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POMPE DISEASE IN A BRAZILIAN SERIES: CLINICAL AND MOLECULAR ANALYSES WITH IDENTIFICATION OF NINE NEW MUTATIONS
Oba-Shinjo, Sueli M. et al. | Date Issued: 2009
Author
Oba-Shinjo, Sueli M.
Silva, Roseli da
Andrade, Fernanda G.
Palmer, Rachel E.
Pomponio, Robert J.
Ciociola, Kristina M.
Carvalho, Mary S.
Gutierrez, Paulo S.
Porta, Gilda
Marrone, Carlo D.
Munoz, Verônica
Grzesiuk, Anderson K.
Llerena Junior, Juan Clinton
Berditchevsky, Célia R.
Sobreira, Claudia
Horovitz, Dafne Dain Gandelman
Hatem, Thamine P.
Frota, Elizabeth R. C.
Pecchini, Rogerio
Kouyoumdjian, João Aris
Werneck, Lineu
Amado, Veronica M.
Camelo Jr., José S.
Mattaliano, Robert J.
Marie, Suely K. N.
Affilliation
Universidade de São Paulo. Faculdade de Medicina. Departamento de Nerologia. Grupo de Miopatias e Biologia Molecular. São Paulo, SP, Brasil.
Universidade de São Paulo. Faculdade de Medicina. Departamento de Nerologia. Grupo de Miopatias e Biologia Molecular. São Paulo, SP, Brasil.
Universidade de São Paulo. Faculdade de Medicina. Departamento de Nerologia. Grupo de Miopatias e Biologia Molecular. São Paulo, SP, Brasil.
Genzyme Corporation. Molecular Genetic Analysis Group. Clinical Laboratory Science. Framingham, MA, USA.
Genzyme Corporation. Molecular Genetic Analysis Group. Clinical Laboratory Science. Framingham, MA, USA.
Genzyme Corporation. Molecular Genetic Analysis Group. Clinical Laboratory Science. Framingham, MA, USA.
Universidade de São Paulo. Faculdade de Medicina. Departamento de Neurologia. Grupo de Miopatias e Biologia Molecular. São Paulo, SP, Brasil.
Universidade de São Paulo. Instituto do Coração. São Paulo, SP, Brasil.
Universidade de Sao Paulo. Faculdade de Medicina. Departamento de Padiatria. São Paulo, SP, Brasil.
Clínica Marrone. Divisão de Anatomia Patológica. Porto Alegre, RS, Brasil.
Hospital das Clínicas de Porto Alegre. Porto Alegre, RS, Brasil.
Instituto Neurológico e da Coluna Vertebral. Cuiabá, MT, Brasil.
Fundação Oswaldo Cruz. Instituto Fernandes Figueira. Rio de Janeiro, RJ, Brasil.
Hospital Servidores do Estado do Rio de Janeiro. Rio de Janeiro, RJ, Brasil.
Universidade de São Paulo. Departamento de Nurologia. Psiquiatria e Psicologia Médica. Ribeirão Preto, SP, Brasil.
Universidade de São Paulo. Faculdade de Medicina de Ribeirão Preto. Departamento de Puericultura e Pediatria. Ribeirão Preto, SP, Brasil.
Unidade de Cardiologia e Medicina Fetal. Recife, PE, Brasil.
Universidade Federal de Minas Gerais. Hospital da Clínicas. Belo Horizonte, MG, Brasil.
Santa Casa de Misericórdia. Faculdade de Medicina. São Paulo, SP, Brasil.
Faculdade de Medicina de São José do Rio Preto. Departamento de Ciências Neurológicas. São Paulo, SP, Brasil.
Universidade do Paraná. Hospital das Clínicas do Paraná. Curitiba, PR, Brasil.
Universidade de Brasília. Faculdade de Medicina. Brasília, DF, Brasil.
Universidade de São Paulo. Faculdade de Medicina de Ribeirão Preto. Departamento de Puericultura e Pediatria. Ribeirão Preto, SP, Brasil.
Genzyme Corporation. Framingham, MA, USA.
Universidade de São Paulo. Escola de Medicina. Departamento de Nerologia. Grupo de Miopatias e Biologia Molecular. São Paulo, SP, Brasil.
Abstract
Pompe disease (glycogen storage disease type II or acid maltase deficiency) is an inherited autosomal recessive deficiency of acid alpha-glucosidase (GAA), with predominant manifestations of skeletal muscle weakness. A broad range of studies have been published focusing on Pompe patients from different countries, but none from Brazil. We investigated 41 patients with either infantile-onset (21 cases) or late-onset (20 cases) disease by muscle pathology, enzyme activity and GAA gene mutation screening. Molecular analyses identified 71 mutant alleles from the probands, nine of which are novel (five missense mutations c.136T > G, c.650C > T, c.1456G > C, c.1834C > T, and c.1905C > A, a splice-site mutation c.1195-2A > G, two deletions c.18_25del and c.2185delC, and one nonsense mutation c.643G > T). Interestingly, the c.1905C > A variant was detected in four unrelated patients and may represent a common Brazilian Pompe mutation. The c.2560C > T severe mutation was frequent in our population suggesting a high prevalence in Brazil. Also, eight out of the 21 infantile-onset patients have two truncating mutations predicted to abrogate protein expression. Of the ten late-onset patients who do not carry the common late-onset intronic mutation c.-32-13T > G, five (from three separate families) carry the recently described intronic mutation, c.-32-3C > A, and one sibpair carries the novel missense mutation c.1781G > C in combination with known severe mutation c.1941C > G. The association of these variants (c.1781G > C and c.-32-3C > A) with late-onset disease suggests that they allow for some residual activity in these patients. Our findings help to characterize Pompe disease in Brazil and support the need for additional studies to define the wide clinical and pathological spectrum observed in this disease.
Keywords
Acid a-glucosidase
Pompe Disease
Glycogen Storage Disease Type II
Acid Maltase Deficiency
Mutation Analysis
Novel Mutation
 
DeCS
Glucosidases
Doença de Depósito de Glicogênio Tipo II
Doença de Depósito de Glicogênio Tipo II
Doença de Depósito de Glicogênio Tipo II
Mutação
 
Publisher
Springer International
Citation
OBA-SHINJO, Sueli M. et al. Pompe disease in a Brazilian series: clinical and molecular analyses with identification of nine new mutations. J. Neurol., Berlim, v. 256, p. 1881-1890, 2009.
DOI
10.1007/s00415-009-5219-y