Src binds cortactin through an SH2 domain cystine-mediated linkage

Evans, Jason V.; Ammer, Amanda G.; Jett, John E.; Bolcato, Chris A.; Breaux, Jason C.; Martin, Karen H.; Culp, Mark V.; Gannett, Peter M.; Weed, Scott A.

doi:10.1242/jcs.121046

Cited by 25 publications

(17 citation statements)

References 73 publications

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“…The contribution of p38 MAPK to the pathogenesis of pemphigus vulgaris is well established (32,33) and previous studies placed p38 MAPK upstream of RhoA in this context (16,18). However, treatment of keratinocytes with the p38 MAPK inhibitor SB202190 for 30 min did not change ␣-adducin phosphorylation (Fig.…”

Section: Volume 289 • Number 21 • May 23 2014mentioning

confidence: 66%

Adducin Is Required for Desmosomal Cohesion in Keratinocytes

Rötzer

Breit

Waschke

et al. 2014

Journal of Biological Chemistry

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Background:The cortical actin cytoskeleton is necessary for keratinocyte adhesion by unclear mechanisms. Results: The actin-binding protein adducin modulates desmosomal adhesion and is a target of protective PKC phosphorylation in response to autoantibodies of the blistering skin disease pemphigus. Conclusion: Adducin promotes adhesion by regulating desmosomes and is part of a protective pathway in pemphigus. Significance: Novel mechanism how cortical actin modulates desmosomal adhesion.

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Section: Volume 289 • Number 21 • May 23 2014mentioning

confidence: 66%

Adducin Is Required for Desmosomal Cohesion in Keratinocytes

Rötzer

Breit

Waschke

et al. 2014

Journal of Biological Chemistry

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“…Perhaps Cdc42-driven N-WASP activation is sufficient, and further enhancement regulated by cortactin phosphorylation is not necessary. Alternatively, a recent report described phosphorylation-independent interactions between cortactin and SH2 domains of its binding partners, suggesting that cortactin phosphorylation may not be required for its effects [32]. …”

Section: Resultsmentioning

confidence: 99%

Vav1 as a Central Regulator of Invadopodia Assembly

et al. 2014

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Summary Invadopodia are protrusive structures used by tumor cells for degradation of the extracellular matrix to promote invasion [1]. Invadopodia formation and function are regulated by cytoskeletal remodeling pathways and the oncogenic kinase Src. The guanine nucleotide exchange factor Vav1, which is an activator of Rho family GTPases, is ectopically expressed in many pancreatic cancers, where it promotes tumor cell survival and migration [2, 3]. We have now determined that Vav1 is also a potent regulator of matrix degradation by pancreatic tumor cells, as depletion of Vav1 by siRNA-mediated knockdown inhibits the formation of invadopodia. This requires the exchange function of Vav1 toward the GTPase Cdc42, which is required for invadopodia assembly [4, 5]. In addition, we have determined that Src-mediated phosphorylation and activation of Vav1 is both required for, and, unexpectedly, sufficient for, invadopodia formation. Expression of Vav1 Y174F, which mimics its activated state, is a potent inducer of invadopodia formation through Cdc42, even in the absence of Src activation and phosphorylation of other Src substrates, such as cortactin. Thus, these data identify a novel mechanism by which Vav1 can enhance the tumorigenicity and invasive potential of cancer cells. These data suggest that Vav1 promotes the matrix-degrading processes underlying tumor cell migration, and further, under conditions of ectopic Vav1 expression, that Vav1 is a central regulator and major driver of invasive matrix remodeling by pancreatic tumor cells.

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“…The shRNA/siRNAs expressing constructs against NEDD9, HDAC6, AURKA, CTTN and the control were purchased from ThermoFisher Scientific (sequences available upon request). Mouse wild type, C- and N-term CTTN truncation mutant constructs were previously described (31). The acetylation-null 9KR cortactin construct was generated by site-directed mutagenesis using full-length mouse cortactin.…”

Section: Methodsmentioning

confidence: 99%

NEDD9 Regulates Actin Dynamics through Cortactin Deacetylation in an AURKA/HDAC6–Dependent Manner

Kozyreva

McLaughlin

Livengood

et al. 2014

Molecular Cancer Research

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The prometastatic protein NEDD9 (Neural precursor cell Expressed, Developmentally Down-regulated 9) is highly expressed in many cancers and is required for mesenchymal individual cell migration and progression to the invasive stage. Nevertheless, the molecular mechanisms of NEDD9-driven migration and the downstream targets effecting metastasis are not well defined. In the current study, knockdown of NEDD9 in highly metastatic tumor cells drastically reduces their migratory capacity due to disruption of actin dynamics at the leading edge. Specifically, NEDD9 deficiency leads to a decrease in the persistence and stability of lamellipodial protrusions similar to knockdown of cortactin (CTTN). Mechanistically, it was shown that NEDD9 binds to and regulates acetylation of CTTN in an Aurora A kinase (AURKA)/HDAC6-dependent manner. The knockdown of NEDD9 or AURKA results in an increase in the amount of acetylated CTTN and a decrease in the binding of CTTN to F-actin. Overexpression of the deacetylation mimicking (9KR) mutant of CTTN is sufficient to restore actin dynamics at the leading edge and migration proficiency of the tumor cells. Inhibition of AURKA and HDAC6 activity by Alisertib and Tubastatin A in xenograft models of breast cancer leads to a decrease in the number of pulmonary metastases. Collectively, these findings identify CTTN as the key downstream component of NEDD9-driven migration and metastatic phenotypes. Implications This study provides a mechanistic platform for therapeutic interventions based on AURKA and HDAC6 inhibition for metastatic breast cancer patients to prevent and/or eradicate metastases.

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Src binds cortactin through an SH2 domain cystine-mediated linkage

Cited by 25 publications

References 73 publications

Adducin Is Required for Desmosomal Cohesion in Keratinocytes

Adducin Is Required for Desmosomal Cohesion in Keratinocytes

Vav1 as a Central Regulator of Invadopodia Assembly

NEDD9 Regulates Actin Dynamics through Cortactin Deacetylation in an AURKA/HDAC6–Dependent Manner

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