Investigação clínica e genética da ataxia por deficiência de vitamina E (AVED), uma forma tratável de doença neuromuscular

Oliveira, Caroline Flores de

doi:10.11606/D.41.2020.tde-11052020-152844

Home

Facilities

Master's Dissertation

DOI

https://doi.org/10.11606/D.41.2020.tde-11052020-152844

Document

Master's Dissertation

Author

Oliveira, Caroline Flores de (Catálogo USP)

Full name

Caroline Flores de Oliveira

E-mail

Institute/School/College

Instituto de Biociências

Knowledge Area

Genetic Counseling and Human Genomics

Date of Defense

2020-02-04

Published

São Paulo, 2019

Supervisor

Kok, Fernando (Catálogo USP)

Committee

Kok, Fernando (President)
Bueno, Clarissa
Kim, Chong Ae

Title in Portuguese

Investigação clínica e genética da ataxia por deficiência de vitamina E (AVED), uma forma tratável de doença neuromuscular

Keywords in Portuguese

Ataxia
Ataxia autossômica recessiva
Ataxia com deficiênciad e vitamina E
Genética
Vitamina E

Abstract in Portuguese

A Ataxia por Deficiencia de Vitamina E (AVED) e uma doenca neurodegenerativa e progressiva caracterizada principalmente por ataxia espinocerebelar progressiva, arreflexia, disartria, propriocepcao prejudicada e acentuada deficiencia de vitamina E no plasma. Possui alta semelhanca clinica com a forma mais comum de ataxia autossomica recessiva, a ataxia de Friedreich (AF), na qual e muitas vezes confundida. A AVED desenvolve-se em decorrencia de mutacao no gene que codifica a proteina de transferencia de alfa-tocoferol (TTPA) e possui padrão de heranca autossomica recessiva. O tratamento consiste em suplementacao com altas doses diarias de vitamina E. O presente estudo teve como objetivo avaliar, do ponto de vista clinico e genetico, uma serie de 9 pacientes diagnosticados com AVED em acompanhamento no Ambulatorio de Neurogenetica do Hospital das Clinicas de Sao Paulo (HC-FMUSP) e comparar os dados obtidos com a literatura mundial, assim como oferecer Aconselhamento Genetico aos pacientes e suas familias. A coleta de dados foi realizada no Ambulatorio de Neurogenetica do HC-FMUSP. Para a avaliacao funcional, foi utilizada a escala Scale for the Assessment and Rating of Ataxia (SARA). O material genético dos participantes foi sequenciado por sequenciamento de nova geração (NGS) e analisado por programas de bioinformatica. Ao todo, 5 mutações foram identificadas, sendo a p.Thr172Leufs*5 a mais frequente, seguida da p.Glu249Asnfs*15, ambas relatadas na literatura como sendo responsáveis por uma forma grave da doenca. Tambem foi identificada a mutacao missense p.Ala120Thr e duas variantes nunca antes descritas na literatura: p.Ala58Pro e p.Arg134Pro. Este estudo demonstrou que, em concordancia com a literatura, a suplementacao com vitamina E em pacientes com AVED cessou a progressao da doenca nos pacientes investigados. De modo geral, mutacoes que causem a perda de funcao do gene estao associadas a inicio precoce dos sintomas e progressao rapida, enquanto que variantes missense tendem a causar um quadro mais leve da doenca. Esta relacao, entretanto, tem exceções. A investigação molecular do gene TTPA dos pacientes com diagnostico clinico e bioquimico de AVED deve ser preconizado, uma vez que auxilia no Aconselhamento Genético e prognóstico da doença

Title in English

Clinical and genetic investigation of ataxia with vitamin E deficiency (AVED), a treatable form of neuro-muscular disease

Keywords in English

Ataxia
Ataxia with Vitamin E deficiency
Genetics
Recessive autossomal ataxia
Vitamin E

Abstract in English

Ataxia with vitamin E deficiency (AVED) is a progressive and neurodegenerative disease mainly characterized by progressive spinocerebellar ataxia, areflexia, dysarthria, impaired proprioception and marked reduced plasma levels of vitamin E. Clinically, it resembles the most common form of recessive autosomal ataxia, Friedreich ataxia (FA). AVED develops as a result of mutation in the gene encoding alpha-tocopherol transfer protein (TTPA) and is inherited in an autosomal recessive inheritance pattern. The treatment consists of supplementation with high doses of vitamin E. The present study aimed to evaluate, from the clinical and genetic point of view, 9 patients diagnosed with AVED under follow-up at the Neurogenetics Out-Patient Service of Hospital das Clinicas de Sao Paulo (HC-FMUSP) and compare the data obtained with the world literature, as well as offer genetic counseling to patients and their families. Data collection was performed at the Neurogenetics Ambulatory of HC-FMUSP. For a functional assessment, the Scale for the Assessment and Rating of Ataxia (SARA) was performed. Participants' genetic material was sequenced by next generation sequencing (NGS) and analyzed by bioinformatics softwares. At all, 5 mutations were identified. The p.Thr172Leufs*5 mutation was the most frequent, followed by p.Glu249Asnfs*15, both reported in the literature associated as a severe form of the disease. It was also identified the missense mutation p.Ala120Thr and two variants never reported in the literature before: p.Ala58Pro and p.Arg134Pro. This study showed that, in accordance with the literature, vitamin E supplementation in patients with AVED ceased disease progression in the investigated patients. In general, mutations that cause loss of gene function are associated with early onset of symptoms and rapid progression, while missense variants tend to cause a milder picture of the disease. This relationship, however, has exceptions. Molecular investigation of the TTPA gene of patients with clinical and biochemical diagnosis of AVED should be recommended, as it helps in genetic counseling and disease prognosis

WARNING - Viewing this document is conditioned on your acceptance of the following terms of use:
This document is only for private use for research and teaching activities. Reproduction for commercial use is forbidden. This rights cover the whole data about this document as well as its contents. Any uses or copies of this document in whole or in part must include the author's name.

CarolineFloresOliveira.pdf (6.97 Mbytes)

Publishing Date

2020-12-08

Derived works

WARNING: Learn what derived works are clicking here.