ENIGMA<i>CHEK2</i>gether Project: A Comprehensive Study Identifies Functionally Impaired<i>CHEK2</i>Germline Missense Variants Associated with Increased Breast Cancer Risk

Stolařová, Lenka; Kleiblová, Petra; Zemánková, Petra; Stastna, Barbora; Janatová, Markéta; Soukupová, Jana; Achatz, Maria Isabel; Ambrosone, Christine B.; Apostolou, Paraskevi; Arun, Banu K.; Auer, Paul L.; Barnard, Mollie; Bertelsen, Birgitte; Matsuda, Koichi; Kamatani, Yoichiro; Morisaki, Takayuki; Nagai, Akiko; Muto, Kaori; Murakami, Yoshinori; Furukawa, Yoichi; Yamanashi, Yuji; Nakamura, Yusuke; Mushiroda, Taisei; Momozawa, Yukihide; Tanaka, Toshihiro; Ohnishi, Yozo; Kubo, Michiaki; Higashiue, Shinichi; Kobayashi, Shuzo; Minami, Shiro; Yamaguhci, Hiroki; Arai, Hajime; Yamaji, Katsuhiko; Okazaki, Yasushi; Asai, Satoshi; Takahashi, Yasuo; Fujioka, Tomoaki; Obara, Wataru; Mori, Seijiro; Murayama, Shigeo; Nagayama, Satoshi; Miki, Yoshio; Masumoto, Akihide; Yamada, Akira; Nishizawa, Yasuko; Higashiyama, Masahiko; Kutsumi, Hiromu; Koretsune, Yukihiro; Yoshiyama, Takashi; Blok, Marinus J.; Boddicker, Nicholas; Brunet, Joan; Burnside, Elizabeth S.; Calvello, Mariarosaria; Campbell, Ian; Chan, Sock Hoai; Chen, Fei; Chiang, Jianbang; Coppa, Anna; Cortesi, Laura; Crujeiras-González, Ana; Borecká, Marianna; Černá, Marta; Hovhannisyan, Milena; Jelínková, Sandra; Nehasil, Petr; Foretová, Lenka; Macháčková, Eva; Krutilkova, Vera; Tavandzis, Spiros; Cerna, Leona; Chvojka, Stepan; Koudová, Monika; Puchmajerová, Alena; Havránek, Ondřej; Novotný, Jan; Veselá, Kamila; Vočka, Michal; Hrušková, Lucie; Michalovska, Renata; Schwetzova, Denisa; Vlčková, Zdeňka; Černá, Monika; Hejnalova, Marketa; Jedlickova, Nikol; Šubrt, I; Zavoral, Tomas; Kosařová, Marcela; Vacínová, Gabriela; Janíková, Mária; Kratochvilova, Romana; Curtisová, Václava; Vrtěl, Radek; Scheinost, Ondrej; Duskova, Petra; Stránecký, Viktor; Leeneer, Kim De; Putter, Robin De; DePersia, Allison; Devereux, Lisa; Domchek, Susan M.; Efremidis, Anna; Engel, Christoph; Ernst, Corinna; Evans, D. Gareth; Feliubadaló, Lídia; Fostira, Florentia; Fuentes-Ríos, Olivia; Gómez-García, Encarna B.; González, Sara; Haiman, Christopher A.; Hansen, Thomas van Overeem; Hauke, Jan; Hodge, James; Hu, Chunling; Huang, Hongyan; Ishak, Nur Diana Binte; Iwasaki, Yusuke; Konstantopoulou, Irene; Kraft, Peter; Lacey, J.; Lázaro, Conxi; Li, Na; Lim, Weng Khong; Lindstrom, Sara; Lori, Adriana; Martinez, Elana; Martins, Alexandra; Matullo, Giuseppe; McInerny, Simone; Michailidou, Kyriaki; Montagna, Marco; Monteiro, Alvaro N.A.; Mori, Luigi; Nathanson, Katherine L.; Neuhausen, Susan L.; Nevanlinna, Heli; Olson, Janet E.; Palmer, Julie R.; Pasini, Barbara; Patel, Alpa V.; Piane, Maria; Poppe, Bruce; Radice, Paolo; Renieri, Alessandra; Resta, Nicoletta; Richardson, Marcy E.; Rosseel, Toon; Ruddy, Kathryn J.; Santamariña, Marta; Santos, Elizabeth Santana Dos; Teras, Lauren R.; Toland, Amanda E.; Trentham‐Dietz, Amy; Vachon, Celine M.; Volk, Alexander E; Weber‐Lassalle, Nana; Weitzel, Jeffrey N.; Wiesmüller, Lisa; Winham, Stacey J.; Yadav, Siddhartha; Yannoukakos, Drakoulis; Yao, Song; Zampiga, Valentina; Zethoven, Magnus; Zhang, Ze Wen; Zima, Tomáš; Spurdle, Amanda B.; Vega, Ana; Rossing, Maria; Valle, Jesús Del; Nicolo, Arcangela De; Hahnen, Eric; Claes, Kathleen; Ngeow, Joanne; James, Paul; Couch, Fergus J.; Macůrek, Libor; Kleibl, Zdeněk

doi:10.1158/1078-0432.ccr-23-0212

Cited by 9 publications

(5 citation statements)

