Eribulin induces micronuclei and enhances the nuclear localization of cGAS in triple-negative breast cancer cells

Author:

Yamada Hideyuki1,Takada Mamoru1,Ghone Dhaval2,Yu Muhan1,Nagashima Takeshi1,Fujimoto Hiroshi1,Sakakibara Junta1,Hasegawa Yoshie3,Takao Shintaro4,Yamada Akimitsu5,Narui Kazutaka6,Ishikawa Takashi7,Suzuki Aussie2,Otsuka Masayuki1

Affiliation:

1. Chiba University

2. University of Wisconsin–Madison

3. Hachinohe City Hospital

4. Konan Medical Center

5. Yokohama City University

6. Yokohama City University Medical Center

7. Tokyo Medical University

Abstract

Abstract Eribulin (ERI), clinically utilized for locally advanced or metastatic breast tumors, has shown potential links to the immune system. Notably, the cGAS-STING pathway, a key component of innate immunity, has gained prominence. Yet, limited reports explore ERI's effects on the cGAS-STING pathway. Additionally, the nuclear presence of cGAS remains poorly understood. This study uniquely delves into ERI's impact on both the cytosolic cGAS-STING pathway and nuclear cGAS. ERI enhances nuclear localization of cGAS, resulting in hyper-activation of the cGAS-STING pathway in triple-negative breast cancer cells. Reduction of cGAS heightened both cell proliferation and ERI sensitivity. In clinical data using ERI in a neo-adjuvant setting, patients with low cGAS cases exhibited reduced likelihood of achieving pathological complete response after ERI treatment. These findings illuminate the potential of cGAS and IFNβ as predictive biomarkers for ERI sensitivity, providing valuable insights for personalized breast cancer treatment strategies.

Publisher

Research Square Platform LLC

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