Gravin-mediated Formation of Signaling Complexes in β2-Adrenergic Receptor Desensitization and Resensitization

Lin, Fubao; Wang, Hsien‐yu; Malbon, Craig C.

doi:10.1074/jbc.275.25.19025

Cited by 119 publications

(98 citation statements)

References 47 publications

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“…Partial support for this hypothesis is that a small fraction of cell surface GalT1 has been cofractionated with caveolin in lipid rafts [21]. Furthermore, long GalT1 has been shown to associate with Src-suppressed C kinase substrate (SSeCKS), a previously defined kinase and cytoskeleton scaffolding protein important for agonist-induced internalization and resensitization of G-protein-linked receptors [20,35]. In this scenario, GalT1-associated GTAP may trigger ubiquitination and degradation of caveolin and/or SSeCKS, thereby affecting efficient internalization and function of GalT1.…”

Section: Discussionmentioning

confidence: 86%

Characterization of a Novel Ubiquitin-Conjugating Enzyme That Regulates β1,4-Galactosyltransferase-1 in Embryonic Stem Cells

Wassler¹,

Shur

Zhou³

et al. 2008

Stem Cells

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In this study we identified a novel galactosyltransferase 1-associating protein (GTAP) by cDNA cloning from a murine embryonic cDNA library using the two-hybrid yeast system. GTAP is expressed in early embryonic tissues, as well as in adult tissues with active cell turnover, and belongs to the class III ubiquitin-conjugating (E2) enzyme family. Its COOH-terminal domain contains a consensus sequence for ubiquitin binding shared by all the ubiquitin-conjugating enzymes, whereas its NH 2 -terminal domain appears critical for the binding and internalization of cell surface galactosyltransferase 1 (GalT1) in embryonic stem cells through a monensin-and MG132-dependent pathway. We have found that GTAP regulates GalT1-associated, laminin-dependent embryonic cell adhesion and the formation of embryoid bodies. Thus, GTAP functions as an evolutionarily conserved E2 enzyme, which may participate in intercellular adhesion and embryonic development. STEM CELLS 2008;

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Section: Discussionmentioning

confidence: 86%

Characterization of a Novel Ubiquitin-Conjugating Enzyme That Regulates β1,4-Galactosyltransferase-1 in Embryonic Stem Cells

Wassler¹,

Shur

Zhou³

et al. 2008

Stem Cells

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“…The AKAP domain provides a reversible, dynamic docking site for the β 2 AR and, presumably, other GPCRs. This would explain the basis for the association of AKAP250 as well as AKAP79 with β 2 AR [48,69]. We propose that, for AKAP79/250, this AKAP domain might be better considered as a 'GPCR-binding domain', reflecting its role in docking the β 2 AR and probably other GPCRs.…”

Section: Working Model Of Dynamic Interactions Of Akap250 and The Gpcrmentioning

confidence: 92%

“…The binding of AKAP250 to β 2 AR is reversible, dynamically regulated by activation of the receptor (Figure 4) and essential for the normal subsequent sequellae in the desensitization, sequestration, resensitization and recycling of the β 2 AR [25,48]. For AKAP79, β 2 AR binding appears to be largely constitutive.…”

Section: Akap Motifs and Gpcrsmentioning

confidence: 99%

“…More detailed analysis of this observation [47] and the cellular context, however, will be needed to fully explore this topic. The suppression of AKAP250 expression by antisense technology leads to a disruption of β 2 AR trafficking and resensitization, demonstrating the central role of this scaffold in AKAP79/ 250-based β 2 AR signalling complexes [19,25,47,48]. In silico analysis of AKAP250 revealed three 'AKAP motifs' at residue positions 603-633, 752-782 and 797-827.…”

Section: Akap Motifs and Gpcrsmentioning

confidence: 99%

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AKAPs (A-kinase anchoring proteins) and molecules that compose their G-protein-coupled receptor signalling complexes

Malbon

Tao

Wang

2004

Biochemical Journal

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100

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Cell signalling mediated via GPCRs (G-protein-coupled receptors) is a major paradigm in biology, involving the assembly of receptors, G-proteins, effectors and downstream elements into complexes that approach in design 'solid-state' signalling devices. Scaffold molecules, such as the AKAPs (A-kinase anchoring proteins), were discovered more than a decade ago and represent dynamic platforms, enabling multivalent signalling. AKAP79 and AKAP250 were the first to be shown to bind to membrane-embedded GPCRs, orchestrating the interactions of various protein kinases (including tyrosine kinases), protein phosphatases (e.g. calcineurin) and cytoskeletal elements with at least one member of the superfamily of GPCRs, the prototypical β 2 -adrenergic receptor. In this review, the multivalent interactions of AKAP250 with the cell membrane, receptor, cytoskeleton and constituent components are detailed, providing a working model for AKAP-based GPCR signalling complexes. Dynamic regulation of the AKAP-receptor complex is mediated by ordered protein phosphorylation.

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“…AKAP12 organizes the complex of PKA and PKC (Nauert et al, 1997), and is an important regulator of the b 2 -adrenergic receptor complex (Shih et al, 1999;Lin et al, 2000a). AKAP12 expression can be induced by several drugs like phorbol ester (Gordon et al, 1992;Nauert et al, 1997) and lysophosphatidylcholine (Sato et al, 1998), which suggests the participation of AKAP12 in diverse signal transduction cascades.…”

Section: Introductionmentioning

confidence: 99%

AKAP12/Gravin is inactivated by epigenetic mechanism in human gastric carcinoma and shows growth suppressor activity

et al. 2004

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AKAP12/Gravin, one of the A-kinase anchoring proteins (AKAPs), functions as a kinase scaffold protein and as a dynamic regulator of the b 2 -adrenergic receptor complex. However, the biological role of AKAP12 in cancer development is not well understood. The AKAP12 gene encodes two major isoforms of 305 and 287 kDa (designated AKAP12A and AKAP12B, respectively, in this report). We found that these two isoforms are independently expressed and that they are probably under the control of two different promoters. Moreover, both isoforms were absent from the majority of human gastric cancer cells. The results from methylation-specific PCR (MSP) and bisulfite sequencing revealed that the 5 0 CpG islands of both AKAP12A and AKAP12B are frequently hypermethylated in gastric cancer cells. Treatment with DNA methyltransferase inhibitor and/or histone deacetylase inhibitor efficiently restored the expression of AKAP12 isoforms, confirming that DNA methylation is directly involved in the transcriptional silencing of AKAP12 in gastric cancer cells. Hypermethylation of AKAP12A CpG island was also detected in 56% (10 of 18) of primary gastric tumors. The restoration of AKAP12A in AKAP12-nonexpressing cells reduced colony formation and induced apoptotic cell death. In conclusion, our results suggest that AKAP12A may function as an important negative regulator of the survival pathway in human gastric cancer.

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Gravin-mediated Formation of Signaling Complexes in β2-Adrenergic Receptor Desensitization and Resensitization

Cited by 119 publications

References 47 publications

Characterization of a Novel Ubiquitin-Conjugating Enzyme That Regulates β1,4-Galactosyltransferase-1 in Embryonic Stem Cells

Characterization of a Novel Ubiquitin-Conjugating Enzyme That Regulates β1,4-Galactosyltransferase-1 in Embryonic Stem Cells

AKAPs (A-kinase anchoring proteins) and molecules that compose their G-protein-coupled receptor signalling complexes

AKAP12/Gravin is inactivated by epigenetic mechanism in human gastric carcinoma and shows growth suppressor activity

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