39 results on '"Soares, Raquel"'
Search Results
2. Phenotypic and proliferative modulation of human mesenchymal stem cells via crosstalk with endothelial cells
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Bidarra, Sílvia J., Barrias, Cristina C., Barbosa, Mário A., Soares, Raquel, Amédée, Joelle, and Granja, Pedro L.
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- 2011
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3. The combination of traditional and auricular acupuncture to prevent xerostomia and anxiety in irradiated patients with HNSCC: a preventive, parallel, single-blind, 2-arm controlled study.
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Menezes, Agna Soares da Silva, Sanches, Gabriela Luize Guimarães, Gomes, Emisael Stênio Batista, Soares, Raquel Gusmão, Durães, Cristina Paixão, Fonseca, Larissa Lopes, Filho, Arlen de Paulo Santiago, Ribeiro, Adriana Aparecida Almeida de Aguiar, Nascimento, Jairo Evangelista, Santos, Sérgio Henrique Sousa, de Paula, Alfredo Maurício Batista, Farias, Lucyana Conceição, and Guimarães, André Luiz Sena
- Abstract
Objective: The purpose of the present study was to investigate the effect of acupuncture on xerostomia in irradiated patients with head and neck squamous cell carcinoma (HNSCC).Study Design: A preventive, 2-arm, parallel, single-blind trial was performed. Patients with HNSCC (N = 296) were checked for eligibility, and 107 patients were enrolled in the study. The study comprised 1 group that did not receive the intervention (n = 55) and the interventional group that received traditional and auricular acupuncture (n = 52). The primary outcome was the reduction of the patients' xerostomia after treatment. In addition, the secondary outcome was the reduction of anxiety.Results: The current acupuncture protocol reduced the xerostomia score and increased saliva volume and density without changing salivary pH. Additionally, acupuncture decreased the Beck Anxiety Inventory (BAI) score after radiation therapy.Conclusion: Combining traditional and auricular acupuncture reduced xerostomia and increased saliva volume without changing the saliva's pH in irradiated patients with HNSCC. Additionally, the combination of traditional and auricular acupuncture reduced BAI scores. [ABSTRACT FROM AUTHOR]- Published
- 2021
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4. Cardiac metastasizing leiomyoma: A case report.
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Reis Soares, Raquel, Ferber Drumond, Leonardo, Soares da Mata, Daniel, Miraglia Firpe, Luiza, Tavares Mendonça Garretto, João Victor, and Ferber Drumond, Matheus
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• We reported the case of Benign Metastasizing Leiomyomatosis (BML) in a female patient emphasizing the cardiac findings. • BML is a rare disorder that affects fertile aged women with a past medical history of treatment of uterine leiomyoma. • We suggest that benign metastasizing leiomyoma should be remembered as a differential diagnoses when a hysterectomized premenopausal woman presents with an intra cardiac mass. Cardiac intracavitary growth of metastasizing tumour is unusual. Benign Metastasizing Leiomyoma (BML) from the uterus to the heart is extremely rare. It affects premenopausal women with a history of uterine leiomyoma. We report a case of a 42-year-old woman who presented three tumours in the right side of the heart, two years after a hysterectomy due to leiomyomatosis. The cardiac tumours were resected and the diagnosis was uterine leiomyoma. The patient developed cardiac failure due to three masses at the right side of the heart. Cardiac involvement in BML is usually asymptomatic and rare. The heart masses were surgically removed and a peri ovarian mass was detected and also removed. Although histologically benign, BML exhibits metastatic qualities. It suggests that BML should be included as a differential diagnosis when a female patient presents an intra cardiac mass and a history of hysterectomy. [ABSTRACT FROM AUTHOR]
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- 2020
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5. Molecular effects of Microcystin-LA in tilapia (Oreochromis niloticus).
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Moreira, Daniel A., Soares, Raquel M., Valente, Richard H., Bebianno, Maria J., and Rebelo, Mauro F.
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NILE tilapia , *FRESHWATER fishes , *GENE expression , *EXPOSURE dose , *PROTEIN expression , *TILAPIA - Abstract
Nile tilapia (Oreochromis niloticus) is a freshwater phytoplanktivorous fish species reported to accumulate and tolerate large amounts of cyanotoxins such as microcystins (MCs). The present study aimed to investigate molecular responses to the acute exposure of Nile tilapia to the Microcystin-LA analogue (MC-LA). Thus, the specimens were sublethally exposed to 1000 μg kg−1 of MC-LA for 12, 24, 48, and 96 h. Gene expression of PP1, PP2A, GST, GPX and actin was analyzed by quantitative PCR. The protein abundance profile of PP2A was determined by immunoblotting, while the integrity of its biological function was assessed by a phosphatase enzymatic assay. PP2A activity was significantly and strongly reduced by MC-LA. A resulting feedback mechanism significantly increased PP2A gene expression and protein abundance in all assessed times. However, a recovery of that phosphatase activity was not observed. In this study, the observed increase in GPX gene expression was the only response that could be directly related to the unknown factors associated to the fish survival to such high dose exposure. • Tilapia survived to MC-LA high dose, even presenting a strong inhibition of PP2A. • PP2A inhibition leads to an increase in the transcription and translation of this protein. • GPX mRNA increasing could be related to the fish survival to such high dose exposure. [ABSTRACT FROM AUTHOR]
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- 2019
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6. Obesity and cancer phenotype: Is angiogenesis a missed link?
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Mendonça, Fernando and Soares, Raquel
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OBESITY , *PHENOTYPES , *NEOVASCULARIZATION , *FATTY acids , *ADIPOSE tissues , *INFLAMMATION , *ANTINEOPLASTIC agents - Abstract
Obesity remains nowadays one of the main threats to human health, being a problem of worldwide proportions. It is characterized by augmented storage of fatty acids in an enlarged adipose tissue. This process is possible thanks to a rich capillary network, supported by a mechanism that has also a crucial role on cancer: angiogenesis. Given that several studies point obesity as a risk factor for cancer development, angiogenesis may be approached as the missed link between these two pathologies. Understanding the different pathways behind angiogenesis becomes essential to break this link by developing new anti-angiogenic therapies or improving the actual ones. In the first phase, this paper will focus the structural and cellular changes that adipose tissue suffers in obesity. Then, the main pro-angiogenic players will be reviewed, taking into account the pathways that explain their putative role in obesity–cancer link. Finally, the clinical implications of the presented mechanisms will also be regarded, being the main focus on the anti-angiogenic therapies. [ABSTRACT FROM AUTHOR]
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- 2015
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7. Angiogenesis in the pathophysiology of schizophrenia — A comprehensive review and a conceptual hypothesis.
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Lopes, Rui, Soares, Raquel, Coelho, Rui, and Figueiredo-Braga, Margarida
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DIAGNOSIS of schizophrenia , *ETIOLOGY of schizophrenia , *MENTAL illness , *VASCULAR diseases , *NEOVASCULARIZATION , *BRAIN imaging , *PATHOLOGICAL physiology ,MEDICAL literature reviews - Abstract
Schizophrenia (SZ) is a severe mental disorder poorly elucidated from the etiopathogenesis prism. Recently, several micro- and macro-vascular abnormalities have been consistently implicated in SZ's pathophysiology. Since angiogenesis is involved in several biological functions and is a fundamental process in vascular formation and angioregulation, it can provide a framework in which some etiological factors and susceptibility genes for SZ can be linked together. We performed a comprehensive non-systematic review of the literature to explore the possible link between SZ and angiogenesis from a vascular perspective, taking into account new insights from genetic, molecular, neurochemical, animal, and neuroimaging functional studies. Recent molecular and neuroimaging studies indicate that angiogenesis could be involved in SZ etiopathogenesis through its role in neurogenesis during neurodevelopment, or by angiomodulation of cerebral blood flow (CBF). Furthermore, it has been hypothesized that the epidemiological finding of lesser predisposition of SZ patients to certain types of cancer could be derived by a putative interplay between SZ pathophysiology and angiogenesis. While it is yet unclear how a complex multivariate interplay between angiogenic factors, neurotrophins, dopamine and other neurotransmitters, brain angiogenic inhibitor molecules (BAI1–3) and patterns of regional blood flow may yield to a biological effect, the importance of further investigation and considering them as potential therapeutic targets for SZ is highlighted. [ABSTRACT FROM AUTHOR]
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- 2015
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8. Metabolic syndrome and risk of cancer: Which link?
