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9 results on '"Galatola, G."'

3. Effects of pellets and impurity injection on runaway control experiments on FTU

Author

Romano, A., Tudisco, O., Rubino, G., Ramogida, G., Napoli, F., Meineri, C., Iafrati, M., Giovannozzi, E., Galatola, G., Fusco, V., Esposito, B., Di Troia, C., D'Arcangelo, O., Cordella, F., Claps, G., Cianfarani, C., Ceccuzzi, S., Botrugno, A., Bagnato, F., Apruzzese, G., Tilia, B., Sibio, S., Gabellieri, L., Buratti, P., Boncagni, L., Bombarda, F., Romano, A., Tudisco, O., Rubino, G.,, Ramogida, G., Napoli, F., Meineri, C., Iafrati, M., Giovannozzi, E., Galatola, G., Fusco, V., Esposito, B., Di Troia, C., D'Arcangelo, O., Cordella, F., Claps, G., Cianfarani, C., Ceccuzzi, S., Botrugno, A., Bagnato, F., Apruzzese, G., Tilia, B., Sibio, S., Gabellieri, L., Buratti, P., Boncagni, L., and Bombarda, F.

Published
2018

4. DTT - Divertor Tokamak Test facility - Interim Design Report

Author

Affinito, L., Almaviva, S., Anemona, A., Angelone, M., Apicella, M. L., Appi, A., Apruzzese, G., Artaserse, G., Barone, G., Baruzzo, M., Batistoni, P., Bombarda, F., Boncagni, L., Buratti, P., Caiffi, B., Caneve, L., Caponero, M., Cardinali, A., Ceccuzzi, S., Centioli, C., Claps, G., Cocilovo, V., Colangeli, A., Colao, F., Contessa, G. M., Corato, V., Cordella, F., Crisanti, F., Cucchiaro, A., D’arcangelo, O., Della Corte, A., Luca, R., Di Pace, L., Di Zenobio, A., Dose, G., Fiamozzi Zignani, C., Flammini, D., Fonnesu, N., Frattolillo, A., Gabellieri, L., Galatola, G., Giannini, L., Giovannozzi, E., Grieco, M. T., Guardati, M., Iafrati, M., Iovinella, I., Lampasi, A., Lanchi, C., Lazic, V., Liuzza, D., Maddaluno, G., Magagnino, S., Mancini, A., Marocco, D., Martelli, E., Mazzitelli, G., Mazzotta, C., Messina, G., Monti, C., Morici, L., Moro, F., Muzzi, L., Pacella, D., Pillon, M., Piron, C., Pizzuto, A., Pollastrone, F., Polli, G. M., Pospodarczyk, M., Ramogida, G., Ravera, G. L., Righetti, R., Roccella, S., Romanelli, G., Romano, A., Romano, R., Rydzy, A., Sandri, S., Starace, F., Tuccillo, A. A., Tudisco, O., Turtù, S., Vellucci, M., Villari, R., Viola, B., Vitale, V., Vlad, G., Zerbini, M., Zito, P., Zoboli, L., Zonca, F., Alessi, E., Baiocchi, B., Bin, W., Bruschi, A., Causa, F., Cremona, A., Fanale, F., Farina, D., Figini, L., Garavaglia, S., Granucci, G., Lontano, M., Moro, A., Muraro, A., Nowak, S., Perelli, E., Ricci, D., Schmuck, S., Sozzi, C., Tardocchi, M., Uccello, A., William, B., Albanese, R., Ambrosino, R., Ariola, M., Castaldo, A., Coccorese, D., Coccorese, V., Magistris, M., Tommasi, G., Di Gironimo, G., Fresa, R., Grazioso, S., Loschiavo, V. P., Martone, R., Marzullo, D., Mattei, M., Mele, A., Mozzillo, R., Orsitto, F. P., Pironti, A., Rubinacci, G., Tarallo, A., Ventre, S., Villone, F., ROBERTO BONIFETTO, Maggiora, Riccardo, DANIELE MILANESIO, Giuseppe Francesco Nallo, Laura Savoldi, Fabio SUBBA, Zanino, Roberto, ANDREA ZAPPATORE, Agostinetti, P., Agostini, M., Barbisan, M., Bolzonella, T., Carraro, L., Castaldo, C., Cavazzana, R., Masi, G., Fassina, A., Ferro, A., Franz, P., Giacomelli, L., Giudicotti, L., Gnesotto, F., Gobbin, M., Innocente, P., Luchetta, A., Manduchi, G., Marrelli, L., Martin, P., Martines, E., Moressa, M., Pasqualotto, R., Peruzzo, S., Piron, L., Puiatti, M. E., Scarin, P., Sonato, P., Spizzo, G., Spolaore, M., Terranova, D., Valisa, M., Vallar, M., Vianello, N., Vincenzi, P., Zaniol, B., Zuin, M., Calabrò, G., Lombroni, R., Minucci, S., Gorini, G., Nocente, M., Santis, A., Maggiacomo, L., Mariano, G., Osipenko, M., Ripani, M., Murtas, F., and Luis, R.

