Comprehensive reanalysis for CNVs in ES data from unsolved rare disease cases results in new diagnoses

Solve-RD Consortium

doi:10.1038/s41525-024-00436-6

Comprehensive reanalysis for CNVs in ES data from unsolved rare disease cases results in new diagnoses

Solve-RD Consortium

Research output: Contribution to a Journal (Peer & Non Peer) › Article › peer-review

4 Citations (Scopus)

Abstract

We report the results of a comprehensive copy number variant (CNV) reanalysis of 9171 exome sequencing datasets from 5757 families affected by a rare disease (RD). The data reanalysed was extremely heterogeneous, having been generated using 28 different enrichment kits by 42 different research groups across Europe partnering in the Solve-RD project. Each research group had previously undertaken their own analysis of the data but failed to identify disease-causing variants. We applied three CNV calling algorithms to maximise sensitivity, and rare CNVs overlapping genes of interest, provided by four partner European Reference Networks, were taken forward for interpretation by clinical experts. This reanalysis has resulted in a molecular diagnosis being provided to 51 families in this sample, with ClinCNV performing the best of the three algorithms. We also identified partially explanatory pathogenic CNVs in a further 34 individuals. This work illustrates the value of reanalysing ES cold cases for CNVs.

Original language	English
Article number	49
Journal	npj Genomic Medicine
Volume	9
Issue number	1
DOIs	https://doi.org/10.1038/s41525-024-00436-6
Publication status	Published - Dec 2024
Externally published	Yes

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10.1038/s41525-024-00436-6

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@article{53c1c5624bc840468854d3cab1faf66d,

title = "Comprehensive reanalysis for CNVs in ES data from unsolved rare disease cases results in new diagnoses",

abstract = "We report the results of a comprehensive copy number variant (CNV) reanalysis of 9171 exome sequencing datasets from 5757 families affected by a rare disease (RD). The data reanalysed was extremely heterogeneous, having been generated using 28 different enrichment kits by 42 different research groups across Europe partnering in the Solve-RD project. Each research group had previously undertaken their own analysis of the data but failed to identify disease-causing variants. We applied three CNV calling algorithms to maximise sensitivity, and rare CNVs overlapping genes of interest, provided by four partner European Reference Networks, were taken forward for interpretation by clinical experts. This reanalysis has resulted in a molecular diagnosis being provided to 51 families in this sample, with ClinCNV performing the best of the three algorithms. We also identified partially explanatory pathogenic CNVs in a further 34 individuals. This work illustrates the value of reanalysing ES cold cases for CNVs.",