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Mendonça, Fernando Miguel, de Sousa, Filipa Rodrigues, Barbosa, Ana Luísa, Martins, Sara Costa, Araújo, Raquel Lage, Soares, Raquel, and Abreu, Cristina
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METABOLIC syndrome ,CANCER risk factors ,DISEASE prevalence ,TUMOR growth ,SOMATOMEDIN ,PLASMINOGEN activator inhibitors - Abstract
Metabolic syndrome (MS) is characterized by a group of metabolic disturbances which lead to an enhanced risk of cardiovascular diseases and type 2 diabetes mellitus. MS constitutes a preoccupant issue with elevated prevalence in the western countries and is often related with cancer development. Elucidating the mechanisms linking these two pathologies is, therefore, essential to identify potential therapeutic molecular targets for cancer treatment in MS patients. The main goals of this review are, to identify the relation between MS and cancer development, handling specifically each one of the main players on this process: insulin and IGF system, estrogen, pro-inflammatory cytokines and others; and, given that colorectal cancer is one of the most prevalent types of cancer in MS patients, we intend to particularly highlight the mechanisms that promote colorectal cancer development in MS individuals. Finally, we will also focus on the clinical implications of the presented mechanisms on cancer therapy and care. [ABSTRACT FROM AUTHOR]
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- 2015
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9. Schizophrenia and cancer: Is angiogenesis a missed link?
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Lopes, Rui, Soares, Raquel, Figueiredo-Braga, Margarida, and Coelho, Rui
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SCHIZOPHRENIA risk factors , *EPIDEMIOLOGY of cancer , *NEOVASCULARIZATION , *PATHOLOGICAL physiology , *DISEASE prevalence , *DISEASE incidence , *ONCOLOGY - Abstract
Abstract: Cancer prevalence and risk in schizophrenia (SZ) patients, as well as their implicated molecular pathways, is a debate that has become increasingly appreciated, despite lacking evidence. Since angiogenesis is imbalanced in both conditions, a non-systematic review of the existing literature using the PubMed database was performed to summarize current knowledge and to elucidate hypothesis regarding the reduced incidence of cancer in SZ, exploring possible angiogenesis biology aspects that can be interrelated both with SZ and cancer. Some lines of evidence based in epidemiology, genetic, molecular and biochemical studies suggest a putative interplay between SZ pathophysiology and angiogenesis, involving different molecular pathways and also influencing cancer biology. Studying angiogenesis in SZ and its implications to cancer is an unexplored field that could provide more insightful knowledge regarding its pathophysiology and promote the development of treatment applications. [Copyright &y& Elsevier]
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- 2014
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10. Neovascularization in diabetes and its complications. Unraveling the angiogenic paradox.
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Costa, Paulo Zoé and Soares, Raquel
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NEOVASCULARIZATION , *DIABETES complications , *VASCULAR endothelial growth factors , *METABOLIC disorders , *HYPERGLYCEMIA , *KIDNEY diseases , *HYPOXIA-inducible factors - Abstract
Abstract: Diabetes mellitus (DM) is a chronic metabolic disease characterized by the presence of hyperglycemia, which can lead to many complications over time. These complications, such as nephropathy, retinopathy, neuropathy, impaired wound healing and accelerated atherosclerosis, are implicated with a large number of cellular and subcellular changes on vessels. In agreement, evidence indicates that in retinopathy, nephropathy and atherosclerotic plaque, there is excessive angiogenesis, whereas in wound healing and myocardial perfusion, blood vessel growth is impaired. Despite the awareness of this angiogenic paradox, many questions remain unanswered. This review aims at highlighting the different microvascular and macrovascular complications that are often concurrent in diabetic patients. A revision of the recent findings published in the literature regarding the angiogenic paradox will be performed. Apparently, endothelial dysfunction, as well as molecules such as vascular endothelial growth factor (VEGF) and hypoxia-inducible factor (HIF) play a major role in diabetic vascular complications. Specific tissues with impaired angiogenesis exhibit microenvironment features, such as increased PAI-1/uPA ratio and decreased blood flow, whereas TGFbeta increases extracellular matrix deposition, preventing the vascularization process. In addition, the monocytes/macrophages are important in endothelium activation for arteriogenesis and its arteriogenic response is reduced, leading to impaired collateral artery growth. Moreover, molecular mechanisms involved will be addressed, including abnormalities in growth factor, cytokines and metabolic derangements. [Copyright &y& Elsevier]
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- 2013
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11. Improving bacterial cellulose for blood vessel replacement: Functionalization with a chimeric protein containing a cellulose-binding module and an adhesion peptide.
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Andrade, Fábia K., Costa, Raquel, Domingues, Lucília, Soares, Raquel, and Gama, Miguel
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BACTERIAL cell surfaces ,CELLULOSE ,BLOOD-vessel transplantation ,CARRIER proteins ,CELL adhesion ,PEPTIDES ,RECOMBINANT proteins ,ENDOTHELIUM - Abstract
Abstract: Chimeric proteins containing a cellulose-binding module (CBM) and an adhesion peptide (RGD or GRGDY) were produced and used to improve the adhesion of human microvascular endothelial cells (HMEC) to bacterial cellulose (BC). The effect of these proteins on the HMEC–BC interaction was studied. The results obtained demonstrated that recombinant proteins containing adhesion sequences were able to significantly increase the attachment of HMEC to BC surfaces, especially the RGD sequence. The images obtained by scanning electron microscopy showed that the cells on the RGD-treated BC present a more elongated morphology 48h after cell seeding. The results also showed that RGD decreased the in-growth of HMEC cells through the BC and stimulated the early formation of cord-like structures by these endothelial cells. Thus, the use of recombinant proteins containing a CBM domain, with high affinity and specificity for cellulose surfaces allows control of the interaction of this material with cells. CBM may be combined with virtually any biologically active protein for the modification of cellulose-based materials, for in vitro or in vivo applications. [ABSTRACT FROM AUTHOR]
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- 2010
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12. Red wine increases adipose tissue aromatase expression and regulates body weight and adipocyte size
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Monteiro, Rosário, Soares, Raquel, Guerreiro, Susana, Pestana, Diogo, Calhau, Conceição, and Azevedo, Isabel
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RED wines , *AROMATASE , *REGULATION of body weight , *GENE expression , *FAT cells , *ADIPOSE tissues , *TISSUE analysis , *LABORATORY rats - Abstract
Abstract: Objective: Obesity is an important component of the metabolic syndrome in constituting a risk factor for cardiovascular disease, diabetes, and cancer. Estrogens influence lipid accumulation in adipocytes, acting indirectly or directly on adipose tissue. In this study we aimed to investigate the influence of red wine ingestion on the expression of aromatase (estrogen synthase) in adipose tissue. Methods: Red wine or ethanol solution, in the concentration found in red wine, was provided to Wistar rats as the sole drinking fluid for 8 wk. Food and drink intakes and body weight were monitored throughout treatment and adipocyte size and aromatase expression in the adipose tissue were determined at the end of the experimental period. Results: Red wine and ethanol increased aromatase expression in the adipose tissue and red wine decreased adipocyte size (P < 0.05). In addition, animals treated with red wine or ethanol had significantly lower weight gain than controls, despite a similar energy intake. Conclusion: Thus, the ingestion of red wine may alter the production of estrogens by adipose tissue, body weight gain, and adipocyte size. Some of these red wine effects are attributable to ethanol. This relation among estrogen availability, adipocyte biology, and weight gain is most interesting and deserves further study because it may lead to new strategies to reduce metabolic syndrome incidence. [Copyright &y& Elsevier]
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- 2009
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13. Effects of microcystin-LR on mouse lungs
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Soares, Raquel M., Cagido, Viviane R., Ferraro, Rodrigo B., Meyer-Fernandes, José Roberto, Rocco, Patrícia R.M., Zin, Walter A., and Azevedo, Sandra M.F.O.
