Juvenile Pompe Disease: Retrospective Clinical Study

Detalhes bibliográficos
Autor(a) principal: Loureiro Neves, Filipa
Data de Publicação: 2013
Outros Autores: Garcia, Paula Cristina, Madureira, Núria, Araújo, Henriqueta, Rodrigues, Fidjy, Estêvão, Maria Helena, Lacerda, Lúcia, Diogo Matos, Luísa Maria
Tipo de documento: Artigo
Idioma: por
Título da fonte: Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos)
Texto Completo: https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180
Resumo: Introduction: Pompe disease or glycogen storage disease type II is an autosomal recessive disorder due to acid maltase deficiency. It is a rare disease with a prevalence of 1/40.000 in the dutch and african-american populations and 1/46000 in the australian population. There are three forms of clinical presentation (infantile-onset, childhood-onset and adult-onset), although the disease presents as a continuum of clinical phenotypes. Enzyme replacement therapy is available in Portugal since 2006.Materials and Methods: The clinical files of four patients (two sisters) were analyzed retrospectively.Results: In all, disease presented in the second year of life and the time to diagnosis ranged from two to eleven years. At diagnosis, all presented myopathic features with a delay in motor skills achievement and two had myocardium hypertrophy. Clinical suspicion arose as the result of respiratory failure during infection in two patients. Plasma creatine kinase and aminotransferases levels were increased in all. All patients progressed to pulmonary restrictive syndrome with chronic respiratory failure. The diagnosis was based on reduced activity of acid maltase in fibroblasts: 0 to 1.5% of the lower normal value. Muscle biopsy, performed in three patients, showedlysosomal glycogen accumulation. A c.1064T > C mutation in exon 6 of GAA (glucosidase-alpha-acid) gene was found in all patients, in homozygosity in one. In the sisters, it was associated to c.1666A > G and c.2065G > A mutations in exons 12 and 15, respectively and in the youngest patient, to c.380G > T mutation in exon 2. All patients started enzyme replacement therapy as soon as it became available, with good tolerance. The youngest patient died. The surviving patients maintain ventilatory support measures and physiotherapy. The oldest patient is wheelchair ridden and her sister keeps independent walking. The youngest uses a walking aid.Conclusions: Our cases are clinically included in the juvenile form of Pompe Disease. Pompe disease should be suspected in progressive myopathies at any age, especially those involving limb-girdle and respiratory muscles and in small infants with cardiomyopathy. High creatine kinase is a sensitive, although nonspecific, marker. Given the great variability of the genetic findings, demonstration of reduced activity of acid maltase (in leukocytes or other tissues) remains the diagnosis cornerstone of this rare disorder.
id RCAP_2ffa20a1560bfbae226dfa4b8ecd12a3
oai_identifier_str oai:ojs.www.actamedicaportuguesa.com:article/180
network_acronym_str RCAP
network_name_str Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos)
repository_id_str 7160
spelling Juvenile Pompe Disease: Retrospective Clinical StudyDoença de Pompe Juvenil: Estudo Retrospetivo de Casuística ClínicaIntroduction: Pompe disease or glycogen storage disease type II is an autosomal recessive disorder due to acid maltase deficiency. It is a rare disease with a prevalence of 1/40.000 in the dutch and african-american populations and 1/46000 in the australian population. There are three forms of clinical presentation (infantile-onset, childhood-onset and adult-onset), although the disease presents as a continuum of clinical phenotypes. Enzyme replacement therapy is available in Portugal since 2006.Materials and Methods: The clinical files of four patients (two sisters) were analyzed retrospectively.Results: In all, disease presented in the second year of life and the time to diagnosis ranged from two to eleven years. At diagnosis, all presented myopathic features with a delay in motor skills achievement and two had myocardium hypertrophy. Clinical suspicion arose as the result of respiratory failure during infection in two patients. Plasma creatine kinase and aminotransferases levels were increased in all. All patients progressed to pulmonary restrictive syndrome with chronic respiratory failure. The diagnosis was based on reduced activity of acid maltase in fibroblasts: 0 to 1.5% of the lower normal value. Muscle biopsy, performed in three patients, showedlysosomal glycogen accumulation. A c.1064T > C mutation in exon 6 of GAA (glucosidase-alpha-acid) gene was found in all patients, in homozygosity in one. In the sisters, it was associated to c.1666A > G and c.2065G > A mutations in exons 12 and 15, respectively and in the youngest patient, to c.380G > T mutation in exon 2. All patients started enzyme replacement therapy as soon as it became available, with good tolerance. The youngest patient died. The surviving patients maintain ventilatory support measures and physiotherapy. The oldest patient is wheelchair ridden