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. 2014 Dec 23;16(6):3419.
doi: 10.1186/s13058-014-0474-y.

Refined histopathological predictors of BRCA1 and BRCA2 mutation status: a large-scale analysis of breast cancer characteristics from the BCAC, CIMBA, and ENIGMA consortia

Amanda B SpurdleFergus J CouchMichael T ParsonsLesley McGuffogDaniel BarrowdaleManjeet K BollaQin WangSue HealeyRita SchmutzlerBarbara WappenschmidtKerstin RhiemEric HahnenChristoph EngelAlfons MeindlNina DitschNorbert ArnoldHansjoerg PlendlDieter NiederacherChristian SutterShan Wang-GohrkeDoris SteinemannSabine Preisler-AdamsKarin KastRaymonda Varon-MateevaSteve EllisDebra FrostRadka PlatteJo PerkinsD Gareth EvansLouise IzattRos EelesJulian AdlardRosemarie DavidsonTrevor ColeGiulietta ScuveraSiranoush ManoukianBernardo BonanniFrederique MarietteStefano FortuzziAlessandra VielBarbara PasiniLaura PapiLiliana VarescoRosemary BalleineKatherine L NathansonSusan M DomchekKenneth OffittAnna JakubowskaNoralane LindorMads ThomassenUffe Birk JensenJohanna RantalaÅke BorgIrene L AndrulisAlexander MironThomas V O HansenTrinidad CaldesSusan L NeuhausenAmanda E TolandHeli NevanlinnaMarco MontagnaJudy GarberAndrew K GodwinAna OsorioRachel E FactorMary B TerryTimothy R RebbeckBeth Y KarlanMelissa SoutheyMuhammad Usman RashidNadine TungPaul D P PharoahFiona M BlowsAlison M DunningElena ProvenzanoPer HallKamila CzeneMarjanka K SchmidtAnnegien BroeksSten CornelissenSenno VerhoefPeter A FaschingMatthias W BeckmannArif B EkiciDennis J SlamonStig E BojesenBørge G NordestgaardSune F NielsenHenrik FlygerJenny Chang-ClaudeDieter Flesch-JanysAnja RudolphPetra SeiboldKristiina AittomäkiTaru A MuranenPäivi HeikkiläCarl BlomqvistJonine FigueroaStephen J ChanockLouise BrintonJolanta LissowskaJanet E OlsonVernon S PankratzEsther M JohnAlice S WhittemoreDee W WestUte HamannDiana TorresHans Ulrich UlmerThomas RüdigerPeter DevileeRobert A E M TollenaarCaroline SeynaeveChristi J Van AsperenDiana M EcclesWilliam J TapperLorraine DurcanLouise JonesJulian PetoIsabel dos-Santos-SilvaOlivia FletcherNichola JohnsonMiriam DwekRuth SwannAnita L BaneGord GlendonAnna M MulliganGraham G GilesRoger L MilneLaura BagliettoCatriona McLeanJane CarpenterChristine ClarkeRodney ScottHiltrud BrauchThomas BrüningYon-Dschun KoAngela CoxSimon S CrossMalcolm W R ReedJan LubinskiKatarzyna Jaworska-BieniekKatarzyna DurdaJacek GronwaldThilo DörkNatalia BogdanovaTjoung-Won Park-SimonPeter HillemannsChristopher A HaimanBrian E HendersonFredrick SchumacherLoic Le MarchandBarbara BurwinkelFrederik MarmeHarald SurovyRongxi YangHoda Anton-CulverArgyrios ZiogasMaartje J HooningJ Margriet ColléeJohn W M MartensMadeleine M A Tilanus-LinthorstHermann BrennerAida Karina DieffenbachVolke ArndtChrista StegmaierRobert WinqvistKatri PylkäsArja Jukkola-VuorinenMervi GripAnnika LindblomSara MargolinVijai JosephMark RobsonRohini Rau-MurthyAnna González-NeiraJosé Ignacio AriasPilar ZamoraJavier BenítezArto MannermaaVesa KatajaVeli-Matti KosmaJaana M HartikainenPaolo PeterlongoDaniela ZaffaroniMonica BarileFabio CapraPaolo RadiceSoo H TeoDouglas F EastonAntonis C AntoniouGeorgia Chenevix-TrenchDavid E GoldgarABCTB InvestigatorsEMBRACE GroupGENICA NetworkHEBON GroupkConFab Investigators