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MICROCYSTINS , *LUNGS , *INFLAMMATION , *LABORATORY mice - Abstract
Abstract: Toxic cyanobacteria blooms in drinking water supplies have been an increasing public health concern all over the world. Human populations can be exposed to microcystins, an important family of cyanotoxins, mainly by oral ingestion. However, inhalation from recreational water and hemodialysis can represent other routes. This study investigated changes in respiratory mechanics, histology, protein phosphatase (PP) 1 and 2A activity and microcystin in lung of adult mice injected intraperitoneally (i.p.) with microcystin-LR. Thirty-six mice were divided into control (CTRL) and test (CYANO) groups. CTRL group received an i.p. injection of saline and the CYANO group received 40μg MCYST-LR/kg i.p. After 2 and 8h, and 1, 2 and 4 days after toxin injection, six mice from each group were sampled for analyses. Resistive and viscoelastic pressures, static and dynamic elastances augmented at 2h in CYANO and so remained until day 4. Alveolar collapse and inflammatory cell infiltration were found 2h after the injection, reaching peak values at 8h. However, no microcystin or inhibition of PPases could be detected in mice lungs. In conclusion, MCYST-LR led to a rapid increase in lung impedance and an inflammatory response with interstitial edema and inflammatory cell recruitment in mice. [Copyright &y& Elsevier]
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- 2007
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14. TAA 25. A New Off-Label Technique for a Total Endovascular Aortic Arch Repair.
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Ferber, Leonardo, Ferber, Matheus, Mata, Daniel Soares, Firpe, Luiza Miraglia, Soares, Raquel Reis, and Ferreira, Marcelo
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- 2019
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15. Accumulation and depuration of microcystins (cyanobacteria hepatotoxins) in Tilapia rendalli (Cichlidae) under laboratory conditions
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Soares, Raquel M., Magalhães, Valéria F., and Azevedo, Sandra M.F.O.
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FISHES , *MICROCYSTINS , *BACTERIAL toxins , *REDBREAST tilapia - Abstract
In order to understand accumulation and depuration of microcystins (MCYSTs) in Tilapia rendalli, three experiments with juveniles were done. The experiments simulated the fish diet during a Microcystis aeruginosa bloom in three different situations. In the first one each fish received daily, during 15 days, fish food plus toxic cells of M. aeruginosa (20.4μg MCYSTs fish-1 day-1). In the following 15 days they were fed without toxic cells. In the second experiment, fish were fed only with toxic cells during 28 days (14.6μg MCYSTs fish-1 day-1) and in the third experiment, during 42 days, fish were fed with fish food plus toxic cells (29.2μg MCYSTs fish-1 day-1) previously disrupted (to simulate a senescent bloom). MCYSTs analyses were done by enzyme-linked immunosorbent assay (ELISA) in liver and muscle samples in all experiments and in faeces in the first one (only in the depuration period). The results demonstrated different profiles of MCYSTs accumulation in liver and muscle of T. rendalli. Comparing the experiments, the highest MCYSTs accumulation in the liver (2.8μgg-1) occurred in the second one, where fish had only toxic cells as feeding source. In the first experiment, the highest MCYSTs accumulation in liver (0.6μg MCYSTs g-1) was observed during the accumulation period, while in muscle, interestingly, the highest concentration (0.05μg MCYSTs g-1) occurred in the depuration period. In this same period, it was also observed elimination of toxins through faeces. The second and third experiments showed almost the same average concentrations in tissues although fish have received more MCYSTs in third one. With respect to implications of the fish comsumption, MCYSTs accumulation in muscle of T. rendalli in all three experiments reached concentrations that would represent an intake of these toxins above the tolerable limit for humans and these results confirmed our previous observations from a field study. In conclusion, in this study it was observed that T. rendalli is able to accumulate MCYSTs and the availability of other feeding sources, besides toxic cells, probably interferes with the accumulation rate. Therefore, the occurrence of toxic cyanobacterial blooms produncing MCYSTs in aquaculture ponds could represent a risk to the quality of fish to the consumers. [Copyright &y& Elsevier]
- Published
- 2004
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16. TOI 4. Endovascular Treatment of Tracheoinnominate Artery Fistula.
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Ferber, Leonardo, Ferber, Matheus, Soares, Raquel Reis, Marcius de Carvalho Valle, Leonardo, Miranda, Pedro Caetano, Soares da Mata, Daniel, and Ferreira, Marcelo
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- 2018
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17. Exploring variations in glycolytic and gluconeogenic enzymes and isoforms across breast cancer cell lines and tissues.
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Luís, Carla, Fernandes, Rúben, and Soares, Raquel
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BREAST cancer , *CELL lines , *BREAST , *AMINO acid metabolism , *CANCER cells , *WARBURG Effect (Oncology) - Abstract
It is well established that tumour cells undergo metabolic changes to acquire biological advantage over normal cells with activation of the glycolytic pathway, a process termed "Warburg effect". Enzyme isoforms are alternative enzymatic forms with the same function but with different biochemical or epigenetic features. Moreover, isoforms may have varying impacts on different metabolic pathways. We challenge ourselves to analyse the glycolytic and gluconeogenic enzymes and isoforms in breast cancer, a complex and heterogeneous pathology, associated with high incidence and mortality rates especially among women. We analysed epithelial and tumour cell lines by RT-PCR and compared values to a publicly available database for the expression profile of normal and tumour tissues (Gepia) of enzymes and enzymatic isoforms from glycolytic and gluconeogenic pathways. Additionally, GeneMANIA was used to evaluate interactions, pathways, and attributes of each glycolytic/gluconeogenic steps. The findings reveal that the enzymes and enzymatic isoforms expressed in cell culture were somewhat different from those in breast tissue. We propose that the tumor microenvironment plays a crucial role in the expression of glycolytic and gluconeogenic enzymes and isoforms in tumour cells. Nonetheless, they not only participate in glycolytic and gluconeogenic enzymatic activities but may also influence other pathways, such as the Pentose-Phosphate-Pathway, TCA cycle, as well as other carbohydrate, lipid, and amino acid metabolism. [Display omitted] • Enzymatic isoforms may have varying impacts on different metabolic pathways. • Enzymatic isoforms expressed differently in cell culture from breast cancer tissue. • Glycolysis and gluconeogenic enzymatic isoforms present a distinct expression. [ABSTRACT FROM AUTHOR]
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- 2024
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18. Severe Chorioretinal Folds after Optical Neuritis.
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Miranda, Vítor, Matias, Maria J., and Soares, Raquel
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- 2023
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19. Inhibition of S1P by polyphenols prevents inflammation and angiogenesis: NFκB, a downstream effector?
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Soares, Raquel and Azevedo, Isabel
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- 2007
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20. Structure of the drug target ClpC1 unfoldase in action provides insights on antibiotic mechanism of action.