and her sister keeps independent walking. The youngest uses a walking aid.Conclusions: Our cases are clinically included in the juvenile form of Pompe Disease. Pompe disease should be suspected in progressive myopathies at any age, especially those involving limb-girdle and respiratory muscles and in small infants with cardiomyopathy. High creatine kinase is a sensitive, although nonspecific, marker. Given the great variability of the genetic findings, demonstration of reduced activity of acid maltase (in leukocytes or other tissues) remains the diagnosis cornerstone of this rare disorder.Introdução: A doença de Pompe ou glicogenose tipo II é uma doença autossómica recessiva por deficiência de maltase ácida. É uma entidade rara, com prevalência de 1/40.000 nas populações holandesa e afro-americana e 1/46000 na população australiana. Embora se distingam três formas de apresentação (infantil, juvenil e do adulto), observa-se um amplo espectro clínico. Em Portugal está disponível terapêutica enzimática de substituição desde 2006.Material e Métodos: Fez-se o estudo retrospetivo de quatro doentes (duas das quais irmãs), baseado na revisão dos processos clínicos.Resultados: Em todas, a doença manifestou-se no segundo ano de vida. O tempo até ao diagnóstico variou entre dois e onze anos. Aquando do diagnóstico, todas apresentavam miopatia com atraso de aquisições motoras e em duas havia hipertrofia miocárdica. A suspeita clínica surgiu por insuficiência respiratória em contexto infeccioso em duas doentes. Em todas havia elevação da creatina quinase e das aminotransferases. Todas evoluíram com insuficiência respiratória crónica por síndrome restritiva. O diagnóstico foi baseado na diminuição da atividade da maltase ácida em fibroblastos (0 a 1,5% do limite inferior do normal). Na biópsia muscular, realizada em três doentes, demonstrou-se acumulação lisossómica de glicogénio. Todas apresentavam a mutação c.1064T > C no exão 6 do gene GAA (glucosidase-alpha-acid), em homozigotia numa delas, associada às mutações c.1666A > G no exão 12 e c.2065G > A no exão 15 nas duas irmãs e à mutação c.380G > T no exão 2 na doente mais nova. Todas iniciaram terapia enzimática de substituiçãologo que disponível, com boa tolerância. A doente mais jovem faleceu pouco depois. As outras mantêm medidas de suporteventilatório e fisioterapia, deslocando-se a mais velha, em cadeira de rodas, mantendo a irmã marcha independente e necessitando a mais nova de andarilho.Conclusão: Os nossos casos incluem-se clinicamente na forma juvenil da doença de Pompe. A hipótese de doença de Pompe deve ser considerada em lactentes com miocardiopatia e nas miopatias progressivas, especialmente as das cinturas e dos músculos respiratórios em qualquer idade. A elevação da creatina quinase é um dado sensível, embora inespecífico. Dada a grande variabilidade dos achados genéticos, a demonstração da redução da atividade da maltase ácida continua a ser o pilar do diagnóstico.Ordem dos Médicos2013-08-30info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/articleapplication/pdfimage/tiffimage/tiffimage/tiffimage/tiffimage/tiffimage/tiffhttps://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180oai:ojs.www.actamedicaportuguesa.com:article/180Acta Médica Portuguesa; Vol. 26 No. 4 (2013): July-August; 361-370Acta Médica Portuguesa; Vol. 26 N.º 4 (2013): Julho-Agosto; 361-3701646-07580870-399Xreponame:Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos)instname:Agência para a Sociedade do Conhecimento (UMIC) - FCT - Sociedade da Informaçãoinstacron:RCAAPporhttps://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/3709https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6789https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6790https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6791https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6792https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6793https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6794Loureiro Neves, FilipaGarcia, Paula CristinaMadureira, NúriaAraújo, HenriquetaRodrigues, FidjyEstêvão, Maria HelenaLacerda, LúciaDiogo Matos, Luísa Mariainfo:eu-repo/semantics/openAccess2022-12-20T10:55:51Zoai:ojs.www.actamedicaportuguesa.com:article/180Portal AgregadorONGhttps://www.rcaap.pt/oai/openaireopendoar:71602024-03-19T16:16:23.100270Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos) - Agência para a Sociedade do Conhecimento (UMIC) - FCT - Sociedade da Informaçãofalse
dc.title.none.fl_str_mv Juvenile Pompe Disease: Retrospective Clinical Study
Doença de Pompe Juvenil: Estudo Retrospetivo de Casuística Clínica
title Juvenile Pompe Disease: Retrospective Clinical Study
spellingShingle Juvenile Pompe Disease: Retrospective Clinical Study
Loureiro Neves, Filipa
title_short Juvenile Pompe Disease: Retrospective Clinical Study
title_full Juvenile Pompe Disease: Retrospective Clinical Study
title_fullStr Juvenile Pompe Disease: Retrospective Clinical Study
title_full_unstemmed Juvenile Pompe Disease: Retrospective Clinical Study
title_sort Juvenile Pompe Disease: Retrospective Clinical Study
author Loureiro Neves, Filipa
