PTENε suppresses tumor metastasis through regulation of filopodia formation |
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| Authors: | Qiaoling Zhang Hui Liang Xuyang Zhao Lin Zheng Yunqiao Li Jingjing Gong Yizhang Zhu Yan Jin Yuxin Yin |
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| Institution: | 1. Department of Pathology, School of Basic Medical Sciences, Institute of Systems Biomedicine, Beijing Key Laboratory of Tumor Systems Biology, Peking‐Tsinghua Center of Life Sciences, Peking University Health Science Center, Beijing China ; 2. Institute of Precision Medicine, Peking University Shenzhen Hospital, Shenzhen China |
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| Abstract: | PTEN is one of the most frequently mutated genes in malignancies and acts as a powerful tumor suppressor. Tumorigenesis is involved in multiple and complex processes including initiation, invasion, and metastasis. The complexity of PTEN function is partially attributed to PTEN family members such as PTENα and PTENβ. Here, we report the identification of PTENε (also named as PTEN5), a novel N‐terminal‐extended PTEN isoform that suppresses tumor invasion and metastasis. We show that the translation of PTENε/PTEN5 is initiated from the CUG816 codon within the 5′UTR region of PTEN mRNA. PTENε/PTEN5 mainly localizes in the cell membrane and physically associates with and dephosphorylates VASP and ACTR2, which govern filopodia formation and cell motility. We found that endogenous depletion of PTENε/PTEN5 promotes filopodia formation and enhances the metastasis capacity of tumor cells. Overall, we identify a new isoform of PTEN with distinct subcellular localization and molecular function compared to the known members of the PTEN family. These findings advance our current understanding of the importance and diversity of PTEN functions. |
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| Keywords: | alternative initiation filopodia formation metastasis PTEN5 PTENε |
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