Matrisbildande hjälpämnen för framställning av spraytorkade partiklar för inhalation

Nazari, Zara

January 2024

No description available.

Spray drying

dry powder inhalation

matrix excipient

lactose

trehalose

mannitol

Pharmaceutical Sciences

Farmaceutiska vetenskaper

Characterization of signaling pathways underlying key growth and development processes in Populus trichocarpa

Rigoulot, Stephen Bradley

05 September 2018

The project goals for this dissertation were to manipulate Populus trichocarpa source-sink relationships to optimize this woody crop species for specific agricultural traits such as increased growth rate, stress tolerance and/or improvements in overall biomass accumulation. We targeted specific tissues such as xylem, where alterations in the relationship of source and sink tissues can lead to the control of xylem cell deposition or of various wood properties. This led to the characterization of 165 protein-protein interactions and 20 protein-DNA interaction which constitute numerous woody tissue related subnetworks. One such network, centered on the DIVARACATA and RADIALIS INTERACTING FACTOR (PtrDRIF), identified PtrWOX13c as an interacting protein. Characterization of PtrWOX13c shows that it displays the ability to control promoters related to lignin biosynthesis genes and overexpression phenotypes show alterations in axillary branch activity. Genes which control the differentiation and specialization of cells such as members of the WOX family are also highly responsive to abiotic stress which can force major changes in plant metabolism and nutrient mobilization. ABA, a prominent plant phytohormone with known roles in the adaptation to stress has shown novel connections in the regulation of growth promoting complexes such as TOR through antagonistic regulatory actions of the SnRK2 protein kinase in Arabidopsis. Characterization of the core ABA signaling in P. trichocarpa has identified a regulatory clade A protein phosphatase which interacts with numerous PtrSnRK2 proteins and when overexpressed in hybrid poplar results in increased height and node production potentially by indirect control of growth promoting complexes like TOR through SnRK2 inhibition. This work has also demonstrated that in addition to the involvement of phytohormones in the regulation of plant development, sugar phosphates such as T6P can exert significant control of plant architecture. Together, these studies comprise the discovery and subsequent characterization of novel wood associated networks, hormone pathways and sugar signaling in the manipulation of P. trichocarpa source-sink relationships for the promotion of biomass accumulation. / PHD / Detailed analyses of gene activity in different tissues or under the influence of various environmental conditions have identified numerous genes that control desirable traits and plant characteristics. However, the activities and functions of the proteins produced from these genes is less understood. One of the ways proteins work is through the formation of complexes with other proteins. Using the commercially valuable tree Populus trichocarpa (poplar) as our research model, we have identified novel complexes of interacting proteins with the potential to sense and respond to the environment and to promote plant growth. We tested the function of some of the members of these newly discovered protein complexes using transgenic poplar. As a result, we revealed previously unknown functions for two poplar proteins: PtrWOX13c promoted increased branching and PtrHAB2 promoted an increase in tree height. Independent of these functional analyses of poplar proteins, we also tested the ability of a sugar phosphate, trehalose6-phosphate, known from previous work to regulate plant growth, for its ability to promote poplar growth. We found that reducing levels of trehalose-6-phosphate resulted in increased branch growth, similar to the impact of the PtrWOX13c protein. In summary, identification of new protein complexes is a valuable strategy for the discovery of proteins that can increase tree growth. Additionally, combining targeted changes in both proteins and regulatory sugars may be a promising path toward future crop improvement and tree domestication.

