Implementación de un panel de genes para el diagnóstico genético de la discinesia ciliar primaria

Noelia Baz-Redón; Sandra Rovira-Amigo; Ida Paramonov; Silvia Castillo-Corullón; Maria Cols Roig; María Antolín; Elena García Arumí; Alba Torrent-Vernetta; Inés de Mir Messa; Silvia Gartner; Ignacio Iglesias Serrano; M. Araceli Caballero-Rabasco; Óscar Asensio de la Cruz; Gerardo Vizmanos-Lamotte; Carlos Martín de Vicente; María del Mar Martínez-Colls; Ana Reula; Amparo Escribano; Francisco Dasí; Miguel Armengot-Carceller; Eva Polverino; Esther Amengual Pieras; Rosanel Amaro-Rodríguez; Marta Garrido-Pontnou; Eduardo Tizzano; Núria Camats-Tarruella; Mónica Fernández-Cancio; Antonio Moreno-Galdó

doi:10.1016/j.arbres.2020.02.010

Implementación de un panel de genes para el diagnóstico genético de la discinesia ciliar primaria

Noelia Baz-Redón, Sandra Rovira-Amigo, Ida Paramonov, Silvia Castillo-Corullón, Maria Cols Roig, María Antolín, Elena García Arumí, Alba Torrent-Vernetta, Inés de Mir Messa, Silvia Gartner, Ignacio Iglesias Serrano, M. Araceli Caballero-Rabasco, Óscar Asensio de la Cruz, Gerardo Vizmanos-Lamotte, Carlos Martín de Vicente, María del Mar Martínez-Colls, Ana Reula, Amparo Escribano, Francisco Dasí, Miguel Armengot-CarcellerEva Polverino, Esther Amengual Pieras, Rosanel Amaro-Rodríguez, Marta Garrido-Pontnou, Eduardo Tizzano, Núria Camats-Tarruella, Mónica Fernández-Cancio, Antonio Moreno-Galdó^*

^*Autor correspondiente de este trabajo

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

8 Citas (Scopus)

Resumen

Introduction: Primary ciliary dyskinesia (PCD) is characterized by an alteration in the ciliary structure causing difficulty in the clearance of respiratory secretions. Diagnosis is complex and based on a combination of techniques. The objective of this study was to design a gene panel including all known causative genes, and to corroborate their diagnostic utility in a cohort of Spanish patients. Methods: This was a multicenter cross-sectional study of patients with a high suspicion of PCD, according to European Respiratory Society criteria, designed around a gene panel for massive sequencing using SeqCap EZ capture technology that included 44 genes associated with PCD. Results: We included 79 patients, 53 of whom had a diagnosis of confirmed or highly probable PCD. The sensitivity of the gene panel was 81.1%, with a specificity of 100%. Candidate variants were found in some of the genes of the panel in 43 patients with PCD, 51.2% (22/43) of whom were homozygotes and 48.8% (21/43) compound heterozygotes. The most common causative genes were DNAH5 and CCDC39. We found 52 different variants, 36 of which were not previously described in the literature. Conclusions: The design and implementation of a tailored gene panel produces a high yield in the genetic diagnosis of PCD. This panel provides a better understanding of the causative factors involved in these patients and lays down the groundwork for future therapeutic approaches.

Título traducido de la contribución	Implementation of a Gene Panel for Genetic Diagnosis of Primary Ciliary Dyskinesia
Idioma original	Español
Publicación	Archivos de Bronconeumologia
DOI	https://doi.org/10.1016/j.arbres.2020.02.010
Estado	Publicada - mar 2021

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Baz-Redón, N., Rovira-Amigo, S., Paramonov, I., Castillo-Corullón, S., Cols Roig, M., Antolín, M., García Arumí, E., Torrent-Vernetta, A., de Mir Messa, I., Gartner, S., Iglesias Serrano, I., Caballero-Rabasco, M. A., Asensio de la Cruz, Ó., Vizmanos-Lamotte, G., Martín de Vicente, C., Martínez-Colls, M. D. M., Reula, A., Escribano, A., Dasí, F., ... Moreno-Galdó, A. (2021). Implementación de un panel de genes para el diagnóstico genético de la discinesia ciliar primaria. Archivos de Bronconeumologia. https://doi.org/10.1016/j.arbres.2020.02.010

