Mutation status of <scp>RAD</scp>51C,<scp>PALB</scp>2 and <scp>BRIP</scp>1 in 100 Japanese familial breast cancer cases without <scp>BRCA</scp>1 and <scp>BRCA</scp>2 mutations

Sato, Kazuo; Koyasu, Mio; Nomura, Sachio; Sato, Yuri; Kita, Mizuho; Ashihara, Yuumi; Adachi, Yasue; Ohno, Shinji; Iwase, Takuji; Kitagawa, Dai; Nakashima, Eri; Yoshida, Reiko; Miki, Yoshio; Arai, Masami

doi:10.1111/cas.13350

Cited by 14 publications

(9 citation statements)

References 52 publications

(133 reference statements)

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“…Accumulating evidence indicates that patients with BRIP1 mutations have HRR deficiency and are consequently hypersensitive to PARP inhibition. 14 BRIP1 is a BRCA1-interacting protein (the BRIP1-BRCA1 interaction is important for HRR) and associates with BRCA1 as cells progress through the S phase of the cell cycle. 15 , 16 BRIP1 is a DNA helicase that interacts with the COOH-terminal BRCT repeat of BRCA1.…”

Section: Discussionmentioning

confidence: 99%

Olaparib Monotherapy for BRIP1-Mutated High-Grade Serous Endometrial Cancer

Nakamura

Aimono

Tanishima

et al. 2020

JCO Precision Oncology

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Section: Discussionmentioning

confidence: 99%

Olaparib Monotherapy for BRIP1-Mutated High-Grade Serous Endometrial Cancer

Nakamura

Aimono

Tanishima

et al. 2020

JCO Precision Oncology

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“…Also mutations in RAD51C have not been found to increase the risk of breast cancer [ 18 – 20 ] and mutations in RAD51D have been associated with high risk of ovarian cancer but not with breast cancer [ 21 ]. Nevertheless, other studies have indicated that mutations in RAD51C [ 22 ] and RAD51D [ 17 , 23 , 24 ] contribute to the risk of both breast and ovarian cancer, and that RAD50 is an intermediate-risk breast cancer susceptibility gene [ 25 ]. Although germline mutations in the DNA mismatch repair genes ( MLH1, MSH2, MSH6, PMS2 ) have been mostly associated with Lynch syndrome, evidence has been established to support the connections between the mutations in the DNA mismatch repair genes and the risk or survival of breast cancer [ 26 – 29 ].…”

Section: Introductionmentioning

confidence: 99%

“…Although germline mutations in the DNA mismatch repair genes ( MLH1, MSH2, MSH6, PMS2 ) have been mostly associated with Lynch syndrome, evidence has been established to support the connections between the mutations in the DNA mismatch repair genes and the risk or survival of breast cancer [ 26 – 29 ]. Similarly, whether BRIP1 is a breast cancer susceptibility gene remains controversial [ 30 ], and perhaps is dependent on the ethnicity of the cohort studied [ 22 ]. NF1 mutations have been known to associate with increased risk of breast cancer in younger population [ 31 ] and poor breast cancer survival [ 32 ].…”

Section: Introductionmentioning

confidence: 99%

Germline breast cancer susceptibility gene mutations and breast cancer outcomes

et al. 2018

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BackgroundIt is unclear whether germline breast cancer susceptibility gene mutations affect breast cancer related outcomes. We wanted to evaluate mutation patterns in 20 breast cancer susceptibility genes and correlate the mutations with clinical characteristics to determine the effects of these germline mutations on breast cancer prognosis.MethodsThe study cohort included 480 ethnic Chinese individuals in Taiwan with at least one of the six clinical risk factors for hereditary breast cancer: family history of breast or ovarian cancer, young age of onset for breast cancer, bilateral breast cancer, triple negative breast cancer, both breast and ovarian cancer, and male breast cancer. PCR-enriched amplicon-sequencing on a next generation sequencing platform was used to determine the germline DNA sequences of all exons and exon-flanking regions of the 20 genes. Protein-truncating variants were identified as pathogenic.ResultsWe detected a 13.5% carrier rate of pathogenic germline mutations, with BRCA2 being the most prevalent and the non-BRCA genes accounting for 38.5% of the mutation carriers. BRCA mutation carriers were more likely to be diagnosed of breast cancer with lymph node involvement (66.7% vs 42.6%; P = 0.011), and had significantly worse breast cancer specific outcomes. The 5-year disease-free survival was 73.3% for BRCA mutation carriers and 91.1% for non-carriers (hazard ratio for recurrence or death 2.42, 95% CI 1.29–4.53; P = 0.013). After adjusting for clinical prognostic factors, BRCA mutation remained an independent poor prognostic factor for cancer recurrence or death (adjusted hazard ratio 3.04, 95% CI 1.40–6.58; P = 0.005). Non-BRCA gene mutation carriers did not exhibit any significant difference in cancer characteristics or outcomes compared to those without detected mutations. Among the risk factors for hereditary breast cancer, the odds of detecting a germline mutation increased significantly with having bilateral breast cancer (adjusted odds ratio 3.27, 95% CI 1.64–6.51; P = 0.0008) or having more than one risk factor (odds ratio 2.07, 95% CI 1.22–3.51; P = 0.007).ConclusionsWithout prior knowledge of the mutation status, BRCA mutation carriers had more advanced breast cancer on initial diagnosis and worse cancer-related outcomes. Optimal approach to breast cancer treatment for BRCA mutation carriers warrants further investigation.Electronic supplementary materialThe online version of this article (10.1186/s12885-018-4229-5) contains supplementary material, which is available to authorized users.

