Your search keyword '"Robert Raffaniello"' showing total 6 results

1. Variations in the multimerization region of the Helicobacter pylori cytotoxin CagA affect virulence

Author

Robert Raffaniello, Tricia Alston, and Daiva Ahire

Subjects

0301 basic medicine, Cancer Research, biology, Virulence, Transfection, Cell cycle, Helicobacter pylori, bacterial infections and mycoses, biology.organism_classification, digestive system, Virology, Molecular biology, Fusion protein, digestive system diseases, Virulence factor, 03 medical and health sciences, 030104 developmental biology, Oncology, bacteria, CagA, Gene

Abstract

Helicobacter pylori colonizes the human stomach by infecting gastric epithelial cells. It is the primary cause of peptic ulcer disease and gastric cancer (GC). Cytotoxin-associated gene A (CagA) is a virulence factor produced by H. pylori. Strains positive for the CagA protein are associated with more severe gastric diseases. The 3' region of the cagA gene exhibits heterogeneity with respect to tyrosine phosphorylation motifs (EPIYA) and CagA multimerization motifs (CM). CagA proteins are categorized as either Western or Eastern based on EPIYA sequences. CM motifs are also identified as Western and Eastern based on CM sequences identified in Western and East Asian countries. It has been suggested that CagA proteins possessing an Eastern CM type are associated with less severe gastric disorders. In the present study, the effects of two CagA peptides with different CM motifs on cell function were compared: CagA with a Western and Eastern CM motif (CagA-WE), and CagA with two Western CM motifs (CagA-WW). CagA sequences were fused with green fluorescent protein (GFP) to form GFP-CagA fusion proteins. GFP-CagA and GFP control constructs were transfected into human gastric adenocarcinoma cells (AGS). GFP-CagA expression was verified by immunoblotting and immunofluorescence. The results demonstrated that, following 18 h, the CagA-WE-transfected cells were less adherent compared with the CagA-WW transfected cells. CagA has also been reported to cause cell elongation in AGS cells. In the current study, cell elongation was more frequent in the CagA-WW-transfected cells compared with the CagA-WE transfected cells (8.34 vs. 3.97% cells, respectively). The CagA peptides did not affect proliferation or apoptosis rates. These results suggest that different CM motif types may affect CagA virulence.

Published

2017

2. Chibby is a weak regulator of β-catenin activity in gastric epithelium

Author

Ken-Ichi Takemaru, Luis Chiriboga, Margaret Black, Robert Raffaniello, and Feng-Qian Li

Subjects

0301 basic medicine, Physiology, Clinical Biochemistry, Cell, Adenocarcinoma, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Stomach Neoplasms, Cell Line, Tumor, medicine, Humans, Wnt Signaling Pathway, beta Catenin, Chemistry, Cell growth, Nuclear Proteins, Cell Biology, Cell biology, Gene Expression Regulation, Neoplastic, 030104 developmental biology, medicine.anatomical_structure, Cell culture, Gastric Mucosa, 030220 oncology & carcinogenesis, Catenin, Immunohistochemistry, Phosphorylation, Cell fractionation, Carrier Proteins, human activities

Abstract

The canonical Wnt-β-catenin pathway is important in normal development. Mutations in β-catenin or proteins involved with regulating its phosphorylation or localization result in its nuclear accumulation where it activates its target genes and stimulates cell proliferation. This pathway is dysregulated in many different types of cancer, including gastric cancer (GC). Chibby (Cby) is a 14-kDa protein that inhibits β-catenin localization to the nucleus and represses β-catenin-induced transcriptional activity. In the current study, we examined the expression and function of Cby in normal and cancerous human gastric tissue. Reverse-transcription polymerase chain reaction and immunohistochemistry revealed that Cby is expressed in human stomach and localized to glandular elements. Immunohistochemical staining intensity of Cby was decreased in GC tissue when compared with normal gastric epithelium. In AGS cells, a human gastric carcinoma cell line, Cby expression was low. Stable AGS cell transfectants overexpressing Cby were prepared. Cby overexpression did not affect proliferation rates or β-catenin levels. However, confocal microscopy and subcellular fractionation studies revealed that Cby overexpression resulted in a small decrease in nuclear β-catenin. Moreover, Cby overexpression caused a molecular weight shift in nuclear β-catenin and resulted in decreased β-catenin signaling in AGS cells as measured by the TopFlash assay. However, Cby overexpression did not affect c-Myc protein levels. To conclude, Cby expression was decreased in GC samples and Cby expression altered β-catenin localization in cultured GC cells. However, Cby did not affect cell proliferation rates or β-catenin-induced protein expression. Cby may be involved in the early events in the pathogenesis of GC.