Populus trichocarpa

Yeast two-hybrid

interaction network

xylem

WOX

ABA signaling

Trehalose-6-phosphate

Glycolipids : from synthesis and self-assembly studies to the design of original bio-based polymers / Glycolipides : de la synthèse et l’étude de l’auto-assemblage à la conception de polymères bio-sourcés originaux

Hibert, Geoffrey

28 November 2016

Ces travaux de thèse traitent de l’étude de glycolipides et plus précisément d’esters de trehalose pour la synthèse de nouveaux polymères bio-sourcés. Des monoesters et diesters de trehalose ont ainsi été synthétisés par estérification des alcools primaires du trehalose avec des acides gras selon deux voies de synthèse. La première utilisant un agent de couplage peptidique ne nécessite pas l’utilisation de groupement protecteur pour estérifier sélectivement les alcools primaires. La deuxième est une estérification sélective catalysée par une lipase. L’auto-assemblage des esters de tréhalose a ensuite été étudié. Les monoesters possèdent des propriétés tensio-actives dans l’eau et le trehalose monoeruçate a la capacité de gélifier l’eau. Les diesters, quant à eux sont de bons gélifiants pour les solvants organiques etles huiles végétales. Par conséquent, des gels ont été préparés dans trois huiles végétales, puis leur morphologie et leur propriété rhéologique ont été étudiées. Ensuite, les diesters ont été fonctionnalisé et polymérisés selon différentes stratégies. Ainsi, des polyuréthanes et des poly(hydroxyuréthane)s ont été synthétisés par polycondensation tandis que des glycopolyesters ont été obtenus par polymérisation par métathèse et addition thiol-ène. Finalement,les propriétés d’auto-assemblage de ces polymères ont été étudiées. Ces derniers peuvent former des nanoparticules par la méthode de déplacement de solvants. / The aim of this thesis was to study glycolipids and particularly trehalose esters for the synthesis of new bio-sourced polymers. Trehalose monoesters and diesters were synthesized by two esterification pathways of the primary alcohol of trehalose with different fatty acids. The first synthetic route is a protective group-free esterification using a peptide coupling agent and the second one is a lipase-catalyzed esterification. The self-assembly properties of the trehalose esters were investigated. Trehalose monoesters showed surfactant properties in water and trehalose monoerucate was even able to form gels in water. The trehalose diesters appeared to be good gelators for organic solvent and vegetable oil. Thus, gels in three vegetable oils were prepared and their morphology and rheological properties were studied. Afterwards, trehalose diesters were functionalized and polymerized with different strategies.Thus, polyurethanes and poly(hydroxyurethane)s were obtained by polycondensation where as glyco-polyesters were synthesized by acyclic diene metathesis (ADMET) and thiol-enepolymerization. Finally, the self-assembly properties of these polymers were investigated. The latter were able to form some nanoparticles by solvent displacement method.

Glycolipides

Esters de trehalose

Auto-assemblage

Tensioactif

Gel

Polyuréthane

Poly(hydroxyuréthane)

Polymérisation par métathèse

Polymérisation par addition thiol-ène

Glycolipids

Trehalose esters

Self-assembly

Surfactant

Gel

Polyurethane

Poly(hydroxyurethane)

