MLPA followed by target-NGS to detect mutations in the dystrophin gene of Peruvian patients suspected of DMD/DMB

María Luisa Guevara-Fujita; Francia Huaman-Dianderas; Daisy Obispo; Rodrigo Sánchez; Victor Barrenechea; Diana Rojas-Málaga; Alejandro Estrada-Cuzcano; Milana Trubnykova; Mario Cornejo-Olivas; Victoria Marca; Bertha Gallardo; Milagros Dueñas-Roque; Ana Protzel; Carlos Castañeda; Hugo Abarca; Luis Celis; Jorge La Serna-Infantes; Ricardo Fujita

doi:10.1002/mgg3.1759

MLPA followed by target-NGS to detect mutations in the dystrophin gene of Peruvian patients suspected of DMD/DMB

María Luisa Guevara-Fujita
, Francia Huaman-Dianderas
, Daisy Obispo
, Rodrigo Sánchez
, Victor Barrenechea
, Diana Rojas-Málaga
, Alejandro Estrada-Cuzcano
, Milana Trubnykova
, Mario Cornejo-Olivas
, Victoria Marca
, Bertha Gallardo
, Milagros Dueñas-Roque
, Ana Protzel
, Carlos Castañeda
, Hugo Abarca
, Luis Celis
, Jorge La Serna-Infantes
, Ricardo Fujita

Producción científica: Contribución a una revista › Artículo › revisión exhaustiva

6 Citas (Scopus)

Resumen

Background: We report the molecular analysis of the DMD gene in a group of Peruvian patients with Duchenne/Becker dystrophinopathy. This is the first study to thoroughly characterize mutations in this population. Methods: We used the combination of multiplex ligation-dependent probe amplification (MLPA) and sequencing analysis of the DMD gene. We recruited Peruvian patients in 2 years from reference national hospitals. We performed DNA tests in 152 patients, checking first exon deletion/duplication by MLPA, and subsequently, if negative, samples were sequenced to detect point mutations. Results: The average age for diagnosis was 9.8 years, suggesting a delay for timely diagnosis and care. We found causal DMD mutations in 125 patients: 72 (57.6%) exon deletions/duplications (41.6% deletions, 16.0% duplications), and 53 (42.4%) point mutations (27.2% nonsense, 9.6% small indels, and 5.6% splice site). Conclusion: Due to our genetic background, we expected a higher number of novel and recurrent causal mutations in our sample. Results showed 16% of novel mutations, similar to other well-studied populations.

Idioma original	Inglés
Número de artículo	e1759
Publicación	Molecular Genetics and Genomic Medicine
Volumen	9
N.º	9
DOI	https://doi.org/10.1002/mgg3.1759
Estado	Publicada - set. 2021
Publicado de forma externa	Sí

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Guevara-Fujita, M. L., Huaman-Dianderas, F., Obispo, D., Sánchez, R., Barrenechea, V., Rojas-Málaga, D., Estrada-Cuzcano, A., Trubnykova, M., Cornejo-Olivas, M., Marca, V., Gallardo, B., Dueñas-Roque, M., Protzel, A., Castañeda, C., Abarca, H., Celis, L., La Serna-Infantes, J., & Fujita, R. (2021). MLPA followed by target-NGS to detect mutations in the dystrophin gene of Peruvian patients suspected of DMD/DMB. Molecular Genetics and Genomic Medicine, 9(9), Artículo e1759. https://doi.org/10.1002/mgg3.1759

@article{e58e31028c1a4f5cbfd35d7ed25b7b5b,

title = "MLPA followed by target-NGS to detect mutations in the dystrophin gene of Peruvian patients suspected of DMD/DMB",

abstract = "Background: We report the molecular analysis of the DMD gene in a group of Peruvian patients with Duchenne/Becker dystrophinopathy. This is the first study to thoroughly characterize mutations in this population. Methods: We used the combination of multiplex ligation-dependent probe amplification (MLPA) and sequencing analysis of the DMD gene. We recruited Peruvian patients in 2 years from reference national hospitals. We performed DNA tests in 152 patients, checking first exon deletion/duplication by MLPA, and subsequently, if negative, samples were sequenced to detect point mutations. Results: The average age for diagnosis was 9.8 years, suggesting a delay for timely diagnosis and care. We found causal DMD mutations in 125 patients: 72 (57.6\%) exon deletions/duplications (41.6\% deletions, 16.0\% duplications), and 53 (42.4\%) point mutations (27.2\% nonsense, 9.6\% small indels, and 5.6\% splice site). Conclusion: Due to our genetic background, we expected a higher number of novel and recurrent causal mutations in our sample. Results showed 16\% of novel mutations, similar to other well-studied populations.",

keywords = "Becker muscular dystrophy, Duchenne muscular dystrophy, molecular diagnosis, multiple ligation probe amplification, targeted Next Generation Sequencing",