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Weinhäupl, Katharina, Gragera, Marcos, Bueno-Carrasco, M. Teresa, Arranz, Rocío, Krandor, Olga, Akopian, Tatos, Soares, Raquel, Rubin, Eric, Felix, Jan, and Fraga, Hugo
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DRUG target , *DRUG development , *MYCOBACTERIUM tuberculosis , *ANTIBIOTICS , *PROTEOLYSIS , *PROTEOLYTIC enzymes , *ADENOSINE triphosphatase - Abstract
The unfoldase ClpC1 is one of the most exciting drug targets against tuberculosis. This AAA+ unfoldase works in cooperation with the ClpP1P2 protease and is the target of at least four natural product antibiotics: cyclomarin, ecumicin, lassomycin, and rufomycin. Although these molecules are promising starting points for drug development, their mechanisms of action remain largely unknown. Taking advantage of a middle domain mutant, we determined the first structure of Mycobacterium tuberculosis ClpC1 in its apo, cyclomarin-, and ecumicin-bound states via cryo-EM. The obtained structure displays features observed in other members of the AAA+ family and provides a map for further drug development. While the apo and cyclomarin-bound structures are indistinguishable and have N-terminal domains that are invisible in their respective EM maps, around half of the ecumicin-bound ClpC1 particles display three of their six N-terminal domains in an extended conformation. Our structural observations suggest a mechanism where ecumicin functions by mimicking substrate binding, leading to ATPase activation and changes in protein degradation profile. [ABSTRACT FROM AUTHOR]
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- 2022
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21. Microcystins in South American aquatic ecosystems: Occurrence, toxicity and toxicological assays
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Dörr, Felipe Augusto, Pinto, Ernani, Soares, Raquel Moraes, and Feliciano de Oliveira e Azevedo, Sandra Maria
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MICROCYSTINS , *ALGAL blooms , *CYANOBACTERIA , *MICROCYSTIS , *HEMODIALYSIS , *AQUATIC ecology , *KIDNEY disease treatments , *TOXICOLOGY , *CONTAMINATION of drinking water - Abstract
Abstract: The acute poisoning of chronic renal patients during hemodialysis sessions in 1996 in Caruaru City (Pernambuco State, Brazil) stimulated an intensive search for the cause of this severe complication. This search culminated in the identification of microcystins (MC), hepatotoxic cyclic heptapeptides produced by cyanobacteria, as the causative agents. More than ten years later, additional research data provides us with a better understanding of the factors related to cyanobacterial bloom occurrence and production of MC in Brazil and other South American countries. The contamination of water bodies and formation of toxic blooms remains a very serious concern, especially in countries in which surface water is used as the main source for human consumption. The purpose of this review is to highlight the discoveries of the past 15 years that have brought South American researchers to their current level of understanding of toxic cyanobacteria species and that have contributed to their knowledge of factors related to MC production, mechanisms of action and consequences for human health and the environment. [ABSTRACT FROM AUTHOR]
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- 2010
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22. Can LASSBio 596 and dexamethasone treat acute lung and liver inflammation induced by microcystin-LR?
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Carvalho, Giovanna M.C., Oliveira, Vinícius R., Soares, Raquel M., Azevedo, Sandra M.F.O., Lima, Lidia M., Barreiro, Eliezer J., Valença, Samuel S., Saldiva, Paulo H.N., Faffe, Débora S., and Zin, Walter A.
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MICROCYSTINS , *INFLAMMATION treatment , *ANTI-inflammatory agents , *LABORATORY mice , *CYANOBACTERIA , *ADRENOCORTICAL hormones , *HISTOPATHOLOGY , *OXIDATIVE stress , *MICROBIAL peptides - Abstract
Abstract: The treatment of microcystin-LR (MCYST-LR)-induced lung inflammation has never been reported. Hence, LASSBio 596, an anti-inflammatory drug candidate, designed as symbiotic agent that modulates TNF-α levels and inhibits phosphodiesterase types 4 and 5, or dexamethasone were tested in this condition. Swiss mice were intraperitoneally (i.p.) injected with 60 μl of saline (CTRL) or a sub-lethal dose of MCYST-LR (40 μg/kg). 6 h later they were treated (i.p.) with saline (TOX), LASSBio 596 (10 mg/kg, L596), or dexamethasone (1 mg/kg, 0.1 mL, DEXA). 8 h after MCYST-LR injection, pulmonary mechanics were determined, and lungs and livers prepared for histopathology, biochemical analysis and quantification of MCYST-LR. TOX showed significantly higher lung impedance than CTRL and L596, which were similar. DEXA could only partially block the mechanical alterations. In both TOX and DEXA alveolar collapse and inflammatory cell influx were higher than in CTRL and L596, being LASSBio 596 more effective than dexamethasone. TOX showed oxidative stress that was not present in CTRL and L596, while DEXA was partially efficient. MCYST-LR was detected in the livers of all mice receiving MCYST-LR and no recovery was apparent. In conclusion, LASSBio 596 was more efficient than dexamethasone in reducing the pulmonary functional impairment induced by MCYST-LR. [Copyright &y& Elsevier]
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- 2010
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23. Effects of saxitoxins exposure on oligodendrocyte development in mouse neonates.
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Lima-Filho, Cesar Macedo, Nogaroli, Luciana, Hedin-Pereira, Cecilia, Azevedo, Sandra M.F.O., and Soares, Raquel M.
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CYANOBACTERIAL toxins , *OLIGODENDROGLIA , *PROGENITOR cells , *NEWBORN infants , *SODIUM channels , *NEURAL development , *INTRAPERITONEAL injections - Abstract
Saxitoxins (STXs) are neurotoxins produced by cyanobacteria and dinoflagellates, and they are primarily known to block voltage-gated sodium channels in neurons. The present study aimed to obtain further information regarding the effects of these toxins on neurodevelopment by investigating the responses of murine subventricular zone (SVZ) neural progenitors to STXs. An in vitro neonatal mouse SVZ explant model was exposed to different concentrations of toxic cyanobacterial extracts to evaluate the migration and differentiation of SVZ-derived progenitor cells. To test the ability of STX to cross the placental barrier, pregnant mice received a single intraperitoneal injection of STXs (7.5 μg/kg body weight) on gestational day fifteen. Immunocytochemistry was performed to detect proliferating and differentiating progenitors, including oligodendrocyte progenitor cells (OPCs). It was found that specific proliferation of OPCs was significantly increased, but there was no corresponding increase in the number of differentiated oligodendrocytes, which may indicate a negative effect on the maturation process of these cells. Additionally, the data showed that STXs crossed the placental barrier. Thus, STXs can be considered a potential risk to fetal neurodevelopment. • Saxitoxins can cross the placental barrier and reach fetuses' brains of mice. • Saxitoxins increases the number of oligodendrocyte progenitor cells, but not immature non-proliferative oligodendrocytes. • Results suggest that Saxitoxins can be considered a potential risk to fetal neurodevelopment. [ABSTRACT FROM AUTHOR]
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- 2020
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24. Warburg Effect Inversion: Adiposity shifts central primary metabolism in MCF-7 breast cancer cells.
