Clinical, splicing, and functional analysis to classify BRCA2 exon 3 variants: Application of a points-based ACMG/AMP approach

Thomassen, M.; Mesman, R.L.S.; Hansen, T.V.O.; Menendez, M.; Rossing, M.; Esteban-Sánchez, A.; Tudini, E.; Törngren, T.; Parsons, M.T.; Pedersen, I.S.; Teo, S.H.; Kruse, T.A.; Møller, P.; Borg, Å.; Jensen, U.B.; Christensen, L.L.; Singer, C.F.; Muhr, D.; Santamariña Pena, Marta; Brandao, R.; Andresen, B.S.; Feng, B.-J.; Canson, D.; Richardson, M.E.; Karam, R.; Pesaran, T.; LaDuca, H.; Conner, B.R.; Abualkheir, N.; Hoang, L.; Calléja, F.M.G.R.; Andrews, L.; James, P.A.; Bunyan, D.; Hamblett, A.; Radice, P.; Goldgar, D.E.; Walker, L.C.; Engel, C.; Claes, K.B.M.; Machá?ková, E.; Baralle, D.; Viel, A.; Wappenschmidt, B.; Lazaro, C.; Vega Gliemmo, Ana; Vreeswijk, M.P.G.; de la Hoya, M.; Spurdle, A.B.

