Clinical and molecular findings in a cohort of ANO5‐related myopathy

OBJECTIVE: ANO5‐related myopathy is an important cause of limb‐girdle muscular dystrophy (LGMD) and hyperCKemia. The main descriptions have emerged from European cohorts, and the burden of the disease worldwide is unclear. We provide a detailed characterization of a large Brazilian cohort of ANO5 pa...

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Autores principales: Silva, André M. S., Coimbra-Neto, Antônio R., Souza, Paulo Victor S., Winckler, Pablo B., Gonçalves, Marcus V. M., Cavalcanti, Eduardo B. U., Carvalho, Alzira A. D. S., Sobreira, Cláudia F. D. R., Camelo, Clara G., Mendonça, Rodrigo D. H., Estephan, Eduardo D. P., Reed, Umbertina C., Machado-Costa, Marcela C., Dourado-Junior, Mario E. T., Pereira, Vanessa C., Cruzeiro, Marcelo M., Helito, Paulo V. P., Aivazoglou, Laís U., Camargo, Leonardo V. D., Gomes, Hudson H., Camargo, Amaro J. S. D., Pinto, Wladimir B. V. D. R., Badia, Bruno M. L., Libardi, Luiz H., Yanagiura, Mario T., Oliveira, Acary S. B., Nucci, Anamarli, Saute, Jonas A. M., França-Junior, Marcondes C., Zanoteli, Edmar
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6649425/
https://www.ncbi.nlm.nih.gov/pubmed/31353849
http://dx.doi.org/10.1002/acn3.50801
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author Silva, André M. S.
Coimbra-Neto, Antônio R.
Souza, Paulo Victor S.
Winckler, Pablo B.
Gonçalves, Marcus V. M.
Cavalcanti, Eduardo B. U.
Carvalho, Alzira A. D. S.
Sobreira, Cláudia F. D. R.
Camelo, Clara G.
Mendonça, Rodrigo D. H.
Estephan, Eduardo D. P.
Reed, Umbertina C.
Machado-Costa, Marcela C.
Dourado-Junior, Mario E. T.
Pereira, Vanessa C.
Cruzeiro, Marcelo M.
Helito, Paulo V. P.
Aivazoglou, Laís U.
Camargo, Leonardo V. D.
Gomes, Hudson H.
Camargo, Amaro J. S. D.
Pinto, Wladimir B. V. D. R.
Badia, Bruno M. L.
Libardi, Luiz H.
Yanagiura, Mario T.
Oliveira, Acary S. B.
Nucci, Anamarli
Saute, Jonas A. M.
França-Junior, Marcondes C.
Zanoteli, Edmar
author_facet Silva, André M. S.
Coimbra-Neto, Antônio R.
Souza, Paulo Victor S.
Winckler, Pablo B.
Gonçalves, Marcus V. M.
Cavalcanti, Eduardo B. U.
Carvalho, Alzira A. D. S.
Sobreira, Cláudia F. D. R.
Camelo, Clara G.
Mendonça, Rodrigo D. H.
Estephan, Eduardo D. P.
Reed, Umbertina C.
Machado-Costa, Marcela C.
Dourado-Junior, Mario E. T.
Pereira, Vanessa C.
Cruzeiro, Marcelo M.
Helito, Paulo V. P.
Aivazoglou, Laís U.
Camargo, Leonardo V. D.
Gomes, Hudson H.
Camargo, Amaro J. S. D.
Pinto, Wladimir B. V. D. R.
Badia, Bruno M. L.
Libardi, Luiz H.
Yanagiura, Mario T.
Oliveira, Acary S. B.
Nucci, Anamarli
Saute, Jonas A. M.
França-Junior, Marcondes C.
Zanoteli, Edmar
author_sort Silva, André M. S.
collection PubMed
description OBJECTIVE: ANO5‐related myopathy is an important cause of limb‐girdle muscular dystrophy (LGMD) and hyperCKemia. The main descriptions have emerged from European cohorts, and the burden of the disease worldwide is unclear. We provide a detailed characterization of a large Brazilian cohort of ANO5 patients. METHODS: A national cross‐sectional study was conducted to describe clinical, histopathological, radiological, and molecular features of patients carrying recessive variants in ANO5. Correlation of clinical and genetic characteristics with different phenotypes was studied. RESULTS: Thirty‐seven patients from 34 nonrelated families with recessive mutations of ANO5 were identified. The most common phenotype was LGMD, observed in 25 (67.5%) patients, followed by pseudometabolic presentation in 7 (18.9%) patients, isolated asymptomatic hyperCKemia in 4 (10.8%) patients, and distal myopathy in a single patient. Nine patients presented axial involvement, including one patient with isolated axial weakness. The most affected muscles according to MRI were the semimembranosus and gastrocnemius, but paraspinal and abdominal muscles, when studied, were involved in most patients. Fourteen variants in ANO5 were identified, and the c.191dupA was present in 19 (56%) families. Sex, years of disease, and the presence of loss‐of‐function variants were not associated with specific phenotypes. INTERPRETATION: We present the largest series of anoctaminopathy outside Europe. The most common European founder mutation c.191dupA was very frequent in our population. Gender, disease duration, and genotype did not determine the phenotype.