ADMET

Thiol-ene polymerization

VITRIFICATION AND CHORIOALLANTOIC MEMBRANE (CAM) CULTURE OF BOVINE OVARIAN TISSUE

2015 May 1900

The overall objectives of this thesis were to develop a short-term culture system and to examine the effects of vitrification and short-term culture on the viability of fresh and vitrified bovine ovarian tissue and the follicles within. The first objective was to compare the health and development of preantral follicles in bovine ovarian tissue, as well as the neovascularization of these tissues, subjected to avian chorioallantoic membrane (CAM) culture with the traditional in vitro culture system. We hypothesized that the chorioallantoic membrane (CAM) of the chicken embryo is a 
more suitable culture system than traditional in vitro culture. Bovine ovaries were retrieved from a local abattoir and cortical pieces (1-2mm3) were randomly assigned to one of the following groups; control (fixed immediately), CAM or in in vitro culture. Ovarian tissue fragments from both groups were removed on D1, D3 and D5 of culture, fixed, sectioned (5μm) and stained with H&E. The numbers of healthy and degenerated follicles, primordial and activated preantral (primary and secondary), and the number of infiltrated bovine and avian blood vessels were determined using standard stereological procedures. All grafts placed on the traumatized CAM demonstrated increased neovascularization over time. The healthy primordial follicle density decreased over time concomitant with an increase in degenerated (primordial and activated preantral) follicles in both treatment groups. Healthy activated preantral follicle density did not differ between the two culture systems at a given time. In CAM group, blood vessel density increased over time (p = 0.015). The second objective of this thesis was to develop a suitable vitrification protocol for bovine ovarian tissue. The viability of bovine ovarian tissue vitrified using two non-permeating cryoprotectants (sucrose and trehalose) and two cryodevices (cryotop and cryovial) was assessed. We hypothesized that during vitrification the higher cooling rate on the cryotop (open vitrification method) will yield better post-thaw viability of bovine ovarian tissue as compared to the cryovial (closed vitrification method). We also hypothesized that trehalose is a superior non-permeating cryoprotectant to sucrose for vitrification of bovine ovarian tissue. The ovarian tissue was fragmented (1-2mm3) and divided into 6 different treatment groups. Tissues were vitrified in TCM199 supplemented with 15% EG, 15% DMSO, 20% calf serum and 0.5M sucrose or trehalose then placed in a cryovial or on a cryotop. After warming, the vitrified tissues were either immediately placed in 10% formalin (control) or on the chorioallantoic membrane of a 10-day old chicken embryo for 5 days. Follicles from control and vitrified tissue were observed under a light microscope for normal morphology and the total, normal and degenerated follicle densities were determined by standard stereological procedures. Sucrose and trehalose did not differ, nor was a difference observed between the cryovial and the cryotop for total, healthy or degenerated follicle density. Proportion of healthy follicles was higher in the control than all treatment tissues grafted to the CAM. All grafts placed on the traumatized CAM demonstrated presence of avian erythrocytes in the blood vessels after 5 days, but no difference was observed for blood vessel density among treatments. Lastly, the cooling rate of bovine ovarian tissue subjected to open and closed system devices for vitrification was evaluated. A thermocouple wire was used to determine the cooling velocity of 1-2mm3 fragments of bovine ovarian tissue placed on a cryotop (open system) or in a sealed cryovial (closed system). The cooling rate of tissues on the cryotop and in the cryovial was 7481±205.9° C/min and 664±26.0° C/min respectively. In conclusion, the CAM supported the bovine ovarian tissue, thus the CAM culture system may be considered an acceptable alternative to traditional in vitro culture system for bovine ovarian tissue. Furthermore, angiogenesis may be an additional indication of ovarian tissue health. The hypotheses of our second study were refuted. Results indicated that sucrose and trehalose, and the cryotop and cryovial were equally effective in vitrifying bovine ovarian tissue.

Avaliação de diferentes compostos contra paralisia e efeitos deletérios em modelo de esclerose lateral amiotrófica em Caenorhabditis elegans / Evaluation of different compounds against paralysis and deleterious effects in a model of amyotrophic lateral sclerosis in Caenorhabditis elegans

