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663 results on '"Reis, Rui M."'

201. In vitro screening of cytotoxic activity of euphol from Euphorbia tirucalli on a large panel of human cancer-derived cell lines.

Author

Silva, Viviane Aline Oliveira, Rosa, Marcela Nunes, Tansini, Aline, Oliveira, Renato J.S., Martinho, Olga, Lima, João Paulo, Pianowski, Luiz F., and Reis, Rui M.

Subjects
EUPHORBIA, PANCREATIC cancer treatment, ANTINEOPLASTIC agents, PACLITAXEL, MEDICAL screening, THERAPEUTICS
Abstract

A large number of classic antineoplastic agents are derived from plants. Euphorbia tirucalli L. (Euphorbiaceae) is a subtropical and tropical plant, used in Brazilian folk medicine against many diseases, including cancer, yet little is known about its true anticancer properties. The present study evaluated the antitumor effect of the tetracyclic triterpene alcohol, euphol, the main constituent of E. tirucalli in a panel of 73 human cancer lines from 15 tumor types. The biological effect of euphol in pancreatic cells was also assessed. The combination index was further used to explore euphol interactions with standard drugs. Euphol showed a cytotoxicity effect against several cancer cell lines (IC50 range, 1.41-38.89 μM), particularly in esophageal squamous cell (11.08 μM) and pancreatic carcinoma cells (6.84 μM), followed by prostate, melanoma, and colon cancer. Cytotoxicity effects were seen in all cancer cell lines, with more than half deemed highly sensitive. Euphol inhibited proliferation, motility and colony formation in pancreatic cancer cells. Importantly, euphol exhibited synergistic interactions with gemcitabine and paclitaxel in pancreatic and esophageal cell lines, respectively. To the best of our knowledge, this study constitutes the largest in vitro screening of euphol efficacy on cancer cell lines and revealed its in vitro anti-cancer properties, particularly in pancreatic and esophageal cell lines, suggesting that euphol, either as a single agent or in combination with conventional chemotherapy, is a potential anti-cancer drug. [ABSTRACT FROM AUTHOR]

Published
2018
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202. Lymphangiogenic VEGF-C and VEGFR-3 expression in genetically characterised gastrointestinal stromal tumours

Author

Torres de Oliveira, Antônio Talvane, Reis, Rui M., Alfonso, Julieta, Martinho, Olga, Matos, Delcio, Lopes Carvalho, André, Buosi Silva, Thiago, Scapulatempo, Cristovam, Sydney Saad, Sarhan, and Longatto-Filho, Adhemar

Subjects
616 - Patología. Medicina clínica. Oncología, cardiovascular system, KIT, Gastrointestinal stromal tumor
Abstract

This study aimed to assess the distribution of VEGF-C and VEGFR-3 expression in gastrointestinal stromal tumours (GISTs), and to analyse the value of lymphatic vessel density (LVD) in a tumour that is believed to preferentially metastasize through blood vessel conduits. A panel of immunohistochemical antibodies was used to evaluate 51 cases of genetically characterised GISTs: VEGF-C, VEGFR-3, D2-40 (for LVD assessment) and CD31 (for blood vessel density – BDV – assessment). The results were correlated with the clinical-pathological data. The large majority of cases (86.2%; 44/51) showed a mutation of the KIT gene, most of them (72.5%; 37/51) revealing mutations in exon 11. VEGFR-3 was predominantly expressed in KIT mutated GISTs (p=0.019). High LVD was correlated with the absence of metastasis (p=0.010) and high BVD showed a positive correlation with the occurrence of metastasis (p=0.049). The strong expression of VEGF-C and VEGFR-3 in GIST’s cells was not correlated with the clinical parameters of aggressiveness, nor with high LVD.