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Luis, Carla, Duarte, Fernanda, Faria, Isabel, Jarak, Ivana, Oliveira, Pedro F., Alves, Marco G., Soares, Raquel, and Fernandes, Rúben
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METABOLISM , *CANCER cells , *BREAST cancer , *CELL metabolism , *OBESITY , *CELL survival - Abstract
Abstract Aims Obesity is a complex health disorder and a trigger to many diseases like Diabetes mellitus (DM) and breast cancer (BrCa), both leading causes of morbidity and mortality worldwide. Also evidence demonstrates that abnormal glucose metabolism termed 'the Warburg effect' in cancer cell is closely associated with malignant phenotypes and promote the aggressiveness of several types of cancer, including BrCa. In this study, we evaluated the breast cancer cell metabolism in normoglycemia, hyperglycemia and in an obesity condition in order to clarify the potential underlined mechanisms that link these disorders. Materials and methods MCF-7 cells were exposed to low and high glucose levels, the latter either in the presence of 3T3-L1 adipocyte conditioned medium (CM), thus mimicking the adiposity observed in obese patients. Cell viability, migration, proliferation, cytotoxicity and cell death assays were performed under the different culture conditions. Hormonal and lipid profile were also characterized by biochemical assays and primary metabolism was determined by Nuclear Magnetic Resonance (NMR)-based metabolomics. Results Our results show an increased aggressiveness in the condition mimicking diabetogenic obesity with an altered energy/lipid metabolism. Interestingly in the experimental obesity-mimicking status, lipids and amino acids were expended while glucose was produced by tumor cells from lactate. These findings reveal a shift on tumor cells metabolism that is opposite to 'the Warburg effect'. Conclusions Overall, this experimentally obesity-mimicking condition not only revealed an increased tumor proliferation and aggressiveness but also disclosed a new mechanism of cancer metabolism, the 'Warburg Effect Inversion'. [ABSTRACT FROM AUTHOR]
- Published
- 2019
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25. Oxidative imbalance in mice intoxicated by microcystin-LR can be minimized.
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Casquilho, Natália V., Moreira-Gomes, Maria Diana, Magalhães, Clarissa B., Okuro, Renata T., Ortenzi, Victor Hugo, Feitosa-Lima, Emanuel K., Lima, Lidia M., Barreiro, Eliezer J., Soares, Raquel M., Azevedo, Sandra M.F.O., Valença, Samuel S., Fortunato, Rodrigo S., Carvalho, Alysson Roncally, and Zin, Walter A.
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MICROCYSTINS , *CYANOBACTERIAL toxins , *ANTIOXIDANT analysis , *PHOSPHODIESTERASES , *MESSENGER RNA - Abstract
Microcystins-LR (MC-LR) is a cyanotoxin produced by cyanobacteria. We evaluated the antioxidant potential of LASSBio-596 (LB-596, inhibitor of phosphodiesterases 4 and 5), per os , and biochemical markers involved in lung and liver injury induced by exposure to sublethal dose of MC-LR. Fifty male Swiss mice received an intraperitoneal injection of 60 μL of saline (CTRL group, n = 20) or a sublethal dose of MC-LR (40 μg/kg, TOX group, n = 20). After 6 h the animals received either saline (TOX and CTRL groups) or LB-596 (50 mg/kg, TOX + LASS group, n = 10) by gavage. At 6 h after exposure, respiratory mechanics was evaluated in 10 CTRL and 10 TOX mice: there was a significant increase of all lung mechanics parameters (static elastance, viscoelastic component of elastance and lung resistive and viscoelastic/inhomogeneous pressures) in TOX compared to CTRL. 8 h after saline or MC-LR administration, i.e., 2 h after treatment with LB-596, blood serum levels of alanine aminotransferase and aspartate aminotransferase, activity of superoxide dismutase, catalase, and content of malondialdehyde and carbonyl in lung and liver, NADPH oxidase 2 and 4 mRNA expressions, dual oxidase enzyme activity and H 2 O 2 generation were analyzed in lung homogenates. All parameters were significantly higher in TOX than in the other groups. There was no significant difference between CTRL and TOX + LASS. MC-LR deteriorated lung and liver functions and induced redox imbalance in them, which was prevented by oral administration of LB-596. [ABSTRACT FROM AUTHOR]
- Published
- 2018
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26. Lung and liver responses to 1- and 7-day treatments with LASSBio-596 in mice subchronically intoxicated by microcystin-LR.
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Oliveira, Vinícius Rosa, Carvalho, Giovanna Marcella Cavalcante, Casquilho, Natália Vasconcelos, Moreira-Gomes, Maria Diana, Soares, Raquel Moraes, Azevedo, Sandra Maria F.O., Lima, Lidia Moreira, Barreiro, Eliezer Jesus, Takiya, Christina Maeda, and Zin, Walter Araujo
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MICROCYSTINS , *IMMUNOGLOBULINS , *POLYLACTIC acid , *HISTOLOGY , *LACTIC acid - Abstract
Microcystin-LR (MC-LR) can cause serious injuries upon short- and long-term exposures that can be prevented by LASSBio-596 (LB-596), an anti-inflammatory compound. We aimed to test LB-596 following subchronic exposure to MC-LR. Swiss mice received 10 intraperitoneal injections of distilled water (DW) or MC-LR (20 μg/kg bw) every 2 days. On the 10th injection animals receiving DW were gavaged with DW or 50 mg/kg bw of LB-596 for 1 or 7 days (C1D, C7D, CL1D and CL7D groups), whereas those exposed to MC-LR received either DW or 50 mg/kg of LB-596 for 1 or 7 days (T1D, T7D, TL1D and TL7D groups). Twelve hours after the last gavage we assessed respiratory mechanics, and extracted lung and liver for histology, apoptosis, inflammatory biomarkers and MC-LR content. C1D, C7D, CL1D and CL7D were all similar. Mechanical parameters were significantly higher in T1D and T7D compared to the other groups. LB-596 reversed these changes on day 1 of administration. LB-596 reduced inflammatory mediators in lung and liver on day 1 of treatment. On day 7 apoptosis in liver and lung fell even more. Briefly, 7-day administration completely reversed lung and liver changes. [ABSTRACT FROM AUTHOR]
- Published
- 2018
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27. Xanthohumol and 8-prenylnaringenin ameliorate diabetic-related metabolic dysfunctions in mice.
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Costa, Raquel, Rodrigues, Ilda, Guardão, Luísa, Rocha-Rodrigues, Sílvia, Silva, Carolina, Magalhães, José, Ferreira-de-Almeida, Manuel, Negrão, Rita, and Soares, Raquel
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METABOLIC disorders , *PEOPLE with diabetes , *TYPE 2 diabetes , *POLYPHENOLS , *LABORATORY mice , *DISEASES - Abstract
Type 2 diabetes mellitus (T2DM) is a chronic disease characterized by metabolic disturbances in specific tissues. The present work aimed to analyze the effects of xanthohumol (XN) and 8-prenylnaringenin (8PN), two beer-derived polyphenols, in liver and skeletal muscle lipid and glycolytic metabolism in T2DM mice model. Thirty C57Bl/6 mice were randomly divided into five groups: standard diet (control), high-fat diet (DM), high-fat diet plus ethanol (DM-Ethanol), high-fat diet plus 10 mg/L XN (DM-XN) and high-fat diet plus 10 mg/L 8PN (DM-8PN) during 20 weeks. Fasting blood glucose and insulin tolerance tests were performed 1 week before sacrifice. At the end of the study, blood, liver and skeletal muscle were collected. Both XN and 8PN treatments prevented body weight gain; decreased glycemia, triglyceride, cholesterol and alkaline phosphatase levels; and improved insulin sensitivity. Polyphenols promoted hepatic and skeletal muscle AMP-activated protein kinase (AMPK) activation, diminishing the expression of target lipogenic enzymes (sterol regulatory element binding protein-1c and fatty acid synthase) and acetyl-CoA carboxylase activity. Moreover, both XN and 8PN treatments decreased VEGFR-1/VEGFB pathway, involved in fatty acid uptake, and increased AS160 expression, involved in GLUT4 membrane translocation. Presented data demonstrated that both XN and 8PN treatment resulted in AMPK signaling pathway activation, thus suppressing lipogenesis. Their consumption prevented body weight gain and improved plasma lipid profile, with significant improvement of insulin resistance and glucose tolerance. XN- or 8PN-enriched diet could ameliorate diabetic-associated metabolic disturbances by regulating glucose and lipid pathways. [ABSTRACT FROM AUTHOR]
- Published
- 2017
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28. Melanoma and obesity: Should antioxidant vitamins be addressed?