author = "Guevara-Fujita, \{Mar{\'i}a Luisa\} and Francia Huaman-Dianderas and Daisy Obispo and Rodrigo S{\'a}nchez and Victor Barrenechea and Diana Rojas-M{\'a}laga and Alejandro Estrada-Cuzcano and Milana Trubnykova and Mario Cornejo-Olivas and Victoria Marca and Bertha Gallardo and Milagros Due{\~n}as-Roque and Ana Protzel and Carlos Casta{\~n}eda and Hugo Abarca and Luis Celis and \{La Serna-Infantes\}, Jorge and Ricardo Fujita",

note = "Publisher Copyright: {\textcopyright} 2021 The Authors. Molecular Genetics \& Genomic Medicine published by Wiley Periodicals LLC",

year = "2021",

month = sep,

doi = "10.1002/mgg3.1759",

language = "Ingl{\'e}s",

volume = "9",

journal = "Molecular Genetics and Genomic Medicine",

issn = "2324-9269",

publisher = "John Wiley and Sons Inc.",

number = "9",

}

Guevara-Fujita, ML, Huaman-Dianderas, F, Obispo, D, Sánchez, R, Barrenechea, V, Rojas-Málaga, D, Estrada-Cuzcano, A, Trubnykova, M, Cornejo-Olivas, M, Marca, V, Gallardo, B, Dueñas-Roque, M, Protzel, A, Castañeda, C, Abarca, H, Celis, L, La Serna-Infantes, J & Fujita, R 2021, 'MLPA followed by target-NGS to detect mutations in the dystrophin gene of Peruvian patients suspected of DMD/DMB', Molecular Genetics and Genomic Medicine, vol. 9, n.º 9, e1759. https://doi.org/10.1002/mgg3.1759

TY - JOUR

T1 - MLPA followed by target-NGS to detect mutations in the dystrophin gene of Peruvian patients suspected of DMD/DMB

AU - Guevara-Fujita, María Luisa

AU - Huaman-Dianderas, Francia

AU - Obispo, Daisy

AU - Sánchez, Rodrigo

AU - Barrenechea, Victor

AU - Rojas-Málaga, Diana

AU - Estrada-Cuzcano, Alejandro

AU - Trubnykova, Milana

AU - Cornejo-Olivas, Mario

AU - Marca, Victoria

AU - Gallardo, Bertha

AU - Dueñas-Roque, Milagros

AU - Protzel, Ana

AU - Castañeda, Carlos

AU - Abarca, Hugo

AU - Celis, Luis

AU - La Serna-Infantes, Jorge

AU - Fujita, Ricardo

PY - 2021/9

Y1 - 2021/9

N2 - Background: We report the molecular analysis of the DMD gene in a group of Peruvian patients with Duchenne/Becker dystrophinopathy. This is the first study to thoroughly characterize mutations in this population. Methods: We used the combination of multiplex ligation-dependent probe amplification (MLPA) and sequencing analysis of the DMD gene. We recruited Peruvian patients in 2 years from reference national hospitals. We performed DNA tests in 152 patients, checking first exon deletion/duplication by MLPA, and subsequently, if negative, samples were sequenced to detect point mutations. Results: The average age for diagnosis was 9.8 years, suggesting a delay for timely diagnosis and care. We found causal DMD mutations in 125 patients: 72 (57.6%) exon deletions/duplications (41.6% deletions, 16.0% duplications), and 53 (42.4%) point mutations (27.2% nonsense, 9.6% small indels, and 5.6% splice site). Conclusion: Due to our genetic background, we expected a higher number of novel and recurrent causal mutations in our sample. Results showed 16% of novel mutations, similar to other well-studied populations.

AB - Background: We report the molecular analysis of the DMD gene in a group of Peruvian patients with Duchenne/Becker dystrophinopathy. This is the first study to thoroughly characterize mutations in this population. Methods: We used the combination of multiplex ligation-dependent probe amplification (MLPA) and sequencing analysis of the DMD gene. We recruited Peruvian patients in 2 years from reference national hospitals. We performed DNA tests in 152 patients, checking first exon deletion/duplication by MLPA, and subsequently, if negative, samples were sequenced to detect point mutations. Results: The average age for diagnosis was 9.8 years, suggesting a delay for timely diagnosis and care. We found causal DMD mutations in 125 patients: 72 (57.6%) exon deletions/duplications (41.6% deletions, 16.0% duplications), and 53 (42.4%) point mutations (27.2% nonsense, 9.6% small indels, and 5.6% splice site). Conclusion: Due to our genetic background, we expected a higher number of novel and recurrent causal mutations in our sample. Results showed 16% of novel mutations, similar to other well-studied populations.

KW - Becker muscular dystrophy

KW - Duchenne muscular dystrophy

KW - molecular diagnosis

KW - multiple ligation probe amplification

KW - targeted Next Generation Sequencing

UR - https://www.scopus.com/pages/publications/85111526488

U2 - 10.1002/mgg3.1759

DO - 10.1002/mgg3.1759

M3 - Artículo

C2 - 34327855

AN - SCOPUS:85111526488

SN - 2324-9269

VL - 9

JO - Molecular Genetics and Genomic Medicine

JF - Molecular Genetics and Genomic Medicine

IS - 9

M1 - e1759

ER -

MLPA followed by target-NGS to detect mutations in the dystrophin gene of Peruvian patients suspected of DMD/DMB

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