Tyrosine phosphorylation of the orphan receptor ESDN/DCBLD2 serves as a scaffold for the signaling adaptor CrkL

Redmond, Miranda; Weaver, Sheila O.; Love, Collin C.; Joy, Ryan; Lapp, Aliya S.; Rivera, Osvaldo D.; Hinkle, Karen L.; Ballif, Bryan A.

doi:10.1016/j.febslet.2013.05.064

Cited by 16 publications

(37 citation statements)

References 33 publications

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“…The human c-Abl construct, with a C-terminal Flag tag was kindly gifted by A. Howe (U. of Vermont), originally constructed in the Kufe lab (Harvard Medical School) [ 23 ]. DCBLD2 mutant constructs: DCBLD2-Y1F (Tyr750Phe), DCBLD2-Y3F (Tyr750Phe, Tyr732Phe, Tyr565Phe), and DCBLD2-Y7F (Tyr750Phe, Tyr732Phe, Tyr677Phe, Tyr666Phe, Tyr655Phe, Tyr621Phe, Tyr565Phe) were described previously [ 6 ]. The C-terminal Myc- and Flag-tagged DCBLD1 WT and mutant DCBLD1-Y8F (Tyr540Phe, Tyr578Phe, Tyr589Phe, Tyr600Phe, Tyr621Phe, Tyr652Phe, Tyr665Phe, and Tyr696Phe) constructs in pCMV6 vectors were synthesized by Bio Basic Inc. (Markham, ON).…”

Section: Methodsmentioning

confidence: 99%

“…Previously, we reported a proteomics screen for novel Src Family Kinase (SFK) substrates that, when phosphorylated, would bind to the CRKL SH2 domain [ 6 ]. This screen identified the transmembrane protein D iscoidin, C U B , and L CCL d omain-containing 2 (DCBLD2; also e ndothelial and s mooth muscle cell- d erived n europilin-like, ESDN) as a novel phosphotyrosine-dependent CRKL-SH2 binding partner.…”

Section: Introductionmentioning

confidence: 99%

“…Furthermore, it was determined that SFKs were sufficient for, but not the only tyrosine kinases capable of, inducing the interaction of DCBLD2 with CRKL. Our initial study also identified four specific sites on DCBLD2 of regulated tyrosine phosphorylation, three of which were in YxxP motifs [ 6 ].…”

Section: Introductionmentioning

confidence: 99%

“…These YxxP motifs are not only highly conserved among DCBLD2 orthologs, but they are also highly conserved in their related paralog, DCBLD1, which harbors eight YxxP motifs ( Figure 1 ). While to date almost all studies involving DCBLD2 have importantly focused on the interaction of DCBLD2 with RTKs, we have proposed that the clustering of DCBLD proteins by unknown ligands could be an important RTK-independent mechanism of DCBLD signaling [ 6 ]. In order to understand how these conserved motifs might participate in non-RTK or RTK signaling pathways it is important to establish the contribution of specific kinases to the phosphorylation of specific YxxP motifs on DCBLD proteins.…”

Section: Introductionmentioning

confidence: 99%

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Dynamic multi-site phosphorylation by Fyn and Abl drives the interaction between CRKL and the novel scaffolding receptors DCBLD1 and DCBLD2

Schmoker

Weinert

Kellett

et al. 2017

Biochemical Journal

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Discoidin, CUB, and LCCL Domain-containing (DCBLD) 2 is a neuropilin-like transmembrane scaffolding receptor with known and anticipated roles in vascular remodeling and neuronal positioning. DCBLD2 is also upregulated in several cancers and can drive glioblastomas downstream of activated Epidermal Growth Factor Receptor. While a few studies have shown either a positive or negative role for DCBLD2 in regulating growth factor receptor signaling, little is known about the conserved signaling features of DCBLD family members that drive their molecular activities. We previously identified DCBLD2 tyrosine phosphorylation sites in intracellular YxxP motifs that are required for the phosphorylation-dependent binding of the signaling adaptors CRK and CRKL (CT10 regulator of kinase and CRK-Like). These intracellular YxxP motifs are highly conserved across vertebrates and between DCBLD family members. Here, we demonstrate that, as for DCBLD2, DCBLD1 YxxP motifs are required for CRKL-SH2 binding. We report Src family kinases (SFKs) and Abl differentially promote the interaction between the CRKL-SH2 domain and DCBLD1 and DCBLD2, and while SFKs and Abl each promotes DCBLD1 and DCBLD2 binding to the CRKL-SH2 domain, the effect of Abl is more pronounced for DCBLD1. Using high performance liquid chromatography coupled with tandem mass spectrometry, we quantified phosphorylation at several YxxP sites in DCBLD1 and DCBLD2, mapping site-specific preferences for SFKs and Abl. Together these data provide a platform to decipher the signaling mechanisms by which these novel receptors drive their biological activities.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Dynamic multi-site phosphorylation by Fyn and Abl drives the interaction between CRKL and the novel scaffolding receptors DCBLD1 and DCBLD2

