G protein-coupled cholecystokinin-B/gastrin receptors are responsible for physiological cell growth of the stomach mucosa in vivo.

Nagata, Aki; Ito, Mitsuhiro; Iwata, Nobuko; Kuno, Junko; Takano, Hiroshi; Minowa, Osamu; Chihara, Kazuo; Matsui, Toshimitsu; Noda, Tetsuo

doi:10.1073/pnas.93.21.11825

Cited by 213 publications

(170 citation statements)

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“…An amplified 155-bp DNA fragment underwent direct DNA sequencing for confirmation using Receptor binding study. To perform the in vitro gastrin binding experiment, we isolated the membrane fraction from GSM06 cells preincubated in the presence or absence of various peptides for 2 days at 33°C by homogenization and centrifugation at 42,000 g for 15 min as reported previously (27). The membrane fraction (1 mg) was labeled for 2 h at 24°C with 50 pM [ 125 I]gastrin in the presence of varying concentrations (10 Ϫ11 to 10 Ϫ6 M) of nonlabeled gastrin, CCK-8, or G-Gly.…”

Section: Animalsmentioning

confidence: 99%

“…CCKA-Rs exhibit a 500-to 1,000-fold higher affinity for sulfated analogs of CCK than for gastrin, whereas CCKB-Rs have approximately equal affinity for both sulfated and non-sulfated peptide analogs of CCK and gastrin (32,34,46,47). CCKB-Rs are present in parietal, ECL, and probably somatostatin cells (2,4,23,27,28,41 (2,28). Immunohistochemical studies have also demonstrated the distribution of CCKB-R in the same cell types (41).…”

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confidence: 99%

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Gastrin stimulates the growth of gastric pit cell precursors by inducing its own receptors

Nakajima

Konda

Izumi

et al. 2002

American Journal of Physiology-Gastrointestinal and Liver Physi

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.-Gastrin/CCK-B receptors (CCKB-Rs) are present on parietal and enterochromaffin-like cells in the gastric mucosa but not on pit cells in the proliferative zone. Because serum gastrin levels are well correlated with the growth of the gastric pit, we examined whether pit precursor cells express CCKB-Rs using hypergastrinemic transgenic mice and a mouse pit precursor cell line, GSM06. In situ hybridization indicated that CCKB-R mRNA was limited to the lower one-third of the mucosa in control mice, whereas it was faintly distributed along the midto low glandular region in the hypergastrinemic transgenic mouse mucosa. CCKB-R-positive midglandular cells appear to have a pit cell lineage; therefore, GSM06 cells were used for an [ 125 I]gastrin binding study. [ 125 I]gastrin bound to the membrane fraction of the GSM06 cells when precultured with gastrin. Gastrin dose dependently induced CCKB-R expression in GSM06 cells and stimulated their growth. Thus these findings suggest that gastrin directly stimulates the growth of the pit cell lineage by inducing its own receptor in pit cell precursors. gastric mucosal growth; gastric surface mucous cell; gastrin/ cholecystokinin-B receptor GASTRIN CONTROLS THE GROWTH of gastric mucosa (14,15). Hypertrophied gastric mucosa is observed in patients with gastrin-producing tumors and also in rats infused continuously with gastrin (5, 31). In contrast, hypotrophic or atrophic mucosa results from fasting in rats whose serum gastrin levels become low (35). The glandular cell components, which include parietal, chief, and enterochromaffin-like (ECL) cells, have relatively long lifespans of 3, 5, and 2 mo, respectively (17). Thus the atrophic change induced by fasting in rats appears to be due mainly to a shortage of pit/gastric surface mucous cells that survive only 3 days in rodents (18). It is not known, however, whether the pit cells and their precursors express gastrin receptors.The physiological roles of gastrin in mucosal growth were recently studied using hypergastrinemic animal models. Wang et al. (45) produced transgenic (TG) mice expressing gastrin under the control of an insulin promoter, which resulted in gastrin production in pancreatic ␤-cells. They reported that gastrin enhances gastric mucosal growth, whereas progastrin preferentially stimulates colonic mucosal growth. They further demonstrated that hypergastrinemic TG mice develop gastric atrophy and eventually gastric cancer (44) and postulated that the hyperplasia of the foveolar pit cell region and the decrease in the parietal cell mass are due, at least in part, to gastrin-stimulated upregulation of growth factors, including heparin binding-epidermal growth factor-like growth factor (HB-EGF) and transforming growth factor-␣ (TGF-␣). Moreover, infection with Helicobacter felis accelerates the formation of gastric cancer in a synergistic manner with hypergastrinemia in hypergastrinemic TG mice (44).We generated TG mice with hypergastrinemia by expressing a human gastrin transgene (19). The gastric mucosa of these mice...