Subjects
Nuclear fusion, Nuclear fusion, Divertor Tokamak Test, Divertor Tokamak Test
Published
2019

6. Helicobacter pylori -induced inflammation masks the underlying presence of low-grade dysplasia on gastric lesions.

Author

Panarese A, Galatola G, Armentano R, Pimentel-Nunes P, Ierardi E, Caruso ML, Pesce F, Lenti MV, Palmitessa V, Coletta S, and Shahini E

Subjects
Adult, Female, Gastric Mucosa pathology, Humans, Hyperplasia pathology, Inflammation pathology, Male, Metaplasia pathology, Middle Aged, Helicobacter Infections complications, Helicobacter Infections drug therapy, Helicobacter Infections pathology, Helicobacter pylori, Stomach Neoplasms pathology
Abstract

Background: Helicobacter pylori (H. pylori) infection has been associated with a long-term risk of precancerous gastric conditions (PGC) even after H. pylori eradication., Aim: To investigate the efficacy of High-Resolution White-Light Endoscopy with Narrow-Band Imaging in detecting PGC, before/after H. pylori eradication., Methods: We studied 85 consecutive patients with H. pylori -related gastritis with/without PGC before and 6 mo after proven H. pylori eradication. Kimura-Takemoto modified and endoscopic grading of gastric intestinal metaplasia classifications, were applied to assess the endoscopic extension of atrophy and intestinal metaplasia. The histological result was considered to be the gold standard. The Sydney System, the Operative-Link on Gastritis-Assessment, and the Operative-Link on Gastric-Intestinal Metaplasia were used for defining histological gastritis, atrophy and intestinal metaplasia, whereas dysplasia was graded according to World Health Organization classification. Serum anti-parietal cell antibody and anti-intrinsic factor were measured when autoimmune atrophic gastritis was suspected., Results: After H. pylori eradication histological signs of mononuclear/polymorphonuclear cell infiltration and Mucosal Associated Lymphoid Tissue-hyperplasia, disappeared or decreased in 100% and 96.5% of patients respectively, whereas the Operative-Link on Gastritis-Assessment and Operative-Link on Gastric-Intestinal Metaplasia stages did not change. Low-Grade Dysplasia prevalence was similar on random biopsies before and after H. pylori eradication (17.6% vs 10.6%, P = 0.19), but increased in patients with visible lesions (0% vs 22.4%, P < 0.0001). At a multivariate analysis, the probability for detecting dysplasia after resolution of H. pylori -related active inflammation was higher in patients with regression or reduction of Mucosal Associated Lymphoid Tissue hyperplasia, greater alcohol consumption, and anti-parietal cell antibody and/or anti-intrinsic factor positivity [odds ratio (OR) = 3.88, 95% confidence interval (CI): 1.31-11.49, P = 0.01; OR = 3.10, 95%CI: 1.05-9.12, P = 0.04 and OR = 5.47, 95%CI: 1.33-22.39, P < 0.04, respectively]., Conclusion: High-Resolution White-Light Endoscopy with Narrow-Band Imaging allows an accurate diagnosis of Low-Grade Dysplasia on visible lesions after regression of H. pylori -induced chronic gastritis. Patients with an overlap between autoimmune/ H. pylori -induced gastritis may require more extensive gastric mapping., Competing Interests: Conflict-of-interest statement: There are no conflicts of interest to report., (©The Author(s) 2020. Published by Baishideng Publishing Group Inc. All rights reserved.)

Published
2020
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7. Comparing CT colonography and flexible sigmoidoscopy: a randomised trial within a population-based screening programme.

Author

Regge D, Iussich G, Segnan N, Correale L, Hassan C, Arrigoni A, Asnaghi R, Bestagini P, Bulighin G, Cassinis MC, Ederle A, Ferraris A, Galatola G, Gallo T, Gandini G, Garretti L, Martina MC, Molinar D, Montemezzi S, Morra L, Motton M, Occhipinti P, Pinali L, Soardi GA, and Senore C

Subjects
Adenoma pathology, Colorectal Neoplasms pathology, Female, Humans, Male, Middle Aged, Patient Acceptance of Health Care statistics & numerical data, Sex Factors, Adenoma diagnostic imaging, Colonic Polyps diagnostic imaging, Colonography, Computed Tomographic, Colorectal Neoplasms diagnostic imaging, Early Detection of Cancer methods, Sigmoidoscopy
Abstract

Importance and Aims: The role of CT colonography (CTC) as a colorectal cancer (CRC) screening test is uncertain. The aim of our trial was to compare participation and detection rate (DR) with sigmoidoscopy (flexible sigmoidoscopy (FS)) and CTC in a screening setting., Design Setting and Participants: We conducted two randomised clinical trials (RCTs). (1) Participation RCT: individuals, aged 58 years, living in Turin (Italy), were randomly assigned to be invited to FS or CTC screening; (2) detection RCT: residents in northern Italy, aged 58-60, giving their consent to recruitment, were randomly allocated to CTC or FS. Polyps ≥6 mm at CTC, or 'high-risk' distal lesions at FS, were referred for colonoscopy (TC)., Main Outcome Measures: Participation rate (proportion of invitees examined); DR of advanced adenomas or CRC (advanced neoplasia (AN))., Results: Participation was 30.4% (298/980) for CTC and 27.4% (267/976) for FS (relative risk (RR) 1.1; 95% CI 0.98 to 1.29). Among men, participation was higher with CTC than with FS (34.1% vs 26.5%, p=0.011). In the detection RCT, 2673 subjects had FS and 2595 had CTC: the AN DR was 4.8% (127/2673, including 9 CRCs) with FS and 5.1% (133/2595, including 10 CRCs) with CTC (RR 1.08; 95% CI 0.85 to 1.37). Distal AN DR was 3.9% (109/2673) with FS and 2.9% (76/2595) with CTC (RR 0.72; 95% CI 0.54 to 0.96); proximal AN DR was 1.2% (34/2595) for FS vs 2.7% (69/2595) for CTC (RR 2.06; 95% CI 1.37 to 3.10)., Conclusions and Relevance: Participation and DR for FS and CTC were comparable. AN DR was twice as high in the proximal colon and lower in the distal colon with CTC than with FS. Men were more likely to participate in CTC screening., Trial Registration Number: NCT01739608; Pre-results., (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://www.bmj.com/company/products-services/rights-and-licensing/.)

Published
2017
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9. Stromal contribution to the colorectal cancer transcriptome.

Author

Isella C, Terrasi A, Bellomo SE, Petti C, Galatola G, Muratore A, Mellano A, Senetta R, Cassenti A, Sonetto C, Inghirami G, Trusolino L, Fekete Z, De Ridder M, Cassoni P, Storme G, Bertotti A, and Medico E

Subjects
Animals, Biomarkers, Tumor genetics, Cell Line, Tumor, Colorectal Neoplasms metabolism, Epithelial-Mesenchymal Transition genetics, Fibroblasts pathology, Gene Expression Regulation, Neoplastic, Heterografts, Humans, Mice, Microarray Analysis, Stromal Cells metabolism, Stromal Cells pathology, Colorectal Neoplasms genetics, Colorectal Neoplasms pathology, Fibroblasts metabolism, Transcriptome
Abstract

Recent studies identified a poor-prognosis stem/serrated/mesenchymal (SSM) transcriptional subtype of colorectal cancer (CRC). We noted that genes upregulated in this subtype are also prominently expressed by stromal cells, suggesting that SSM transcripts could derive from stromal rather than epithelial cancer cells. To test this hypothesis, we analyzed CRC expression data from patient-derived xenografts, where mouse stroma supports human cancer cells. Species-specific expression analysis showed that the mRNA levels of SSM genes were mostly due to stromal expression. Transcriptional signatures built to specifically report the abundance of cancer-associated fibroblasts (CAFs), leukocytes or endothelial cells all had significantly higher expression in human CRC samples of the SSM subtype. High expression of the CAF signature was associated with poor prognosis in untreated CRC, and joint high expression of the stromal signatures predicted resistance to radiotherapy in rectal cancer. These data show that the distinctive transcriptional and clinical features of the SSM subtype can be ascribed to its particularly abundant stromal component.

Published
2015
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