A Functional Dissection of PTEN N-Terminus: Implications in PTEN Subcellular Targeting and Tumor Suppressor Activity

被引:24
作者
Gil, Anabel [1 ,3 ]
Rodriguez-Escudero, Isabel [2 ]
Stumpf, Miriam [1 ,3 ,4 ]
Molina, Maria [2 ]
Cid, Victor J. [2 ]
Pulido, Rafael [5 ,6 ]
机构
[1] Ctr Invest Principe Felipe, Valencia, Spain
[2] Univ Complutense Madrid, Fac Farm, Dept Microbiol 2, Madrid, Spain
[3] Inst Ramon & Cajal Invest Sanitarias IRYCIS, Madrid, Spain
[4] Hubrecht Inst, Utrecht, Netherlands
[5] BioCruces Hlth Res Inst, Baracaldo, Spain
[6] Ikerbasque, Basque Fdn Sci, E-48011 Bilbao, Spain
关键词
NUCLEAR PTEN; PHOSPHATIDYLINOSITOL 4,5-BISPHOSPHATE; MEMBRANE ASSOCIATION; PHOSPHATASE-ACTIVITY; BINDING MOTIF; PROTEIN; CANCER; LOCALIZATION; ACTIVATION; CELLS;
D O I
10.1371/journal.pone.0119287
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Spatial regulation of the tumor suppressor PTEN is exerted through alternative plasma membrane, cytoplasmic, and nuclear subcellular locations. The N-terminal region of PTEN is important for the control of PTEN subcellular localization and function. It contains both an active nuclear localization signal (NLS) and an overlapping PIP2-binding motif (PBM) involved in plasma membrane targeting. We report a comprehensive mutational and functional analysis of the PTEN N-terminus, including a panel of tumor-related mutations at this region. Nuclear/cytoplasmic partitioning in mammalian cells and PIP3 phosphatase assays in reconstituted S. cerevisiae defined categories of PTEN N-terminal mutations with distinct PIP3 phosphatase and nuclear accumulation properties. Noticeably, most tumor-related mutations that lost PIP3 phosphatase activity also displayed impaired nuclear localization. Cell proliferation and soft-agar colony formation analysis in mammalian cells of mutations with distinctive nuclear accumulation and catalytic activity patterns suggested a contribution of both properties to PTEN tumor suppressor activity. Our functional dissection of the PTEN N-terminus provides the basis for a systematic analysis of tumor-related and experimentally engineered PTEN mutations.
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页数:18
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