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Dive into the research topics where Yasmine Nonose is active.

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Featured researches published by Yasmine Nonose.


Neuroscience Letters | 2012

Morphine treatment in early life alters glutamate uptake in the spinal synaptosomes of adult rats.

Joanna Ripoll Rozisky; Deusa Vendite; Fernanda Urruth Fontella; Yasmine Nonose; Gabriela Laste; Carla Dalmaz; Wolnei Caumo; Iraci Lucena da Silva Torres

Morphine exposure during the neonatal period can promote changes in pain signaling pathways that can be expressed as an increased nociceptive response in adult life. Glutamate is the major excitatory neurotransmitter in primary afferent terminals and plays a critical role in normal spinal excitatory synaptic transmission. Considering the importance of a better understanding of the mechanisms that underlie nociceptive changes throughout the life course, the aim of this study was investigate the effects of repeated morphine administration at postnatal days 8 (P8) to 14 (P14) on glutamate uptake in spinal synaptosomes at P30 and P60. The morphine group showed decreased [3H]-glutamate uptake as compared to control groups in both P30 and P60. These findings suggest that morphine exposure in early life leads to changes in glutamatergic signaling at least until the 60th day of age, which may lead to increased levels of glutamate in the spinal synaptic cleft and, consequently, an increased nociceptive response in adult life. Thus, this study highlights the importance of conducting research in this field to provide a comprehensive knowledge of the long-term effects of early-life morphine treatment on nociceptive pathways.


Journal of Experimental Pharmacology | 2012

Morphine treatment alters nucleotidase activities in rat blood serum

Joanna Ripoll Rozisky; Yasmine Nonose; Gabriela Laste; Vinícius Souza dos Santos; Isabel Cristina de Macedo; Ana Maria Oliveira Battastini; Wolnei Caumo; Iraci Ls Torres

Morphine has been widely used in neonatal pain management. However, this treatment may produce adaptive changes in several physiologic systems. Our laboratory has demonstrated that morphine treatment in neonate rats alters nucleoside triphosphate diphosphohydrolase (NTPDase) activity and gene expression in central nervous system structures. Considering the relationship between the opioid and purinergic systems, our aim was to verify whether treatment with morphine from postnatal days 8 (P8) through 14 (P14) at a dose of 5 μg per day alters NTPDase and 5′-nucleotidase activities in rat serum over the short, medium, and long terms. After the in vivo assay, the morphine group showed increased hydrolysis of all nucleotides at P30, and a decrease in adenosine 5′-diphosphate hydrolysis at P60. Moreover, we found that nucleotidase activities change with age; adenosine 5′-triphosphate hydrolysis activity was lower at P16, and adenosine 5′-monophosphate hydrolysis activity was higher at P60. These changes are very important because these enzymes are the main regulators of blood nucleotide levels and, consequently, nucleotide signaling. Our findings showed that in vivo morphine treatment alters nucleotide hydrolysis in rat blood serum, suggesting that purine homeostasis can be influenced by opioid treatment during the neonatal period.


Frontiers in Neuroscience | 2016

Cerebral Ketone Body Oxidation Is Facilitated by a High Fat Diet Enriched with Advanced Glycation End Products in Normal and Diabetic Rats

Adriano Martimbianco de Assis; Jussemara Souza da Silva; Anderson Rech; Aline Longoni; Yasmine Nonose; Cendrine Repond; Matheus Augusto de Bittencourt Pasquali; José Cláudio Fonseca Moreira; Diogo O. Souza; Luc Pellerin

Diabetes mellitus (DM) causes important modifications in the availability and use of different energy substrates in various organs and tissues. Similarly, dietary manipulations such as high fat diets also affect systemic energy metabolism. However, how the brain adapts to these situations remains unclear. To investigate these issues, control and alloxan-induced type I diabetic rats were fed either a standard or a high fat diet enriched with advanced glycation end products (AGEs) (HAGE diet). The HAGE diet increased their levels of blood ketone bodies, and this effect was exacerbated by DM induction. To determine the effects of diet and/or DM induction on key cerebral bioenergetic parameters, both ketone bodies (β-hydroxybutyric acid) and lactate oxidation were measured. In parallel, the expression of Monocarboxylate Transporter 1 (MCT1) and 2 (MCT2) isoforms in hippocampal and cortical slices from rats submitted to these diets was assessed. Ketone body oxidation increased while lactate oxidation decreased in hippocampal and cortical slices in both control and diabetic rats fed a HAGE diet. In parallel, the expression of both MCT1 and MCT2 increased only in the cerebral cortex in diabetic rats fed a HAGE diet. These results suggest a shift in the preferential cerebral energy substrate utilization in favor of ketone bodies in animals fed a HAGE diet, an effect that, in DM animals, is accompanied by the enhanced expression of the related transporters.


