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Start Over Author "Vaz, Fátima" Publisher elsevier b.v.
7 results on '"Vaz, Fátima"'

3. Evening and morning peroxiredoxin-2 redox/oligomeric state changes in obstructive sleep apnea red blood cells: Correlation with polysomnographic and metabolic parameters.

Author

Feliciano, Amélia, Vaz, Fátima, Torres, Vukosava M, Valentim-Coelho, Cristina, Silva, Rita, Prosinecki, Vesna, Alexandre, Bruno M, Carvalho, Ana S, Matthiesen, Rune, Malhotra, Atul, Pinto, Paula, Bárbara, Cristina, and Penque, Deborah

Subjects
*SLEEP apnea syndromes, *METABOLIC disorders, *POLYSOMNOGRAPHY, *PEROXIREDOXINS, *ERYTHROCYTES, *MOLECULAR chaperones, *DIAGNOSIS
Abstract

We have examined the effects of Obstructive Sleep Apnea (OSA) on red blood cell (RBC) proteome variation at evening/morning day time to uncover new insights into OSA-induced RBC dysfunction that may lead to OSA manifestations. Dysregulated proteins mainly fall in the group of catalytic enzymes, stress response and redox regulators such as peroxiredoxin 2 (PRDX2). Validation assays confirmed that at morning the monomeric/dimeric forms of PRDX2 were more overoxidized in OSA RBC compared to evening samples. Six month of positive airway pressure (PAP) treatment decreased this overoxidation and generated multimeric overoxidized forms associated with chaperone/transduction signaling activity of PRDX2. Morning levels of overoxidized PRDX2 correlated with polysomnographic (PSG)-arousal index and metabolic parameters whereas the evening level of disulfide-linked dimer (associated with peroxidase activity of PRDX2) correlated with PSG parameters. After treatment, morning overoxidized multimer of PRDX2 negatively correlated with fasting glucose and dopamine levels. Overall, these data point toward severe oxidative stress and altered antioxidant homeostasis in OSA RBC occurring mainly at morning time but with consequences till evening. The beneficial effect of PAP involves modulation of the redox/oligomeric state of PRDX2, whose mechanism and associated chaperone/transduction signaling functions deserves further investigation. RBC PRDX2 is a promising candidate biomarker for OSA severity and treatment monitoring, warranting further investigation and validation. [ABSTRACT FROM AUTHOR]

Published
2017
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5. 235 Nasopharyngeal cancer chemotherapy – before or after curative chemoradiation?

Author

Magno, Sara, Freitas, Rita, Dunões, Inês, Vicente, Inês, Machado, Madalena, Pereira, Margarida, Vaz, Fátima, and Sargento, Isabel

Subjects
*CANCER chemotherapy, *NASOPHARYNX cancer, *TERMINATION of treatment, *CHEMORADIOTHERAPY, *HEALTH facilities
Abstract

