Somatic mutations in benign breast disease tissue and risk of subsequent invasive breast cancer

Thomas E Rohan,Yihong Wang,Olivier Loudig,Mindy Ginsberg,Andrew Glass,Christopher A Miller,Elaine Mardis,Tiandao Li

doi:10.1038/s41416-018-0089-7

Abstract

BackgroundInsights into the molecular pathogenesis of breast cancer might come from molecular analysis of tissue from early stages of the disease.MethodsWe conducted a case–control study nested in a cohort of women who had biopsy-confirmed benign breast disease (BBD) diagnosed between 1971 and 2006 at Kaiser Permanente Northwest and who were followed to mid-2015 to ascertain subsequent invasive breast cancer (IBC); cases (n = 218) were women with BBD who developed subsequent IBC and controls, individually matched (1:1) to cases, were women with BBD who did not develop IBC in the same follow-up interval as that for the corresponding case. Targeted sequence capture and sequencing were performed for 83 genes of importance in breast cancer.ResultsThere were no significant case–control differences in mutation burden overall, for non-silent mutations, for individual genes, or with respect either to the nature of the gene mutations or to mutational enrichment at the pathway level. For seven subjects with DNA from the BBD and ipsilateral IBC, virtually no mutations were shared.ConclusionsThis study, the first to use a targeted multi-gene sequencing approach on early breast cancer precursor lesions to investigate the genomic basis of the disease, showed that somatic mutations detected in BBD tissue were not associated with breast cancer risk.

Highlights

One model of the natural history of breast cancer posits that it develops as a result of the progression of breast tissue through specific histological forms of benign breast disease (BBD) and carcinoma in situ before developing into invasive breast cancer (IBC)[1]
In the prospective study reported here, we examined the association between somatic mutations detected in BBD tissue and risk of subsequent IBC
28 mutations were observed, and none was shown definitively to be shared between the BBD and IBC (Fig. 1b, Supplementary Table 2b). This is the first study that has used a targeted multi-gene sequencing approach on early breast cancer precursor lesions to investigate the genomic basis of the disease

Summary

Introduction

One model of the natural history of breast cancer posits that it develops as a result of the progression of breast tissue through specific histological forms of benign breast disease (BBD) and carcinoma in situ before developing into invasive breast cancer (IBC)[1]. Predicting the behavior of BBD requires an understanding of its underlying biology[2] In this regard, insights into the molecular pathogenesis of breast cancer will potentially come from analyses conducted on tissue from early stages of the disease[2,3]. In the prospective study reported here, we examined the association between somatic mutations detected in BBD tissue and risk of subsequent IBC. CONCLUSIONS: This study, the first to use a targeted multi-gene sequencing approach on early breast cancer precursor lesions to investigate the genomic basis of the disease, showed that somatic mutations detected in BBD tissue were not associated with breast cancer risk

Methods

Results

Conclusion