Literature DB >> 27829436

The PALB2 p.Leu939Trp mutation is not associated with breast cancer risk.

Irene Catucci1, Paolo Radice2, Roger L Milne3,4, Fergus J Couch5, Melissa C Southey6, Paolo Peterlongo7.   

Abstract

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Keywords:  Breast cancer genetic risk factor; Breast cancer predisposition; PALB2 p.Leu939Trp; VUS

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Year:  2016        PMID: 27829436      PMCID: PMC5101669          DOI: 10.1186/s13058-016-0762-9

Source DB:  PubMed          Journal:  Breast Cancer Res        ISSN: 1465-5411            Impact factor:   6.466


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Missense mutations in breast cancer predisposition genes are a substantial clinical problem. These are usually considered variants of uncertain significance (VUS) until genetic, clinical, and functional data provide statistical evidence for reclassification as pathogenic or neutral. Recently, Park et al. [1] suggested that the WD40 domain of the protein encoded by the breast cancer predisposition gene PALB2 may scaffold RAD51C, RAD51, and BRCA2 proteins into a complex involved in DNA repair mediated by homologous recombination (HR). The authors studied the effect of p.Leu939Trp and other missense mutations located within the PALB2 WD40 domain that had been identified in the germline of women with breast cancer. They reported that the p.Leu939Trp mutation resulted in altered PALB2BRCA2 binding, decreased capacity for DNA double-strand break-induced HR, and increased sensitivity to ionizing radiation. Based on these observations and their assertion that this mutation occurs more frequently in women with breast cancer than in unaffected women, Park et al. [1] concluded that the p.Leu939Trp mutation may be pathogenic and proposed that their assays could be used for the functional characterization of other PALB2 missense variants. Case-control, rather than case-only studies are required to estimate the relative risk associated with a genetic variant. Park et al. refer to p.Leu939Trp as a breast cancer-associated mutation; however, among the studies they cited to sustain this hypothesis, only one was a case-control study [2]. Further, case-control data from Rahman et al. [3] were not considered, even though this study is referenced in their report. These two studies [2, 3] together identified the p.Leu939Trp mutation in 10/1741 (0.57 %) women with breast cancer and 8/1534 (0.52 %) unaffected controls, suggesting that this mutation is not associated with breast cancer risk. Further, we later published a third study corroborating this null finding [4] and have subsequently reported additional evidence that the p.Leu939Trp mutation is not associated with breast cancer risk, based on genotyping of 42,671 breast cancer cases and 42,164 controls (odds ratio = 1.05, 95 % confidence interval = 0.83–1.32, p value = 0.70) [5]. Finally, we observed that the p.Leu939Trp mutation does not disrupt the HR-mediated DNA repair activity of PALB2 (Fig. 1).
Fig. 1

Homologous recombination assay for the p.Leu939Trp mutation. B400 palb2−/−; tp53−/− mouse mammary tumor cells were co-transfected with direct repeat-green fluorescent protein (DR-GFP) reporter and recombinant constructs expressing normal (used as positive control), p.Tyr551* (used as negative control) and p.Leu939Trp mutated PALB2 alleles. The error bars represent the Standard Error (SE) of the mean from three independent experiments. GFP-positive cells were assessed by flow cytometry. Comparable expression level of normal and p.Leu939Trp mutated PALB2 proteins was observed by western blot (data not shown)

Homologous recombination assay for the p.Leu939Trp mutation. B400 palb2−/−; tp53−/− mouse mammary tumor cells were co-transfected with direct repeat-green fluorescent protein (DR-GFP) reporter and recombinant constructs expressing normal (used as positive control), p.Tyr551* (used as negative control) and p.Leu939Trp mutated PALB2 alleles. The error bars represent the Standard Error (SE) of the mean from three independent experiments. GFP-positive cells were assessed by flow cytometry. Comparable expression level of normal and p.Leu939Trp mutated PALB2 proteins was observed by western blot (data not shown) Results from functional assays with undefined sensitivity and specificity are not sufficient to classify VUS. In this instance, the p.Leu939Trp mutation may have some influence on response to ionizing radiation but it appears to have little to no impact on HR-mediated DNA repair. In conclusion, our findings suggest that the PALB2 p.Leu939Trp mutation should be classified as a neutral variant with no clinical relevance to risk of breast cancer.
  5 in total

1.  Germline mutations in the PALB2 gene are population specific and occur with low frequencies in familial breast cancer.

