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A functional dissection of PTEN N-terminus: implications in PTEN subcellular targeting and tumor suppressor activity.

机译:PTEN N末端的功能解剖:对PTEN亚细胞靶向和肿瘤抑制活性的影响。

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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.
机译:抑癌基因PTEN的空间调节是通过其他质膜,胞质和核亚细胞位置来实现的。 PTEN的N端区域对于控制PTEN亚细胞定位和功能很重要。它既包含活性核定位信号(NLS),又包含参与质膜靶向的重叠PIP2结合基序(PBM)。我们报告了P​​TEN N末端的全面的突变和功能分析,包括该区域的一组与肿瘤相关的突变。重组酿酒酵母中哺乳动物细胞中的核/细胞质分配和PIP3磷酸酶测定确定了具有不同PIP3磷酸酶和核积累特性的PTEN N末端突变类别。值得注意的是,大多数失去PIP3磷酸酶活性的肿瘤相关突变也显示出受损的核定位。哺乳动物细胞中具有独特核积累和催化活性模式的突变的细胞增殖和软琼脂菌落形成分析表明,这两种特性均对PTEN肿瘤抑制活性有贡献。我们对PTEN N末端的功能解剖为系统分析肿瘤相关和实验改造的PTEN突变提供了基础。

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