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Detalhes Referência

Tipo
Artigos em Revista

Tipo de Documento
Artigo Completo

Título
Molecular and Clinical Investigations on Portuguese Patients with Multiple acyl-CoA Dehydrogenase Deficiency

Participantes na publicação
Bárbara J. Henriques (Author)
Dep. Química e Bioquímica
BioISI
Tânia G. Lucas (Author)
Esmeralda Martins (Author)
Ana Gaspar (Author)
Anabela Bandeira (Author)
Célia Nogueira (Author)
Otilia Brandão (Author)
Hugo Rocha (Author)
Laura Vilarinho (Author)
Cláudio M. Gomes (Author)
Dep. Química e Bioquímica
BioISI

Resumo
BACKGROUND:\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\nMultiple Acyl-CoA Dehydrogenase Deficiency (MADD) is a congenital rare metabolic disease with broad clinical phenotypes and variable evolution. This inborn error of metabolism is caused by mutations in the ETFA, ETFB or ETFDH genes, which encode for the mitochondrial ETF and ETF:QO proteins. A considerable group of patients has been described to respond positively to riboflavin oral supplementation, which constitutes the prototypic treatment for the pathology.\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\n\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\nOBJECTIVES:\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\nTo report mutations in ETFA, ETFB and ETFDH genes identified in Portuguese patients, correlating, whenever possible, biochemical and clinical outcomes with the effects of mutations on the structure and stability of the affected proteins, to better understand MADD pathogenesis at the molecular level.\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\n\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\nMETHODS:\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\nMADD patients were identified based on the characteristic urinary profile of organic acids and/or acylcarnitine profiles in blood spots during newborn screening. Genotypic, clinical and biochemical data were collected for all patients. In silico structural analysis was employed using bioinformatic tools carried out in an ETF:QO molecular model for the identified missense mutations.\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\n\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\nRESULTS:\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\nA survey describing clinical and biochemical features of eight Portuguese MADD patients was made. Genotype analysis identified five ETFDH mutations, including one extension (p.X618QextX*14), two splice mutations (c.34+5G>C and c.405+3A>T) and two missense mutations (ETF:QO-p.Arg155Gly and ETF:QO-p.Pro534Leu), and one ETFB mutation (ETFβ- p.Arg191Cys). Homozygous patients containing the ETFDH mutations p.X618QextX*14, c.34+5G>C and ETF:QO-p.Arg155Gly, all presented severe (lethal) MADD phenotypes. However, when any of these mutations are in heterozygosity with the known ETF:QO-p.Pro534Leu mild variant, the severe clinical effects are partly and temporarily attenuated. Indeed, the latter destabilizes an ETF-interacting loop, with no major functional consequences. However, the position 155 in ETF:QO is localized at the ubiquinone binding and membrane interacting domain, and is thus expected to perturb protein structure and membrane insertion, with severe functional effects. Structural analysis of molecular models is therefore demonstrated to be a valuable tool to rationalize the effects of mutations in the context of the clinical phenotype severity.\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\n\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\nCONCLUSION:\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\\nAdvanced molecular diagnosis, structural analysis and clinical correlations reveal that MADD patients harboring a severe prognosis mutation in one allele can actually revert to a milder phenotype by complementation with a milder mutation in the other allele. However, such patients are nevertheless in a precarious metabolic balance which can revert to severe fatal outcomes during catabolic stress or secondary pathology, thus requiring strict clinical follow-up.

Data de Publicação
2019-08-02

Instituição
Biosystems & Integrative Sciences Institute, Faculdade de Ciências, Universidade de Lisboa, Portugal.

Suporte
Current Molecular Medicine

Identificadores da Publicação
ISSN - 1566-5240

Editora
Bentham Science Publishers Ltd.

Volume
19
Fascículo
7

Número de Páginas
6
Página Inicial
487
Página Final
493

Identificadores do Documento
DOI - https://doi.org/10.2174/1566524019666190507114748
URL - http://dx.doi.org/10.2174/1566524019666190507114748

Identificadores de Qualidade
SCIMAGO Q2 (2019) - 0.694 - Biochemistry (Q2)
SCIMAGO Q2 (2019) - 0.694 - Medicine (miscellaneous) (Q2)


Exportar referência

APA
Bárbara J. Henriques, Tânia G. Lucas, Esmeralda Martins, Ana Gaspar, Anabela Bandeira, Célia Nogueira, Otilia Brandão, Hugo Rocha, Laura Vilarinho, Cláudio M. Gomes, (2019). Molecular and Clinical Investigations on Portuguese Patients with Multiple acyl-CoA Dehydrogenase Deficiency. Current Molecular Medicine, 19, 487-493. ISSN 1566-5240. eISSN . http://dx.doi.org/10.2174/1566524019666190507114748

IEEE
Bárbara J. Henriques, Tânia G. Lucas, Esmeralda Martins, Ana Gaspar, Anabela Bandeira, Célia Nogueira, Otilia Brandão, Hugo Rocha, Laura Vilarinho, Cláudio M. Gomes, "Molecular and Clinical Investigations on Portuguese Patients with Multiple acyl-CoA Dehydrogenase Deficiency" in Current Molecular Medicine, vol. 19, pp. 487-493, 2019. 10.2174/1566524019666190507114748

BIBTEX
@article{39374, author = {Bárbara J. Henriques and Tânia G. Lucas and Esmeralda Martins and Ana Gaspar and Anabela Bandeira and Célia Nogueira and Otilia Brandão and Hugo Rocha and Laura Vilarinho and Cláudio M. Gomes}, title = {Molecular and Clinical Investigations on Portuguese Patients with Multiple acyl-CoA Dehydrogenase Deficiency}, journal = {Current Molecular Medicine}, year = 2019, pages = {487-493}, volume = 19 }