Keratin 19 Regulates Cell Cycle Pathway and Sensitivity of Breast Cancer Cells to CDK Inhibitors

Overview

Journal Sci Rep

Specialty Science

Date 2019 Oct 12

PMID 31601969

Citations 19

Authors

Pooja Sharma

Sarah Alsharif

Karina Bursch

Swetha Parvathaneni

Dimitrios G Anastasakis

Joeffrey Chahine

Arwa Fallatah

Kevin Nicolas

Sudha Sharma

Markus Hafner

Bhaskar Kallakury

Byung Min Chung

Affiliations

Soon will be listed here.

Abstract

Keratin 19 (K19) belongs to the keratin family of proteins, which maintains structural integrity of epithelia. In cancer, K19 is highly expressed in several types where it serves as a diagnostic marker. Despite the positive correlation between higher expression of K19 in tumor and worse patient survival, the role of K19 in breast cancer remains unclear. Therefore, we ablated K19 expression in MCF7 breast cancer cells and found that K19 was required for cell proliferation. Transcriptome analyses of KRT19 knockout cells identified defects in cell cycle progression and levels of target genes of E2F1, a key transcriptional factor for the transition into S phase. Furthermore, proper levels of cyclin dependent kinases (CDKs) and cyclins, including D-type cyclins critical for E2F1 activation, were dependent on K19 expression, and K19-cyclin D co-expression was observed in human breast cancer tissues. Importantly, K19 interacts with cyclin D3, and a loss of K19 resulted in decreased protein stability of cyclin D3 and sensitivity of cells towards CDK inhibitor-induced cell death. Overall, these findings reveal a novel function of K19 in the regulation of cell cycle program and suggest that K19 may be used to predict the efficacy of CDK inhibitors for treatments of breast cancer.

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