Dal Forno, Ana Helena de Castro

17 March 2017

Submitted by Marcos Anselmo (marcos.anselmo@unipampa.edu.br) on 2018-12-03T17:42:10Z No. of bitstreams: 1 ANA HELENA DE CASTRO DAL FORNO.pdf: 1125113 bytes, checksum: bac2174a37c6246d7048e40640b14f02 (MD5) / Approved for entry into archive by Marcos Anselmo (marcos.anselmo@unipampa.edu.br) on 2018-12-03T17:42:22Z (GMT) No. of bitstreams: 1 ANA HELENA DE CASTRO DAL FORNO.pdf: 1125113 bytes, checksum: bac2174a37c6246d7048e40640b14f02 (MD5) / Made available in DSpace on 2018-12-03T17:42:22Z (GMT). No. of bitstreams: 1 ANA HELENA DE CASTRO DAL FORNO.pdf: 1125113 bytes, checksum: bac2174a37c6246d7048e40640b14f02 (MD5) Previous issue date: 2017-03-17 / A esclerose lateral amiotrófica (ELA) é uma doença paralisante e fatal caracterizada por degeneração e morte dos neurônios motores que é geralmente fatal dentro de cinco anos após diagnóstico e sem tratamento eficaz atual. Aproximadamente 10% dos casos de ELA são familiares (ELAf) e cerca de 20% de ELAf estão associados a mutações no gene superóxido dismutase 1 (sod1). Em busca de modelos experimentais alternativos que possam substituir e oferecer novas possibilidades de ensaio de toxicidade xenobiótica, o nematóide Caenorhabditis elegans foi considerado favorável como um valioso organismo bioindicador. Utilizando cepas transgênicas de C. elegans como modelo ELA HA2619, HA2622, HA2425, HA2426 testamos diferentes compostos para avaliar sua eficácia nas alterações resultantes da mutação em modelo da ELA. Foram testados trealose (5 mM) com vitamina E (200 μg/mL) e os compostos orgânicos (1 μM) 4-fenilselanil-7-cloroquinolina (PSQ) e 4-feniltellanil-7-cloroquinolina (PTQ). Nenhum dos tratamentos testados apresentou resultados positivos para o aumento da longevidade ou diminuição na paralisia, o que nos levou a questionar se os tratamentos podem ter desencadeado um aumento dos sintomas e consequentemente uma piora nos vermes. Também observamos que o tratamento com os compostos orgânicos contra o dano oxidativo causado pelo peróxido de hidrogênio (0,6 mM) não foi revertido. Em nossas perspectivas, mais estudos são necessários para encontrar terapias que podem prolongar a longevidade e diminuir ou retardar a paralisia. / Amyotrophic lateral sclerosis (ALS) is a fatal paralytic disorder characterized by degeneration of motorneuron which is generally fatal within five years of diagnosis and with no current effective treatment. Approximately 10% of the ALS cases are familial ALS (fALS) and about 20% of fALS are associated with mutations in the superoxide dismutase 1 gene (sod1). Seeking for alternative experimental models that may substitute and offer new possibilities to assay xenobiotics toxicity, the nematode Caenorhabditis elegans has been found favorable as a valuable bioindicator organism. Using C. elegans transgenic strains as ALS model HA2619, HA2622, HA2425, HA2426 we tested compounds to evaluate the efficacy in treatment of ALS. Trehalose (5mM) with vitamin E (200μg/mL) and the organocompounds (1μM) 4-phenylselanyl-7-chloroquinoline (PSQ) and 4-phenyltellanyl-7-chloroquinoline (PTQ) were tested. None of the treatments tested positive for increased longevity or delayed or decreased paralysis, which led us to wonder if the treatments may have triggered an increase in symptoms and worsening of the worms. We also observed the treatment with the organocompounds against the oxidative damage caused by hydrogen peroxide (0.6mM) was not reversed. In our perspectives further studies are needed to find therapies that may prolong longevity and decrease or delay paralysis.

CNPQ::CIENCIAS BIOLOGICAS

Esclerose lateral amiotrófica

Trealose

Vitamina E

Organocompostos

Caenorhabditis elegans

Amyotrophic lateral sclerosis

Trehalose

Vitamin E

Organocompounds

Caenorhabditis elegans

A trealase periplasmática e o operon de metabolismo de β-glicosídeos afetam a virulência in vivo na cepa Escherichia coli patogênica extraintestinal MT78