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“…U nosiček mutace genu RAD51C by ale měla být zvážena preventivní adnexektomie ve 45-50 le tech (event. dříve, věk posuzovat podle nejčasnějšího výskytu karcinomu ovaria v rodině, podobně jako u nosiček mu tace genu BRIP1) [18,20,22,23].…”

Section: Nbnunclassified

“…Souvislost mutací genu BRIP1 se zvýšeným rizikem karci nomu prsu nebyla jednoznačně proká zána, i když je v ně kte rých publikacích možná souvislost uváděna vč. databází OMIM a ClinVar [21][22][23].…”

Section: Nbnunclassified

Risks of Solid Tumors in Heterozygous Carriers of Recessive Syndromes

Koudová¹,

Puchmajerová²

2019

Klin Onkol

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Centrum lékařské genetiky a reprodukční medicíny GENNET, Praha SouhrnRozšířené panelové testování dědičných nádorových dispozic metodou masivně paralelního sek venování vede k nálezu heterozygotních patogenních variant v genech pro autozomálně recesivně dědičné nádorové syndromy. Ke stanovení míry rizika rozvoje solidních nádorů a vhodné dispenza rizace pro heterozygoty nejsou u většiny těchto genů v současnosti k dispozici klinická guidelines ani není definován postup pro další genetické vyšetření v rodině a u jejich partnerů. Naším cílem bylo na základě současných poznatků vytvořit "české guidelines" pro tyto případy. V předkládané práci uvádíme přehled vybraných genů pro autozomálně recesivně dědičné nádorové syndromy, rozdělený do dvou skupin -geny pro Fanconiho anémii a geny pro ostatní autozomálně recesivně dědičné nádorové syndromy. V každé části je vytvořena souhrnná tabulka, která obsahuje frekvenci heterozygotů mutace daného genu v populaci, riziko nádorů u heterozygotů a návrh dispenzarizace a doporučení pro predikce v rodině a ke genetickému vyšetření partnerů heterozygotů. Prediktivní vyšetření je vhodné provádět tam, kde je u heterozygotů zvýšené riziko nádorových onemocnění a/ nebo je předpoklad další reprodukce a vyšší frekvence heterozygotů v populaci, tedy i zvýšeného rizika autozomálně recesivního syndromu pro děti nosiče mutace. Uvedené návrhy a doporučení vycházejí ze současných poznatků a v budoucnosti je bude potřeba dále korigovat dle přibývajících znalostí o stávajících nebo dalších, dosud neprozkoumaných, genech. Klíčová slovadědičné nádorové syndromy -autozomálně recesivní dědičnost -heterozygot -mutace -ri ziko nádorů -prediktivní testování SummaryExpanded gene panel test ing for hereditary cancer predispositions us ing massive parallel sequenc ing can identify heterozygous pathogenic variants of genes that cause autosomal recessive inheri ted cancer syndromes. There are no clinical guidelines regard ing assessment of the risk of develop ing solid tumors or for develop ing appropriate surveillance strategies for heterozygotes for most of these genes, nor is there delineation with respect to the management for genetic testing of relatives and partners. Based on current knowledge, our aim was to create "Czech guidelines" for these cases. Here, we present an overview of the selected genes for autosomal recessive inherited tumor syndromes. The genes were divided into two groups: genes caus ing Fanconi anemia and genes caus ing other autosomal recessive inherited tumor syndromes. A summary table was crea ted for each group. The table shows the population frequency of heterozygotes, the cancer risk for heterozygotes, the proposed surveillance strategy, and recommendations for family prediction and genetic test ing of partners. Predictive testing should be performed in the case of heterozygotes that have an increased risk of cancer and/or as prerequisite to further reproduction of heterozygo tes for a given gene with significant population frequency (this allows an estimation of the risk of a...

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Mutation status of RAD51C,PALB2 and BRIP1 in 100 Japanese familial breast cancer cases without BRCA1 and BRCA2 mutations

Cited by 14 publications

References 52 publications

Olaparib Monotherapy for BRIP1-Mutated High-Grade Serous Endometrial Cancer

Olaparib Monotherapy for BRIP1-Mutated High-Grade Serous Endometrial Cancer

Germline breast cancer susceptibility gene mutations and breast cancer outcomes

Risks of Solid Tumors in Heterozygous Carriers of Recessive Syndromes

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