author_facet Loureiro Neves, Filipa
Garcia, Paula Cristina
Madureira, Núria
Araújo, Henriqueta
Rodrigues, Fidjy
Estêvão, Maria Helena
Lacerda, Lúcia
Diogo Matos, Luísa Maria
author_role author
author2 Garcia, Paula Cristina
Madureira, Núria
Araújo, Henriqueta
Rodrigues, Fidjy
Estêvão, Maria Helena
Lacerda, Lúcia
Diogo Matos, Luísa Maria
author2_role author
author
author
author
author
author
author
dc.contributor.author.fl_str_mv Loureiro Neves, Filipa
Garcia, Paula Cristina
Madureira, Núria
Araújo, Henriqueta
Rodrigues, Fidjy
Estêvão, Maria Helena
Lacerda, Lúcia
Diogo Matos, Luísa Maria
description Introduction: Pompe disease or glycogen storage disease type II is an autosomal recessive disorder due to acid maltase deficiency. It is a rare disease with a prevalence of 1/40.000 in the dutch and african-american populations and 1/46000 in the australian population. There are three forms of clinical presentation (infantile-onset, childhood-onset and adult-onset), although the disease presents as a continuum of clinical phenotypes. Enzyme replacement therapy is available in Portugal since 2006.Materials and Methods: The clinical files of four patients (two sisters) were analyzed retrospectively.Results: In all, disease presented in the second year of life and the time to diagnosis ranged from two to eleven years. At diagnosis, all presented myopathic features with a delay in motor skills achievement and two had myocardium hypertrophy. Clinical suspicion arose as the result of respiratory failure during infection in two patients. Plasma creatine kinase and aminotransferases levels were increased in all. All patients progressed to pulmonary restrictive syndrome with chronic respiratory failure. The diagnosis was based on reduced activity of acid maltase in fibroblasts: 0 to 1.5% of the lower normal value. Muscle biopsy, performed in three patients, showedlysosomal glycogen accumulation. A c.1064T > C mutation in exon 6 of GAA (glucosidase-alpha-acid) gene was found in all patients, in homozygosity in one. In the sisters, it was associated to c.1666A > G and c.2065G > A mutations in exons 12 and 15, respectively and in the youngest patient, to c.380G > T mutation in exon 2. All patients started enzyme replacement therapy as soon as it became available, with good tolerance. The youngest patient died. The surviving patients maintain ventilatory support measures and physiotherapy. The oldest patient is wheelchair ridden and her sister keeps independent walking. The youngest uses a walking aid.Conclusions: Our cases are clinically included in the juvenile form of Pompe Disease. Pompe disease should be suspected in progressive myopathies at any age, especially those involving limb-girdle and respiratory muscles and in small infants with cardiomyopathy. High creatine kinase is a sensitive, although nonspecific, marker. Given the great variability of the genetic findings, demonstration of reduced activity of acid maltase (in leukocytes or other tissues) remains the diagnosis cornerstone of this rare disorder.
publishDate 2013
dc.date.none.fl_str_mv 2013-08-30
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/article
format article
status_str publishedVersion
dc.identifier.uri.fl_str_mv https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180
oai:ojs.www.actamedicaportuguesa.com:article/180
url https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180
identifier_str_mv oai:ojs.www.actamedicaportuguesa.com:article/180
dc.language.iso.fl_str_mv por
language por
dc.relation.none.fl_str_mv https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180
https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/3709
https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6789
https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6790
https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6791
https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6792
https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6793
https://www.actamedicaportuguesa.com/revista/index.php/amp/article/view/180/6794
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
image/tiff
image/tiff
image/tiff
image/tiff
image/tiff
image/tiff
dc.publisher.none.fl_str_mv Ordem dos Médicos
publisher.none.fl_str_mv Ordem dos Médicos
dc.source.none.fl_str_mv Acta Médica Portuguesa; Vol. 26 No. 4 (2013): July-August; 361-370
Acta Médica Portuguesa; Vol. 26 N.º 4 (2013): Julho-Agosto; 361-370
1646-0758
0870-399X
reponame:Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos)
instname:Agência para a Sociedade do Conhecimento (UMIC) - FCT - Sociedade da Informação
instacron:RCAAP
instname_str Agência para a Sociedade do Conhecimento (UMIC) - FCT - Sociedade da Informação
instacron_str RCAAP
institution RCAAP
reponame_str Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos)
collection Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos)
repository.name.fl_str_mv Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos) - Agência para a Sociedade do Conhecimento (UMIC) - FCT - Sociedade da Informação
repository.mail.fl_str_mv
_version_ 1799130617782206464

Registros relacionados