6q Deletion is Frequent but Unrelated to Patient Prognosis in Breast Cancer

Overview

Journal Breast Cancer

Specialty Oncology

Date 2021 Oct 9

PMID 34625909

Citations 1

Authors

Patrick Lebok

Hannah Bonte

Martina Kluth

Christina Moller-Koop

Isabell Witzel

Linn Wolber

Peter Paluchowski

Christian Wilke

Uwe Heilenkotter

Volkmar Muller

Barbara Schmalfeldt

Ronald Simon

Guido Sauter

Luigi Terracciano

Rainer Horst Krech

Albert von der Assen

Eike Burandt

Affiliations

Soon will be listed here.

Abstract

Background: Deletions involving the long arm of chromosome 6 have been reported to occur in breast cancer, but little is known about the clinical relevance of this alteration.

Methods: We made use of a pre-existing tissue microarray with 2197 breast cancers and employed a 6q15/centromere 6 dual-labeling probe for fluorescence in situ (FISH) analysis RESULTS: Heterozygous 6q15 deletions were found in 202 (18%) of 1099 interpretable cancers, including 19% of 804 cancers of no special type (NST), 3% of 29 lobular cancers, 7% of 41 cribriform cancers, and 28% of 18 cancers with papillary features. Homozygous deletions were not detected. In the largest subset of NST tumors, 6q15 deletions were significantly linked to advanced tumor stage and high grade (p < 0.0001 each). 6q deletions were also associated with estrogen receptor negativity (p = 0.0182), high Ki67 proliferation index (p < 0.0001), amplifications of HER2 (p = 0.0159), CCND1 (p = 0.0069), and cMYC (p = 0.0411), as well as deletions of PTEN (p = 0.0003), 8p21 (p < 0.0001), and 9p21 (p = 0.0179). However, 6q15 deletion was unrelated to patient survival in all cancers, in NST cancers, or in subsets of cancers defined by the presence or absence of lymph-node metastases.

Conclusion: Our data demonstrate that 6q deletion is a frequent event in breast cancer that is statistically linked to unfavorable tumor phenotype and features of genomic instability. The absence of any prognostic impact argues against a clinical applicability of 6q15 deletion testing in breast cancer patients.

Citing Articles

Genetic inconsistency at the D6S1043 locus caused by microdeletion at 6q15.

Wu H, Zhang L, Fan A, Wu H, Wang K Int J Legal Med. 2023; 137(5):1413-1419.

PMID: 37414920 DOI: 10.1007/s00414-023-03044-8.

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