Your search keyword '"Carvalho-Tavares, Juliana"' showing total 7 results

1. Automatic detection of motion blur in intravital video microscopy image sequences via directional statistics of log-Gabor energy maps

Author

Ferrari, Ricardo J., Villa Pinto, Carlos H., Gregório da Silva, Bruno C., Bernardes, Danielle, and Carvalho-Tavares, Juliana

Published

2015

2. Salivation pattern of Rhodnius prolixus (Reduviidae; Triatominae) in mouse skin

Author

Soares, Adriana Coelho, Carvalho-Tavares, Juliana, Gontijo, Nelder de Figueiredo, dos Santos, Vânia Cristina, Teixeira, Mauro Martins, and Pereira, Marcos Horácio

Subjects

*RHODNIUS prolixus, *INSECT feeding & feeds, *ACRIDINE, *TRIATOMA, *SALIVARY glands, *IMMUNE response

Abstract

Abstract: The objective of this work was to study the pattern of salivation of triatomines during feeding in mouse skin. Rhodnius prolixus was fed with a solution of the dye acridine orange or fluorescein. The saliva was efficiently labelled with acridine orange, probably due to the difference in pH between the salivary gland (⩽6.0) and the hemolymph (6.5–7.0). This procedure was not effective at labelling the saliva of Triatoma infestans, however, fluorescent labelling of R. prolixus saliva allowed us to demonstrate that salivation occurs during entire feeding process. The saliva is released soon after the bite. In the probing phase, saliva is pumped continuously in the host skin, including around the blood vessels. During the engorgement phase, saliva is observed in a bolus within the blood vessel and some of it is sucked up by the insect, together with blood. The frequency of saliva emission inside the vessels was low (0.51±0.18Hz). The saliva deposition in the microcirculation is continuous and modulated by the frequency of the cibarial pump because, when functioning at high frequency, cibarial pump sucks almost all saliva to the insect gut. This mechanism would determine the quantity of saliva deposited in the microcirculation as necessary, and consequently minimizing the host''s immune response to salivary antigens. [Copyright &y& Elsevier]

Published

2006

3. Differential brain and spinal cord cytokine and BDNF levels in experimental autoimmune encephalomyelitis are modulated by prior and regular exercise.

Author

Bernardes, Danielle, Oliveira-Lima, Onésia Cristina, da Silva, Thiago Vitarelli, Faraco, Camila Cristina Fraga, Leite, Hércules Ribeiro, Juliano, Maria Aparecida, dos Santos, Daniel Moreira, Bethea, John R., Brambilla, Roberta, Orian, Jacqueline M., Arantes, Rosa Maria Esteves, and Carvalho-Tavares, Juliana

Subjects

*BRAIN-derived neurotrophic factor, *SPINAL cord, *CYTOKINES, *ENCEPHALOMYELITIS, *AUTOIMMUNE diseases, *EXERCISE physiology

Abstract

Abstract: The interactions between a prior program of regular exercise and the development of experimental autoimmune encephalomyelitis (EAE)-mediated responses were evaluated. In the exercised EAE mice, although there was no effect on infiltrated cells, the cytokine and derived neurotrophic factor (BDNF) levels were altered, and the clinical score was attenuated. Although, the cytokine levels were decreased in the brain and increased in the spinal cord, BDNF was elevated in both compartments with a tendency of lesser demyelization volume in the spinal cord of the exercised EAE group compared with the unexercised. [Copyright &y& Elsevier]

Published

2013

4. Plasmodium berghei NK65 induces cerebral leukocyte recruitment in vivo: An intravital microscopic study

Author

Lacerda-Queiroz, Norinne, Lima, Onésia Cristina Oliveira, Carneiro, Cláudia Martins, Vilela, Márcia Carvalho, Teixeira, Antônio Lúcio, Carvalho, Andrea Teixeira-, Araújo, Márcio Sobreira Silva, Martins-Filho, Olindo Assis, Braga, Érika Martins, and Carvalho-Tavares, Juliana

Subjects

*PLASMODIUM, *LEUCOCYTES, *MALARIA, *MICROCIRCULATION, *CHEMOKINES, *ENCEPHALITIS, *HISTOPATHOLOGY, *IMMUNE response

Abstract

Abstract: Malaria is second only to tuberculosis as the leading cause of morbidity and mortality as a consequence of a single infectious agent. Much of the pathology of malaria arises from the inappropriate or excessive immune response mounted by the host in an attempt to eliminate the parasite. We here report the inflammatory changes observed in the cerebral microvasculature of C57BL/6 and BALB/c mice that had been inoculated with Plasmodium berghei NK65, a lethal strain of rodent malaria. Although no neurological signs were observed in experimentally infected mice, inflammation of the cerebral microvasculature was clearly evident. Histopathological analysis demonstrated that alterations in cerebral tissue were more intense in infected C57Bl/6 mice than in infected BALB/c animals. Intravital microscopic examination of the cerebral microvasculature revealed increased leukocyte rolling and adhesion in pial venules of infected mice compared with non-infected animals. The extravasation of Evans blue dye into the cerebral parenchyma was also elevated in infected mice in comparison with their non-infected counterparts. Additionally, protein levels of TNF-α, MIG/CXCL9, MCP-1/CCL2, MIP-1α/CCL3 and RANTES/CCL5 were up-regulated in brain samples derived from infected C57Bl/6 mice. Taken together, the data reported here illustrate the complex strain-dependent relationships between leukocyte recruitment, blood brain barrier permeability and chemokine production. [Copyright &y& Elsevier]

