Phospholipase Cδ1 Is a Guanine Nucleotide Exchanging Factor for Transglutaminase II (Gαh) and Promotes α1B-Adrenoreceptor-mediated GTP Binding and Intracellular Calcium Release

Baek, Kwang Jin; Kang, Sung Koo; Damron, Derek S.; Im, Mie‐Jae

doi:10.1074/jbc.m008252200

Cited by 57 publications

(63 citation statements)

References 41 publications

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“…1). As observed previously, transfection of PLC-⑀ alone resulted in a small increase in [ 3 H]inositol phosphates that was substantially augmented by cotransfection with G␤ 1 ␥ 2 or GTPase-deficient mutants of G␣ 12 , G␣ 13 , or H-Ras (Fig 1A). Surprisingly, constitutively active forms of RhoA, RhoB, and RhoC also markedly stimulated inositol phosphate accumulation after cotransfection with PLC-⑀ ( Fig 1B, and data not shown).…”

Section: Activation Of Plc-⑀ By the Small Gtpase Rho-previous Studiessupporting

confidence: 58%

“…Identification of an Insertion in the Y Box of PLC-⑀ -As illustrated in the experiments above, PLC-⑀ is unique among PLC isozymes in requiring only the catalytic core for activation by Rho, G␣ 12 , and G␣ 13 . To identify unique regions within the catalytic core of PLC-⑀ that potentially could impart this responsiveness, pair-wise and multiple sequence alignments were performed comparing PLC-⑀ isoforms with the other …”

Section: Definition Of Regions Of Plc-⑀ Essential For Activation By Rmentioning

confidence: 99%

“…The heterotrimeric G protein subunits G␣ q (3)(4)(5)(6) and G␤␥ (7-9) directly activate PLC-␤ isozymes, whereas the activity of PLC-␥ isozymes is increased via phosphorylation and translocation as a consequence of the activation of tyrosine kinase receptors (10 -12). The mechanism(s) of regulation of PLC-␦ is less clear, but it has been suggested to involve Gh proteins (13) as well as Ca 2ϩ mobilization (14). A fourth member of the family of PLC enzymes, PLC-⑀, was identified recently (15)(16)(17)(18).…”

mentioning

confidence: 99%

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Direct Activation of Phospholipase C-ϵ by Rho

Wing

Snyder

Sondek³

et al. 2003

Journal of Biological Chemistry

107

109

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Unique among the phospholipase C isozymes, the recently identified phospholipase C-⑀ (PLC- Comparative sequence analysis of mammalian phospholipase C isozymes revealed a unique ϳ65 amino acid insert within the catalytic core of PLC-⑀ not present in PLC-␤, ␥, ␦, or . A PLC-⑀ construct lacking this region was no longer activated by Rho or G␣ 12/13 but retained regulation by G␤␥ and H-Ras. GTP-dependent interaction of Rho with PLC-⑀ was illustrated in pull-down experiments with GST-Rho, and this interaction was retained in the PLC-⑀ construct lacking the unique insert within the catalytic core. These results are consistent with the conclusion that Rho family GTPases directly interact with PLC-⑀ by a mechanism independent of the CDC25 or RA domains. A unique insert within the catalytic core of PLC-⑀ imparts responsiveness to Rho, which may signal downstream of G␣ 12/13 in the regulation of PLC-⑀, because activation by both Rho and G␣ 12/13 is lost in the absence of this sequence.⑀

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Section: Activation Of Plc-⑀ By the Small Gtpase Rho-previous Studiessupporting

confidence: 58%

Section: Definition Of Regions Of Plc-⑀ Essential For Activation By Rmentioning

confidence: 99%

mentioning

confidence: 99%

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Direct Activation of Phospholipase C-ϵ by Rho