Nasopharyngeal carcinomas (NPC) are endemic in southeast Asia and rare in Europe with an incidence of 0.07/100.000 persons. Five-year survival is about 50%. Diagnosis is provided by histological findings and staging classification is done according to AJCC. EBV DNA serum levels should be determined before and after local treatment, carry prognostic significance and can be used in the active surveillance of cancer survivors. The best method for serum determination of EBV DNA is still under discussion. Advanced locoregional disease carries a greater risk of distant spread, highlighting the need of treatment intensification in higher risk patients. The best treatment plan is still under discussion: concurrent chemoradiation followed by adjuvant chemotherapy (ACT) or induction chemotherapy (ICT) followed by chemoradiation. ACT/ICT regimens should consist of two-/three-drug regimens, including a platinum agent and the best drug regimen is still under investigation. ACT carries great toxicity (50% require dose reductions, 60% complete treatment) and has a relatively low PFS and OS benefit. ICT is better tolerated, but may compromise cisplatin cumulative dose in concomitant chemoradiation and delay radiation start, possibly compromising the effectiveness of local treatment. Nonetheless, ICT improves PFS and OS when compared to chemoradiation alone, mostly because of better metastasis free survival (MFS), making this a promising strategy in properly selected high risk patients. Most NPC trials were conducted in countries where NPC is endemic, primarily non-queratinizing and EBV-related. Data in non-endemic countries are lacking. Our study aims to compare ACT and ICT in locally advanced and oligometastatic NPC patients treated in a European reference centre. Retrospective, observational study of patients with NPC diagnosis between January 2017 and September 2023 and disease stage III-IVb. Data were collected from patient records and included patient characteristics (gender, age, smoking history, ECOG performance status), tumor characteristics (T, N, staging, histology, EBV-status) and treatment characteristics (ACT, ICT, toxicities). PFS and OS were analyzed. Toxicity grading is according to CTCAE 5.0 and statistical analysis is descriptive. A total of 69 patients were included. Most patients were male (56.5%, n=39) with a median age of 53.0 years (18-75). Most patients had a good performance status (0 or 1 in 98.5%, n=68). Stage IVa was the most frequent initial staging (50.7%, n=35), with a majority of patients having T4 (33.3%, n=23) and N3 (39.1%, n=27) tumours. All tumours were undifferentiated queratinizing carcinomas and 86.9% (n=60) were EBV-positive. EBV DNA was rarely determined. [Display omitted] Until 2019 the most frequent treatment strategy was ACT with cisplatin-5FU (57.9%, n=40), after which ICT became more frequently used (15.9%, n=11), mostly with cisplatin-gemcitabin (45.4%, n=5). ICT had less acute toxicities that lead to treatment discontinuation (0.9% (n=1) versus 39.7% (n=23)). All patients completed radiotherapy after ICT, but in 4 patients optimal concomitant cisplatin dose (≥200mg/m2) was compromised. Both ICT and ACT showed good response rates, with a complete response in 63.6% versus 79.3%, respectively. Median follow up was 45 months in the ACT group (4-125) and 27 months (1-55) in the ICT group. PFS with ACT was 45.0 months (95%CI 34.8-55.2) and OS was 46.0 months (95%CI 38.5-53.4). The ICT group is small and has a short follow-up time; PFS and OS data will be determined in the future. [Display omitted] The best course of treatment of advanced NPC is still unclear - which patients and histologies benefit most from treatment intensification? What is the role of EBV DNA and what is the best method for its determination? Should ACT or ICT be preferred? Which chemotherapy regimen is better? Treatment center expertise and the ability to provide timely treatment may also play a role in treatment decisions. Our study presents the experience of a European reference centre where ACT was the preferred treatment for a longer period of time and therefore has a significantly larger patient population with longer follow-up time. ACT seems to provide good patient outcomes, despite a worse toxicity profile and more related treatment discontinuations, but group comparison is not yet possible since our centre only recently changed strategies in managing advanced NPC patients, preferring ICT over ACT. ICT patients are still underrepresented in this analysis, with fewer patients and shorter follow-up time. Moreover, the ICT patient group has more advanced disease, including IVb oligometastatic disease (that was not included in the intensification ACT and ICT studies), making head-to-head comparisons difficult. The management of advanced NPC is a clinical challenge and more data are needed to better select both patients and treatment strategies for treatment intensification, while taking into consideration the differences between endemic and non-endemic NPC. [ABSTRACT FROM AUTHOR]

Published
2024
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7. Supramolecular organizations in the aerobic respiratory chain of Escherichia coli

Author

Sousa, Pedro M.F., Silva, Sara T.N., Hood, Brian L., Charro, Nuno, Carita, João N., Vaz, Fátima, Penque, Deborah, Conrads, Thomas P., and Melo, Ana M.P.

Subjects
*ESCHERICHIA coli, *MICROBIAL respiration, *BIOENERGETICS, *OXIDOREDUCTASES, *MASS spectrometry, *PHENAZINE, *ETHYLENEDIAMINETETRAACETIC acid, *SULFONIC acids, *LIQUID chromatography, *DEHYDROGENASES
Abstract

Abstract: The organization of respiratory chain complexes in supercomplexes has been shown in the mitochondria of several eukaryotes and in the cell membranes of some bacteria. These supercomplexes are suggested to be important for oxidative phosphorylation efficiency and to prevent the formation of reactive oxygen species. Here we describe, for the first time, the identification of supramolecular organizations in the aerobic respiratory chain of Escherichia coli, including a trimer of succinate dehydrogenase. Furthermore, two heterooligomerizations have been shown: one resulting from the association of the NADH:quinone oxidoreductases NDH-1 and NDH-2, and another composed by the cytochrome bo 3 quinol:oxygen reductase, cytochrome bd quinol:oxygen reductase and formate dehydrogenase (fdo). These results are supported by blue native-electrophoresis, mass spectrometry and kinetic data of wild type and mutant E . coli strains. [Copyright &y& Elsevier]

Published
2011
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