisa Bishop; Elizabeth A Sellars; Lisa A Schimmenti; Natalie Gallant; Carlos E Prada; Robert J Hopkin; Nancy D Leslie; Susan A Berry; David S Rosenblatt; Amy L Fair; Dietrich Matern; Kimiyo Raymond; Devin Oglesbee; Piero Rinaldo; Dimitar Gavrilov
Journal:  Genet Med       Date:  2015-04-09       Impact factor: 8.822

8.  Association Study between Folate Pathway Gene Single Nucleotide Polymorphisms and Gastric Cancer in Koreans.

Authors:  Jae-Young Yoo; Sook-Young Kim; Jung-Ah Hwang; Seung-Hyun Hong; Aesun Shin; Il Ju Choi; Yeon-Su Lee
Journal:  Genomics Inform       Date:  2012-09-28

9.  The deep intronic c.903+469T>C mutation in the MTRR gene creates an SF2/ASF binding exonic splicing enhancer, which leads to pseudoexon activation and causes the cblE type of homocystinuria.

Authors:  Katerina Homolova; Petra Zavadakova; Thomas Koed Doktor; Lisbeth Dahl Schroeder; Viktor Kozich; Brage S Andresen
Journal:  Hum Mutat       Date:  2010-04       Impact factor: 4.878

Review 10.  Newborn screening for homocystinurias and methylation disorders: systematic review and proposed guidelines.

Authors:  Martina Huemer; Viktor Kožich; Piero Rinaldo; Matthias R Baumgartner; Begoña Merinero; Elisabetta Pasquini; Antonia Ribes; Henk J Blom
Journal:  J Inherit Metab Dis       Date:  2015-03-12       Impact factor: 4.982
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