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Oliveira, Sofia, Coelho, Pedro, Prudêncio, Cristina, Vieira, Mónica, Soares, Raquel, Guerreiro, Susana G., and Fernandes, Rúben
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MELANOMA treatment , *OBESITY treatment , *THERAPEUTIC use of antioxidants , *VITAMIN therapy , *EPIDEMICS - Abstract
Melanoma is an aggressive form of skin cancer refractory to conventional therapies. Obesity has reached epidemic dimensions acting as a risk factor for several cancer types, such as melanoma. Several reactive species of oxygen are also involved in melanoma initiation and progression. Low levels of antioxidant content and/or activity in lightly pigmented cells could expose them to an extremely oxidative environment and rise the susceptibility to oxidative damage and consequently loss of cell homeostasis. Despite the knowledge about melanoma biology, pathogenesis and developed therapies, is extremely important to understand the antioxidant modulation of melanoma under an environment of obesity, especially the effect of some natural compounds of the diet, such as antioxidant vitamins A, C and E and selenium in order to establish alternatives to conventional therapies, which are known to be ineffective against melanoma. [ABSTRACT FROM AUTHOR]
- Published
- 2016
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29. Pulmonary and hepatic injury after sub-chronic exposure to sublethal doses of microcystin-LR.
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Carvalho, Giovanna Marcella Cavalcante, Oliveira, Vinícius Rosa, Casquilho, Natália Vasconcelos, Araujo, Andressa Cristine Pereira, Soares, Raquel Moraes, Azevedo, Sandra Maria F.O., Pires, Karla Maria Pereira, Valença, Samuel Santos, and Zin, Walter Araujo
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MICROCYSTINS , *LUNG diseases , *LIVER diseases , *LABORATORY mice , *INTRAPERITONEAL injections - Abstract
We had previously shown that microcystin-LR (MCLR) could induce lung and liver inflammation after acute exposure. The biological outcomes following prolonged exposure to MCLR, although more frequent, are still poorly understood. Thus, we aimed to verify whether repeated doses of MCLR could damage lung and liver and evaluate the dose-dependence of the results. Male Swiss mice received 10 intraperitoneal injections ( i . p .) of distilled water (60 μL, CTRL) or different doses of MCLR (5 μg/kg, TOX5), 10 μg/kg (TOX10), 15 μg/kg (TOX15) and 20 μg/kg (TOX20) every other day. On the tenth injection respiratory mechanics (lung resistive and viscoelastic/inhomogeneous pressures, static elastance, and viscoelastic component of elastance) was measured. Lungs and liver were prepared for histology (morphometry and cellularity) and inflammatory mediators (KC and MIP-2) determination. All mechanical parameters and alveolar collapse were significantly higher in TOX5, 10, 15 and 20 than CTRL, but did not differ among them. Lung inflammatory cell content increased dose-dependently in all TOX groups in relation to CTRL, being TOX20 the largest. The production of KC was increased in lung and liver homogenates. MIP-2 increased in the liver of all TOX groups, but in lung homogenates it was significantly higher only in TOX20 group. All TOX mice livers showed steatosis, necrosis, inflammatory foci and a high degree of binucleated hepatocytes. In conclusion, sub-chronic exposure to MCLR damaged lung and liver in all doses, with a more important lung inflammation in TOX20 group. [ABSTRACT FROM AUTHOR]
- Published
- 2016
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30. Synthesis, antiangiogenesis evaluation and molecular docking studies of 1-aryl-3-[(thieno[3,2-b]pyridin-7-ylthio)phenyl]ureas: Discovery of a new substitution pattern for type II VEGFR-2 Tyr kinase inhibitors.
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Machado, Vera A., Peixoto, Daniela, Costa, Raquel, Froufe, Hugo J.C., Calhelha, Ricardo C., Abreu, Rui M.V., Ferreira, Isabel C.F.R., Soares, Raquel, and Queiroz, Maria-João R.P.
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PHENYLUREA compounds , *NEOVASCULARIZATION inhibitors , *PROTEIN-tyrosine kinase inhibitors , *CHEMICAL synthesis , *MOLECULAR docking , *DRUG development , *VASCULAR endothelial growth factor receptors , *IMMUNOSTAINING - Abstract
The synthesis and biological evaluation of novel 1-aryl-3-[2-, 3- or 4-(thieno[3,2- b ]pyridin-7-ylthio)phenyl]ureas 3 , 4 and 5 as VEGFR-2 tyrosine kinase inhibitors, are reported. The 1-aryl-3-[3-(thieno[3,2- b ]pyridin-7-ylthio)phenyl]ureas 4a – 4h , with the arylurea in the meta position to the thioether, showed the lowest IC 50 values in enzymatic assays (10–206 nM), the most potent compounds 4d – 4h (IC 50 10–28 nM) bearing hydrophobic groups (Me, F, CF 3 and Cl) in the terminal phenyl ring. A convincing rationalization was achieved for the highest potent compounds 4 as type II VEGFR-2 inhibitors, based on the simultaneous presence of: (1) the thioether linker and (2) the arylurea moiety in the meta position. For compounds 4 , significant inhibition of Human Umbilical Vein Endothelial Cells (HUVECs) proliferation (BrdU assay), migration (wound-healing assay) and tube formation were observed at low concentrations. These compounds have also shown to increase apoptosis using the TUNEL assay. Immunostaining for total and phosphorylated (active) VEGFR-2 was performed by Western blotting. The phosphorylation of the receptor was significantly inhibited at 1.0 and 2.5 μM for the most promising compounds. Altogether, these findings point to an antiangiogenic effect in HUVECs. [ABSTRACT FROM AUTHOR]
- Published
- 2015
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31. Repeated intranasal exposure to microcystin-LR affects lungs but not nasal epithelium in mice.
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Oliveira, Vinícius R., Mancin, Viviane G.L., Pinto, Eliete F., Soares, Raquel M., Azevedo, Sandra M.F.O., Macchione, Mariangela, Carvalho, Alysson R., and Zin, Walter A.
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MICROCYSTINS , *EPITHELIUM , *LABORATORY mice , *HEALTH outcome assessment , *RESPIRATORY disease diagnosis , *LUNG disease diagnosis , *PHYSIOLOGY - Abstract
Microcystin-LR (MC-LR) is a harmful cyanotoxin able to induce adverse outcomes in the respiratory system. We aimed to examine the lungs and nasal epithelium of mice following a sub-chronic exposure to MC-LR. Swiss mice were intranasally instilled with 10 μL of distilled water (CTRL, n = 10) or 6.7 ng/kg of MC-LR diluted in 10 μL of distilled water (TOX, n = 8) during 30 consecutive days. Respiratory mechanics was measured in vivo and histology measurements (morphology and inflammation) were assessed in lungs and nasal epithelium samples 24 h after the last intranasal instillation. Despite the lack of changes in the nasal epithelium, TOX mice displayed an increased amount of PMN cells in the lungs (× 10 −3 /μm 2 ), higher lung static elastance (cmH 2 O/mL), resistive and viscoelastic/inhomogeneous pressures (cmH 2 O) (7.87 ± 3.78, 33.96 ± 2.64, 1.03 ± 0.12, 1.01 ± 0.08, respectively) than CTRL (5.37 ± 4.02, 26.65 ± 1.24, 0.78 ± 0.06, 0.72 ± 0.05, respectively). Overall, our findings suggest that the nasal epithelium appears more resistant than lungs in this model of MC-LR intoxication. [ABSTRACT FROM AUTHOR]
- Published
- 2015
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32. Vascular biomarkers and correlation with peripheral vasculopathy in systemic sclerosis.