Pavanelo, Daniel Brisotto

January 2017

Escherichia coli patogênicas extraintestinais (ExPEC) causam colibacilose aviária, infecções do trato urinário e meningite neonatal em humanos. A cepa ExPEC MT78 é virulenta in vitro e in vivo, e possui a habilidade de invadir células eucarióticas. Para melhor entender o fenótipo invasivo dessa cepa, foi criada uma biblioteca de mutantes aleatórios pela técnica de mutagênese marcada com assinatura, e os mutantes foram selecionados negativamente em ensaio de invasão a fibroblastos aviários. Mutantes atenuados apresentaram mutação em genes do operon da fímbria do tipo 1 e nos genes de metabolismo de açúcares treA e bglB. Foram feitos mutantes específicos para o gene que codifica a enzima trealase periplasmática (TreA) e para o operon de metabolismo de β-glicosídeos (bgl). O mutante MT78ΔtreA apresentou, frente à cepa selvagem, diminuição na capacidade de adesão e invasão a fibroblastos aviários, na expressão da fímbria do tipo 1 e na capacidade de colonizar a bexiga de camundongos em modelo de infecção urinária. O mutante MT78Δbgl também apresentou, frente à cepa selvagem, diminuição na capacidade de adesão e invasão a fibroblastos aviários e na capacidade de colonizar a bexiga de camundongos em modelo de infecção urinária, mas não mostrou alteração na expressão da fímbria do tipo 1, medida por aglutinação de leveduras. Os resultados deste trabalho mostraram que a trealase periplasmática afeta a expressão da fímbria do tipo 1 e a virulência in vivo da cepa ExPEC MT78, enquanto o operon do metabolismo de β-glicosídeos afeta a virulência in vivo da cepa ExPEC MT78 por um mecanismo ainda não-elucidado. / Extraintestinal pathogenic E. coli (ExPEC) cause colibacillosis in birds, urinary tract infections and neonatal meningitis in humans. The ExPEC strain MT78 is virulent in vitro and in vivo, and is able to invade eukaryotic cells. In order to better understand the invasive phenotype of this strain, a library of random mutants was made using the signature-tagged mutagenesis approach. The mutants were negatively selected in invasion assays of avian fibroblasts. Attenuated mutants presented mutation in the type 1 fimbria operon and in the genes of sugar metabolism treA and bglB. Specific mutants were created for the periplasmic trehalase (TreA) gene and for the β-glycosides metabolism operon (bgl). The MT78ΔtreA mutant displayed, in comparison with the wild type strain, a reduction on the capacity of adhesion and invasion to avian fibroblastos, on type 1 fimbriae expression and on the capacity to colonize the bladder in a murine model of urinary tract infection. The MT78Δbgl mutant, compared to the wild type strain, also displayed a reduction on the capacity of adhesion and invasion to avian fibroblastos and on the capacity to colonize the bladder in a murine model of urinary tract infection, but did not show any difference on type 1 fimbriae expression as detected by yeast agglutination. Taken together, our results show that the periplasmic trehalase affects type 1 expression and in vivo virulence of the ExPEC strain MT78, and the operon for β-glycosides metabolism affects in vivo virulence by an as yet unidentified mechanism.

Escherichia coli

Mutagenese

Trealase

β-glycosides

Trehalose

Type 1 fimbriae

Signature-tagged mutagenesis

Characterization by optical methods of the heat denaturation of bovine serum albumin (BSA) as affected by protein concentration, pH, ionic strength and sugar concentration

