FSBP suppresses tumor cell migration by inhibiting the JNK pathway

Fangyu Song; Wenshuo Zhang; Xiaohui Li; Xiaoqing Chen; Xuejun Yuan; Mingjin Jiang; Yunhe Zhao; Qingxin Liu; Zizhang Zhou

iScience (Apr 2023)

FSBP suppresses tumor cell migration by inhibiting the JNK pathway

Fangyu Song,
Wenshuo Zhang,
Xiaohui Li,
Xiaoqing Chen,
Xuejun Yuan,
Mingjin Jiang,
Yunhe Zhao,
Qingxin Liu,
Zizhang Zhou

Affiliations

Fangyu Song: College of Life Sciences, Shandong Agricultural University, Tai’an 271018, China
Wenshuo Zhang: College of Life Sciences, Shandong Agricultural University, Tai’an 271018, China; Fang Zongxi Center, MoE Key Laboratory of Marine Genetics and Breeding, College of Marine Life Sciences, Ocean University of China, Qingdao, China
Xiaohui Li: College of Life Sciences, Shandong Agricultural University, Tai’an 271018, China
Xiaoqing Chen: College of Life Sciences, Shandong Agricultural University, Tai’an 271018, China
Xuejun Yuan: College of Life Sciences, Shandong Agricultural University, Tai’an 271018, China
Mingjin Jiang: Jiangxi Provincial Institute of Translational Medicine, The First Affiliated Hospital of Nanchang University, Nanchang, China
Yunhe Zhao: College of Life Sciences, Shandong Agricultural University, Tai’an 271018, China; Corresponding author
Qingxin Liu: College of Life Sciences, Shandong Agricultural University, Tai’an 271018, China; Corresponding author
Zizhang Zhou: College of Life Sciences, Shandong Agricultural University, Tai’an 271018, China; Corresponding author

Journal volume & issue: Vol. 26, no. 4
p. 106440

Abstract

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Summary: The main cause of high mortality in cancer patients is tumor metastasis. Exploring the underlying mechanism of tumor metastasis is of great significance for clinical treatments. Here, we identify the transcription factor Apt/FSBP is a suppressor for tumor metastasis. In Drosophila wing disc, knockdown of apt is able to trigger cell migration, whereas overexpression of apt hampers scrib-RNAi-induced tumor cell migration. Further studies show that loss of apt promotes cell migration through activating the JNK pathway. To investigate the role of FSBP, the homolog of Apt in mammals, we construct Fsbp liver-specific knockout mice. Knockout of Fsbp in liver does not cause any detectable physiological defects, but predisposes to tumorigenesis on DEN and CCl4 treatment. In addition, loss of Fsbp accelerates tumor metastasis from liver to diaphragm. Taken together, this study uncovers FSBP is a novel tumor suppressor, and provides it as a considerable drug target for tumor treatment.

Published in iScience

ISSN: 2589-0042 (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Science
Website: http://www.cell.com/iscience/home

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