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Chora, Inês, Guiducci, Serena, Manetti, Mirko, Romano, Eloisa, Mazzotta, Celestina, Bellando-Randone, Silvia, Ibba-Manneschi, Lidia, Matucci-Cerinic, Marco, and Soares, Raquel
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PERIPHERAL vascular disease treatment , *BIOMARKERS , *CAPILLAROSCOPY , *NEOVASCULARIZATION , *STATISTICAL correlation , *CHEMOKINE receptors - Abstract
Vascular disease is a hallmark of systemic sclerosis (SSc). It is present in every patient, being responsible both for the earliest clinical manifestations and the major life-threatening complications of the disease, and thus determining important morbidity and mortality. In SSc, progressive vascular injury leads to vascular tone dysfunction and reduced capillary blood flow, with consequent tissue ischemia and chronic hypoxia. These phenomena are often accompanied by abnormal levels of vascular factors. Microangiopathy in SSc may be easily assessed by nailfold videocapillaroscopy. The variety of derangements detected in the nailfold capillaries is accompanied by abnormal levels of different vascular mediators and appears to be the best evaluable predictor of the development of peripheral vascular complications, such as digital ulcers. The purpose of this review is to summarize in SSc the most relevant vascular biomarkers and the main associations between vascular biomarkers and capillaroscopic parameters and/or the presence of digital ulcers. Vascular biomarkers could become useful predictive factors of vascular damage in SSc, allowing an earlier management of vascular complications. [ABSTRACT FROM AUTHOR]
- Published
- 2015
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33. The independent contribution of diabetic foot ulcer on lower extremity amputation and mortality risk.
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Martins-Mendes, Daniela, Monteiro-Soares, Matilde, Boyko, Edward John, Ribeiro, Manuela, Barata, Pedro, Lima, Jorge, and Soares, Raquel
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PEOPLE with diabetes , *LEG amputation , *ULCERS , *CAUSES of death , *RETROSPECTIVE studies , *COHORT analysis , *OUTPATIENT medical care , *DISEASE risk factors - Abstract
Aims: To estimate 3-year risk for diabetic foot ulcer (DFU), lower extremity amputation (LEA) and death; determine predictive variables and assess derived models accuracy. Material and Methods: Retrospective cohort study including all subjects with diabetes enrolled in our diabetic foot outpatient clinic from beginning 2002 until middle 2010. Data were collected from clinical records. Results: 644 subjects with mean age of 65.1 (±11.2) and diabetes duration of 16.1 (±10.8) years. Cumulative incidence was 26.6% for DFU, 5.8% for LEA and 14.0% for death. In multivariate analysis, physical impairment, peripheral arterial disease complication history, complication count and previous DFU were associated with DFU; complication count, foot pulses and previous DFU with LEA and age, complication count and previous DFU with death. Predictive models' areas under the ROC curves ranged from 0.80 to 0.83. A simplified model including previous DFU and complication count presented high accuracy. Previous DFU was associated with all outcomes, even when adjusted for complication count, in addition to more complex models. Conclusions: DFU seems more than a marker of complication status, having independent impact on LEA and mortality risk. Proposed models may be applicable in healthcare settings to identify patients at higher risk of DFU, LEA and death. [ABSTRACT FROM AUTHOR]
- Published
- 2014
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34. Neurokinin-1 receptor, a new modulator of lymphangiogenesis in obese-asthma phenotype.
- Author
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Ramalho, Renata, Almeida, Joana, Fernandes, Rubén, Costa, Raquel, Pirraco, Ana, Guardão, Luísa, Delgado, Luís, Moreira, André, and Soares, Raquel
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SUBSTANCE P receptors , *IMMUNOMODULATORS , *LYMPHANGIOGRAPHY , *OVERWEIGHT persons , *ASTHMA , *PHENOTYPES , *DISEASE prevalence , *PATHOLOGICAL physiology , *LABORATORY mice - Abstract
Abstract: Aims: Obesity and asthma are widely prevalent and associated disorders. Recent studies of our group revealed that Substance P (SP) is involved in pathophysiology of obese-asthma phenotype in mice through its selective NK1 receptor (NK1-R). Lymphangiogenesis is impaired in asthma and obesity, and SP activates contractile and inflammatory pathways in lymphatics. Our aim was to study whether NK1-R expression was involved in lymphangiogenesis on visceral (VAT) and subcutaneous (SAT) adipose tissues and in the lungs, in obese-allergen sensitized mice. Main methods: Diet-induced obese and ovalbumin (OVA)-sensitized Balb/c mice were treated with a selective NK1-R antagonist (CJ 12,255, Pfizer Inc., USA) or placebo. Lymphatic structures (LYVE-1+) and NK1-R expression were analyzed by immunohistochemistry. A semi-quantitative score methodology was used for NK1-R expression. Key findings: Obesity and allergen-sensitization together increased the number of LYVE-1+ lymphatics in VAT and decreased it in SAT and lungs. NK1-R was mainly expressed on adipocyte membranes of VAT, blood vessel areas of SAT, and in lung epithelium. Obesity and allergen-sensitization combined increased the expression of NK1-R in VAT, SAT and lungs. NK1-R antagonist treatment reversed the effects observed in lymphangiogenesis in those tissues. Significance: The obese-asthma phenotype in mice is accompanied by increased expression of NK1-R on adipose tissues and lung epithelium, reflecting that SP released during inflammation may act directly on these tissues. Blocking NK1-R affects lymphangiogenesis, implying a role of SP, with opposite physiological consequences in VAT, and in SAT and lungs. Our results provide a clue for a novel SP role in the obese-asthma phenotype. [Copyright &y& Elsevier]
- Published
- 2013
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35. Different effects of catechin on angiogenesis and inflammation depending on VEGF levels
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Negrão, Rita, Costa, Raquel, Duarte, Delfim, Gomes, Tiago Taveira, Azevedo, Isabel, and Soares, Raquel
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CATECHIN , *NEOVASCULARIZATION , *INFLAMMATION , *VASCULAR endothelial growth factors , *PATHOLOGICAL physiology , *ENDOTHELIAL cells , *POLYPHENOLS - Abstract
Abstract: Although physiological and pathological angiogenesis develop through similar processes, during pathological angiogenesis, proangiogenic factors are exacerbated. Polyphenols have been considered therapeutic tools for conditions exhibiting enhanced angiogenesis. However, the possibility that these compounds may also prevent vascularization in physiological situations is a major drawback for their use. The purpose of the current study was to investigate the effects of 0.1–100 μM catechin on endothelial cells (EC) and vascular smooth muscle cells (VSMC) regarding angiogenic and inflammatory processes. Catechin modulation of angiogenesis and inflammation was also evaluated in vivo using different models of angiogenesis: one physiological (skin wound-healing assay) and another one resembling pathological angiogenesis, exhibiting higher vascular endothelial growth factor (VEGF)-A stimulation (Matrigel plug assay). The in vitro results showed that 100 μM catechin increased viability (to 165.58% and to 165.34%) and decreased apoptosis (53.45% and 92.65%) and proliferation (33.19% and 23.36%) of EC and VSMC, respectively. Catechin affected migration and invasion, tending to increase both in EC and decreasing them in VSMC; however, it did not change sprouting angiogenesis. Nevertheless, catechin diminished in vitro inflammatory modulators such as tumor necrosis factor α (58.66% for human umbilical vein endothelial cells and 85.46% for human aortic smooth muscle cells) and nuclear factor kappa-B (38.43% for VSMC). The in vivo results demonstrated that catechin did not change angiogenesis and inflammation in skin wound-healing model and substantially decreased these processes in Matrigel plug assay. Altogether, the current study showed that catechin has different effects in angiogenesis and inflammation depending on VEGF-A levels. The absence of adverse effects in mature vasculature favors catechin potential use against pathological situations where angiogenesis is stimulated. [Copyright &y& Elsevier]
- Published
- 2013
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36. Injectable in situ crosslinkable RGD-modified alginate matrix for endothelial cells delivery
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Bidarra, Sílvia J., Barrias, Cristina C., Fonseca, Keila B., Barbosa, Mário A., Soares, Raquel A., and Granja, Pedro L.