Kongraksawech, Teepakorn

14 March 2007

The thermal denaturation of proteins has been extensively studied using several methods including differential scanning calorimetry (DSC). A custom-built optical system was used to study thermal effects on protein as an alternative method to DSC measurements. It was used to investigate the thermal stability of bovine serum albumin (BSA) with a focus on comparisons with published DSC data. In the first study, the effect of protein concentration on the thermal denaturation (Td) of BSA was determined and validated using published DSC data for bovine serum albumin (BSA). The optical rotation (OR) and transmitted light (TL) signals indicating protein conformational changes and gel formation, respectively, were collected during the heating of BSA solutions at ~6��C/min from room temperature to ~85��C. The experiments were performed on 1, 2.5 and 5% (w/v) BSA in 0.01 M phosphate buffer at pH 7 and ionic strength (IS) 0.08. BSA���s Td values obtained from this investigation were consistent with published values and had low experimental variability (CV<2.5%). In agreement with some but not all published data, increasing BSA concentration did not affect its thermal stability. Protein gel formation, however, increased with protein concentration. In the second study, changes in the OR and TL signal of BSA in 0.01 M phosphate buffer at pH 6.1, 7 and 7.9 with IS maintained at 0.04, 0.08 and 0.16 were recorded during the heating of BSA solutions at ~6��C/min from room temperature to ~85��C. BSA showed a maximum and minimum thermostability at pH 7 and 7.9, respectively, consistent with published values determined by DSC. BSA formed opaque gel at pH 6.1 approaching the BSA���s pI values. Increasing IS level did not have a significant effect on BSA���s Td value but promoted gel formation. In the third study, the optical method was applied to investigate the heat stability of BSA as affected by low concentrations of sucrose, trehalose or sorbitol. BSA solutions (2.5% w/v) in the presence of 0 5% sucrose, trehalose and sorbitol were heated at ~6��C/min from ambient temperature to ~85��C. In contrast with published work on the thermal stability of BSA in the presence of higher sugar concentrations, this study showed that increasing sugar concentration did not enhance the thermal stability of this protein. Also, the ability to promote protein stability among sucrose, trehalose and sorbitol were not significantly different. The significance of these studies is that they demonstrate that the custom-built optical methods here developed can be used to study heat-induced protein denaturation and the effect of environmental conditions. Future studies will examine other proteins such as ��-lactoglobulin or ��-lacactalbumin. A further advantage of optical systems is their ability to conduct real-time measurements which could be used for food processing control. / Graduation date: 2007

bovine serum albumin (BSA)

optical rotation

thermal denaturation temperature

sucrose

trehalose

sorbitol

Serum albumin -- Denaturation

Serum albumin -- Optical properties

DESENVOLVIMENTO TECNOLÓGICO DE PRODUTOS SECOS REDISPERSÍVEIS A PARTIR DE NANOESTRUTURAS CONTENDO TIOCONAZOL / TECHNOLOGICAL DEVELOPMENT OF REDISPERSIBLE DRIED PRODUCTS FROM NANOSTRUCTURES CONTAINING TIOCONAZOLE

Ribeiro, Roseane Fagundes

29 April 2013

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / Spray-drying and freeze-drying are dehydration techniques which serve as alternative to increase the stability of formulations which are in aqueous medium. Therefore, this study objectived the development of redispersible dried products prepared from suspensions of polymeric nanocapsules and nanoemulsions using tioconazole, an antifungal. The suspension of nanocapsules, prepared using poli(-caprolactona) - PCL and Eudragit® RS100 polymers, and nanoemulsions containing tioconazole (1.0 mg/ml) were evaluated in relation to mean particles size, drug content, pH and encapsulation efficiency, and after preparation, showed physicochemical characteristics suitable: mean particles size in the nanometer range (110 210 nm), polydispersity index below 0.20, drug content near to theoretical and encapsulation efficiency of approximately 100 % and 86 % for the PCL and Eudragit® RS100 nanocapsules, respectively. Furthermore, the formulations have been stable for 30 days. After, the liquid formulations were subjected to spray-drying and/or freeze-drying using lactose and trehalose as adjuvants in a proportion of 10 % (w/v). The dried products were characterized in relation to yield, index resuspension in water, drug content, moisture and morphology. Regardless of the method of dehydration and adjuvant, the dried products presented satisfactory physicochemical characteristics: yield 50 100 % (depending on the technique of dehydration), drug content near to theoretical, percentage of moisture of less than 4.2 %, good redispersion in water, is possible to verify the presence of nanometric and micrometric particles (by laser diffraction), and the recovery of nanometer size similar to the original liquid formulation, after filtration (photon correlation spectroscopy). Morphological analysis showed the presence of rounded particles for the powders obtained by spray-drying and irregular to those obtained by freeze-drying. Dried products were stable for 30 days, however, the powders obtained from nanoemulsions and nanocapsules of Eudragit® RS100, by spray-drying and lactose as adjuvant showed a decrease in tioconazole content. The suspensions of nanocapsules and nanoemulsions and their respective dried products containing tioconazole showed antifungal activity against the yeast C. albicans, demonstrating that the dehydration process did not affect the action of the drug. