Biallelic germline BRCA1 mutations in a patient with early onset breast cancer, mild Fanconi anemia‐like phenotype, and no chromosome fragility
Katharina Keupp,Stephanie Hampp,Annette Hübbel,M Maringa,Sarah Kostezka,Kerstin Rhiem,Anke Waha,Barbara Wappenschmidt,Roser Pujol,Roser Pujol,Jordi Surrallés,Jordi Surrallés,Rita K. Schmutzler,Lisa Wiesmüller,Eric Hahnen +14 more
41
TL;DR: Biallelic BRCA1 mutations are reported in a woman with breast cancer diagnosed at the age of 30 years and the common European founder mutation p.Cys61Gly confers high cancer risk, whereas the deleterious p.Arg1699Gln is hypomorphic and was suggested to confer intermediate cancer risk.
read more
Abstract: Background Biallelic BRCA1 mutations are regarded either embryonically lethal or to cause Fanconi anemia (FA), a genomic instability syndrome characterized by bone marrow failure, developmental abnormalities, and cancer predisposition. We report biallelic BRCA1 mutations c.181T > G (p.Cys61Gly) and c.5096G > A (p.Arg1699Gln) in a woman with breast cancer diagnosed at the age of 30 years. The common European founder mutation p.Cys61Gly confers high cancer risk, whereas the deleterious p.Arg1699Gln is hypomorphic and was suggested to confer intermediate cancer risk. Methods and results Aside from significant toxicity from chemotherapy, the patient showed mild FA-like features (e.g., short stature, microcephaly, skin hyperpigmentation). Chromosome fragility, a hallmark of FA patient cells, was not present in patient-derived peripheral blood lymphocytes. We demonstrated that the p.Arg1699Gln mutation impairs DNA double-strand break repair, elevates RAD51 foci levels at baseline, and compromises BRCA1 protein function in protecting from replication stress. Although the p.Arg1699Gln mutation compromises BRCA1 function, the residual activity of the p.Arg1699Gln allele likely prevents from chromosome fragility and a more severe FA phenotype. Conclusion Our data expand the clinical spectrum associated with biallelic BRCA1 mutations, ranging from embryonic lethality to a mild FA-like phenotype and no chromosome fragility.
read more
Chat with Paper
AI Agents for this Paper
Find similar papers on Google Scholar, PubMed and Arxiv
Write a critical review of this paper
Analyze citations of this paper to find unaddressed research gaps
Citations
Genetic/familial high-risk assessment: Breast, ovarian, and pancreatic, version 2.2021
Mary B. Daly,Tuya Pal,Michael Berry,Saundra S. Buys,Patricia I. Dickson,Susan M. Domchek,Ahmed Elkhanany,Susan Hatters Friedman,Michael Goggins,Mollie L. Hutton,Beth Y. Karlan,Seema A. Khan,Catherine Klein,Wendy Kohlmann,Allison W. Kurian,Christine Laronga,Jennifer K. Litton,Julie S. Mak,Carolyn S. Menendez,Sofia D. Merajver,Barbara S. Norquist,Kenneth Offit,Holly J. Pederson,Gwen Reiser,Leigha Senter-Jamieson,Kristen M. Shannon,Rebecca Shatsky,Kala Visvanathan,Jeffrey N. Weitzel,Myra J. Wick,Kari B. Wisinski,Matthew B. Yurgelun,Susan Darlow,Mary A. Dwyer +33 more
TL;DR: The NCCN Guidelines for Genetic/Familial High-Risk Assessment: Breast, Ovarian, and Pancreatic focus primarily on assessment of pathogenic or likely pathogenic variants associated with increased risk of breast, ovarian, and pancreatic cancer and recommended approaches to genetic testing/counseling and management strategies as mentioned in this paper.
Genetic Predisposition to Breast and Ovarian Cancers: How Many and Which Genes to Test?
TL;DR: The past and more recent findings in the field of cancer predisposition genes are summarized, with insights into the role of the encoded proteins and the associated genetic disorders.
93
BRCA1 Mutational Complementation Induces Synthetic Viability
Joseph Nacson,Joseph Nacson,Daniela Di Marcantonio,Yifan Wang,Andrea J. Bernhardy,Emma Clausen,Xiang Hua,Kathy Q. Cai,Esteban Martínez,Wanjuan Feng,Elsa Callen,Wei Wu,Gaorav P. Gupta,Joseph R. Testa,André Nussenzweig,Stephen M. Sykes,Neil Johnson +16 more
TL;DR: Brca1CC and Brca1Δ11 alleles represent separation-of-function mutations that combine to provide a level of HR sufficient for normal development and hematopoiesis.
50
Clinical experience with carrier screening in a general population: support for a comprehensive pan-ethnic approach.
Maggie Westemeyer,Jennifer Saucier,Jody Wallace,Sarah A. Prins,Aparna Shetty,Meenakshi Malhotra,Zachary Demko,Christine M. Eng,Louis Weckstein,Robert Boostanfar,Matthew Rabinowitz,Peter Benn,Dianne Keen-Kim,Paul Billings +13 more
TL;DR: Compared with standard screening, NGS-based CS provides additional information that may impact reproductive choices and Pan-ethnic CS leads to substantially increased identification of at-risk couples.
49
Rubinstein-Taybi syndrome in diverse populations.