Published

2018

3. Rab3D regulates amylase levels, not agonist-induced amylase release, in AR42J cells

Author

Saima Limi, Robert Raffaniello, and George K. Ojakian

Subjects

Recombinant Fusion Proteins, rab3 GTP-Binding Proteins, Gene Expression, GTP-binding protein, Biochemistry, Exocytosis, Dexamethasone, Sincalide, Proto-Oncogene Proteins c-myc, Cell Line, Tumor, Animals, Secretion, Amylase, Molecular Biology, Pancreas, biology, Rab3D, Granule (cell biology), Cell Biology, Zymogen granule, Digestive enzyme, Molecular biology, Rats, Cell culture, Amylases, Mutation, biology.protein, AR42J cells, Zymogen granules, Cell fractionation, Cholecystokinin, Exocrine, Research Article

Abstract

Rab3D is a low molecular weight GTP-binding protein that associates with secretory granules in exocrine cells. AR42J cells are derived from rat pancreatic exocrine tumor cells and develop an acinar cell-like phenotype when treated with dexamethasone (Dex). In the present study, we examined the role of Rab3D in Dex-treated AR42J cells. Rab3D expression and localization were analyzed by subcellular fractionation and immunoblotting. The role of Rab3D was examined by overexpressing myc-labeled wild-type-Rab3D and a constitutively active form of Rab3D (Rab3D-Q81L) in AR42J cells. We found that Rab3D is predominantly membrane-associated in AR42J cells and co-localizes with zymogen granules (ZG). Following CCK-8-induced exocytosis, amylase-positive ZGs appeared to move towards the periphery of the cell and co-localization between Rab3D and amylase was less complete when compared to basal conditions. Overexpression of WT, but not mutant Rab3D, resulted in an increase in cellular amylase levels. Overexpression of mutant and WT Rab3D did not affect granule morphology, CCK-8-induced secretion, long-term (48 hr) basal amylase release or granule density. We conclude that Rab3D is not involved in agonist-induced exocytosis in AR42J cells. Instead, Rab3D may regulate amylase content in these cells.

Published

2012

4. Hsp90 Co-localizes with Rab-GDI-1 and Regulates Agonist-induced Amylase Release in AR42J Cells

Author

Robert Raffaniello, Dawn Ip, Sarwish Rafiq, and Daria Fedorova

Subjects

Gene isoform, Physiology, Lactams, Macrocyclic, GTPase, Dexamethasone, Sincalide, Cell Line, Tumor, Heat shock protein, Benzoquinones, Centrifugation, Density Gradient, polycyclic compounds, Animals, Immunoprecipitation, Protein Isoforms, rho-Specific Guanine Nucleotide Dissociation Inhibitors, Secretion, HSP90 Heat-Shock Proteins, Guanine Nucleotide Dissociation Inhibitors, Original Paper, biology, fungi, Hsp90, Molecular biology, Rats, Cell biology, rab GTP-Binding Proteins, Cell culture, Amylases, biology.protein, Chaperone complex, Rab

Abstract

Rab proteins are small GTPases required for vesicle trafficking through the secretory and endocytic pathways. Rab GDP-dissociation inhibitor (rab-GDI) regulates Rab protein function and localization by maintaining Rab proteins in the GDP-bound conformation. Two isoforms of rab-GDI are present in most mammalian cells: GDI-1 and GDI-2. It has recently been demonstrated that a Heat shock protein 90 (Hsp90) chaperone complex regulates the interactions between Rab proteins and Rab-GDI-1. The AR42J cell line is derived from rat pancreatic exocrine tumor cells and develops an acinar-like phenotype when treated with dexamethasone (Dex). The aim of the present study was to examine the expression of rab-GDI isoforms and Hsp90 in AR42J cells in the presence or absence of Dex. Rab-GDI: Hsp90 interactions were also examined. Both rab-GDI isoforms were detected in AR42J cells by immunoblotting. In Dex-treated cells, quantitative immunoblotting revealed that rab-GDI-1 expression increased by 28%, although this change was not statistically significant. Rab-GDI-2 levels were unaltered by Dex treatment. Approximately 21% rab-GDI-1 was membrane associated, whereas rab-GDI-2 was exclusively cytosolic. Dex treatment did not affect the subcellular distribution of rab-GDI isoforms. Hsp90 was present in the cytosolic and membrane fractions of AR42J cells and co-immunoprecipitated with cytosolic rab-GDI-1. Moreover, density gradient centrifugation of AR42J cell membranes revealed that Hsp90 and rab-GDI-1 co-localize on low- and high-density membrane fractions, including amylase-containing secretory granules. The Hsp90 inhibitor, geldanamycin, inhibited CCK-8-induced amylase release from these cells in a dose-dependent manner. Our results indicate that as AR42J cells differentiate into acinar-like cells, rab-GDI isoform expression and localization is not significantly altered. Moreover, our findings suggest that Hsp90 regulates agonist-induced secretion in exocrine cells by interacting with rab-GDI-1.