@article{24edc5ef12574fb2885a00fab23854ea,

title = "Implementaci{\'o}n de un panel de genes para el diagn{\'o}stico gen{\'e}tico de la discinesia ciliar primaria",

abstract = "Introduction: Primary ciliary dyskinesia (PCD) is characterized by an alteration in the ciliary structure causing difficulty in the clearance of respiratory secretions. Diagnosis is complex and based on a combination of techniques. The objective of this study was to design a gene panel including all known causative genes, and to corroborate their diagnostic utility in a cohort of Spanish patients. Methods: This was a multicenter cross-sectional study of patients with a high suspicion of PCD, according to European Respiratory Society criteria, designed around a gene panel for massive sequencing using SeqCap EZ capture technology that included 44 genes associated with PCD. Results: We included 79 patients, 53 of whom had a diagnosis of confirmed or highly probable PCD. The sensitivity of the gene panel was 81.1%, with a specificity of 100%. Candidate variants were found in some of the genes of the panel in 43 patients with PCD, 51.2% (22/43) of whom were homozygotes and 48.8% (21/43) compound heterozygotes. The most common causative genes were DNAH5 and CCDC39. We found 52 different variants, 36 of which were not previously described in the literature. Conclusions: The design and implementation of a tailored gene panel produces a high yield in the genetic diagnosis of PCD. This panel provides a better understanding of the causative factors involved in these patients and lays down the groundwork for future therapeutic approaches.",

keywords = "Electron microscopy, Gene panel, High-speed optical video microscopy, Massive sequencing, Primary ciliary dyskinesia",

author = "Noelia Baz-Red{\'o}n and Sandra Rovira-Amigo and Ida Paramonov and Silvia Castillo-Corull{\'o}n and {Cols Roig}, Maria and Mar{\'i}a Antol{\'i}n and {Garc{\'i}a Arum{\'i}}, Elena and Alba Torrent-Vernetta and {de Mir Messa}, In{\'e}s and Silvia Gartner and {Iglesias Serrano}, Ignacio and Caballero-Rabasco, {M. Araceli} and {Asensio de la Cruz}, {\'O}scar and Gerardo Vizmanos-Lamotte and {Mart{\'i}n de Vicente}, Carlos and Mart{\'i}nez-Colls, {Mar{\'i}a del Mar} and Ana Reula and Amparo Escribano and Francisco Das{\'i} and Miguel Armengot-Carceller and Eva Polverino and {Amengual Pieras}, Esther and Rosanel Amaro-Rodr{\'i}guez and Marta Garrido-Pontnou and Eduardo Tizzano and N{\'u}ria Camats-Tarruella and M{\'o}nica Fern{\'a}ndez-Cancio and Antonio Moreno-Gald{\'o}",

year = "2021",

month = mar,

doi = "10.1016/j.arbres.2020.02.010",

language = "Espa{\~n}ol",

}

Baz-Redón, N, Rovira-Amigo, S, Paramonov, I, Castillo-Corullón, S, Cols Roig, M, Antolín, M, García Arumí, E, Torrent-Vernetta, A, de Mir Messa, I, Gartner, S, Iglesias Serrano, I, Caballero-Rabasco, MA, Asensio de la Cruz, Ó, Vizmanos-Lamotte, G, Martín de Vicente, C, Martínez-Colls, MDM, Reula, A, Escribano, A, Dasí, F, Armengot-Carceller, M, Polverino, E, Amengual Pieras, E, Amaro-Rodríguez, R, Garrido-Pontnou, M, Tizzano, E, Camats-Tarruella, N, Fernández-Cancio, M & Moreno-Galdó, A 2021, 'Implementación de un panel de genes para el diagnóstico genético de la discinesia ciliar primaria', Archivos de Bronconeumologia. https://doi.org/10.1016/j.arbres.2020.02.010

TY - JOUR

T1 - Implementación de un panel de genes para el diagnóstico genético de la discinesia ciliar primaria