author = "\{Solve-RD Consortium\} and German Demidov and Burcu Yaldiz and Jos{\'e} Garcia-Pelaez and \{de Boer\}, Elke and Nika Schuermans and \{Van de Vondel\}, Liedewei and Ida Paramonov and Johansson, \{Lennart F.\} and Francesco Musacchia and Elisa Benetti and Gemma Bullich and Karolis Sablauskas and Sergi Beltran and Christian Gilissen and Alexander Hoischen and Stephan Ossowski and \{de Voer\}, Richarda and Katja Lohmann and Carla Oliveira and Ana Topf and Vissers, \{Lisenka E.L.M.\} and Kristina Zguro and Federico Zara and Ioannis Zaganas and Y{\'e}pez, \{Vicente A.\} and Brunhilde Wirth and David Webb and Hannah Verdin and \{Van Nieuwenhove\}, Erika and \{van Montfrans\}, Joris and \{van Heurck\}, Roxane and \{van der Veken\}, Lars and Laura Valle and Paolo Uva and Bjarne Udd and Aurelien Trimouille and Rachel Thompson and Marco Tartaglia and Yves Sznajer and Pasquale Striano and Verena Steinke-Lange and Martha Spilioti and Paolo Scudieri and Evelin Schr{\"o}ck and Katherine Schon and Marcello Scala and Marco Savarese and Santen, \{Gijs W.E.\} and Andreas Rump and Ruivenkamp, \{Claudia A.L.\} and Andreas Roos and Caroline Rooryck and Antonella Riva and Alessandra Renieri and Thiloka Ratnaike and Radio, \{Francesca Clementina\} and Flavia Privitera and \{De la Paz\}, \{Manuel Posada\} and Bruce Poppe and Kiran Polavarapu and Konrad Platzer and Borut Peterlin and Bel{\'e}n P{\'e}rez-Due{\~n}as and Martje Pauly and Elena Parrini and Catarina Olimpio and Reghan, \{Mary O.\} and \{de Benito\}, \{Daniel Natera\} and Osorio, \{Andr{\'e}s Nascimento\} and Francina Munell and Alexander M{\"u}nchau and St{\'e}phanie Moortgat and Olivier Monestier and Molnar, \{Maria Judit\} and Colombine Meunier and Christian Mertes and Davide Mei and Isabelle Maystadt and Patrick May and Ales Maver and Lambros Mathioudakis and Fr{\'e}d{\'e}ric Masclaux and Sandrine Mary and Delgado, \{Beatriz Mart{\'i}nez\} and Anna Marc{\'e}-Grau and Sivasankar Malaichamy and Alfons Macaya and Rebeka Lukn{\'a}rov{\'a} and Mart{\'i}n, \{Estrella L{\'o}pez\} and Hanns Lochm{\"u}ller and Elsa Leit{\~a}o and Damien Lederer and Helen Leavis and Andreas Laner and Didier Lacombe and Leon Krass and Christian Korff and Evgenia Kokosali and Mert Karakaya and Nicholas Allen",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2024.",

year = "2024",

month = dec,

doi = "10.1038/s41525-024-00436-6",

language = "English",

volume = "9",

journal = "npj Genomic Medicine",

issn = "2056-7944",

publisher = "Nature Research",

number = "1",

}

TY - JOUR

T1 - Comprehensive reanalysis for CNVs in ES data from unsolved rare disease cases results in new diagnoses

AU - Solve-RD Consortium

AU - Demidov, German

AU - Yaldiz, Burcu

AU - Garcia-Pelaez, José

AU - de Boer, Elke

AU - Schuermans, Nika

AU - Van de Vondel, Liedewei

AU - Paramonov, Ida

AU - Johansson, Lennart F.

AU - Musacchia, Francesco

AU - Benetti, Elisa

AU - Bullich, Gemma

AU - Sablauskas, Karolis

AU - Beltran, Sergi

AU - Gilissen, Christian

AU - Hoischen, Alexander

AU - Ossowski, Stephan

AU - de Voer, Richarda

AU - Lohmann, Katja

AU - Oliveira, Carla

AU - Topf, Ana

AU - Vissers, Lisenka E.L.M.

AU - Zguro, Kristina

AU - Zara, Federico

AU - Zaganas, Ioannis

AU - Yépez, Vicente A.

AU - Wirth, Brunhilde

AU - Webb, David

AU - Verdin, Hannah

AU - Van Nieuwenhove, Erika

AU - van Montfrans, Joris

AU - van Heurck, Roxane

AU - van der Veken, Lars

AU - Valle, Laura

AU - Uva, Paolo

AU - Udd, Bjarne

AU - Trimouille, Aurelien

AU - Thompson, Rachel

AU - Tartaglia, Marco

AU - Sznajer, Yves

AU - Striano, Pasquale

AU - Steinke-Lange, Verena

AU - Spilioti, Martha

AU - Scudieri, Paolo

AU - Schröck, Evelin

AU - Schon, Katherine

AU - Scala, Marcello

AU - Savarese, Marco

AU - Santen, Gijs W.E.

AU - Rump, Andreas

AU - Ruivenkamp, Claudia A.L.