Authors:  Heide Hellebrand; Christian Sutter; Ellen Honisch; Eva Gross; Barbara Wappenschmidt; Christian Schem; Helmut Deissler; Nina Ditsch; Verena Gress; Marion Kiechle; Claus R Bartram; Rita K Schmutzler; Dieter Niederacher; Norbert Arnold; Alfons Meindl
Journal:  Hum Mutat       Date:  2011-02-24       Impact factor: 4.878

2.  PALB2, which encodes a BRCA2-interacting protein, is a breast cancer susceptibility gene.

Authors:  Nazneen Rahman; Sheila Seal; Deborah Thompson; Patrick Kelly; Anthony Renwick; Anna Elliott; Sarah Reid; Katarina Spanova; Rita Barfoot; Tasnim Chagtai; Hiran Jayatilake; Lesley McGuffog; Sandra Hanks; D Gareth Evans; Diana Eccles; Douglas F Easton; Michael R Stratton
Journal:  Nat Genet       Date:  2006-12-31       Impact factor: 38.330

3.  PALB2 sequencing in Italian familial breast cancer cases reveals a high-risk mutation recurrent in the province of Bergamo.

Authors:  Irene Catucci; Paolo Peterlongo; Sara Ciceri; Mara Colombo; Graziella Pasquini; Monica Barile; Bernardo Bonanni; Paolo Verderio; Sara Pizzamiglio; Claudia Foglia; Anna Falanga; Marina Marchetti; Laura Galastri; Tiziana Bianchi; Chiara Corna; Fernando Ravagnani; Loris Bernard; Stefano Fortuzzi; Domenico Sardella; Giulietta Scuvera; Bernard Peissel; Siranoush Manoukian; Carlo Tondini; Paolo Radice
Journal:  Genet Med       Date:  2014-02-20       Impact factor: 8.822

4.  Breast cancer-associated missense mutants of the PALB2 WD40 domain, which directly binds RAD51C, RAD51 and BRCA2, disrupt DNA repair.

Authors:  J-Y Park; T R Singh; N Nassar; F Zhang; M Freund; H Hanenberg; A R Meetei; P R Andreassen
Journal:  Oncogene       Date:  2013-10-21       Impact factor: 9.867

