Clinicopathologic and genetic analysis of invasive breast carcinomas in women with germline CHEK2 variants.

Christopher J Schwartz Nikka Khorsandi Amie Blanco Rita A Mukhtar Yunn-Yi Chen Gregor Krings

Breast Cancer Res Treat

Department of Pathology, University of California San Francisco (UCSF), 1825 4th Street, San Francisco, CA, 94143, USA.

Published: February 2024

CHEK2 germline variants are linked to a moderate increase in breast cancer risk, primarily affecting younger women, with a median age of 45.
The study analyzed 44 CHEK2-associated breast cancer cases, finding that most tumors were invasive ductal carcinomas (86%) and predominantly estrogen receptor positive (95%).
Despite variable responses to chemotherapy, 85% of patients remained disease-free during the follow-up, although some experienced metastasis, and one patient died over an average follow-up period of 50 months.

Purpose: Germline pathogenic variants in checkpoint kinase 2 (CHEK2) are associated with a moderately increased risk of breast cancer (BC). The spectrum of clinicopathologic features and genetics of these tumors has not been fully established.

Methods: We characterized the histopathologic and clinicopathologic features of 44 CHEK2-associated BCs from 35 women, and assessed responses to neoadjuvant chemotherapy. A subset of cases (n = 23) was additionally analyzed using targeted next-generation DNA sequencing (NGS).

Results: Most (94%, 33/35) patients were heterozygous carriers for germline CHEK2 variants, and 40% had the c.1100delC allele. Two patients were homozygous, and five had additional germline pathogenic variants in ATM (2), PALB2 (1), RAD50 (1), or MUTYH (1). CHEK2-associated BCs occurred in younger women (median age 45 years, range 25-75) and were often multifocal (20%) or bilateral (11%). Most (86%, 38/44) were invasive ductal carcinomas of no special type (IDC-NST). Almost all (95%, 41/43) BCs were ER + (79% ER + HER2-, 16% ER + HER2 + , 5% ER-HER2 +), and most (69%) were luminal B. Nottingham grade, proliferation index, and results of multiparametric molecular testing were heterogeneous. Biallelic CHEK2 alteration with loss of heterozygosity was identified in most BCs (57%, 13/23) by NGS. Additional recurrent alterations included GATA3 (26%), PIK3CA (226%), CCND1 (22%), FGFR1 (22%), ERBB2 (17%), ZNF703 (17%), TP53 (9%), and PPM1D (9%), among others. Responses to neoadjuvant chemotherapy were variable, but few patients (21%, 3/14) achieved pathologic complete response. Most patients (85%) were without evidence of disease at time of study (n = 34). Five patients (15%) developed distant metastasis, and one (3%) died (mean follow-up 50 months).

Conclusion: Almost all CHEK2-associated BCs were ER + IDC-NST, with most classified as luminal B with or without HER2 overexpression. NGS supported the luminal-like phenotype and confirmed CHEK2 as an oncogenic driver in the majority of cases. Responses to neoadjuvant chemotherapy were variable but mostly incomplete.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10806021	PMC
http://dx.doi.org/10.1007/s10549-023-07176-8	DOI Listing

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