Comprehensive Functional Characterization and Clinical Interpretation of 20 Splice-Site Variants of the RAD51C Gene

Sanoguera-Miralles, Lara; Valenzuela-Palomo, Alberto; Bueno-Martínez, Elena; Llovet, Patricia; Díez-Gómez, Beatriz; Caloca, María J.; Pérez‐Segura, Pedro; Fraile-Bethencourt, Eugenia; Colmena, Marta; Carvalho, Sara; Allen, Jamie; Easton, Douglas F.; Devilee, Peter; Vreeswijk, Maaike P.G.; Hoya, Miguel de la; Velasco, Eladio A.

doi:10.3390/cancers12123771

Cited by 11 publications

(33 citation statements)

References 82 publications

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“…Many studies, including previous work by our group, support the ability of minigene assays to accurately reproduce splicing alterations as observed in RNA from carriers [ 16 , 24 , 25 , 47 , 48 , 49 ]. Unfortunately, as far as we know, none of the RAD51D variants here assessed have been tested previously in RNA from carriers (the only exception being a sub-optimal study performed in a c.738+1G>A carrier, see footnote to Table 1 ).…”

Section: Discussionmentioning

confidence: 83%

“…Forty-seven variants from the intron–exon boundaries (3′ splice-site: intron/exon [IVS-10_IVS-1/2nt]; 5′ splice-site: exon/intron [2nt/IVS+1_IVS+10]) [ 16 ] and 34 from RAD51D exon 3 were collected from the BRIDGES sequencing data [ 5 ]. RNA outcomes and predicted protein products were described according to the Human Genome Variation Society guidelines ( , accessed on 1 April 2021) using Ensembl reference transcript ID ENST00000345365.10 (GenBank NM_002878.3).…”

Section: Methodsmentioning

confidence: 99%

“…To identify potential splicing variants, in silico studies were performed using MaxEntScan (MES, , accessed on 1 April 2021) (cut-off ≥ 3.0) [ 18 ] and NNSplice ( , accessed on 1 April 2021) [ 19 ] when MES was not informative. Potential spliceogenic variants were selected according to the following criteria: (i) MES score changes (>15%) [ 16 , 20 ] and (ii) creation of alternative sites ( Table S2 ).…”

Section: Methodsmentioning

confidence: 99%

“…MCF-7 cell growth, transfection and inhibition of the nonsense-mediated decay were performed as previously described [ 16 ]. The triple-negative breast cancer (TNBC) cell line MDA-MB-231 was cultured in Dulbecco’s Modified Eagle Medium (DMEM) supplemented with 10% fetal bovine serum, 2 mM glutamine, 1% non-essential amino acids and 1% penicillin/streptomycin solution.…”

Section: Methodsmentioning

confidence: 99%

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RAD51D Aberrant Splicing in Breast Cancer: Identification of Splicing Regulatory Elements and Minigene-Based Evaluation of 53 DNA Variants

Bueno-Martínez

Sanoguera-Miralles

Valenzuela-Palomo

et al. 2021

Cancers

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RAD51D loss-of-function variants increase lifetime risk of breast and ovarian cancer. Splicing disruption is a frequent pathogenic mechanism associated with variants in susceptibility genes. Herein, we have assessed the splicing and clinical impact of splice-site and exonic splicing enhancer (ESE) variants identified through the study of ~113,000 women of the BRIDGES cohort. A RAD51D minigene with exons 2–9 was constructed in splicing vector pSAD. Eleven BRIDGES splice-site variants (selected by MaxEntScan) were introduced into the minigene by site-directed mutagenesis and tested in MCF-7 cells. The 11 variants disrupted splicing, collectively generating 25 different aberrant transcripts. All variants but one produced negligible levels (<3.4%) of the full-length (FL) transcript. In addition, ESE elements of the alternative exon 3 were mapped by testing four overlapping exonic microdeletions (≥30-bp), revealing an ESE-rich interval (c.202_235del) with critical sequences for exon 3 recognition that might have been affected by germline variants. Next, 26 BRIDGES variants and 16 artificial exon 3 single-nucleotide substitutions were also assayed. Thirty variants impaired splicing with variable amounts (0–65.1%) of the FL transcript, although only c.202G > A demonstrated a complete aberrant splicing pattern without the FL transcript. On the other hand, c.214T > C increased efficiency of exon 3 recognition, so only the FL transcript was detected (100%). In conclusion, 41 RAD51D spliceogenic variants (28 of which were from the BRIDGES cohort) were identified by minigene assays. We show that minigene-based mapping of ESEs is a powerful approach for identifying ESE hotspots and ESE-disrupting variants. Finally, we have classified nine variants as likely pathogenic according to ACMG/AMP-based guidelines, highlighting the complex relationship between splicing alterations and variant interpretation.