Published

2009

5. Variations in the multimerization region of the

Author

Daiva, Ahire, Tricia, Alston, and Robert, Raffaniello

Subjects

bacteria, Articles, bacterial infections and mycoses, digestive system, digestive system diseases

Abstract

Helicobacter pylori colonizes the human stomach by infecting gastric epithelial cells. It is the primary cause of peptic ulcer disease and gastric cancer (GC). Cytotoxin-associated gene A (CagA) is a virulence factor produced by H. pylori. Strains positive for the CagA protein are associated with more severe gastric diseases. The 3′ region of the cagA gene exhibits heterogeneity with respect to tyrosine phosphorylation motifs (EPIYA) and CagA multimerization motifs (CM). CagA proteins are categorized as either Western or Eastern based on EPIYA sequences. CM motifs are also identified as Western and Eastern based on CM sequences identified in Western and East Asian countries. It has been suggested that CagA proteins possessing an Eastern CM type are associated with less severe gastric disorders. In the present study, the effects of two CagA peptides with different CM motifs on cell function were compared: CagA with a Western and Eastern CM motif (CagA-WE), and CagA with two Western CM motifs (CagA-WW). CagA sequences were fused with green fluorescent protein (GFP) to form GFP-CagA fusion proteins. GFP-CagA and GFP control constructs were transfected into human gastric adenocarcinoma cells (AGS). GFP-CagA expression was verified by immunoblotting and immunofluorescence. The results demonstrated that, following 18 h, the CagA-WE-transfected cells were less adherent compared with the CagA-WW transfected cells. CagA has also been reported to cause cell elongation in AGS cells. In the current study, cell elongation was more frequent in the CagA-WW-transfected cells compared with the CagA-WE transfected cells (8.34 vs. 3.97% cells, respectively). The CagA peptides did not affect proliferation or apoptosis rates. These results suggest that different CM motif types may affect CagA virulence.

Published

2016

6. Calcium dependence of muscarinic receptor-mediated catecholamine secretion from the perfused rat adrenal medulla

Author

Orna E. Harish, Arun R. Wakade, Allan S. Schneider, Lung-Sen Kao, and Robert Raffaniello

Subjects

Atropine, medicine.medical_specialty, Nicotine, medicine.drug_class, chemistry.chemical_element, Calcium channel blocker, Hexamethonium Compounds, Calcium, In Vitro Techniques, Biochemistry, Hexamethonium, Calcium in biology, Cellular and Molecular Neuroscience, Catecholamines, Internal medicine, Muscarine, Muscarinic acetylcholine receptor, medicine, Animals, Egtazic Acid, T-type calcium channel, Muscarinic acetylcholine receptor M3, Receptors, Muscarinic, Electric Stimulation, Rats, Calcium ATPase, Perfusion, Endocrinology, medicine.anatomical_structure, chemistry, Verapamil, Adrenal Medulla, Adrenal medulla

Abstract

It had previously been thought that muscarinic cholinergic receptors utilize an influx of extracellular calcium for activation of adrenomedullary catecholamine secretion. However, it has recently been demonstrated that muscarinic receptors on isolated adrenal chromaffin cells can elevate cytosolic free calcium levels in a manner independent of extracellular calcium, presumably by mobilizing intracellular calcium stores. We now demonstrate that muscarinic receptor-mediated catecholamine secretion from perfused rat adrenal glands can occur under conditions of extracellular calcium deprivation that are sufficient to block both nicotine- and electrically stimulated release. Three independent conditions of extracellular calcium deprivation were used: nominally calcium-free perfusion solution (no calcium added), EGTA-containing calcium-free perfusion solution, and perfusion solution containing the calcium channel blocker verapamil. Secretion was evoked from the perfused glands by either transmural electrical stimulation or injection of nicotine or muscarine into the perfusion stream. Each condition of calcium deprivation was able to block nicotine- and electrically stimulated catecholamine release in an interval that left muscarine-evoked release largely unaffected. The above results demonstrate that muscarine-evoked catecholamine secretion from perfused rat adrenal glands can occur in the absence of extracellular calcium, presumably by mobilization of intracellular calcium. The latter may be due to muscarinic receptor-mediated generation of inositol trisphosphate.

Published

1987