5.  PALB2, CHEK2 and ATM rare variants and cancer risk: data from COGS.

Authors:  Melissa C Southey; David E Goldgar; Robert Winqvist; Katri Pylkäs; Fergus Couch; Marc Tischkowitz; William D Foulkes; Joe Dennis; Kyriaki Michailidou; Elizabeth J van Rensburg; Tuomas Heikkinen; Heli Nevanlinna; John L Hopper; Thilo Dörk; Kathleen Bm Claes; Jorge Reis-Filho; Zhi Ling Teo; Paolo Radice; Irene Catucci; Paolo Peterlongo; Helen Tsimiklis; Fabrice A Odefrey; James G Dowty; Marjanka K Schmidt; Annegien Broeks; Frans B Hogervorst; Senno Verhoef; Jane Carpenter; Christine Clarke; Rodney J Scott; Peter A Fasching; Lothar Haeberle; Arif B Ekici; Matthias W Beckmann; Julian Peto; Isabel Dos-Santos-Silva; Olivia Fletcher; Nichola Johnson; Manjeet K Bolla; Elinor J Sawyer; Ian Tomlinson; Michael J Kerin; Nicola Miller; Federik Marme; Barbara Burwinkel; Rongxi Yang; Pascal Guénel; Thérèse Truong; Florence Menegaux; Marie Sanchez; Stig Bojesen; Sune F Nielsen; Henrik Flyger; Javier Benitez; M Pilar Zamora; Jose Ignacio Arias Perez; Primitiva Menéndez; Hoda Anton-Culver; Susan Neuhausen; Argyrios Ziogas; Christina A Clarke; Hermann Brenner; Volker Arndt; Christa Stegmaier; Hiltrud Brauch; Thomas Brüning; Yon-Dschun Ko; Taru A Muranen; Kristiina Aittomäki; Carl Blomqvist; Natalia V Bogdanova; Natalia N Antonenkova; Annika Lindblom; Sara Margolin; Arto Mannermaa; Vesa Kataja; Veli-Matti Kosma; Jaana M Hartikainen; Amanda B Spurdle; kConFab Investigators; Els Wauters; Dominiek Smeets; Benoit Beuselinck; Giuseppe Floris; Jenny Chang-Claude; Anja Rudolph; Petra Seibold; Dieter Flesch-Janys; Janet E Olson; Celine Vachon; Vernon S Pankratz; Catriona McLean; Christopher A Haiman; Brian E Henderson; Fredrick Schumacher; Loic Le Marchand; Vessela Kristensen; Grethe Grenaker Alnæs; Wei Zheng; David J Hunter; Sara Lindstrom; Susan E Hankinson; Peter Kraft; Irene Andrulis; Julia A Knight; Gord Glendon; Anna Marie Mulligan; Arja Jukkola-Vuorinen; Mervi Grip; Saila Kauppila; Peter Devilee; Robert A E M Tollenaar; Caroline Seynaeve; Antoinette Hollestelle; Montserrat Garcia-Closas; Jonine Figueroa; 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Janet L Stanford; William J Blot; Stephen Thibodeau; Daniel J Schaid; Joseph L Kelley; Christiane Maier; Adam S Kibel; Cezary Cybulski; Lisa Cannon-Albright; Katja Butterbach; Jong Park; Radka Kaneva; Jyotsna Batra; Manuel R Teixeira; Zsofia Kote-Jarai; Ali Amin Al Olama; Sara Benlloch; Stefan P Renner; Arndt Hartmann; Alexander Hein; Matthias Ruebner; Diether Lambrechts; Els Van Nieuwenhuysen; Ignace Vergote; Sandrina Lambretchs; Jennifer A Doherty; Mary Anne Rossing; Stefan Nickels; Ursula Eilber; Shan Wang-Gohrke; Kunle Odunsi; Lara E Sucheston-Campbell; Grace Friel; Galina Lurie; Jeffrey L Killeen; Lynne R Wilkens; Marc T Goodman; Ingo Runnebaum; Peter A Hillemanns; Liisa M Pelttari; Ralf Butzow; Francesmary Modugno; Robert P Edwards; Roberta B Ness; Kirsten B Moysich; Andreas du Bois; Florian Heitz; Philipp Harter; Stefan Kommoss; Beth Y Karlan; Christine Walsh; Jenny Lester; Allan Jensen; Susanne Krüger Kjaer; Estrid Høgdall; Bernard Peissel; Bernardo Bonanni; Loris Bernard; Ellen L Goode; Brooke L Fridley; Robert A Vierkant; Julie M Cunningham; Melissa C Larson; Zachary C Fogarty; Kimberly R Kalli; Dong Liang; Karen H Lu; Michelle A T Hildebrandt; Xifeng Wu; Douglas A Levine; Fanny Dao; Maria Bisogna; Andrew Berchuck; Edwin S Iversen; Jeffrey R Marks; Lucy Akushevich; Daniel W Cramer; Joellen Schildkraut; Kathryn L Terry; Elizabeth M Poole; Meir Stampfer; Shelley S Tworoger; Elisa V Bandera; Irene Orlow; Sara H Olson; Line Bjorge; Helga B Salvesen; Anne M van Altena; Katja K H Aben; Lambertus A Kiemeney; Leon F A G Massuger; Tanja Pejovic; Yukie Bean; Angela Brooks-Wilson; Linda E Kelemen; Linda S Cook; Nhu D Le; Bohdan Górski; Jacek Gronwald; Janusz Menkiszak; Claus K Høgdall; Lene Lundvall; Lotte Nedergaard; Svend Aage Engelholm; Ed Dicks; Jonathan Tyrer; Ian Campbell; Iain McNeish; James Paul; Nadeem Siddiqui; Rosalind Glasspool; Alice S Whittemore; Joseph H Rothstein; Valerie McGuire; Weiva Sieh; Hui Cai; Xiao-Ou Shu; Rachel T Teten; Rebecca Sutphen; John R McLaughlin; Steven A Narod; Catherine M Phelan; Alvaro N Monteiro; David Fenstermacher; Hui-Yi Lin; Jennifer B Permuth; Thomas A Sellers; Y Ann Chen; Ya-Yu Tsai; Zhihua Chen; Aleksandra Gentry-Maharaj; Simon A Gayther; Susan J Ramus; Usha Menon; Anna H Wu; Celeste L Pearce; David Van Den Berg; Malcolm C Pike; Agnieszka Dansonka-Mieszkowska; Joanna Plisiecka-Halasa; Joanna Moes-Sosnowska; Jolanta Kupryjanczyk; Paul Dp Pharoah; Honglin Song; Ingrid Winship; Georgia Chenevix-Trench; Graham G Giles; Sean V Tavtigian; Doug F Easton; Roger L Milne
Journal:  J Med Genet       Date:  2016-09-05       Impact factor: 6.318
  5 in total
  4 in total

