Constitutive activation of the gastrin-releasing peptide receptor expressed by the nonmalignant human colon epithelial cell line NCM460.

Ferris, Heather A.; Carroll, Robert E.; Rasenick, Mark M.; Benya, Richard V.

doi:10.1172/jci119795

Cited by 32 publications

(19 citation statements)

References 44 publications

(41 reference statements)

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“…It is also known that constitutively activated G␣ 13 can act as a potent oncogene (31)(32)(33) and that Rho function is necessary for transformation (55). In addition, constitutive or autocrine stimulation of heptahelical receptors that couple to G␣ 13 and Rho are also implicated in tumorogenesis (56,57). Our results identifying a novel link between G␣ 13 , Rho, and COX-2 suggest that this pathway may contribute to tumor development in at least some cell types, a proposition that warrants further experimental work.…”

Section: Results and Conclusionmentioning

confidence: 70%

Gα13 Stimulates Rho-dependent Activation of the Cyclooxygenase-2 Promoter

Slice¹,

Walsh²,

Rozengurt³

1999

Journal of Biological Chemistry

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Cyclooxygenase-2 (COX-2) gene expression is rapidly increased by cytokines, tumor promoters, and growth factors and is markedly enhanced in various cancer cells. Here, we examine the regulation of COX-2 promoter activity by ␣ subunits of heterotrimeric G proteins in NIH 3T3 cells. Using a transient transfection assay with a reporter vector in which the murine COX-2 promoter drives the production of luciferase and expression vectors encoding for ␣ subunits of G-proteins, we show that overexpression of wild type and constitutively active G␣ 13 and G␣ q induced transcription from the COX-2 promoter. The highest level of induced luciferase activity (5.8-fold) occurred in cells expressing the constitutively active G␣ 13 (Q226L). We also show that expression of a constitutively active mutant of Rho (RhoQ63L) also induced transcription from the COX-2 promoter. Co-expression of Clostridium botulinum C3 toxin specifically blocked induction of the COX-2 promoter by either G␣ 13 Q226L or RhoQ63L but did not prevent the activation of this promoter by Ras, Rac, v-src, or forskolin. We conclude that G␣ 13 signals through a Rho-dependent pathway leading to activation of the COX-2 promoter. This pathway is not inhibited by either cytochalasin D, which disrupts actin filament organization, or genistein, a broad spectrum tyrosine kinase inhibitor, indicating a bifurcation of the signaling pathway used by G␣ 13 /Rho to induce COX-2 expression from that used to induce stress fiber formation and tyrosine phosphorylation of focal adhesion proteins.Prostaglandins play a pivotal role in a broad range of physiological and pathological processes including inflammation, pain transmission, maintenance of gastrointestinal integrity, and progression of colorectal cancer (1-3). The rate-limiting enzymes for production of prostaglandins are cyclooxygenases (COX) 1 type 1 and 2 (4 -6). COX-1 is constitutively expressed in nearly all cells, whereas COX-2 expression is induced as an immediate-early gene in response to pro-inflammatory cytokines, tumor promoters, and growth factors (7-10). COX-2 is overexpressed in cancers of the colon, stomach, and breast (11)(12)(13)(14), and chronic inhibition of COX activity has been associated with chemopreventive effects on colon cancer (15). Consequently, the identification of the pathways and regulatory elements that lead to COX-2 expression are the subject of major interest.An increase in the rate of COX-2 gene transcription is mediated by several cis-acting promoter elements that respond to multiple signal transduction pathways (8, 16 -21). Plateletderived growth factor, serum, and v-src promote COX-2 expression through Ras-mediated increases in c-Jun NH2-terminal kinase and extracellular signal-related kinase pathways in NIH 3T3 cells (22)(23)(24). Agonists that signal through cAMP induce COX-2 expression through the cAMP response element binding transcription factor (25). These pathways converge onto a common regulatory region, the ATF/cAMP response element located between Ϫ56 and Ϫ48 of the murine COX...

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Section: Results and Conclusionmentioning

confidence: 70%

Gα13 Stimulates Rho-dependent Activation of the Cyclooxygenase-2 Promoter

Slice¹,

Walsh²,

Rozengurt³

1999

Journal of Biological Chemistry

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“…As a model we used Caco-2 and HT-29 colon cancer cell lines, which express functional GRP receptor and form moderately well-differentiated adenocarcinoma in nude mice (Carroll et al, 2000). To determine RhoA activation, we conducted a time-course experiment, stimulating Caco-2 and HT-29 cells in serum free conditions with a concentration of GRP (100 nM) that has been used for previous colon cancer studies (Ferris et al, 1997;Glover et al, 2005).The level of RhoA activation was assessed using RhoA pulldown assay (Ren and Schwartz, 2000) (Fig. 1, A and B).…”

