Inducible Knockout of 14-3-3β Attenuates Proliferation and Spheroid Formation in a Human Glioblastoma Cell Line U87MG

Author:

Gallo Kellie1,Srinageshwar Bhairavi23ORCID,Ward Avery3,Diola Carlos3ORCID,Dunbar Gary24,Rossignol Julien123ORCID,Bakke Jesse12

Affiliation:

1. Biochemistry, Cellular, and Molecular Biology, College of Science and Engineering, Central Michigan University, Mount Pleasant, MI 48559, USA

2. Program of Neuroscience, Central Michigan University, Mount Pleasant, MI 48859, USA

3. Foundational Sciences Department, College of Medicine, Central Michigan University, Mount Pleasant, MI 48859, USA

4. Department of Psychology, Central Michigan University, Mount Pleasant, MI 48859, USA

Abstract

Glioblastomas (GBs) are the most common and malignant brain tumors in adults. A protein encoded by the gene YWHAB, 14-3-3β, is commonly found to be upregulated throughout the initiation and progression of GB. The 14-3-3β has oncogenic roles in several different types of cancer cells through interactions with proteins such as Bad, FBI1, Raf-1, Cdc25b, and others. Previous RNA interference studies have shown that 14-3-3β promotes proliferation, cell cycle progression, and migration and invasion of GB cells. However, despite the many oncogenic functions of 14-3-3β, a CRISPR/Cas9 knockout model of 14-3-3β has not been investigated. This study confirmed previous findings and showed that siRNA inhibition of 14-3-3β results in reduced cellular proliferation in a human glioblastoma cell line, U87MG. We also used a YWHAB Tet-On CRISPR/Cas9 U87MG cell line that, upon doxycycline induction, leads to robust Cas9 expression and subsequent knockout of 14-3-3β. Using this model, we show that loss of 14-3-3β significantly reduces cellular proliferation and spheroid formation of U87MG cells.

Funder

Central Michigan University College of Medicine

Office of Research and Graduate Studies at Central Michigan University for an Graduate Research Grant

John G. Kulhavi Professorship

E. Malcolm Field Endowed Chair in Neuroscience

Publisher

MDPI AG

Subject

General Neuroscience

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