Wing

Snyder

Sondek³

et al. 2003

Journal of Biological Chemistry

107

109

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“…In addition to catalysing the calcium-dependent post-translation modification of proteins, TG2 can also catalyse calciumindependent hydrolysis of guanosine triphosphate (GTP) and adenosine triphosphate, the protein disulfide isomerase reaction (Chandrashekar et al, 1998) and serine/threonine kinase activity (Chen and Mehta, 1999;Fesus and Piacentini, 2002;Lorand and Graham, 2003;Mishra and Murphy, 2004). The ability of TG2 to hydrolyse GTP enables it to serve as a signaling molecule in transmitting outside signal from a 1b adrenergic receptors to a downstream cytoplasmic target, phospholipase C (Baek et al, 2001). Although, predominantly a cytosolic protein, TG2 can also be secreted outside the cell where it regulates cell-matrix interactions (Aeschlimann and Thomazy, 2000); can translocate to the nucleus where it associates with pRb, p53 and histones to regulate certain cellular functions (Milakovic et al, 2004;; and can be expressed on the cell membrane in association with b-integrins where it serves as a coreceptor for integrin-mediated binding to fibronectin (Fn) (Akimov and Belkin, 2001).…”

Section: Introductionmentioning

confidence: 99%

Tissue transglutaminase expression promotes cell attachment, invasion and survival in breast cancer cells

et al. 2006

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Distant metastasis is frequently observed in patients with breast cancer and is a major cause of cancer-related deaths in these patients. Currently, very little is known about the mechanisms that underlie the development of the metastatic phenotype in breast cancer cells. We previously found that metastatic breast cancer cells express high levels of tissue transglutaminase (TG2), but established no direct link between TG2 and metastasis. In this study, we hypothesized that TG2 plays a role in conferring the metastatic phenotype to breast cancer cells. The results obtained suggested that increased expression of TG2 in breast cancer cells contributes to their increased survival, invasion and motility. We further found that TG2 protein in a metastatic breast cancer MDA-MB231 cells was present on the cell surface in close association with integrins b1, b4 and b5. Downregulation of endogenous TG2 by small interfering RNA inhibited fibronectin (Fn)-mediated cell attachment, survival and invasion. Conversely, ectopic expression of TG2 augmented invasion of breast cancer cells and attachment to Fn-coated surfaces. We conclude that TG2 expression in breast cancer cells plays an important role in the development of the metastatic phenotype.

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“…PLC-␥ isozymes are activated by protein phosphorylation following from activation of tyrosine kinase receptors or from receptors linked to tyrosine kinases (10 -12). Although there is evidence for Ca 2ϩ -and transglutaminase II-promoted regulation of PLC-␦ (13,14), the importance of hormonal regulation of this PLC isozyme remains unclear (15).…”

Section: Plcmentioning

confidence: 99%

Activation of Phospholipase C-ε by Heterotrimeric G Protein βγ-Subunits

Wing

Houston

Kelley

et al. 2001

Journal of Biological Chemistry

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PLC-⑀ was identified recently as a phosphoinositidehydrolyzing phospholipase C (PLC) containing catalytic domains (X, Y, and C2) common to all PLC isozymes as well as unique CDC25-and Ras-associating domains. Novel regulation of this PLC isozyme by the Ras oncoprotein and ␣-subunits (G␣ 12 ) of heterotrimeric G proteins was illustrated. Sequence analyses of PLC-⑀ revealed previously unrecognized PH and EF-hand domains in the amino terminus. The known interaction of G␤␥ subunits with the PH domains of other proteins led us to examine the capacity of G␤␥ to activate PLC-⑀.

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Phospholipase Cδ1 Is a Guanine Nucleotide Exchanging Factor for Transglutaminase II (Gαh) and Promotes α1B-Adrenoreceptor-mediated GTP Binding and Intracellular Calcium Release

Cited by 57 publications

References 41 publications

Direct Activation of Phospholipase C-ϵ by Rho

Direct Activation of Phospholipase C-ϵ by Rho

Tissue transglutaminase expression promotes cell attachment, invasion and survival in breast cancer cells

Activation of Phospholipase C-ε by Heterotrimeric G Protein βγ-Subunits

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