1.  PALB2 mutations in BRCA1/2-mutation negative breast and ovarian cancer patients from Poland.

Authors:  Anna Kluska; Aneta Balabas; Magdalena Piatkowska; Katarzyna Czarny; Katarzyna Paczkowska; Dorota Nowakowska; Michal Mikula; Jerzy Ostrowski
Journal:  BMC Med Genomics       Date:  2017-03-09       Impact factor: 3.063

2.  Two Missense Variants Detected in Breast Cancer Probands Preventing BRCA2-PALB2 Protein Interaction.

Authors:  Laura Caleca; Irene Catucci; Gisella Figlioli; Loris De Cecco; Tina Pesaran; Maggie Ward; Sara Volorio; Anna Falanga; Marina Marchetti; Maria Iascone; Carlo Tondini; Alberto Zambelli; Jacopo Azzollini; Siranoush Manoukian; Paolo Radice; Paolo Peterlongo
Journal:  Front Oncol       Date:  2018-10-25       Impact factor: 6.244

3.  Criteria of the German Consortium for Hereditary Breast and Ovarian Cancer for the Classification of Germline Sequence Variants in Risk Genes for Hereditary Breast and Ovarian Cancer.

Authors:  Barbara Wappenschmidt; Jan Hauke; Ulrike Faust; Dieter Niederacher; Lisa Wiesmüller; Gunnar Schmidt; Evi Groß; Andrea Gehrig; Christian Sutter; Juliane Ramser; Andreas Rump; Norbert Arnold; Alfons Meindl
Journal:  Geburtshilfe Frauenheilkd       Date:  2020-04-21       Impact factor: 2.915

4.  A global functional analysis of missense mutations reveals two major hotspots in the PALB2 tumor suppressor.

Authors:  Amélie Rodrigue; Guillaume Margaillan; Thiago Torres Gomes; Yan Coulombe; Gemma Montalban; Simone da Costa E Silva Carvalho; Larissa Milano; Mandy Ducy; Giuliana De-Gregoriis; Graham Dellaire; Wilson Araújo da Silva; Alvaro N Monteiro; Marcelo A Carvalho; Jacques Simard; Jean-Yves Masson
Journal:  Nucleic Acids Res       Date:  2019-11-18       Impact factor: 16.971
  4 in total

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