Refined histopathological predictors of BRCA1 and BRCA2 mutation status: a large-scale analysis of breast cancer characteristics from the BCAC, CIMBA, and ENIGMA consortia

Amanda B Spurdle et al. Breast Cancer Res. .

Abstract

Introduction: The distribution of histopathological features of invasive breast tumors in BRCA1 or BRCA2 germline mutation carriers differs from that of individuals with no known mutation. Histopathological features thus have utility for mutation prediction, including statistical modeling to assess pathogenicity of BRCA1 or BRCA2 variants of uncertain clinical significance. We analyzed large pathology datasets accrued by the Consortium of Investigators of Modifiers of BRCA1/2 (CIMBA) and the Breast Cancer Association Consortium (BCAC) to reassess histopathological predictors of BRCA1 and BRCA2 mutation status, and provide robust likelihood ratio (LR) estimates for statistical modeling.

Methods: Selection criteria for study/center inclusion were estrogen receptor (ER) status or grade data available for invasive breast cancer diagnosed younger than 70 years. The dataset included 4,477 BRCA1 mutation carriers, 2,565 BRCA2 mutation carriers, and 47,565 BCAC breast cancer cases. Country-stratified estimates of the likelihood of mutation status by histopathological markers were derived using a Mantel-Haenszel approach.

Results: ER-positive phenotype negatively predicted BRCA1 mutation status, irrespective of grade (LRs from 0.08 to 0.90). ER-negative grade 3 histopathology was more predictive of positive BRCA1 mutation status in women 50 years or older (LR = 4.13 (3.70 to 4.62)) versus younger than 50 years (LR = 3.16 (2.96 to 3.37)). For BRCA2, ER-positive grade 3 phenotype modestly predicted positive mutation status irrespective of age (LR = 1.7-fold), whereas ER-negative grade 3 features modestly predicted positive mutation status at 50 years or older (LR = 1.54 (1.27 to 1.88)). Triple-negative tumor status was highly predictive of BRCA1 mutation status for women younger than 50 years (LR = 3.73 (3.43 to 4.05)) and 50 years or older (LR = 4.41 (3.86 to 5.04)), and modestly predictive of positive BRCA2 mutation status in women 50 years or older (LR = 1.79 (1.42 to 2.24)).

Conclusions: These results refine likelihood-ratio estimates for predicting BRCA1 and BRCA2 mutation status by using commonly measured histopathological features. Age at diagnosis is an important variable for most analyses, and grade is more informative than ER status for BRCA2 mutation carrier prediction. The estimates will improve BRCA1 and BRCA2 variant classification and inform patient mutation testing and clinical management.

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Figures

Figure 1
Figure 1
Proposed strategy for application of pathology likelihood ratios in multifactorial likelihood analysis of BRCA1 or BRCA2 rare sequence variants. Cases carrying a variant of uncertain clinical significance, and with information on relevant pathology variables, are first assessed to determine that breast tumor pathology information was not a criterion used to trigger gene testing. ER, estrogen-receptor breast tumor status; PR, progesterone-receptor breast tumor status; HER2, HER2 breast tumor status; TN, triple-negative breast tumor status; Not TN, breast tumor status not triple-negative, after measurement of ER, PR, and HER2 status; ER-neg, ER-negative status; ER-pos, ER-positive status; G, grade; <50, breast cancer diagnosis at younger than 50 years for tumor with relevant pathology data; ≥50, breast cancer diagnosis at 50 to 70 years for tumor with relevant pathology data.

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