RIN1 orchestrates the activation of RAB5 GTPases and ABL tyrosine kinases to determine the fate of EGFR

Balaji, Kavitha; Mooser, Chelsea K.; Janson, Christine; Bliss, Joanne M.; Hojjat, Houmehr; Colicelli, John

doi:10.1242/jcs.113688

Cited by 54 publications

(76 citation statements)

References 67 publications

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“…Because Ras potentiates the Rab5 nucleotide exchange activity of Rin1, this interaction augments Rab5A-dependent endosome fusion and EGFRmediated endocytosis. In contrast, Rin1-Abl signaling stabilizes EGFR and inhibits macropinocytosis (Balaji et al 2012).…”

Section: Endocytosis and Cancermentioning

confidence: 99%

Endocytosis and Cancer

Mellman¹,

Yarden

2013

Cold Spring Harbor Perspectives in Biology

339

300

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Section: Endocytosis and Cancermentioning

confidence: 99%

Endocytosis and Cancer

Mellman¹,

Yarden

2013

Cold Spring Harbor Perspectives in Biology

339

300

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“…EGFR endocytosis is also regulated by RAB5 (also known as RABGEF1), a GTPase that promotes early endosome fusion and subsequent degradation of EGFR in the lysosome (Chen et al, 2009). The activity of RAB5 is regulated by the Ras and Rab interactor 1 (RIN1) that binds and activates the Abl kinases, and is also a guanine nucleotide exchange factor (GEF) for RAB5 (Balaji et al, 2012;Hu et al, 2005). Recent data suggest that binding of the RIN1 SH2 domain to EGFR phosphorylated at tyrosine residues balances RIN1-RAB5-mediated EGFR endocytosis and lysosomal degradation with RIN1-ABLdependent EGFR stabilization by blocking macropinocytosis of the receptor (Balaji et al, 2012) (see poster).…”

Section: Abl-dependent Regulation Of Membrane and Organelle Traffickingmentioning

confidence: 99%

“…The activity of RAB5 is regulated by the Ras and Rab interactor 1 (RIN1) that binds and activates the Abl kinases, and is also a guanine nucleotide exchange factor (GEF) for RAB5 (Balaji et al, 2012;Hu et al, 2005). Recent data suggest that binding of the RIN1 SH2 domain to EGFR phosphorylated at tyrosine residues balances RIN1-RAB5-mediated EGFR endocytosis and lysosomal degradation with RIN1-ABLdependent EGFR stabilization by blocking macropinocytosis of the receptor (Balaji et al, 2012) (see poster). Although overexpression of active ABL1 inhibits EGFR internalization, the activity of endogenous ABL1 has been reported to be required for antigen-induced endocytosis of the B-cell receptor (Jacob et al, 2009).…”

Section: Abl-dependent Regulation Of Membrane and Organelle Traffickingmentioning

confidence: 99%

Multifunctional Abl kinases in health and disease

Khatri

Wang

Pendergast

2016

Journal of Cell Science

115

145

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The Abelson tyrosine kinases were initially identified as drivers of leukemia in mice and humans. The Abl family kinases Abl1 and Abl2 regulate diverse cellular processes during development and normal homeostasis, and their functions are subverted during inflammation, cancer and other pathologies. Abl kinases can be activated by multiple stimuli leading to cytoskeletal reorganization required for cell morphogenesis, motility, adhesion and polarity. Depending on the cellular context, Abl kinases regulate cell survival and proliferation. Emerging data support important roles for Abl kinases in pathologies linked to inflammation. Among these are neurodegenerative diseases and inflammatory pathologies. Unexpectedly, Abl kinases have also been identified as important players in mammalian host cells during microbial pathogenesis. Thus, the use of Abl kinase inhibitors might prove to be effective in the treatment of pathologies beyond leukemia and solid tumors. In this Cell Science at a Glance article and in the accompanying poster, we highlight the emerging roles of Abl kinases in the regulation of cellular processes in normal cells and diverse pathologies ranging from cancer to microbial pathogenesis.

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“…EGF treatment of HeLa cells promoted the formation of large plasma membrane ruffles that are characterized by highly dynamic actin rearrangements in their lamellipodia (Fig. 4 A and B; EGF, Dox−) (31,32). Dox-induced expression of hCDC14A inhibited this EGF-induced ruffling of the membranes (Fig.…”

Section: Phosphomentioning

confidence: 91%

Human phosphatase CDC14A regulates actin organization through dephosphorylation of epithelial protein lost in neoplasm

Chen

Uddin

Hardt

et al. 2017

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

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CDC14 is an essential dual-specificity phosphatase that counteracts CDK1 activity during anaphase to promote mitotic exit in Saccharomyces cerevisiae. Surprisingly, human CDC14A is not essential for cell cycle progression. Instead, it regulates cell migration and cell adhesion. Little is known about the substrates of hCDC14A and the counteracting kinases. Here, we combine phospho-proteome profiling and proximity-dependent biotin identification to identify hCDC14A substrates. Among these targets were actin regulators, including the tumor suppressor eplin. hCDC14A counteracts EGF-induced rearrangements of actin cytoskeleton by dephosphorylating eplin at two known extracellular signal-regulated kinase sites, serine 362 and 604. hCDC14A(PD) and eplin knockout cell lines exhibited down-regulation of E-cadherin and a reduction in alpha/beta-catenin at cell-cell adhesions. Reduction in the levels of hCDC14A and eplin mRNA is frequently associated with colorectal carcinoma and is correlated with poor prognosis. We therefore propose that eplin dephosphorylation by hCDC14A reduces actin dynamics to restrict tumor malignancy

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RIN1 orchestrates the activation of RAB5 GTPases and ABL tyrosine kinases to determine the fate of EGFR

Cited by 54 publications

References 67 publications

Endocytosis and Cancer

Endocytosis and Cancer

Multifunctional Abl kinases in health and disease

Human phosphatase CDC14A regulates actin organization through dephosphorylation of epithelial protein lost in neoplasm

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