DNA Damage Induces the Accumulation of Tiam1 by Blocking β-TrCP-dependent Degradation

Zhu, Guixin; Fan, Zhongyun; Ding, Miao; Mu, Libing; Liang, Juan Boo; Ding, Yuchuan; Fu, Yu; Huang, Biao; Wu, Wei

doi:10.1074/jbc.m114.553388

Cited by 14 publications

(17 citation statements)

References 57 publications

(71 reference statements)

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“…Interestingly, it has been recently reported that constitutive mTOR-S6K signaling sensitizes cells to p53-dependent cell death in response to stress conditions (33). In agreement with these studies, a recent report has shown that cells expressing the degradation-resistant Tiam1-C1199 mutant are more sensitive to DNA-damaging drug-induced apoptosis (34).…”

Section: Discussionsupporting

confidence: 76%

Degradation of Tiam1 by Casein Kinase 1 and the SCFβTrCP Ubiquitin Ligase Controls the Duration of mTOR-S6K Signaling

Magliozzi

Kim

Low

et al. 2014

Journal of Biological Chemistry

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Section: Discussionsupporting

confidence: 76%

Degradation of Tiam1 by Casein Kinase 1 and the SCFβTrCP Ubiquitin Ligase Controls the Duration of mTOR-S6K Signaling

Magliozzi

Kim

Low

et al. 2014

Journal of Biological Chemistry

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“…This prompted us to investigate whether TIAM1 was a component of the WNT-regulated destruction complex. By immunoprecipitating endogenous TIAM1 from cytosolic and nuclear fractions of confluent HEK293 cells, which carry a functional destruction complex, we found that TIAM1 interacted with AXIN, β-catenin, and (as shown previously by Magliozzi et al., 2014, Zhu et al., 2014, and above) βTrCP, which are established elements of the destruction complex as well as TAZ and YAP (Figure 5A). Even though low levels of TIAM1 were detected in the nucleus, TIAM1 interaction with AXIN, β-catenin, βTrCP, TAZ, and YAP was observed only in the cytoplasm of HEK293 cells.…”

Section: Resultsmentioning

confidence: 99%

TIAM1 Antagonizes TAZ/YAP Both in the Destruction Complex in the Cytoplasm and in the Nucleus to Inhibit Invasion of Intestinal Epithelial Cells

et al. 2017

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SummaryAberrant WNT signaling drives colorectal cancer (CRC). Here, we identify TIAM1 as a critical antagonist of CRC progression through inhibiting TAZ and YAP, effectors of WNT signaling. We demonstrate that TIAM1 shuttles between the cytoplasm and nucleus antagonizing TAZ/YAP by distinct mechanisms in the two compartments. In the cytoplasm, TIAM1 localizes to the destruction complex and promotes TAZ degradation by enhancing its interaction with βTrCP. Nuclear TIAM1 suppresses TAZ/YAP interaction with TEADs, inhibiting expression of TAZ/YAP target genes implicated in epithelial-mesenchymal transition, cell migration, and invasion, and consequently suppresses CRC cell migration and invasion. Importantly, high nuclear TIAM1 in clinical specimens associates with increased CRC patient survival. Together, our findings suggest that in CRC TIAM1 suppresses tumor progression by regulating YAP/TAZ activity.

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“…However, we do not fully understand how this RAC1 activator is locally turned off again. For example, CUL1 SKP1/BTRC was shown to regulate TIAM1 (Magliozzi et al, 2014;Zhu et al, 2014), though its ubiquitylation and proteasomal degradation involved total protein amounts and not a subcellular pool of TIAM1. Our results expand the concept of spatially restricted regulation to TIAM1.…”

Section: Discussionmentioning

confidence: 98%

CUL3-KBTBD6/KBTBD7 Ubiquitin Ligase Cooperates with GABARAP Proteins to Spatially Restrict TIAM1-RAC1 Signaling

et al. 2015

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The small Rho GTPase RAC1 is an essential regulator of cellular signaling that controls actin rearrangements and cell motility. Here, we identify a novel CUL3 RING ubiquitin ligase complex, containing the substrate adaptors KBTBD6 and KBTBD7, that mediates ubiquitylation and proteasomal degradation of TIAM1, a RAC1-specific GEF. Increasing the abundance of TIAM1 by depletion of KBTBD6 and/or KBTBD7 leads to elevated RAC1 activity, changes in actin morphology, loss of focal adhesions, reduced proliferation, and enhanced invasion. KBTBD6 and KBTBD7 employ ATG8 family-interacting motifs to bind preferentially to GABARAP proteins. Surprisingly, ubiquitylation and degradation of TIAM1 by CUL3(KBTBD6/KBTBD7) depends on its binding to GABARAP proteins. Our study reveals that recruitment of CUL3(KBTBD6/KBTBD7) to GABARAP-containing vesicles regulates the abundance of membrane-associated TIAM1 and subsequently spatially restricted RAC1 signaling. Besides their role in autophagy and trafficking, we uncovered a previously unknown function of GABARAP proteins as membrane-localized signaling scaffolds.

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DNA Damage Induces the Accumulation of Tiam1 by Blocking β-TrCP-dependent Degradation

Cited by 14 publications

References 57 publications

Degradation of Tiam1 by Casein Kinase 1 and the SCFβTrCP Ubiquitin Ligase Controls the Duration of mTOR-S6K Signaling

Degradation of Tiam1 by Casein Kinase 1 and the SCFβTrCP Ubiquitin Ligase Controls the Duration of mTOR-S6K Signaling

TIAM1 Antagonizes TAZ/YAP Both in the Destruction Complex in the Cytoplasm and in the Nucleus to Inhibit Invasion of Intestinal Epithelial Cells

CUL3-KBTBD6/KBTBD7 Ubiquitin Ligase Cooperates with GABARAP Proteins to Spatially Restrict TIAM1-RAC1 Signaling

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