Cedrik Tekendo-Ngongang,Babajide Owosela,Nicole Fleischer,Yonit A. Addissie,Bryan Malonga,Ebenezer Badoe,Neerja Gupta,Angélica Moresco,Victoria Huckstadt,Engy A. Ashaat,Dalia Farouk Hussen,Ho Ming Luk,Ivan F M Lo,Brian H.Y. Chung,Jasmine L.F. Fung,Danilo Moretti-Ferreira,Leticia Cassimiro Batista,Stephanie Lotz-Esquivel,Manuel Saborio-Rocafort,Ramses Badilla-Porras,Monica Penon Portmann,Monica Penon Portmann,Kelly L. Jones,Omar A. Abdul-Rahman,Annette Uwineza,Eloise J. Prijoles,Ifeanyi Kanayo Ifeorah,Arianne Llamos Paneque,Nirmala D. Sirisena,Leah Dowsett,Sansan Lee,Gerarda Cappuccio,Carolyn Sian Kitchin,Alicia Diaz-Kuan,Meow-Keong Thong,María Gabriela Obregon,Leon Mutesa,Vajira H. W. Dissanayake,Mona O. El Ruby,Nicola Brunetti-Pierri,Ekanem N. Ekure,Roger E. Stevenson,Maximilian Muenke,Paul Kruszka +43 more
TL;DR: Clinical examination combined with facial analysis technology may enable earlier and improved diagnosis of RSTS in diverse populations, demonstrating excellent discrimination efficacy.
28
References
Development of a WHO growth reference for school-aged children and adolescents
Mercedes de Onis,Adelheid W. Onyango,Elaine Borghi,Amani Siyam,Chizuru Nishida,Jonathan Siekmann +5 more
TL;DR: The new curves are closely aligned with the WHO Child Growth Standards at 5 years, and the recommended adult cut-offs for overweight and obesity at 19 years.
Specific killing of BRCA2-deficient tumours with inhibitors of poly(ADP-ribose) polymerase
Helen E. Bryant,Nilklas Schultz,Huw D. Thomas,Kayan M. Parker,Dan Flower,Elena Lopez,Suzanne Kyle,Mark Meuth,Nicola J. Curtin,Thomas Helleday,Thomas Helleday +10 more
TL;DR: It is proposed that, in the absence of PARP1, spontaneous single-strand breaks collapse replication forks and trigger homologous recombination for repair and exploited in order to kill BRCA2-deficient tumours by PARP inhibition alone.
4.9K
Elaboración de valores de referencia de la OMS para el crecimiento de escolares y adolescentes
Mercedes de Onis,Adelheid W. Onyango,Elaine Borghi,Amani Siyam,Chizuru Nishida,Jonathan Siekmann +5 more
TL;DR: The methods used to reconstruct the 1977 NCHS/WHO growth reference are reported, to compare the resulting new curves with the 2007 WHO reference, and to describe the transition at 5 years of age from the WHO standards for under-fives to these new curves for school-aged children and adolescents.
Risks of Breast, Ovarian, and Contralateral Breast Cancer for BRCA1 and BRCA2 Mutation Carriers
Karoline Kuchenbaecker,Karoline Kuchenbaecker,John L. Hopper,Daniel R. Barnes,Kelly-Anne Phillips,T.M. Mooij,Marie-José Roos-Blom,Marie-José Roos-Blom,Sarah Jervis,Sarah Jervis,Flora E. van Leeuwen,Roger L. Milne,Roger L. Milne,Nadine Andrieu,David E. Goldgar,Mary Beth Terry,Matti A. Rookus,Douglas F. Easton,Antonis C. Antoniou,Lesley McGuffog,D. Gareth Evans,Daniel Barrowdale,Debra Frost,Julian Adlard,Kai-ren Ong,Louise Izatt,Marc Tischkowitz,Ros Eeles,Rosemarie Davidson,Shirley Hodgson,Steve Ellis,Catherine Noguès,Christine Lasset,Dominique Stoppa-Lyonnet,Dominique Stoppa-Lyonnet,Jean-Pierre Fricker,Laurence Faivre,Pascaline Berthet,Maartje J. Hooning,Lizet E. van der Kolk,Carolien M. Kets,Muriel A. Adank,Esther M. John,Wendy K. Chung,Irene L. Andrulis,Irene L. Andrulis,Melissa C. Southey,Mary B. Daly,Saundra S. Buys,Ana Osorio,Christoph Engel,Karin Kast,Rita K. Schmutzler,Trinidad Caldés,Anna Jakubowska,Jacques Simard,Michael Friedlander,Sue-Anne McLachlan,Sue-Anne McLachlan,Eva Machackova,Lenka Foretova,Yen Y. Tan,Yen Y. Tan,Christian F. Singer,Edith Olah,Anne-Marie Gerdes,Brita Arver,Håkan Olsson +67 more
TL;DR: To estimate age-specific risks of breast, ovarian, and contralateral breast cancer for mutation carriers and to evaluate risk modification by family cancer history and mutation location, a large cohort study recruited in 1997-2011 provides estimates of cancer risk based on BRCA1 and BRCa2 mutation carrier status.
A Distinct Replication Fork Protection Pathway Connects Fanconi Anemia Tumor Suppressors to RAD51-BRCA1/2
TL;DR: A repair-independent requirement for FA genes, including FANCD2, and BRCA1 in protecting stalled replication forks from degradation is shown, implying a unified molecular mechanism for repair- independent functions of FA, RAD51, and PSA1/2 proteins in preventing genomic instability and suppressing tumorigenesis.
931
Related Papers (5)
[...]
Sarah Reid,Detlev Schindler,Helmut Hanenberg,Helmut Hanenberg,Karen Barker,Sandra Hanks,Reinhard Kalb,Kornelia Neveling,Patrick Kelly,Sheila Seal,Marcel Freund,Melanie Wurm,Sat Dev Batish,Sat Dev Batish,Francis P. Lach,Sevgi Yetgin,Heidemarie Neitzel,Hany Ariffin,Marc Tischkowitz,Marc Tischkowitz,Christopher G. Mathew,Arleen D. Auerbach,Nazneen Rahman +22 more