References 41 publications

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“…Such an approach is supported by the finding that concordant data from multiple assays has significantly more overlap with independent VEP predictions than data from a single assay. The value of a second, confirming assay is further supported by an analysis of ENIGMA patient data and two functional assays (KAP1 phosphorylation and CHK2 phosphorylation) carried out by Stolarova et al 22 , which shows that CHK2 variants confirmed to be damaging in more assays are associated with increasing risk for breast cancer. For example, the 140 variants that either of their functional assays classified as damaging, even if the two assays were discordant, showed a combined increased risk for breast cancer (OR 2.29; 95% CI 1.97 – 2.66), while the 91-variant subset of these that were confirmed to be damaging in our screen showed a marginally increased risk (OR 2.95; 95% CI 2.36 – 3.69), and the risk conferred by 74 variants confirmed to be damaging in all three assays was even higher (OR 3.05; 2.39 – 3.90) (Supplemental Table 3 and 22 ).…”

Section: Discussionmentioning

confidence: 82%

“…Another recent large study functionally characterized 427 CHEK2 VUSs selected by the international ENIGMA (Evidence-based Network for the Interpretation of Germline Mutant Alleles) consortium for variants with an association to an increased risk of breast cancer 22 . That study used two parallel functional assays that quantified the phosphorylation of the KRAB-associated protein (KAP1) at S473 and autophosphorylation of CHK2 at S516.…”

Section: Resultsmentioning

confidence: 99%

“…When compared to our functionally characterized CHK2 variants, the phosphorylation of KAP1 and CHK2 autophosphorylation experiments agreed in 322/427 (75.4%) and 318/327 (91.2%) of the variant classifications, respectively. However, this analysis does not include those classified as “functionally intermediate” in the ENIGMA 22 assays; the KAP1 phosphorylation and CHEK2 phosphorylation assays classified as intermediate 46 and 28 variants, respectively, that were tolerated in our screen, and another 12 and 16 variants, respectively, that were damaging in our screen. Compared with the concordant experimental data, our variant classifications were consistent in 337/427 (78.9%) of the variants.…”

Section: Resultsmentioning

confidence: 99%

“…Several different functional assays have been used to test individual and small sets of CHK2 missense variants identified in patients, including tests of protein stability, kinase activity toward various substrates, and activation by DNA damaging agents 22,23,29–32 . Another method to assay the function of CHK2 variants is to test their ability to complement a yeast RAD53 loss-of-function mutant ( rad53 ).…”

Section: Introductionmentioning

confidence: 99%

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Comprehensive analysis of the functional impact of single nucleotide variants of humanCHEK2

McCarthy-Leo,

Brush,

Pique-Regi

et al. 2023

Preprint

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Loss of function mutations in the checkpoint kinase geneCHEK2are associated with increased risk of breast and other cancers. Most of the 3,188 unique amino acid changes that can result from non-synonymous single nucleotide variants (SNVs) ofCHEK2, however, have not been tested for their impact on the function of theCHEK2-enocded protein (CHK2). One successful approach to testing the function of variants has been to test for their ability to complement mutations in the yeast ortholog ofCHEK2,RAD53. This approach has been used to provide functional information on over 100CHEK2SNVs and the results align with functional assays in human cells and known pathogenicity. Here we tested all but two of the 4,887 possible SNVs in theCHEK2open reading frame for their ability to complementRAD53mutants using a novel high throughput technique. Among the non-synonymous changes, 770 were damaging to protein function while 2,417 were tolerated. The results correlate well with previous structure and function data and provide a first or additional functional assay for all the variants of uncertain significance identified in clinical databases. Combined, this approach can be used to help predict the pathogenicity ofCHEK2variants of uncertain significance that are found in patient screening and could be applied to other cancer risk genes.