doi:10.1002/humu.24449

dc.contributor.author	Thomassen, M.
dc.contributor.author	Mesman, R.L.S.
dc.contributor.author	Hansen, T.V.O.
dc.contributor.author	Menendez, M.
dc.contributor.author	Rossing, M.
dc.contributor.author	Esteban-Sánchez, A.
dc.contributor.author	Tudini, E.
dc.contributor.author	Törngren, T.
dc.contributor.author	Parsons, M.T.
dc.contributor.author	Pedersen, I.S.
dc.contributor.author	Teo, S.H.
dc.contributor.author	Kruse, T.A.
dc.contributor.author	Møller, P.
dc.contributor.author	Borg, Å.
dc.contributor.author	Jensen, U.B.
dc.contributor.author	Christensen, L.L.
dc.contributor.author	Singer, C.F.
dc.contributor.author	Muhr, D.
dc.contributor.author	Santamariña Pena, Marta
dc.contributor.author	Brandao, R.
dc.contributor.author	Andresen, B.S.
dc.contributor.author	Feng, B.-J.
dc.contributor.author	Canson, D.
dc.contributor.author	Richardson, M.E.
dc.contributor.author	Karam, R.
dc.contributor.author	Pesaran, T.
dc.contributor.author	LaDuca, H.
dc.contributor.author	Conner, B.R.
dc.contributor.author	Abualkheir, N.
dc.contributor.author	Hoang, L.
dc.contributor.author	Calléja, F.M.G.R.
dc.contributor.author	Andrews, L.
dc.contributor.author	James, P.A.
dc.contributor.author	Bunyan, D.
dc.contributor.author	Hamblett, A.
dc.contributor.author	Radice, P.
dc.contributor.author	Goldgar, D.E.
dc.contributor.author	Walker, L.C.
dc.contributor.author	Engel, C.
dc.contributor.author	Claes, K.B.M.
dc.contributor.author	Machá?ková, E.
dc.contributor.author	Baralle, D.
dc.contributor.author	Viel, A.
dc.contributor.author	Wappenschmidt, B.
dc.contributor.author	Lazaro, C.
dc.contributor.author	Vega Gliemmo, Ana
dc.contributor.author	Vreeswijk, M.P.G.
dc.contributor.author	de la Hoya, M.
dc.contributor.author	Spurdle, A.B.
dc.date.accessioned	2025-08-26T11:23:41Z
dc.date.available	2025-08-26T11:23:41Z
dc.date.issued	2022
dc.identifier.citation	Thomassen M, Mesman RLS, Hansen TVO, Menendez M, Rossing M, Esteban-Sánchez A, et al. Clinical, splicing, and functional analysis to classify BRCA2 exon 3 variants: Application of a points-based ACMG/AMP approach. Human Mutation. 2022;43(12):1921-44.
dc.identifier.issn	1098-1004
dc.identifier.other	https://portalcientifico.sergas.gal/documentos/636708ed688cd71757e145b3	*
dc.identifier.uri	http://hdl.handle.net/20.500.11940/20931
dc.description.abstract	Skipping of BRCA2 exon 3 (?E3) is a naturally occurring splicing event, complicating clinical classification of variants that may alter ?E3 expression. This study used multiple evidence types to assess pathogenicity of 85 variants in/near BRCA2 exon 3. Bioinformatically predicted spliceogenic variants underwent mRNA splicing analysis using minigenes and/or patient samples. ?E3 was measured using quantitative analysis. A mouse embryonic stem cell (mESC) based assay was used to determine the impact of 18 variants on mRNA splicing and protein function. For each variant, population frequency, bioinformatic predictions, clinical data, and existing mRNA splicing and functional results were collated. Variant class was assigned using a gene-specific adaptation of ACMG/AMP guidelines, following a recently proposed points-based system. mRNA and mESC analysis combined identified six variants with transcript and/or functional profiles interpreted as loss of function. Cryptic splice site use for acceptor site variants generated a transcript encoding a shorter protein that retains activity. Overall, 69/85 (81%) variants were classified using the points-based approach. Our analysis shows the value of applying gene-specific ACMG/AMP guidelines using a points-based approach and highlights the consideration of cryptic splice site usage to appropriately assign PVS1 code strength.	en