Neuropeptides | 2015

Chronic stress associated with hypercaloric diet changes the hippocampal BDNF levels in male Wistar rats

Isabel Cristina de Macedo; Joanna Ripoll Rozisky; Cleverson Moraes de Oliveira; C.M. Oliveira; Gabriela Laste; Yasmine Nonose; Vinícius Souza dos Santos; P.R. Marques; Maria Flavia Marques Ribeiro; Wolnei Caumo; I.L.S. Torres


Molecular Neurobiology | 2018

Homocysteine Induces Glial Reactivity in Adult Rat Astrocyte Cultures

Aline Longoni; Bruna Bellaver; Larissa Daniele Bobermin; Camila Leite Santos; Yasmine Nonose; Janaína Kolling; Tiago dos Santos; Adriano Martimbianco de Assis; André Quincozes-Santos; Angela Terezinha de Souza Wyse


Molecular Neurobiology | 2018

Cortical Bilateral Adaptations in Rats Submitted to Focal Cerebral Ischemia: Emphasis on Glial Metabolism

Yasmine Nonose; Pedro E. Gewehr; Roberto Farina de Almeida; Jussemara Souza da Silva; Bruna Bellaver; Leo Anderson Meira Martins; Eduardo Rigon Zimmer; Samuel Greggio; Gianina Teribele Venturin; Jaderson Costa da Costa; André Quincozes-Santos; Luc Pellerin; Diogo O. Souza; Adriano Martimbianco de Assis


Archive | 2016

Metabolismo energético cerebral é modulado em modelo experimental de isquemia focal permanente

P.E. Gewehr; Yasmine Nonose; Roberto Farina de Almeida; Jussemara Souza da Silva; Vitoria Brum da Silva Nunes; Leonardo Hekman D'Avila; Bruna Bellaver; André Quincozes-Santos; Diogo Onofre Gomes de Souza; Adriano Martimbianco de Assis


Archive | 2016

Modelo experimental de isquemia cerebral altera parâmetros astrocitários

Vitoria Brum da Silva Nunes; P.E. Gewehr; Yasmine Nonose; Jaderson Costa da Costa; Leo Anderson Meira Martins; Eduardo Rigon Zimmer; Gianina Teribele Venturin; Samuel Greggio; Diogo de Souza; Adriano Martimbianco de Assis


Archive | 2014

Efeito neuroprotetor da administração de guanosina em modelo experimental de hiperamonemia aguda em ratos

Diogo Onofre Gomes de Souza; P. Guazelli; D. M. Garcia; Lucas Guazzelli Paim Paniz; G. Santos; Karine Duarte Curvello; Yasmine Nonose; J. Souza; Adriano Martimbianco de Assis; Maria Elisa Calcagnotto


Archive | 2012

Neonathal morphine treatment alters glutamate uptake in spinal cord of rats

Vinícius Souza dos Santos; Joanna Ripoll Rozisky; Yasmine Nonose; Fernanda Urruth Fontella; Deusa Vendite; Carla Dalmaz; Wolnei Caumo; Iraci Lucena da Silva Torres

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Joanna Ripoll Rozisky

Universidade Federal do Rio Grande do Sul

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Iraci Lucena da Silva Torres

Universidade Federal do Rio Grande do Sul

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Gabriela Laste

Universidade Federal do Rio Grande do Sul

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Vinícius Souza dos Santos

Universidade Federal do Rio Grande do Sul

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Isabel Cristina de Macedo

Universidade Federal do Rio Grande do Sul

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Adriano Martimbianco de Assis

Universidade Federal do Rio Grande do Sul

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Ana Maria Oliveira Battastini

Universidade Federal do Rio Grande do Sul

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Cleverson Moraes de Oliveira

Universidade Federal do Rio Grande do Sul

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Carla de Oliveira

Universidade Federal do Rio Grande do Sul

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Wolnei Caumo

Universidade Federal do Rio Grande do Sul

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