Published
2011

204. KIAA1549

Author

Becker, Aline Paixão, primary, Scapulatempo-Neto, Cristovam, additional, Carloni, Adriana C., additional, Paulino, Alessandra, additional, Sheren, Jamie, additional, Aisner, Dara L., additional, Musselwhite, Evelyn, additional, Clara, Carlos, additional, Machado, Hélio R., additional, Oliveira, Ricardo S., additional, Neder, Luciano, additional, Varella-Garcia, Marileila, additional, and Reis, Rui M., additional

Published
2015
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206. A transcriptomic signature mediated by HOXA9 promotes human glioblastoma initiation, aggressiveness and resistance to temozolomide

Author

Pojo, Marta, primary, Gonçalves, Céline S., additional, Xavier-Magalhães, Ana, additional, Oliveira, Ana Isabel, additional, Gonçalves, Tiago, additional, Correia, Sara, additional, Rodrigues, Ana J., additional, Costa, Sandra, additional, Pinto, Luísa, additional, Pinto, Afonso A., additional, Lopes, José M., additional, Reis, Rui M., additional, Rocha, Miguel, additional, Sousa, Nuno, additional, and Costa, Bruno M., additional

Published
2015
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208. Lack of microsatellite instability in gastrointestinal stromal tumors.

Author

CAMPANELLA, NATHÁLIA C., SCAPULATEMPO-NETO, CRISTOVAM, ABRAHÃO-MACHADO, LUCAS FARIA, TORRES DE OLIVERIA, ANTÔNIO TALVANE, BERARDINELLI, GUSTAVO N., GUIMARÃES, DENISE PEIXOTO, and REIS, RUI M.

Subjects
MICROSATELLITE repeats, GASTROINTESTINAL stromal tumors, HUMAN phenotype, BIOMARKERS, CANCER immunotherapy
Abstract

The microsatellite instability (MSI) phenotype may constitute an important biomarker for patient response to immunotherapy, particularly to anti-programmed death-1 inhibitors. MSI is a type of genomic instability caused by a defect in DNA mismatch repair (MMR) proteins, which is present mainly in colorectal cancer and its hereditary form, hereditary nonpolyposis colorectal cancer. Gastrointestinal stromal tumor (GIST) development is associated with activating mutations of KIT proto-oncogene receptor tyrosine kinase (KIT) or platelet-derived growth factor receptor α (PDGFRA), which are oncogenes that predict the response to imatinib mesylate. In addition to KIT/PDGFRA mutations, other molecular alterations are important in GIST development. In GISTs, the characterization of the MSI phenotype is scarce and the results are not consensual. The present study aimed to assess MSI in a series of 79 GISTs. The evaluation of MSI was performed by pentaplex polymerase chain reaction comprising five markers, followed by capillary electrophoresis. The expression of MMR proteins was evaluated by immunohistochemistry. Regarding the KIT/PDGFRA/B-Raf proto-oncogene, serine/threonine kinase molecular profile of the 79 GISTs, 83.6% of the tumors possessed KIT mutations, 10.1% had PDGFRA mutations and 6.3% were triple wild-type. The mutated-PDGFRA cases were associated with gastric location and a lower mitotic index compared with KIT-mutated and wild-types, and these patients were more likely to be alive and without cancer. MSI analysis identified 4 cases with instability in one marker, however, additional evaluation of normal tissue and immunohistochemical staining of MMR proteins confirmed their microsatellite-stable nature. The results of the present study indicated that MSI is not involved in GIST tumorigenesis and, therefore, cannot serve as a biomarker to immunotherapy response in GIST. [ABSTRACT FROM AUTHOR]

Published
2017
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209. Low frequency of TERT promoter mutations in gastrointestinal stromal tumors (GISTs)

Author

Campanella, Nathália C, primary, Celestino, Ricardo, additional, Pestana, Ana, additional, Scapulatempo-Neto, Cristovam, additional, de Oliveira, Antonio Talvane, additional, Brito, Maria José, additional, Gouveia, António, additional, Lopes, José Manuel, additional, Guimarães, Denise Peixoto, additional, Soares, Paula, additional, and Reis, Rui M, additional

Published
2014
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211. Characterization of monocarboxylate transporters (MCTs) expression in soft tissue sarcomas: distinct prognostic impact of MCT1 sub-cellular localization

Author

Pinheiro, Céline, primary, Penna, Valter, additional, Morais-Santos, Filipa, additional, Abrahão-Machado, Lucas F, additional, Ribeiro, Guilherme, additional, Curcelli, Emílio C, additional, Olivieri, Marcus V, additional, Morini, Sandra, additional, Valença, Isabel, additional, Ribeiro, Daniela, additional, Schmitt, Fernando C, additional, Reis, Rui M, additional, and Baltazar, Fátima, additional

Published
2014
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212. Immunoglobulin genes implicated in glioma risk

Author

Pandey, Janardan P, primary, Kaur, Navtej, additional, Costa, Sandra, additional, Amorim, Julia, additional, Nabico, Rui, additional, Linhares, Paulo, additional, Vaz, Rui, additional, Viana-Pereira, Marta, additional, and Reis, Rui M, additional

Published
2014
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214. Histone H3.3. mutations drive pediatric glioblastoma through upregulation of MYCN.

Author

Bjerke, Lynn, Bjerke, Lynn, Mackay, Alan, Nandhabalan, Meera, Burford, Anna, Jury, Alexa, Popov, Sergey, Bax, Dorine A, Carvalho, Diana, Taylor, Kathryn R, Vinci, Maria, Bajrami, Ilirjana, McGonnell, Imelda M, Lord, Christopher J, Reis, Rui M, Hargrave, Darren, Ashworth, Alan, Workman, Paul, Jones, Chris, Bjerke, Lynn, Bjerke, Lynn, Mackay, Alan, Nandhabalan, Meera, Burford, Anna, Jury, Alexa, Popov, Sergey, Bax, Dorine A, Carvalho, Diana, Taylor, Kathryn R, Vinci, Maria, Bajrami, Ilirjana, McGonnell, Imelda M, Lord, Christopher J, Reis, Rui M, Hargrave, Darren, Ashworth, Alan, Workman, Paul, and Jones, Chris

Abstract

UnlabelledChildren and young adults with glioblastoma (GBM) have a median survival rate of only 12 to 15 months, and these GBMs are clinically and biologically distinct from histologically similar cancers in older adults. They are defined by highly specific mutations in the gene encoding the histone H3.3 variant H3F3A , occurring either at or close to key residues marked by methylation for regulation of transcription—K27 and G34. Here, we show that the cerebral hemisphere-specific G34 mutation drives a distinct expression signature through differential genomic binding of the K36 trimethylation mark (H3K36me3). The transcriptional program induced recapitulates that of the developing forebrain, and involves numerous markers of stem-cell maintenance, cell-fate decisions, and self-renewal.Critically, H3F3A G34 mutations cause profound upregulation of MYCN , a potent oncogene that is causative of GBMs when expressed in the correct developmental context. This driving aberration is selectively targetable in this patient population through inhibiting kinases responsible for stabilization of the protein.SignificanceWe provide the mechanistic explanation for how the fi rst histone gene mutation inhuman disease biology acts to deliver MYCN, a potent tumorigenic initiator, into a stem-cell compartment of the developing forebrain, selectively giving rise to incurable cerebral hemispheric GBM. Using synthetic lethal approaches to these mutant tumor cells provides a rational way to develop novel and highly selective treatment strategies

Published
2013

218. Abstract C118: TERT promoter mutations in human gliomas.

Author

Lima, Jorge, primary, Reis, Rui M., additional, Catarino, Telmo, additional, Peixoto, Joana, additional, Vinagre, Joao, additional, Batista, Rui, additional, Castro, Ligia, additional, Pardal, Fernando, additional, Sobrinho-Simoes, Manuel, additional, Maximo, Valdemar, additional, and Soares, Paula, additional

Published
2013
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219. Novel Oncogenic PDGFRA Mutations in Pediatric High-Grade Gliomas

Author

Paugh, Barbara S., primary, Zhu, Xiaoyan, additional, Qu, Chunxu, additional, Endersby, Raelene, additional, Diaz, Alexander K., additional, Zhang, Junyuan, additional, Bax, Dorine A., additional, Carvalho, Diana, additional, Reis, Rui M., additional, Onar-Thomas, Arzu, additional, Broniscer, Alberto, additional, Wetmore, Cynthia, additional, Zhang, Jinghui, additional, Jones, Chris, additional, Ellison, David W., additional, and Baker, Suzanne J., additional

Published
2013
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221. Histone H3.3 Mutations Drive Pediatric Glioblastoma through Upregulation of MYCN

Author

Bjerke, Lynn, primary, Mackay, Alan, additional, Nandhabalan, Meera, additional, Burford, Anna, additional, Jury, Alexa, additional, Popov, Sergey, additional, Bax, Dorine A., additional, Carvalho, Diana, additional, Taylor, Kathryn R., additional, Vinci, Maria, additional, Bajrami, Ilirjana, additional, McGonnell, Imelda M., additional, Lord, Christopher J., additional, Reis, Rui M., additional, Hargrave, Darren, additional, Ashworth, Alan, additional, Workman, Paul, additional, and Jones, Chris, additional

Published
2013
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227. Monocarboxylate transporters (MCTs) in gliomas: expression and exploitation as therapeutic targets

Author

Miranda-Gonçalves, Vera, primary, Honavar, Mrinalini, additional, Pinheiro, Céline, additional, Martinho, Olga, additional, Pires, Manuel M., additional, Pinheiro, Célia, additional, Cordeiro, Michelle, additional, Bebiano, Gil, additional, Costa, Paulo, additional, Palmeirim, Isabel, additional, Reis, Rui M., additional, and Baltazar, Fátima, additional

Published
2012
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228. KO-Homology and Type I String Theory

Author

Reis, Rui M. G., Szabo, Richard J., Valentino, Alessandro, Reis, Rui M. G., Szabo, Richard J., and Valentino, Alessandro

Abstract

We study the classification of D-branes and Ramond-Ramond fields in Type I string theory by developing a geometric description of KO-homology. We define an analytic version of KO-homology using KK-theory of real C*-algebras, and construct explicitly the isomorphism between geometric and analytic KO-homology. The construction involves recasting the Cl(n)-index theorem and a certain geometric invariant into a homological framework which is used, along with a definition of the real Chern character in KO-homology, to derive cohomological index formulas. We show that this invariant also naturally assigns torsion charges to non-BPS states in Type I string theory, in the construction of classes of D-branes in terms of topological KO-cycles. The formalism naturally captures the coupling of Ramond-Ramond fields to background D-branes which cancel global anomalies in the string theory path integral. We show that this is related to a physical interpretation of bivariant KK-theory in terms of decay processes on spacetime-filling branes. We also provide a construction of the holonomies of Ramond-Ramond fields in Type II string theory in terms of topological K-chains., Comment: 40 pages; v4: Clarifying comments added, more detailed proof of main isomorphism theorem given; Final version to be published in Reviews in Mathematical Physics

Published
2006
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229. Geometric K-Homology of Flat D-Branes

Author

Reis, Rui M. G., Szabo, Richard J., Reis, Rui M. G., and Szabo, Richard J.

Abstract

We use the Baum-Douglas construction of K-homology to explicitly describe various aspects of D-branes in Type II superstring theory in the absence of background supergravity form fields. We rigorously derive various stability criteria for states of D-branes and show how standard bound state constructions are naturally realized directly in terms of topological K-cycles. We formulate the mechanism of flux stabilization in terms of the K-homology of non-trivial fibre bundles. Along the way we derive a number of new mathematical results in topological K-homology of independent interest., Comment: 45 pages; v2: References added; v3: Some substantial revision and corrections, main results unchanged but presentation improved, references added; to be published in Communications in Mathematical Physics

Published
2005
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232. Strand-Specific miR-28-5p and miR-28-3p Have Distinct Effects in Colorectal Cancer Cells

Author

Almeida, Maria I., primary, Nicoloso, Milena S., additional, Zeng, Lizhi, additional, Ivan, Cristina, additional, Spizzo, Riccardo, additional, Gafà, Roberta, additional, Xiao, Lianchun, additional, Zhang, Xinna, additional, Vannini, Ivan, additional, Fanini, Francesca, additional, Fabbri, Muller, additional, Lanza, Giovanni, additional, Reis, Rui M., additional, Zweidler–McKay, Patrick A., additional, and Calin, George A., additional

Published
2012
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235. Impact ofEGFRGenetic Variants on Glioma Risk and Patient Outcome

Author

Costa, Bruno Marques, primary, Viana-Pereira, Marta, additional, Fernandes, Ricardo, additional, Costa, Sandra, additional, Linhares, Paulo, additional, Vaz, Rui, additional, Pinheiro, Céline, additional, Lima, Jorge, additional, Soares, Paula, additional, Silva, Ana, additional, Pardal, Fernando, additional, Amorim, Júlia, additional, Nabiço, Rui, additional, Almeida, Rui, additional, Alegria, Carlos, additional, Pires, Manuel Melo, additional, Pinheiro, Célia, additional, Carvalho, Ernesto, additional, Oliveira, Pedro, additional, Lopes, José M., additional, and Reis, Rui M., additional

Published
2011
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236. Monocarboxylate transporter 4 (MCT4) and CD147 overexpression is associated with poor prognosis in prostate cancer

Author

Pértega-Gomes, Nelma, primary, Vizcaíno, José R, additional, Miranda-Gonçalves, Vera, additional, Pinheiro, Céline, additional, Silva, Joana, additional, Pereira, Helena, additional, Monteiro, Pedro, additional, Henrique, Rui M, additional, Reis, Rui M, additional, Lopes, Carlos, additional, and Baltazar, Fátima, additional

Published
2011
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241. MGMT-Independent Temozolomide Resistance in Pediatric Glioblastoma Cells Associated with a PI3-Kinase–Mediated HOX/Stem Cell Gene Signature

Author

Gaspar, Nathalie, primary, Marshall, Lynley, additional, Perryman, Lara, additional, Bax, Dorine A., additional, Little, Suzanne E., additional, Viana-Pereira, Marta, additional, Sharp, Swee Y., additional, Vassal, Gilles, additional, Pearson, Andrew D.J., additional, Reis, Rui M., additional, Hargrave, Darren, additional, Workman, Paul, additional, and Jones, Chris, additional

Published
2010
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242. A Distinct Spectrum of Copy Number Aberrations in Pediatric High-Grade Gliomas

Author

Bax, Dorine A., primary, Mackay, Alan, additional, Little, Suzanne E., additional, Carvalho, Diana, additional, Viana-Pereira, Marta, additional, Tamber, Narinder, additional, Grigoriadis, Anita E., additional, Ashworth, Alan, additional, Reis, Rui M., additional, Ellison, David W., additional, Al-Sarraj, Safa, additional, Hargrave, Darren, additional, and Jones, Chris, additional

Published
2010
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244. The selective COX-2 inhibitor Etoricoxib reduces acute inflammatory markers in a model of neurogenic laryngitis but loses its efficacy with prolonged treatment

Author

Lima-Rodrigues, Manuel, primary, Lamas, Nuno, additional, Valle-Fernandes, Ana, additional, Cruz, Andrea, additional, Vieira, Artur, additional, Oliveira, Pedro, additional, Pedrosa, Jorge, additional, Castro, António G., additional, Reis, Rui M., additional, Baltazar, Fátima, additional, and Almeida, Armando, additional

Published
2010
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246. Reversing HOXA9 Oncogene Activation by PI3K Inhibition: Epigenetic Mechanism and Prognostic Significance in Human Glioblastoma

Author

Costa, Bruno M., primary, Smith, Justin S., additional, Chen, Ying, additional, Chen, Justin, additional, Phillips, Heidi S., additional, Aldape, Kenneth D., additional, Zardo, Giuseppe, additional, Nigro, Janice, additional, James, C. David, additional, Fridlyand, Jane, additional, Reis, Rui M., additional, and Costello, Joseph F., additional

Published
2010
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249. EGFRvIII Deletion Mutations in Pediatric High-Grade Glioma and Response to Targeted Therapy in Pediatric Glioma Cell Lines

Author

Bax, Dorine A., primary, Gaspar, Nathalie, additional, Little, Suzanne E., additional, Marshall, Lynley, additional, Perryman, Lara, additional, Regairaz, Marie, additional, Viana-Pereira, Marta, additional, Vuononvirta, Raisa, additional, Sharp, Swee Y., additional, Reis-Filho, Jorge S., additional, Stávale, João N., additional, Al-Sarraj, Safa, additional, Reis, Rui M., additional, Vassal, Gilles, additional, Pearson, Andrew D.J., additional, Hargrave, Darren, additional, Ellison, David W., additional, Workman, Paul, additional, and Jones, Chris, additional

Published
2009
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