Schmoker

Weinert

Kellett

et al. 2017

Biochemical Journal

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“…The extracellular domain of ESDN consists of complement C1r/C1s, Uegf, Bmp1 (CUB); LCCL; and discoidin (FV/VIII) domains. Unlike neuropilins, which are composed of two CUB, two discoidin, a MAM, and a short intracellular domain, ESDN has a relatively long intracellular domain that can function as a scaffold for CT10 regulator of kinase like (4). It is conceivable that ESDN intracellular domain can similarly be involved in its interactions with IR and adaptor proteins, APS and Grb10.…”

Section: Discussionmentioning

confidence: 99%

The neuropilin-like protein ESDN regulates insulin signaling and sensitivity

Jung

Nie

et al. 2016

American Journal of Physiology-Heart and Circulatory Physiology

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Insulin effects on cell metabolism, growth, and survival are mediated by its binding to, and activation of, insulin receptor. With increasing prevalence of insulin resistance and diabetes there is considerable interest in identifying novel regulators of insulin signal transduction. The transmembrane protein endothelial and smooth muscle cell-derived neuropilinlike protein (ESDN) is a novel regulator of vascular remodeling and angiogenesis. Here, we investigate a potential role of ESDN in insulin signaling, demonstrating that Esdn gene deletion promotes insulininduced vascular smooth muscle cell proliferation and migration. This is associated with enhanced protein kinase B and mitogen-activated protein kinase activation as well as insulin receptor phosphorylation. Likewise, insulin signaling in the liver, muscle, and adipose tissue is enhanced in Esdn Ϫ/Ϫ mice, and these animals exhibit improved insulin sensitivity and glucose homeostasis in vivo. The effect of ESDN on insulin signaling is traced back to its interaction with insulin receptor, which alters the receptor interaction with regulatory adaptor protein-E3 ubiquitin ligase pairs, adaptor protein with pleckstrin homology and Src homology 2 domain-c-Cbl and growth factor receptor bound protein 10-neuronal precursor cell-expressed developmentally downregulated 4. In conclusion, our findings establish ESDN as an inhibitor of insulin receptor signal transduction through a novel regulatory mechanism. Loss of ESDN potentiates insulin's metabolic and mitotic effects and provides insights into a novel therapeutic avenue.

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Novel autophosphorylation sites of Src family kinases regulate kinase activity and SH2 domain‐binding capacity

et al. 2016

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Src family tyrosine kinases (SFKs) are critical players in normal and aberrant biological processes. While phosphorylation importantly-regulates SFKs at two known tyrosines, large-scale phosphoproteomics have revealed four additional tyrosines commonly-phosphorylated in SFKs. We found these novel tyrosines to be autophosphorylation sites. Mimicking phosphorylation at the site C-terminal to the activation loop decreased Fyn activity. Phosphomimetics and direct phosphorylation at the three SH2 domain sites increased Fyn activity while reducing phosphotyrosine-dependent interactions. While 68% of human SH2 domains exhibit conservation of at least one of these tyrosines, few have been found phosphorylated except when found in cis to a kinase domain.

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Tyrosine phosphorylation of the orphan receptor ESDN/DCBLD2 serves as a scaffold for the signaling adaptor CrkL

Cited by 16 publications

References 33 publications

Dynamic multi-site phosphorylation by Fyn and Abl drives the interaction between CRKL and the novel scaffolding receptors DCBLD1 and DCBLD2

Dynamic multi-site phosphorylation by Fyn and Abl drives the interaction between CRKL and the novel scaffolding receptors DCBLD1 and DCBLD2

The neuropilin-like protein ESDN regulates insulin signaling and sensitivity

Novel autophosphorylation sites of Src family kinases regulate kinase activity and SH2 domain‐binding capacity

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