Section: Grp Stimulation Increases Rhoa Activation In Colonmentioning

confidence: 99%

Gα₁₃/PDZ-RhoGEF/RhoA Signaling Is Essential for Gastrin-Releasing Peptide Receptor–Mediated Colon Cancer Cell Migration

et al. 2014

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Gastrin-releasing peptide receptor (GRPR) is ectopically expressed in over 60% of colon cancers. GRPR expression has been correlated with increased colon cancer cell migration. However, the signaling pathway by which GRPR activation leads to increased cancer cell migration is not well understood. We set out to molecularly dissect the GRPR signaling pathways that control colon cancer cell migration through regulation of small GTPase RhoA. Our results show that GRP stimulation activates RhoA predominantly through G13 heterotrimeric G-protein signaling. We also demonstrate that postsynaptic density 95/disk-large/ZO-1 (PDZ)-RhoGEF (PRG), a member of regulator of G-protein signaling (RGS)-homology domain (RH) containing guanine nucleotide exchange factors (RH-RhoGEFs), is the predominant activator of RhoA downstream of GRPR. We found that PRG is required for GRP-stimulated colon cancer cell migration, through activation of RhoA-Rhoassociated kinase (ROCK) signaling axis. In addition, PRG-RhoA-ROCK pathway also contributes to cyclo-oxygenase isoform 2 (Cox-2) expression. Increased Cox-2 expression is correlated with increased production of prostaglandin-E 2 (PGE 2 ), and Cox-2-PGE 2 signaling contributes to total GRPR-mediated cancer cell migration. Our analysis reveals that PRG is overexpressed in colon cancer cell lines. Overall, our results have uncovered a key mechanism for GRPR-regulated colon cancer cell migration through the Ga 13 -PRG-RhoA-ROCK pathway.

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“…Apparent constitutive activity of a wild-type GPCR may vary substantially in various systems. Differences in GPCR expression level, GPCR desensitisation, G-protein complement and GPCR/G-protein stochiometry can all contribute to such differences (Seifert and Wenzel-Seifert, 2002) This could explain why GRP receptors expressed in NCM460 cells, a nonmalignant human colon epithelial cell line, are constitutively active (Ferris et al, 1997) but are not in other cell types (Benya et al, 1994). Our findings are unlikely to be due to an overexpression artefact as the receptors in this study were expressed at levels not greater than those measured from a variety of other cancers (100 -50 000 sites/ cell, Jensen et al, 2001) So at these moderate levels, wild-type receptor was sufficient to activate downstream signals that promote cell survival under anchorage-independent conditions.…”

Section: Discussionmentioning

confidence: 99%

Expression of V1A and GRP receptors leads to cellular transformation and increased sensitivity to substance-P analogue-induced growth inhibition

et al. 2005

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Small-cell lung cancer (SCLC) is a particularly aggressive cancer, which metastasises early. Despite initial sensitivity to radio-and chemo-therapy, it invariably relapses, so that the 2-year survival remains less than 5%. Neuropeptides particularly arginine vasopressin (AVP) and gastrin-releasing peptide (GRP) act as autocrine and paracrine growth factors and the expression of these and their receptors are a hallmark of the disease. ,N me Phe 8 ]-substance-P (6 -11) (SP-G) inhibit the growth of SCLC cells by modulating neuropeptide signalling. We show that GRP and V 1A receptors expression leads to the development of a transformed phenotype. Addition of neuropeptide provides some protection from etoposide-induced cytotoxicity. Receptor expression also leads to an increased sensitivity to substance-P analogue-induced growth inhibition. We show that SP-D and SP-G act as biased agonists at GRP and V 1A receptors causing blockade of G q -mediated Ca 2 þ release while directing signalling to activate ERK via a pertussis toxin-sensitive pathway. This is the first description of biased agonism at V 1A receptors. This unique pharmacology governs the antiproliferative properties of these agents and highlights their potential therapeutic potential for the treatment of SCLC and particularly in tumours, which have developed resistance to chemotherapy.

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Constitutive activation of the gastrin-releasing peptide receptor expressed by the nonmalignant human colon epithelial cell line NCM460.

Cited by 32 publications

References 44 publications

Gα13 Stimulates Rho-dependent Activation of the Cyclooxygenase-2 Promoter

Gα13 Stimulates Rho-dependent Activation of the Cyclooxygenase-2 Promoter

Gα₁₃/PDZ-RhoGEF/RhoA Signaling Is Essential for Gastrin-Releasing Peptide Receptor–Mediated Colon Cancer Cell Migration

Expression of V1A and GRP receptors leads to cellular transformation and increased sensitivity to substance-P analogue-induced growth inhibition

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Constitutive activation of the gastrin-releasing peptide receptor expressed by the nonmalignant human colon epithelial cell line NCM460.

Cited by 32 publications

References 44 publications

Gα13 Stimulates Rho-dependent Activation of the Cyclooxygenase-2 Promoter

Gα13 Stimulates Rho-dependent Activation of the Cyclooxygenase-2 Promoter

Gα13/PDZ-RhoGEF/RhoA Signaling Is Essential for Gastrin-Releasing Peptide Receptor–Mediated Colon Cancer Cell Migration

Expression of V1A and GRP receptors leads to cellular transformation and increased sensitivity to substance-P analogue-induced growth inhibition

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Gα₁₃/PDZ-RhoGEF/RhoA Signaling Is Essential for Gastrin-Releasing Peptide Receptor–Mediated Colon Cancer Cell Migration