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spelling pubmed-66494252019-07-31 Clinical and molecular findings in a cohort of ANO5‐related myopathy Silva, André M. S. Coimbra-Neto, Antônio R. Souza, Paulo Victor S. Winckler, Pablo B. Gonçalves, Marcus V. M. Cavalcanti, Eduardo B. U. Carvalho, Alzira A. D. S. Sobreira, Cláudia F. D. R. Camelo, Clara G. Mendonça, Rodrigo D. H. Estephan, Eduardo D. P. Reed, Umbertina C. Machado-Costa, Marcela C. Dourado-Junior, Mario E. T. Pereira, Vanessa C. Cruzeiro, Marcelo M. Helito, Paulo V. P. Aivazoglou, Laís U. Camargo, Leonardo V. D. Gomes, Hudson H. Camargo, Amaro J. S. D. Pinto, Wladimir B. V. D. R. Badia, Bruno M. L. Libardi, Luiz H. Yanagiura, Mario T. Oliveira, Acary S. B. Nucci, Anamarli Saute, Jonas A. M. França-Junior, Marcondes C. Zanoteli, Edmar Ann Clin Transl Neurol Research Articles OBJECTIVE: ANO5‐related myopathy is an important cause of limb‐girdle muscular dystrophy (LGMD) and hyperCKemia. The main descriptions have emerged from European cohorts, and the burden of the disease worldwide is unclear. We provide a detailed characterization of a large Brazilian cohort of ANO5 patients. METHODS: A national cross‐sectional study was conducted to describe clinical, histopathological, radiological, and molecular features of patients carrying recessive variants in ANO5. Correlation of clinical and genetic characteristics with different phenotypes was studied. RESULTS: Thirty‐seven patients from 34 nonrelated families with recessive mutations of ANO5 were identified. The most common phenotype was LGMD, observed in 25 (67.5%) patients, followed by pseudometabolic presentation in 7 (18.9%) patients, isolated asymptomatic hyperCKemia in 4 (10.8%) patients, and distal myopathy in a single patient. Nine patients presented axial involvement, including one patient with isolated axial weakness. The most affected muscles according to MRI were the semimembranosus and gastrocnemius, but paraspinal and abdominal muscles, when studied, were involved in most patients. Fourteen variants in ANO5 were identified, and the c.191dupA was present in 19 (56%) families. Sex, years of disease, and the presence of loss‐of‐function variants were not associated with specific phenotypes. INTERPRETATION: We present the largest series of anoctaminopathy outside Europe. The most common European founder mutation c.191dupA was very frequent in our population. Gender, disease duration, and genotype did not determine the phenotype. John Wiley and Sons Inc. 2019-06-11 /pmc/articles/PMC6649425/ /pubmed/31353849 http://dx.doi.org/10.1002/acn3.50801 Text en © 2019 The Authors. Annals of Clinical and Translational Neurology published by Wiley Periodicals, Inc on behalf of American Neurological Association. This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc-nd/4.0/ License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Research Articles
Silva, André M. S.
Coimbra-Neto, Antônio R.
Souza, Paulo Victor S.
Winckler, Pablo B.
Gonçalves, Marcus V. M.
Cavalcanti, Eduardo B. U.
Carvalho, Alzira A. D. S.
Sobreira, Cláudia F. D. R.
Camelo, Clara G.
Mendonça, Rodrigo D. H.
Estephan, Eduardo D. P.
Reed, Umbertina C.
Machado-Costa, Marcela C.
Dourado-Junior, Mario E. T.
Pereira, Vanessa C.
Cruzeiro, Marcelo M.
Helito, Paulo V. P.
Aivazoglou, Laís U.
Camargo, Leonardo V. D.
Gomes, Hudson H.
Camargo, Amaro J. S. D.
Pinto, Wladimir B. V. D. R.
Badia, Bruno M. L.
Libardi, Luiz H.
Yanagiura, Mario T.
Oliveira, Acary S. B.
Nucci, Anamarli
Saute, Jonas A. M.
França-Junior, Marcondes C.
Zanoteli, Edmar
Clinical and molecular findings in a cohort of ANO5‐related myopathy
title Clinical and molecular findings in a cohort of ANO5‐related myopathy
title_full Clinical and molecular findings in a cohort of ANO5‐related myopathy
title_fullStr Clinical and molecular findings in a cohort of ANO5‐related myopathy
title_full_unstemmed Clinical and molecular findings in a cohort of ANO5‐related myopathy
title_short Clinical and molecular findings in a cohort of ANO5‐related myopathy
title_sort clinical and molecular findings in a cohort of ano5‐related myopathy
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6649425/
https://www.ncbi.nlm.nih.gov/pubmed/31353849
http://dx.doi.org/10.1002/acn3.50801
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