AU - Roos, Andreas

AU - Rooryck, Caroline

AU - Riva, Antonella

AU - Renieri, Alessandra

AU - Ratnaike, Thiloka

AU - Radio, Francesca Clementina

AU - Privitera, Flavia

AU - De la Paz, Manuel Posada

AU - Poppe, Bruce

AU - Polavarapu, Kiran

AU - Platzer, Konrad

AU - Peterlin, Borut

AU - Pérez-Dueñas, Belén

AU - Pauly, Martje

AU - Parrini, Elena

AU - Olimpio, Catarina

AU - Reghan, Mary O.

AU - de Benito, Daniel Natera

AU - Osorio, Andrés Nascimento

AU - Munell, Francina

AU - Münchau, Alexander

AU - Moortgat, Stéphanie

AU - Monestier, Olivier

AU - Molnar, Maria Judit

AU - Meunier, Colombine

AU - Mertes, Christian

AU - Mei, Davide

AU - Maystadt, Isabelle

AU - May, Patrick

AU - Maver, Ales

AU - Mathioudakis, Lambros

AU - Masclaux, Frédéric

AU - Mary, Sandrine

AU - Delgado, Beatriz Martínez

AU - Marcé-Grau, Anna

AU - Malaichamy, Sivasankar

AU - Macaya, Alfons

AU - Luknárová, Rebeka

AU - Martín, Estrella López

AU - Lochmüller, Hanns

AU - Leitão, Elsa

AU - Lederer, Damien

AU - Leavis, Helen

AU - Laner, Andreas

AU - Lacombe, Didier

AU - Krass, Leon

AU - Korff, Christian

AU - Kokosali, Evgenia

AU - Karakaya, Mert

AU - Allen, Nicholas

PY - 2024/12

Y1 - 2024/12

N2 - We report the results of a comprehensive copy number variant (CNV) reanalysis of 9171 exome sequencing datasets from 5757 families affected by a rare disease (RD). The data reanalysed was extremely heterogeneous, having been generated using 28 different enrichment kits by 42 different research groups across Europe partnering in the Solve-RD project. Each research group had previously undertaken their own analysis of the data but failed to identify disease-causing variants. We applied three CNV calling algorithms to maximise sensitivity, and rare CNVs overlapping genes of interest, provided by four partner European Reference Networks, were taken forward for interpretation by clinical experts. This reanalysis has resulted in a molecular diagnosis being provided to 51 families in this sample, with ClinCNV performing the best of the three algorithms. We also identified partially explanatory pathogenic CNVs in a further 34 individuals. This work illustrates the value of reanalysing ES cold cases for CNVs.

AB - We report the results of a comprehensive copy number variant (CNV) reanalysis of 9171 exome sequencing datasets from 5757 families affected by a rare disease (RD). The data reanalysed was extremely heterogeneous, having been generated using 28 different enrichment kits by 42 different research groups across Europe partnering in the Solve-RD project. Each research group had previously undertaken their own analysis of the data but failed to identify disease-causing variants. We applied three CNV calling algorithms to maximise sensitivity, and rare CNVs overlapping genes of interest, provided by four partner European Reference Networks, were taken forward for interpretation by clinical experts. This reanalysis has resulted in a molecular diagnosis being provided to 51 families in this sample, with ClinCNV performing the best of the three algorithms. We also identified partially explanatory pathogenic CNVs in a further 34 individuals. This work illustrates the value of reanalysing ES cold cases for CNVs.

UR - https://www.scopus.com/pages/publications/85207830154

U2 - 10.1038/s41525-024-00436-6

DO - 10.1038/s41525-024-00436-6

M3 - Article

AN - SCOPUS:85207830154

SN - 2056-7944

VL - 9

JO - npj Genomic Medicine

JF - npj Genomic Medicine

IS - 1

M1 - 49

ER -

Comprehensive reanalysis for CNVs in ES data from unsolved rare disease cases results in new diagnoses

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