dc.description.sponsorship	Italian Ministry of Health; Den Norske Kreftforening; Spanish Health Research Foundation, Grant/Award Numbers: INT15/ 00070, INT16/00154, INT17/00133, INT20/ 000; NIHR Research Professorship, Grant/Award Number: RP-2016-07- 011; Ministry of Health of the Czech Republic MH CZ - DRO, Grant/Award Numbers: MMCI, 00209805 and NU20-03-00285; Federal Ministry of Education and Research, Grant/Award Number: 01GY1901; Government of Catalonia, Grant/Award Number: 2017SGR1282 and 2017SGR496; CERCA Program/ Generalitat de Catalunya and the Carlos III National Health Institute, Grant/Award Number: PI19/00553; PI16/00563; SAF2015-68016-R and CIBERO; German Cancer Aid, Grant/Award Number: 110837 and 70114178; Autonomous Government of Galicia, Grant/Award Number: IN607B; Dutch Cancer Society KWF, Grant/Award Number: UL2012-5649 and Pink Ribbon-11704; NHMRC, Grant/Award Numbers: APP177524, APP1104808; Centro de Investigacion Biomedica en Red de Enfermedades Raras CIBERER, Grant/Award Number: ACCI 2016: ER17P1AC7112/2018; Spanish Instituto de Salud Carlos III (ISCIII), Grant/Award Number: PI 20/00110; Fundacion Mutua Madrilena	en
dc.language.iso	eng
dc.rights	Attribution-NonCommercial-NoDerivatives 4.0 International	*
dc.rights.uri	https://creativecommons.org/licenses/by-nc-nd/4.0/
dc.title	Clinical, splicing, and functional analysis to classify BRCA2 exon 3 variants: Application of a points-based ACMG/AMP approach	*
dc.type	Article	en
dc.authorsophos	Thomassen, A. B. M.
dc.authorsophos	Mesman, R. L. S.
dc.authorsophos	Hansen, T. V. O.
dc.authorsophos	Menendez, M.
dc.authorsophos	Rossing, M.
dc.authorsophos	Esteban-Sánchez, A.
dc.authorsophos	Tudini, E.
dc.authorsophos	Törngren, T.
dc.authorsophos	Parsons, M. T.
dc.authorsophos	Pedersen, I. S.
dc.authorsophos	Teo, S. H.
dc.authorsophos	Kruse, T. A.
dc.authorsophos	Møller, P.
dc.authorsophos	Borg, Å
dc.authorsophos	Jensen, U. B.
dc.authorsophos	Christensen, L. L.
dc.authorsophos	Singer, C. F.
dc.authorsophos	Muhr, D.
dc.authorsophos	Santamarina, M.
dc.authorsophos	Brandao, R.
dc.authorsophos	Andresen, B. S.
dc.authorsophos	Feng, B. J.
dc.authorsophos	Canson, D.
dc.authorsophos	Richardson, M. E.
dc.authorsophos	Karam, R.
dc.authorsophos	Pesaran, T.
dc.authorsophos	LaDuca, H.
dc.authorsophos	Conner, B. R.
dc.authorsophos	Abualkheir, N.
dc.authorsophos	Hoang, L.
dc.authorsophos	Calléja, F. M. G. R.
dc.authorsophos	Andrews, L.
dc.authorsophos	James, P. A.
dc.authorsophos	Bunyan, D.
dc.authorsophos	Hamblett, A.
dc.authorsophos	Radice, P.
dc.authorsophos	Goldgar, D. E.
dc.authorsophos	Walker, L. C.
dc.authorsophos	Engel, C.
dc.authorsophos	Claes, K. B. M.
dc.authorsophos	Machá?ková, E.
dc.authorsophos	Baralle, D.
dc.authorsophos	Viel, A.
dc.authorsophos	Wappenschmidt, B.
dc.authorsophos	Lazaro, C.
dc.authorsophos	Vega, A.
dc.authorsophos	Vreeswijk, M. P. G.
dc.authorsophos	de la Hoya, M.
dc.authorsophos	Spurdle
dc.identifier.doi	10.1002/humu.24449
dc.identifier.sophos	636708ed688cd71757e145b3
dc.issue.number	12
dc.journal.title	Human Mutation	*
dc.page.initial	1921
dc.page.final	1944
dc.relation.projectID	Italian Ministry of Health; Den Norske Kreftforening; Spanish Health Research Foundation [INT15/00070, INT16/00154, INT17/00133, INT20/000]; NIHR Research Professorship [RP-2016-07-011]; Ministry of Health of the Czech Republic MH CZ - DRO [00209805, NU20-03-00285]; Federal Ministry of Education and Research [01GY1901]; Government of Catalonia [2017SGR1282, 2017SGR496]; CERCA Program/Generalitat de Catalunya [PI19/00553, PI16/00563, SAF2015-68016-R]; Carlos III National Health Institute [PI19/00553, PI16/00563, SAF2015-68016-R]; CIBERO; German Cancer Aid [110837, 70114178]; Autonomous Government of Galicia [IN607B]; Dutch Cancer Society KWF [UL2012-5649, Pink Ribbon-11704]; NHMRC [APP177524, APP1104808]; Centro de Investigacion Biomedica en Red de Enfermedades Raras CIBERER [ACCI 2016: ER17P1AC7112/2018]; Spanish Instituto de Salud Carlos III (ISCIII) [PI 20/00110]; Fundacion Mutua Madrilena; National Institute for Health Research [RP-2016-07-011] Funding Source: researchfish; Wellcome Trust [203477/Z/16/Z] Funding Source: researchfish
dc.relation.publisherversion	https://onlinelibrary.wiley.com/doi/pdfdirect/10.1002/humu.24449;https://onlinelibrary.wiley.com/doi/pdfdirect/10.1002/humu.24449?download=true	es
dc.rights.accessRights	openAccess
dc.subject.keyword	FPGMX	es
dc.subject.keyword	IDIS	es
dc.typefides	Artículo Científico (incluye Original, Original breve, Revisión Sistemática y Meta-análisis)	es
dc.typesophos	Artículo Original	es
dc.volume.number	43

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Clinical, splicing, and functional analysis to classify BRCA2 exon 3 variants: Application of a points-based ACMG/AMP approach

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