Kank regulates RhoA-dependent formation of actin stress fibers and cell migration via 14-3-3 in PI3K–Akt signaling

Kakinuma, Naoto; Roy, Badal C.; Zhu, Yun; Wang, Yong; Kiyama, Ryoiti

doi:10.1083/jcb.200707022

Cited by 102 publications

(110 citation statements)

References 60 publications

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“…Other 14-3-3 family members were shown previously to regulate intermediate filament architecture by functioning as K8/K18 solubility cofactors in a PKCζ-dependent mechanism (40)(41)(42). In addition, a number of studies have highlighted different mechanisms by which 14-3-3 family members regulate actin dynamics either through stabilizing cofilin phosphorylation or by inhibiting signals through the AKT-RhoA pathway (12,(43)(44)(45).…”

Section: Discussionmentioning

confidence: 99%

14-3-3σ stabilizes a complex of soluble actin and intermediate filament to enable breast tumor invasion

Boudreau

Tanner

Wang

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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Significance We characterize a mechanism by which 14-3-3σ directs cell migration and tumor invasion through regulating cytoskeletal solubility and dynamics. Our data suggest that 14-3-3σ expression, rather than being a tumor suppressor, in fact, aids in breast tumor invasion at least in a subset of carcinomas. Our findings warrant further investigation into the role of this molecule in normal mammary gland and breast tumors and, indeed, in epithelial tissues and tumors where 14-3-3σ is expressed.

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Section: Discussionmentioning

confidence: 99%

14-3-3σ stabilizes a complex of soluble actin and intermediate filament to enable breast tumor invasion

Boudreau

Tanner

Wang

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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“…40 This stimulates the formation of actin stress fibers through the activation of RhoA. 41 Therefore, PI3K signaling evoked by truncated Tie2 ( Figure 5) may be involved in the formation of actin stress fibers in endothelial cells ( Figure 6A), leading to endothelial cell retraction. Third, when epithinexpressing cells escape the vasculature, the matrix-degrading activity of epithin 19 can generate a pathway for the cells to invade further into the layers of the extracellular matrix.…”

Section: Roles Of Epithin-mediated Tie2 Regulation In Transendotheliamentioning

confidence: 99%

Epithin/PRSS14 proteolytically regulates angiopoietin receptor Tie2 during transendothelial migration

Kim

Lee

et al. 2011

Blood

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“…Recently, we found that liprin-b1 interacts with KANK1 (van der Vaart et al, 2013), one of the four members of the KANK family of proteins, which were proposed to act as tumor suppressors and regulators of cell polarity and migration through Rho GTPase signaling (Gee et al, 2015;Kakinuma et al, 2008Li et al, 2011;Roy et al, 2009). KANK1 recruits the kinesin-4 KIF21A to CMSCs, which inhibits microtubule polymerization and prevents microtubule overgrowth at the cell edge van der Vaart et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

Talin-KANK1 interaction controls the recruitment of cortical microtubule stabilizing complexes to focal adhesions

Bouchet

Gough

Willige

et al. 2016

Preprint

108

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The cross-talk between dynamic microtubules and integrin-based adhesions to the extracellular matrix plays a crucial role in cell polarity and migration. Microtubules regulate the turnover of adhesion sites, and, in turn, focal adhesions promote the cortical microtubule capture and stabilization in their vicinity, but the underlying mechanism is unknown. Here, we show that cortical microtubule stabilization sites containing CLASPs, KIF21A, LL5b and liprins are recruited to focal adhesions by the adaptor protein KANK1, which directly interacts with the major adhesion component, talin. Structural studies showed that the conserved KN domain in KANK1 binds to the talin rod domain R7. Perturbation of this interaction, including a single point mutation in talin, which disrupts KANK1 binding but not the talin function in adhesion, abrogates the association of microtubule-stabilizing complexes with focal adhesions. We propose that the talin-KANK1 interaction links the two macromolecular assemblies that control cortical attachment of actin fibers and microtubules.

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Kank regulates RhoA-dependent formation of actin stress fibers and cell migration via 14-3-3 in PI3K–Akt signaling

Cited by 102 publications

References 60 publications

14-3-3σ stabilizes a complex of soluble actin and intermediate filament to enable breast tumor invasion

14-3-3σ stabilizes a complex of soluble actin and intermediate filament to enable breast tumor invasion

Epithin/PRSS14 proteolytically regulates angiopoietin receptor Tie2 during transendothelial migration

Talin-KANK1 interaction controls the recruitment of cortical microtubule stabilizing complexes to focal adhesions

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