Published

2011

5. Effect of mutalysin II on vascular recanalization after thrombosis induction in the ear of the hairless mice model

Author

Agero, Ubirajara, Arantes, Rosa M.E., Lacerda-Queiroz, Norinne, Mesquita, Oscar N., Magalhães, A., Sanchez, Eladio F., and Carvalho-Tavares, Juliana

Subjects

*FIBRINOLYTIC agents, *MICE, *ANIMAL models in research, *SCIENTIFIC method

Abstract

Abstract: Mutalysin II (mut-II) is an α-fibrinogenase isolated from Lachesis muta muta (bushmaster) snake venom. The enzyme lyses fibrin clots in vitro, and this activity does not depend on plasminogen activation.The aim of this study was to assess by intravital microscopy the effect of Mutalysin II on the recanalization of microvessels after thrombus induction in the ears of hairless mice. Photochemical thrombus formation was induced after i.v. injection of 5% fluorescein isothiocyanate labelled dextran (FITC-dextran) followed by mercury light exposure of individual microvessels of the ear of five anesthetized animals. Video playback analysis of intravital microscopy images of the ear microcirculation permitted us to measure blood flow velocity (μm/s) under control conditions (before thrombus formation) in the ear microvessels. Thirty minutes after thrombus formation (blood flow velocity stopped completely), each animal (n=5) was infused with Mutalysin II (2.0mg/kg, i.v.). All animals treated with Mutalysin II showed evident thrombolysis after approximately 12min, followed by recanalization. A separate group of mice (n=5) which received urokinase type-plasminogen activator (u-PA, 250U/mouse, i.v.) showed blood flow restoration within the same interval (12min). These in vivo data suggest that Mutalysin II has the potential to be an effective thrombolytic agent. [Copyright &y& Elsevier]

Published

2007

6. CCL2 and CCL5 mediate leukocyte adhesion in experimental autoimmune encephalomyelitis—an intravital microscopy study

Author

dos Santos, Adriana Carvalho, Barsante, Michele Mendes, Esteves Arantes, Rosa Maria, Bernard, Claude C.A., Teixeira, Mauro Martins, and Carvalho-Tavares, Juliana

Subjects

*CENTRAL nervous system diseases, *MULTIPLE sclerosis, *CYTOKINES, *INFLAMMATORY mediators

Abstract

Abstract: Experimental autoimmune encephalomyelitis (EAE) models multiple sclerosis (MS) and is characterized by marked mononuclear cell influx in the brain. Several studies have demonstrated a role for chemokines during EAE. It remains to be determined whether these mediators modulate EAE primarily by mediating leukocyte influx into the CNS or by modifying lymphocyte activation and/or trafficking into lymphoid organs. After induction of EAE with MOG35–55, leukocyte recruitment peaked on day 14 and correlated with symptom onset, TNF-α production and production of CCL2 and CCL5. Levels of CXCL-10 and CCL3 were not different from control animals. Using intravital microscopy, we demonstrated that leukocyte rolling and adhesion also peaked at day 14. Treatment with anti-CCL2 or anti-CCL5 antibodies just prior to the intravital microscopy prevented leukocyte adhesion, but not rolling. Our data suggest that induction of leukocyte adhesion to the brain microvasculature is an important mechanism by which CCL2 and CCL5 participate in the pathophysiology of EAE. [Copyright &y& Elsevier]

Published

2005

7. The thrombolytic action of a proteolytic fraction (P1G10) from Carica candamarcensis

Author

Bilheiro, Rogério P., Braga, Ariadne D., Filho, Marcelo Limborço, Carvalho-Tavares, Juliana, Agero, Ubirajara, Carvalho, Maria das Graças, Sanchez, Eladio F., Salas, Carlos E., and Lopes, Miriam T.P.

Subjects

*FIBRINOLYTIC agents, *PROTEOLYTIC enzymes, *CARICACEAE, *CYSTEINE, *BLOOD flow measurement, *ANTICOAGULANTS

Abstract

Abstract: A group of cysteine-proteolytic enzymes from C. candamarcensis latex, designated as P1G10 displays pharmacological properties in animal models following various types of lesions. This enzyme fraction expresses in vitro fibrinolytic effect without need for plasminogen activation. Based on this evidence, we assessed by intravital microscopy the effect of P1G10 on recanalization of microvessels after thrombus induction in the ear of hairless mice. Video playback of intravital microscopic images allowed measurement of blood flow velocity (mm/s) during the experimental procedure. Groups treated with 5 or 7.5mg/Kg P1G10 showed thrombolysis between 7–15min, without vessel obstruction. Ex vivo experiments demonstrated that platelet activation by ADP is impaired in a dose dependent manner following treatment with P1G10. The P1G10 action on plasma coagulation also showed that prothrombin time (PT), thrombin time (TT) and activated partial thromboplastin time (aPTT, μg/uL) are increased in a dose dependent manner. In addition, P1G10 displayed fibrinogenolytic and fibrinolytic activities, both in a dose dependent manner. Each of these effects was suppressed by inhibition of the proteolytic activity of the fraction. The antithrombotic action of P1G10 can be explained by proteolytic cleavage of fibrinogen and fibrin, both key factors during formation of a stable thrombus. These results combined with prior evidence suggest that P1G10 has potential as thrombolytic agent. [Copyright &y& Elsevier]

Published

2013