Your search keyword '"Silva, I.D."' showing total 4 results

1. Relationship between Genetic Polymorphism of CYP1A1at Codon 462 (Ile462Val) in Colorectal Cancer

Author

Serafim, P.V. Pereira, da Silva, I.D. Cotrim Guerreiro, and Forones, N. Manoukian

Abstract

Aims and background The enzyme cytochrome P450 plays an important role in the metabolization and detoxification of various compounds. CYP1A1 is a polymorphic enzyme and some of its alleles have been correlated with an increased risk of developing various types of cancer. The aim of this study was to investigate the incidence of the polymorphism A→G (Ile462Val, exon 7) in colorectal cancer patients and the correlation of this polymorphism with others risk factors.Patients and methods 114 Brazilian patients with colorectal cancer were matched by age and sex to 114 healthy individuals. DNA was extracted from peripheral blood and the genotypes of the polymorphisms were assessed by PCR-restriction fragment length polymorphism.Results In the case group 64 subjects were male, 53 were alcohol users and 68 were smokers. In the control group 61 were male, 67 were alcohol users and 53 smokers. There were 14 subjects with wild-type homozygous A/A, 97 with heterozygous A/G, and 3 with homozygous mutated G/G in the cancer group versus 81 subjects with wild-type homozygous A/A and 33 with heterozygous A/G in the control group. The presence of the G allele (OR 5.14, 95%CI 3.15–10.80) was associated with an increased risk of colorectal cancer (p=0.001). The prevalence of smokers was higher in the cancer group (p=0.047, OR 1.71, 95%CI 1.03–3.11).Conclusion These results suggest a positive association between the A→G polymorphism and the risk of colorectal cancer. In addition, smoking was also a colorectal cancer risk. We did not find any correlation between this polymorphism and sex, grade of differentiation, stage, or evolution of the disease.

Published

2008

2. Molecular Structure and Alternative Splicing of the Human Carboxypeptidase M Gene

Author

Pessoa, L.G., Silva, I.D. Guerreiro da, Baptista, H.A., Pesquero, J.L., Paiva, A.C.M., Bader, M., and Pesquero, J.B.

Abstract

AbstractUsing RACE technology the 5 and 3 ends of human carboxypeptidase M (CPM) mRNA were determined and found to be divergent from the published sequence. With these results the complete structure of the human CPM gene was established based on the human genome sequence in the GenBank database. The gene was shown to contain 9 exons comprising at least 75 kb of genomic sequence. A novel first exon of 30 bp was identified and an upstream promoter sequence containing several transcription factor binding sites was found by computer analysis. Furthermore, the ATG starting codon was detected defining an open reading frame of 1329 bp that codes for a protein of 443 residues. Additionally, the polyadenylation site was discovered, determining a 3 noncoding region of 2000 nucleotides. The exonintron boundaries diverged substantially compared to those of the other basic carboxypeptidases, CPD, CPE, CPN, and AEBP1. Cloning and sequencing of RTPCR products from different tissues revealed alternative splicing of exons 3 and 5, which results in the generation of four different mRNA isoforms. RNA extracted from tumor tissues contained more CPM mRNA than control tissue, suggesting an upregulation of CPM expression in tumors and raising the question of the role of this enzyme in cancer.

Published

2002

3. OR36: Changes in Expression in Intestinal Tissue of BMPS of Type 2 Diabetes Patients Submitted to ROUX-EN-Y Gastricbypass.

Author

Belarmino, G., Sala, P., Machado, N.M., Fonseca, D.C., Ishida, R.K., Guarda, I.F., Moura, E.G., Sakai, P., Santo, M.A., Silva, I.D., Heymsfield, S.B., Torrinhas, R.S., Giannella-Neto, D., and Waitzberg, D.L.

Published

2016

4. PP098. Lipidic fingerprinting in women with early-onset preeclampsia: A first look.

Author

Oliveira, L. De, Korkes, H., Turco, E. Lo, Bertola, R., Sass, N., Bonetti, T., Moron, A.F., and Silva, I.D. Da

Subjects

PREECLAMPSIA, PREGNANT women, INFLAMMATION, NEOVASCULARIZATION inhibitors, OBESITY in women, ENDOTHELIUM, GESTATIONAL age, HEALTH outcome assessment

Abstract

Introduction: preeclampsia is characterized by intense inflammatory response and an anti-angiogenic state. Maternal obesity has been considered to have important impact on the genesis of preeclampsia as lipotoxicity leads to maternal endothelial dysfunction and chronic inflammation. Here we investigate the plasma lipid profile of preeclamptic women. Objectives: identify possible lipid biomarkers for preeclampsia. Methods: this study included 8 pregnant women with early-onset preeclampsia (before 34weeks gestation) and 8 normal pregnant women. Each patient in the preeclampsia group was matched to a patient in the control group according to gestational age at the time of sample collection. All patients in the control group were followed until term and had normal outcomes. To investigate the lipid profile, lipids were extracted from plasma samples using the Bligh-Dyer protocol and the extracts were subjected to MALDI-TOF Mass Spectrometry. Data matrix was exported for partial least squares discriminant analysis. All the variables analysed were sorted by a score number named Variable Importance in the Projection. The major discriminant variables were selected and underwent to Mann–Whitney U test. Results: a total of 1290 ions were initially identified during lipidomic assessment. Twelve m/z signals were highlighted as the most important lipids for the discrimination of patients with preeclampsia. The identification of these differential lipids was carried out through Lipid Database Search. The main classes identified were Glycerophosphocholines [GP01], Glycerophosphoserines [GP03], Glycerophosphoglycerols [GP04], Glycosyldiradylglycerols [GL05] and Glycerophosphates [GP10]. Conclusion: Our results suggest that some lipid species may be potential biomarkers for early-onset preeclampsia. [Copyright &y& Elsevier]

Published

2012