AU - Baz-Redón, Noelia

AU - Rovira-Amigo, Sandra

AU - Paramonov, Ida

AU - Castillo-Corullón, Silvia

AU - Cols Roig, Maria

AU - Antolín, María

AU - García Arumí, Elena

AU - Torrent-Vernetta, Alba

AU - de Mir Messa, Inés

AU - Gartner, Silvia

AU - Iglesias Serrano, Ignacio

AU - Caballero-Rabasco, M. Araceli

AU - Asensio de la Cruz, Óscar

AU - Vizmanos-Lamotte, Gerardo

AU - Martín de Vicente, Carlos

AU - Martínez-Colls, María del Mar

AU - Reula, Ana

AU - Escribano, Amparo

AU - Dasí, Francisco

AU - Armengot-Carceller, Miguel

AU - Polverino, Eva

AU - Amengual Pieras, Esther

AU - Amaro-Rodríguez, Rosanel

AU - Garrido-Pontnou, Marta

AU - Tizzano, Eduardo

AU - Camats-Tarruella, Núria

AU - Fernández-Cancio, Mónica

AU - Moreno-Galdó, Antonio

PY - 2021/3

Y1 - 2021/3

N2 - Introduction: Primary ciliary dyskinesia (PCD) is characterized by an alteration in the ciliary structure causing difficulty in the clearance of respiratory secretions. Diagnosis is complex and based on a combination of techniques. The objective of this study was to design a gene panel including all known causative genes, and to corroborate their diagnostic utility in a cohort of Spanish patients. Methods: This was a multicenter cross-sectional study of patients with a high suspicion of PCD, according to European Respiratory Society criteria, designed around a gene panel for massive sequencing using SeqCap EZ capture technology that included 44 genes associated with PCD. Results: We included 79 patients, 53 of whom had a diagnosis of confirmed or highly probable PCD. The sensitivity of the gene panel was 81.1%, with a specificity of 100%. Candidate variants were found in some of the genes of the panel in 43 patients with PCD, 51.2% (22/43) of whom were homozygotes and 48.8% (21/43) compound heterozygotes. The most common causative genes were DNAH5 and CCDC39. We found 52 different variants, 36 of which were not previously described in the literature. Conclusions: The design and implementation of a tailored gene panel produces a high yield in the genetic diagnosis of PCD. This panel provides a better understanding of the causative factors involved in these patients and lays down the groundwork for future therapeutic approaches.

AB - Introduction: Primary ciliary dyskinesia (PCD) is characterized by an alteration in the ciliary structure causing difficulty in the clearance of respiratory secretions. Diagnosis is complex and based on a combination of techniques. The objective of this study was to design a gene panel including all known causative genes, and to corroborate their diagnostic utility in a cohort of Spanish patients. Methods: This was a multicenter cross-sectional study of patients with a high suspicion of PCD, according to European Respiratory Society criteria, designed around a gene panel for massive sequencing using SeqCap EZ capture technology that included 44 genes associated with PCD. Results: We included 79 patients, 53 of whom had a diagnosis of confirmed or highly probable PCD. The sensitivity of the gene panel was 81.1%, with a specificity of 100%. Candidate variants were found in some of the genes of the panel in 43 patients with PCD, 51.2% (22/43) of whom were homozygotes and 48.8% (21/43) compound heterozygotes. The most common causative genes were DNAH5 and CCDC39. We found 52 different variants, 36 of which were not previously described in the literature. Conclusions: The design and implementation of a tailored gene panel produces a high yield in the genetic diagnosis of PCD. This panel provides a better understanding of the causative factors involved in these patients and lays down the groundwork for future therapeutic approaches.

KW - Electron microscopy

KW - Gene panel

KW - High-speed optical video microscopy

KW - Massive sequencing

KW - Primary ciliary dyskinesia

UR - http://www.scopus.com/inward/record.url?scp=85082848375&partnerID=8YFLogxK

UR - https://www.mendeley.com/catalogue/61ffc85e-a556-3eee-8f3b-c179973dae8d/

U2 - 10.1016/j.arbres.2020.02.010

DO - 10.1016/j.arbres.2020.02.010

M3 - Artículo

C2 - 32253119

AN - SCOPUS:85082848375

SN - 0300-2896

JO - Archivos de Bronconeumologia

JF - Archivos de Bronconeumologia

ER -

Implementación de un panel de genes para el diagnóstico genético de la discinesia ciliar primaria

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