The genetic architecture of breast papillary lesions as a predictor of progression to carcinoma

Author:

Kader TanjinaORCID,Elder Kenneth,Zethoven Magnus,Semple Timothy,Hill Prue,Goode David L.,Thio Niko,Cheasley DaneORCID,Rowley Simone M.,Byrne David J.ORCID,Pang Jia-Min,Miligy Islam M.,Green Andrew R.,Rakha Emad A.,Fox Stephen B.,Mann G. Bruce,Campbell Ian G.ORCID,Gorringe Kylie L.

Abstract

AbstractIntraductal papillomas (IDP) are challenging breast findings because of their variable risk of progression to malignancy. The molecular events driving IDP development and genomic features of malignant progression are poorly understood. In this study, genome-wide CNA and/or targeted mutation analysis was performed on 44 cases of IDP, of which 20 cases had coexisting ductal carcinoma in situ (DCIS), papillary DCIS or invasive ductal carcinoma (IDC). CNA were rare in pure IDP, but 69% carried an activating PIK3CA mutation. Among the synchronous IDP cases, 55% (11/20) were clonally related to the synchronous DCIS and/or IDC, only one of which had papillary histology. In contrast to pure IDP, PIK3CA mutations were absent from clonal cases. CNAs in any of chromosomes 1, 16 or 11 were significantly enriched in clonal IDP lesions compared to pure and non-clonal IDP. The observation that 55% of IDP are clonal to DCIS/IDC indicates that IDP can be a direct precursor for breast carcinoma, not limited to the papillary type. The absence of PIK3CA mutations and presence of CNAs in IDP could be used clinically to identify patients at high risk of progression to carcinoma.

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Radiology Nuclear Medicine and imaging,Oncology

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