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Section: Discussionmentioning

confidence: 82%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Comprehensive analysis of the functional impact of single nucleotide variants of humanCHEK2

McCarthy-Leo,

Brush,

Pique-Regi

et al. 2023

Preprint

View full text Add to dashboard Cite

show abstract

“…These assays are designed to assess the impact of a particular variant on the structure and functionality of the corresponding protein, providing an estimated VUS pathogenicity [37]. Large investigator consortia, like ENIGMA or INSIGHT, have started to form, with the aim of collecting a large amount of data on VUSs and subsequently using machine learning prediction models or functional assays in determining the significance of variants [39][40][41].…”

Section: Discussionmentioning

confidence: 99%

Prevalence of Variants of Uncertain Significance in Patients Undergoing Genetic Testing for Hereditary Breast and Ovarian Cancer and Lynch Syndrome

Chrysafi,

Jani,

Lotz

et al. 2023

Cancers

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Hereditary Breast and Ovarian Cancer (HBOC) and Lynch Syndrome (LS) are the most common inherited cancer syndromes identified with genetic testing. Testing, though, commonly reveals variants of uncertain significance (VUSs). This is a retrospective observational study designed to determine the prevalence of pathogenic mutations and VUSs in patients tested for HBOC and/or LS and to explore the characteristics of the VUS population. Patients 18–80 years old that met NCCN criteria for HBOC and/or LS genetic screening were tested between 2006 and 2020 at Mount Auburn Hospital in Cambridge, Massachusetts. A total of 663 patients were included in the study, with a mean age of 50 years old and 90% being females. Pathogenic mutations were identified in 12.5% and VUSs in 28.3%. VUS prevalence was associated with race (p-value = 0.019), being particularly higher in Asian populations. Patients with a personal history of breast cancer or family history of breast or ovarian cancer were more likely to have a VUS (personal breast: OR: 1.55; CI: 1.08–2.25; family breast: OR: 1.68; CI: 1.08–2.60, family ovarian OR: 2.29; CI: 1.04–5.45). In conclusion, VUSs appear to be detected in almost one third patients tested for cancer genetic syndromes, and thus future work is warranted to determine their significance in cancer development.

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Comprehensive splicing analysis of the alternatively spliced CHEK2 exons 8 and 10 reveals three enhancer/silencer‐rich regions and 38 spliceogenic variants

Sanoguera‐Miralles,

Llinares‐Burguet,

Bueno‐Martínez

et al. 2024

The Journal of Pathology

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Splicing is controlled by a large set of regulatory elements (SREs) including splicing enhancers and silencers, which are involved in exon recognition. Variants at these motifs may dysregulate splicing and trigger loss‐of‐function transcripts associated with disease. Our goal here was to study the alternatively spliced exons 8 and 10 of the breast cancer susceptibility gene CHEK2. For this purpose, we used a previously published minigene with exons 6–10 that produced the expected minigene full‐length transcript and replicated the naturally occurring events of exon 8 [Δ(E8)] and exon 10 [Δ(E10)] skipping. We then introduced 12 internal microdeletions of exons 8 and 10 by mutagenesis in order to map SRE‐rich intervals by splicing assays in MCF‐7 cells. We identified three minimal (10‐, 11‐, 15‐nt) regions essential for exon recognition: c.863_877del [ex8, Δ(E8): 75%] and c.1073_1083del and c.1083_1092del [ex10, Δ(E10): 97% and 62%, respectively]. Then 87 variants found within these intervals were introduced into the wild‐type minigene and tested functionally. Thirty‐eight of them (44%) impaired splicing, four of which (c.883G>A, c.883G>T, c.884A>T, and c.1080G>T) induced negligible amounts (<5%) of the minigene full‐length transcript. Another six variants (c.886G>A, c.886G>T, c.1075G>A, c.1075G>T, c.1076A>T, and c.1078G>T) showed significantly strong impacts (20–50% of the minigene full‐length transcript). Thirty‐three of the 38 spliceogenic variants were annotated as missense, three as nonsense, and two as synonymous, underlying the fact that any exonic change is capable of disrupting splicing. Moreover, c.883G>A, c.883G>T, and c.884A>T were classified as pathogenic/likely pathogenic variants according to ACMG/AMP (American College of Medical Genetics and Genomics/Association for Molecular Pathology)‐based criteria. © 2024 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of The Pathological Society of Great Britain and Ireland.

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ENIGMACHEK2gether Project: A Comprehensive Study Identifies Functionally ImpairedCHEK2Germline Missense Variants Associated with Increased Breast Cancer Risk

Cited by 9 publications

References 41 publications

Comprehensive analysis of the functional impact of single nucleotide variants of humanCHEK2

Comprehensive analysis of the functional impact of single nucleotide variants of humanCHEK2

Prevalence of Variants of Uncertain Significance in Patients Undergoing Genetic Testing for Hereditary Breast and Ovarian Cancer and Lynch Syndrome

Comprehensive splicing analysis of the alternatively spliced CHEK2 exons 8 and 10 reveals three enhancer/silencer‐rich regions and 38 spliceogenic variants

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