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ALGINATES , *CELL adhesion , *TISSUE scaffolds , *ENDOTHELIUM , *CELLULAR therapy , *REGENERATION (Biology) , *CELL proliferation , *VASCULAR endothelium , *TISSUES - Abstract
Abstract: Cell-based therapies offer an attractive approach for revascularization and regeneration of tissues. However, and despite the pressing clinical needs for effective revascularization strategies, the successful immobilization of viable vascular cells within 3D matrices has been difficult to achieve. In this paper the in vitro potential of a natural, injectable RGD-alginate hydrogel as an in situ forming matrix to deliver endothelial cells was evaluated. Several techniques were employed to investigate how these microenvironments could influence the behavior of vascular cells, namely their ability to promote the outward migration of viable, proliferative cells, retaining the ability to form a 3D arrangement. Cells within RGD-grafted alginate hydrogel were able to proliferate and maintained 80% of viability for at least 48 h post-immobilization. Additionally, entrapped cells created a 3D organization into cellular networks and, when put in contact with matrigel, cells migrated out of the RGD-matrix. Overall, the obtained results support the idea that the RGD peptides conjugated to alginate provide a 3D environment for endothelial cells adhesion, survival, migration and organization. [Copyright &y& Elsevier]
- Published
- 2011
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37. LASSBio 596 per os avoids pulmonary and hepatic inflammation induced by microcystin-LR
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Casquilho, Natália V., Carvalho, Giovanna M.C., Alves, João L.C.R., Machado, Mariana N., Soares, Raquel M., Azevedo, Sandra M.F.O., Lima, Lidia M., Barreiro, Eliezer J., Valença, Samuel S., Carvalho, Alysson R., Faffe, Débora S., and Zin, Walter A.
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HEPATITIS prevention , *PNEUMONIA treatment , *MICROCYSTINS , *ANTI-inflammatory agents , *CYANOBACTERIAL blooms , *LUNG injury treatment , *LIVER injuries , *THERAPEUTICS , *HISTOLOGY - Abstract
Abstract: Cyanobacterial blooms that generate microcystins (MCYSTs) are increasingly recognized as an important health problem in aquatic ecosystems. We have previously reported the impairment of pulmonary structure and function by microcystin-LR (MCYST-LR) exposure as well as the pulmonary improvement by intraperitoneally injected (i.p.) LASSBio 596. In the present study, we aimed to evaluate the usefulness of LASSBio 596 per os on the treatment of pulmonary and hepatic injuries induced by MCYST-LR. Swiss mice received an intraperitoneal injection of 40 μl of saline (CTRL) or a sub-lethal dose of MCYST-LR (40 μg/kg). After 6 h the animals received either saline (TOX and CTRL groups) or LASSBio 596 (50 mg/kg, LASS group) by gavage. Eight hours after the first instillation, lung impedance (static elastance, elastic component of viscoelasticity and resistive, viscoelastic and total pressures) was determined by the end-inflation occlusion method. Left lung and liver were prepared for histology. In lung and hepatic homogenates MCYST-LR, TNF-α, IL-1β and IL-6 were determined by ELISA. LASSBio 596 per os (LASS mice) kept all lung mechanical parameters, polymorphonuclear (PMN) cells, pro-inflammatory mediators, and alveolar collapse similar to control mice (CTRL), whereas in TOX these findings were higher than CTRL. Likewise, liver structural deterioration (hepatocytes inflammation, necrosis and steatosis) and inflammatory process (high levels of pro-inflammatory mediators) were less evident in the LASS than TOX group. LASS and CTRL did not differ in any parameters studied. In conclusion, orally administered LASSBio 596 prevented lung and hepatic inflammation and completely blocked pulmonary functional and morphological changes induced by MCYST-LR. [Copyright &y& Elsevier]
- Published
- 2011
- Full Text
- View/download PDF
38. Wound healing activity of the human antimicrobial peptide LL37
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Ramos, Reinaldo, Silva, João Pedro, Rodrigues, Ana Cristina, Costa, Raquel, Guardão, Luísa, Schmitt, Fernando, Soares, Raquel, Vilanova, Manuel, Domingues, Lucília, and Gama, Miguel
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ANTIMICROBIAL peptides , *WOUND healing , *IMMUNE system , *NEOVASCULARIZATION , *PEPTIDES , *RECOMBINANT proteins , *LABORATORY mice , *REGENERATION (Biology) - Abstract
Abstract: Antimicrobial peptides (AMPs) are part of the innate immune system and are generally defined as cationic, amphipathic peptides, with less than 50 amino acids, including multiple arginine and lysine residues. The human cathelicidin antimicrobial peptide LL37 can be found at different concentrations in many different cells, tissues and body fluids and has a broad spectrum of antimicrobial and immunomodulatory activities. The healing of wound is a complex process that involves different steps: hemostasis, inflammation, remodeling/granulation tissue formation and re-epithelialization. Inflammation and angiogenesis are two fundamental physiological conditions implicated in this process. We have recently developed a new method for the expression and purification of recombinant LL37. In this work, we show that the recombinant peptide P-LL37 with a N-terminus proline preserves its immunophysiological properties in vitro and in vivo. P-LL37 neutralized the activation of macrophages by lipopolysaccharide (LPS). Besides, the peptide induced proliferation, migration and tubule-like structures formation by endothelial cells. Wound healing experiments were performed in dexamethasone-treated mice to study the effect of LL37 on angiogenesis and wound regeneration. The topical application of synthetic and recombinant LL37 increased vascularization and re-epithelialization. Taken together, these results clearly demonstrate that LL37 may have a key role in wound regeneration through vascularization. [Copyright &y& Elsevier]
- Published
- 2011
- Full Text
- View/download PDF
39. Distinct modulation of alkaline phosphatase isoenzymes by 17β-estradiol and xanthohumol in breast cancer MCF-7 cells
- Author
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Guerreiro, Susana, Monteiro, Rosário, Martins, Maria João, Calhau, Conceição, Azevedo, Isabel, and Soares, Raquel
- Subjects
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ISOENZYMES , *ALKALINE phosphatase , *BREAST cancer , *CELL proliferation - Abstract
Abstract: Objectives: : To examine the effect of 17β-estradiol and xanthohumol in alkaline phosphatase (ALP) expression and activity in breast cancer MCF-7 cells. Design and methods: : ALP isoenzymes expression was evaluated by RT-PCR and Western blotting. ALP activity was measured by spectrophotometry. Cell proliferation and apoptosis were examined by MTT and immunostaining for KI67 and TUNEL, respectively. Results: : ALP isoenzymes expression and activity were decreased by 1 nM 17β-estradiol. Pure estrogenic antagonist (ICI 182,780) reversed 17β-estradiol-inhibiting effect in TNS-ALP expression. RNA and protein expression of IALP, but not TNS-ALP, was also decreased by incubation with 10 μM xanthohumol (IC50) and was accompanied by a significant reduction in ALP activity. Treatment with 17β-estradiol enhanced cell proliferation and decreased apoptosis. Conversely, xanthohumol incubation inhibited cell viability and apoptosis. Conclusion: : Estrogens and xanthohumol differently modulate ALP isoenzymes. ALP loss associated with increased cell proliferation. Modulation of this enzyme by 17β-estradiol and xanthohumol might provide therapeutic strategies against hormone-dependent breast cancer. [Copyright &y& Elsevier]
- Published
- 2007
- Full Text
- View/download PDF
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