Your search keyword '"Tatiana Gomes Ribeiro"' showing total 5 results

1. DESENVOLVIMENTO E VALIDAÇÃO DE MÉTODO ANALÍTICO ESPECTROFOTOMÉTRICO PARA QUANTIFICAÇÃO DE NEROLIDOL EM UM DISPOSITIVO POLIMÉRICO DE LIBERAÇÃO PROLONGADA, APÓS DERIVATIZAÇÃO COM VANILINA

Author

Tatiana Gomes Ribeiro, Juçara Ribeiro Franca, André Mesquita Marques, Maria Auxiliadora Coelho Kaplan, André Augusto Gomes Faraco, and Rachel Oliveira Castilho

Subjects

Chemistry, QD1-999

Abstract

This work describes the development and validation of analytical method to assay nerolidol in a hydrophilic matrix of quitosan by UV/visible spectroscopy. The method is based on the formation of purple derivative between nerolidol and vanillin. The validated method was linear (2.5 - 50 mg mL-1, concentration range, r > 0.99), precise (RSD 0.44% for repeatability and 0.32% for intermediate precision), accurate (100.04% recovery), robust and specific. Detection and quantitation limits were 0.74 mg mL-1 and 2.26 mg mL-1, respectively. The method is simple and fast and it was applied successfully. Alternatively, the described method may be applied for the analysis of alcohols and unsaturated lipids.

Published

2018

2. New delivery systems for amphotericin B applied to the improvement of leishmaniasis treatment

Author

Miguel Angel Chávez-Fumagalli, Tatiana Gomes Ribeiro, Rachel Oliveira Castilho, Simone Odília Antunes Fernandes, Valbert Nascimento Cardoso, Cecília Steinberg Perilo Coelho, Débora Vasconcelos Costa Mendonça, Manuel Soto, Carlos Alberto Pereira Tavares, André Augusto Gomes Faraco, and Eduardo Antonio Ferraz Coelho

Subjects

Amphotericin B, Leishmaniasis, Nanoparticles, Toxicity, Treatment, Lipid-based formulations, Arctic medicine. Tropical medicine, RC955-962

Abstract

Leishmaniasis is one of the six major tropical diseases targeted by the World Health Organization. It is a life-threatening disease of medical, social and economic importance in endemic areas. No vaccine is yet available for human use, and chemotherapy presents several problems. Pentavalent antimonials have been the drugs of choice to treat the disease for more than six decades; however, they exhibit high toxicity and are not indicated for children, for pregnant or breastfeeding women or for chronically ill patients. Amphotericin B (AmpB) is a second-line drug, and although it has been increasingly used to treat visceral leishmaniasis (VL), its clinical use has been hampered due to its high toxicity. This review focuses on the development and in vivo usage of new delivery systems for AmpB that aim to decrease its toxicity without altering its therapeutic efficacy. These new formulations, when adjusted with regard to their production costs, may be considered new drug delivery systems that promise to improve the treatment of leishmaniasis, by reducing the side effects and the number of doses while permitting a satisfactory cost-benefit ratio.

Published

2015

3. Ocular Inserts for Sustained Release of the Angiotensin-Converting Enzyme 2 Activator, Diminazene Aceturate, to Treat Glaucoma in Rats.

Author

Giselle Foureaux, Juçara Ribeiro Franca, José Carlos Nogueira, Gustavo de Oliveira Fulgêncio, Tatiana Gomes Ribeiro, Rachel Oliveira Castilho, Maria Irene Yoshida, Leonardo Lima Fuscaldi, Simone Odília Antunes Fernandes, Valbert Nascimento Cardoso, Sebastião Cronemberger, André Augusto Gomes Faraco, and Anderson José Ferreira

Subjects

Medicine, Science

Abstract

The aim of this study was to develop and evaluate the effects of chitosan inserts for sustained release of the angiotensin-converting enzyme 2 (ACE2) activator, diminazene aceturate (DIZE), in experimental glaucoma. Monolayer DIZE loaded inserts (D+I) were prepared and characterized through swelling, attenuated total reflectance Fourier transformed infrared spectroscopy (ATR-FTIR), differential scanning calorimetry (DSC) and in vitro drug release. Functionally, the effects of D+I were tested in glaucomatous rats. Glaucoma was induced by weekly injections of hyaluronic acid (HA) into the anterior chamber and intraocular pressure (IOP) measurements were performed. Retinal ganglion cells (RGC) and optic nerve head cupping were evaluated in histological sections. Biodistribution of the drug was accessed by scintigraphic images and ex vivo radiation counting. We found that DIZE increased the swelling index of the inserts. Also, it was molecularly dispersed and interspersed in the polymeric matrix as a freebase. DIZE did not lose its chemical integrity and activity when loaded in the inserts. The functional evaluation demonstrated that D+I decreased the IOP and maintained the IOP lowered for up to one month (last week: 11.0 ± 0.7 mmHg). This effect of D+I prevented the loss of RGC and degeneration of the optic nerve. No toxic effects in the eyes related to application of the inserts were observed. Moreover, biodistribution studies showed that D+I prolonged the retention of DIZE in the corneal site. We concluded that D+I provided sustained DIZE delivery in vivo, thereby evidencing the potential application of polymeric-based DIZE inserts for glaucoma management.