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Section: Discussionmentioning

confidence: 83%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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RAD51D Aberrant Splicing in Breast Cancer: Identification of Splicing Regulatory Elements and Minigene-Based Evaluation of 53 DNA Variants

Bueno-Martínez

Sanoguera-Miralles

Valenzuela-Palomo

et al. 2021

Cancers

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“…The importance of the RAD51 paralogs was further underlined by genetic studies showing an increased risk of developing breast and/or ovarian cancer in women bearing RAD51C, RAD51D or XRCC2 mutations [115][116][117]. This association was confirmed in breast and/or ovarian cancer families and cohorts with no known BRCA1 or BRCA2 mutations, leading to the proposition to include RAD51D and RAD51C to the list of genes screened for breast cancer predisposition [118][119][120].…”

Section: Rad51 Loading and Stability At Dsb Site By Protein-protein Interactionsmentioning

confidence: 99%

Regulation of RAD51 at the Transcriptional and Functional Levels: What Prospects for Cancer Therapy?

Orhan

Velázquez

Tabet

et al. 2021

Cancers

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The RAD51 recombinase is a critical effector of Homologous Recombination (HR), which is an essential DNA repair mechanism for double-strand breaks. The RAD51 protein is recruited onto the DNA break by BRCA2 and forms homopolymeric filaments that invade the homologous chromatid and use it as a template for repair. RAD51 filaments are detectable by immunofluorescence as distinct foci in the cell nucleus, and their presence is a read out of HR proficiency. RAD51 is an essential gene, protecting cells from genetic instability. Its expression is low and tightly regulated in normal cells and, contrastingly, elevated in a large fraction of cancers, where its level of expression and activity have been linked with sensitivity to genotoxic treatment. In particular, BRCA-deficient tumors show reduced or obliterated RAD51 foci formation and increased sensitivity to platinum salt or PARP inhibitors. However, resistance to treatment sets in rapidly and is frequently based on a complete or partial restoration of RAD51 foci formation. Consequently, RAD51 could be a highly valuable therapeutic target. Here, we review the multiple levels of regulation that impact the transcription of the RAD51 gene, as well as the post-translational modifications that determine its expression level, recruitment on DNA damage sites and the efficient formation of homofilaments. Some of these regulation levels may be targeted and their impact on cancer cell survival discussed.

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Splicing predictions, minigene analyses, and ACMG‐AMP clinical classification of 42 germline PALB2 splice‐site variants

Valenzuela-Palomo

Bueno-Martínez

Sanoguera-Miralles

et al. 2021

The Journal of Pathology

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PALB2 loss-of-function variants confer high risk of developing breast cancer. Here we present a systematic functional analysis of PALB2 splice-site variants detected in approximately 113,000 women in the large-scale sequencing project Breast Cancer After Diagnostic Gene Sequencing (BRIDGES; https://bridges-research.eu/). Eighty-two PALB2 variants at the intron-exon boundaries were analyzed with MaxEntScan. Forty-two variants were selected for the subsequent splicing functional assays. For this purpose, three splicing reporter minigenes comprising exons 1-12 were constructed. The 42 potential spliceogenic variants were introduced into the minigenes by sitedirected mutagenesis and assayed in MCF-7/MDA-MB-231 cells. Splicing anomalies were observed in 35 variants, 23 of which showed no traces or minimal amounts of the expected full-length transcripts of each minigene. More than 30 different variant-induced transcripts were characterized, 23 of which were predicted to truncate the PALB2 protein. The pathogenicity of all variants was interpreted according to an in-house adaptation of the American College of Medical Genetics and Genomics and the Association for Molecular Pathology (ACMG-AMP) variant classification scheme. Up to 23 variants were classified as pathogenic/likely pathogenic. Remarkably, three AE1,2 variants (c.49-2A>T, c.108+2T>C, and c.211+1G>A) were classified as variants of unknown significance, as they produced significant amounts of either in-frame transcripts of unknown impact on the PALB2 protein function or the minigene full-length transcripts. In conclusion, we have significantly contributed to the ongoing effort of identifying spliceogenic variants in the clinically relevant PALB2 cancer susceptibility gene. Moreover, we suggest some approaches to classify the findings in accordance with the ACMG-AMP rationale.

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Comprehensive Functional Characterization and Clinical Interpretation of 20 Splice-Site Variants of the RAD51C Gene

Cited by 11 publications

References 82 publications

RAD51D Aberrant Splicing in Breast Cancer: Identification of Splicing Regulatory Elements and Minigene-Based Evaluation of 53 DNA Variants

RAD51D Aberrant Splicing in Breast Cancer: Identification of Splicing Regulatory Elements and Minigene-Based Evaluation of 53 DNA Variants

Regulation of RAD51 at the Transcriptional and Functional Levels: What Prospects for Cancer Therapy?

Splicing predictions, minigene analyses, and ACMG‐AMP clinical classification of 42 germline PALB2 splice‐site variants

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