A Highlights from MBoC Selection: LKB1 kinase-dependent and -independent defects disrupt polarity and adhesion signaling to drive collagen remodeling during invasion

Jessica Konen; Scott Wilkinson; Byoungkoo Lee; Haian Fu; Wei Zhou; Yi Jiang; Adam I. Marcus

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A Highlights from MBoC Selection: LKB1 kinase-dependent and -independent defects disrupt polarity and adhesion signaling to drive collagen remodeling during invasion

机译：MBoC选择的亮点：LKB1激酶依赖性和非依赖性缺陷会破坏极性和粘附信号，从而在入侵过程中驱动胶原蛋白重塑

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LKB1 is a serine/threonine kinase and a commonly mutated gene in lung adenocarcinoma. The majority of LKB1 mutations are truncations that disrupt its kinase activity and remove its C-terminal domain (CTD). Because LKB1 inactivation drives cancer metastasis in mice and leads to aberrant cell invasion in vitro, we sought to determine how compromised LKB1 function affects lung cancer cell polarity and invasion. Using three-dimensional models, we show that LKB1 kinase activity is essential for focal adhesion kinase–mediated cell adhesion and subsequent collagen remodeling but not cell polarity. Instead, cell polarity is overseen by the kinase-independent function of its CTD and more specifically its farnesylation. This occurs through a mesenchymal-amoeboid morphological switch that signals through the Rho-GTPase RhoA. These data suggest that a combination of kinase-dependent and -independent defects by LKB1 inactivation creates a uniquely invasive cell with aberrant polarity and adhesion signaling that drives invasion into the microenvironment.

机译：LKB1是丝氨酸/苏氨酸激酶，是肺腺癌中常见的突变基因。大多数LKB1突变是截断，会破坏其激酶活性并去除其C末端结构域（CTD）。因为LKB1失活驱动小鼠的癌症转移并导致体外细胞异常侵袭，所以我们试图确定受损的LKB1功能如何影响肺癌细胞的极性和侵袭。使用三维模型，我们显示LKB1激酶活性对于粘着斑激酶介导的细胞粘附和随后的胶原重塑（而不是细胞极性）至关重要。取而代之的是，细胞的极性由其CTD的激酶独立功能（特别是其法呢基化）监督。这是通过通过Rho-GTPase RhoA发出信号的间质-类腺形态转换发生的。这些数据表明，通过LKB1失活，激酶依赖性和非依赖性缺陷的组合产生了具有异常极性和粘附信号的独特侵袭性细胞，其驱动侵袭进入微环境。

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《Cell Regulation》 |2016年第7期|共16页
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Jessica Konen; Scott Wilkinson; Byoungkoo Lee; Haian Fu; Wei Zhou; Yi Jiang; Adam I. Marcus;
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1. LKB1 kinase-dependent and -independent defects disrupt polarity and adhesion signaling to drive collagen remodeling during invasion [J] . Konen Jessica, Wilkinson Scott, Lee Byoungkoo, Molecular biology of the cell . 2016,第7期

机译：LKB1激酶依赖性和非依赖性缺陷可破坏极性和粘附信号，从而在入侵过程中驱动胶原蛋白重塑
2. A Highlights from MBoC Selection: Adenomatous Polyposis Coli Regulates Endothelial Cell Migration Independent of Roles in β-Catenin Signaling and Cell–Cell Adhesion [J] . Elizabeth S. Harris, W. James Nelson Molecular biology of the cell . 2010,第15期

机译：MBoC选择的亮点：腺瘤性息肉病可调节内皮细胞迁移，而独立于β-Catenin信号传导和细胞间粘附的作用
3. A Highlights from MBoC Selection: γ-Tubulin controls neuronal microtubule polarity independently of Golgi outposts [J] . Michelle M. Nguyen, Christie J. McCracken, E. S. Milner, Molecular biology of the cell . 2014,第13期

机译：MBoC选择的亮点：γ-微管蛋白独立于高尔基体前哨控制神经元微管极性
4. A Highlights from MBoC Selection: LKB1 kinase-dependent and -independent defects disrupt polarity and adhesion signaling to drive collagen remodeling during invasion [O] . Jessica Konen, Scott Wilkinson, Byoungkoo Lee, 2016

机译：MBoC选择的亮点：LKB1激酶依赖性和非依赖性缺陷会破坏极性和粘附信号从而在入侵过程中驱动胶原蛋白重塑
5. LKB1 kinase-dependent and -independent defects disrupt polarity and adhesion signaling to drive collagen remodeling during invasion [O] . Jessica Konen, Scott Wilkinson, Byoungkoo Lee, 2016

机译：LKB1激酶依赖性和依赖性缺陷破坏极性和粘合信号，以在侵袭过程中驱动胶原蛋白重塑

A Highlights from MBoC Selection: LKB1 kinase-dependent and -independent defects disrupt polarity and adhesion signaling to drive collagen remodeling during invasion

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