Published

2015

4. Bimatoprost-loaded ocular inserts as sustained release drug delivery systems for glaucoma treatment: in vitro and in vivo evaluation.

Author

Juçara Ribeiro Franca, Giselle Foureaux, Leonardo Lima Fuscaldi, Tatiana Gomes Ribeiro, Lívia Bomfim Rodrigues, Renata Bravo, Rachel Oliveira Castilho, Maria Irene Yoshida, Valbert Nascimento Cardoso, Simone Odília Fernandes, Sebastião Cronemberger, Anderson José Ferreira, and André Augusto Gomes Faraco

Subjects

Medicine, Science

Abstract

The purpose of the present study was to develop and assess a novel sustained-release drug delivery system of Bimatoprost (BIM). Chitosan polymeric inserts were prepared using the solvent casting method and characterized by swelling studies, infrared spectroscopy, differential scanning calorimetry, drug content, scanning electron microscopy and in vitro drug release. Biodistribution of 99mTc-BIM eye drops and 99mTc-BIM-loaded inserts, after ocular administration in Wistar rats, was accessed by ex vivo radiation counting. The inserts were evaluated for their therapeutic efficacy in glaucomatous Wistar rats. Glaucoma was induced by weekly intracameral injection of hyaluronic acid. BIM-loaded inserts (equivalent to 9.0 µg BIM) were administered once into conjunctival sac, after ocular hypertension confirmation. BIM eye drop was topically instilled in a second group of glaucomatous rats for 15 days days, while placebo inserts were administered once in a third group. An untreated glaucomatous group was used as control. Intraocular pressure (IOP) was monitored for four consecutive weeks after treatment began. At the end of the experiment, retinal ganglion cells and optic nerve head cupping were evaluated in the histological eye sections. Characterization results revealed that the drug physically interacted, but did not chemically react with the polymeric matrix. Inserts sustainedly released BIM in vitro during 8 hours. Biodistribution studies showed that the amount of 99mTc-BIM that remained in the eye was significantly lower after eye drop instillation than after chitosan insert implantation. BIM-loaded inserts lowered IOP for 4 weeks, after one application, while IOP values remained significantly high for the placebo and untreated groups. Eye drops were only effective during the daily treatment period. IOP results were reflected in RGC counting and optic nerve head cupping damage. BIM-loaded inserts provided sustained release of BIM and seem to be a promising system for glaucoma management.

Published

2014

5. Mimotope-based vaccines of Leishmania infantum antigens and their protective efficacy against visceral leishmaniasis.

Author

Lourena Emanuele Costa, Luiz Ricardo Goulart, Nathália Cristina de Jesus Pereira, Mayara Ingrid Sousa Lima, Mariana Costa Duarte, Vivian Tamietti Martins, Paula Sousa Lage, Daniel Menezes-Souza, Tatiana Gomes Ribeiro, Maria Norma Melo, Ana Paula Fernandes, Manuel Soto, Carlos Alberto Pereira Tavares, Miguel Angel Chávez-Fumagalli, and Eduardo Antonio Ferraz Coelho

Subjects

Medicine, Science

Abstract

BACKGROUND: The development of cost-effective prophylactic strategies to prevent leishmaniasis has become a high-priority. The present study has used the phage display technology to identify new immunogens, which were evaluated as vaccines in the murine model of visceral leishmaniasis (VL). Epitope-based immunogens, represented by phage-fused peptides that mimic Leishmania infantum antigens, were selected according to their affinity to antibodies from asymptomatic and symptomatic VL dogs' sera. METHODOLOGY/MAIN FINDINGS: Twenty phage clones were selected after three selection cycles, and were evaluated by means of in vitro assays of the immune stimulation of spleen cells derived from naive and chronically infected with L. infantum BALB/c mice. Clones that were able to induce specific Th1 immune response, represented by high levels of IFN-γ and low levels of IL-4 were selected, and based on their selectivity and specificity, two clones, namely B10 and C01, were further employed in the vaccination protocols. BALB/c mice vaccinated with clones plus saponin showed both a high and specific production of IFN-γ, IL-12, and GM-CSF after in vitro stimulation with individual clones or L. infantum extracts. Additionally, these animals, when compared to control groups (saline, saponin, wild-type phage plus saponin, or non-relevant phage clone plus saponin), showed significant reductions in the parasite burden in the liver, spleen, bone marrow, and paws' draining lymph nodes. Protection was associated with an IL-12-dependent production of IFN-γ, mainly by CD8+ T cells, against parasite proteins. These animals also presented decreased parasite-mediated IL-4 and IL-10 responses, and increased levels of parasite-specific IgG2a antibodies. CONCLUSIONS/SIGNIFICANCE: This study describes two phage clones that mimic L. infantum antigens, which were directly used as immunogens in vaccines and presented Th1-type immune responses, and that significantly reduced the parasite burden. This is the first study that describes phage-displayed peptides as successful immunogens in vaccine formulations against VL.

Published

2014