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Section: Animalsmentioning

confidence: 99%

mentioning

confidence: 99%

Gastrin stimulates the growth of gastric pit cell precursors by inducing its own receptors

Nakajima

Konda

Izumi

et al. 2002

American Journal of Physiology-Gastrointestinal and Liver Physi

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“…Mice that lack the gastrin gene or the gastrin/ cholecystokinin-B receptor have altered gastric mucosal architecture and differentiation (Nagata et al, 1996;Koh et al, 1997;Friis-Hansen et al, 1998). Gastrin and gastrin receptor-null mice exhibit reduced numbers of enterochromaffin-like cells and an expansion of mucous and surface epithelial cells (Nagata et al, 1996;Koh et al, 1997;Friis-Hansen et al, 1998).…”

Section: Introductionmentioning

confidence: 99%

Chronic gastritis in the hypochlorhydric gastrin-deficient mouse progresses to adenocarcinoma

et al. 2005

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The current study tests the hypothesis that chronic atrophic gastritis from hypochlorhydria in the gastrindeficient mouse predisposes the stomach to gastric cancer. Gross morphology and histology of 12-month-old wildtype (WT), gastrin-deficient (GÀ/À) and somatostatindeficient (SOMÀ/À) mice were examined. Parietal and G cells, Ki67, TUNEL, villin and MUC2 expression were analysed by immunohistochemistry. RUNX3 and STAT3 expression was analysed by Western blot. Anchorageindependent growth was determined by cell cluster formation in soft agar. Compared to the WT and SOMÀ/À mice, hypochlorhydric GÀ/À mice developed parietal cell atrophy, significant antral inflammation and intestinal metaplasia. Areas of metaplasia within the GÀ/ À mouse stomach showed decreased RUNX3 expression with elevated MUC2 and villin expression. Cells isolated from the tumor grew in soft agar. However, the cells isolated from WT, nontransformed GÀ/À and SOMÀ/À gastric tissue did not form colonies in soft agar. Consistent with elevated antral proliferation, tumor tissue isolated from the GÀ/À mice showed elevated phosphorylated STAT3 expression. We then examined the mechanism by which STAT3 was constitutively expressed in the tumor tissue of the GÀ/À mice. We found that IFNc expression was also significantly higher in the tumor tissue of GÀ/À mice compared to WT and SOMÀ/À animals. To determine whether STAT3 was regulated by IFNc, MKN45 cells were cocultured with IFNc or gastrin. IFNc significantly stimulated phosphorylation of STAT3 in the MKN45 cell line, but not gastrin. Therefore, we show here that in the hypochlorhydric mouse stomach, the chronic gastritis, atrophy, metaplasia, dysplasia paradigm can be recapitulated in mice. Moreover, neoplastic transformation of the antral gastric mucosa does not require gastrin.

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“…Gi-mediated GPCRs, were shown to produce a mitogenic response which was blocked by the tyrosine A recent study has shown, using gene knock-out studies, that certain GPCRs are essential for ce11 growth under physiologicd conditions (Nagata et al, 1996). Activation of GPCRs l a d s to rapid phosphorylation and activation of MAP kinases.…”

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confidence: 99%

SH3 Binding Domains in the Dopamine D4 Receptor

Oldenhof

Vickery²,

Anafi³

et al. 1998

Biochemistry

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The dopamine D4 receptor is a G protein-coupled receptor (GPCR) that belongs to the dopamine D2-like receptor family. Functionally, the D2-like receptors are characterized by their ability to inhibit adenylyl cyclase. The dopamine D4 receptor as well as many other catecholaminergic receptors contain several putative SH3 binding domains. Most of these sites in the D4 receptor are located in a polymorphic repeat sequence and flanking sequences in the third intracellular loop. Here we demonstrate that this region of the D4 receptor can interact with a large variety of SH3 domains of different origin. The strongest interactions were seen with the SH2−SH3 adapter proteins Grb2 and Nck. The repeat sequence itself is not essential in this interaction. The data presented indicate that the different SH3 domains in the adapter proteins interact in a cooperative fashion with two distinct sites immediately upstream and downstream from the repeat sequence. Removal of all the putative SH3 binding domains in the third intracellular loop of the dopamine D4 receptor resulted in a receptor that could still bind spiperone and dopamine. Dopamine could not modulate the coupling of these mutant receptors to adenylyl cyclase and MAPK, although dopamine modulated receptor−G protein interaction appeared normal. The receptor deletion mutants show strong constitutive internalization that may account for the deficiency in functional activation of second messengers. The data indicates that the D4 receptor contains SH3 binding sites and that these sites fall within a region involved in the control of receptor internalization.

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G protein-coupled cholecystokinin-B/gastrin receptors are responsible for physiological cell growth of the stomach mucosa in vivo.

Cited by 213 publications

References 50 publications

Gastrin stimulates the growth of gastric pit cell precursors by inducing its own receptors

Gastrin stimulates the growth of gastric pit cell precursors by inducing its own receptors

Chronic gastritis in the hypochlorhydric gastrin-deficient mouse progresses to adenocarcinoma

SH3 Binding Domains in the Dopamine D4 Receptor

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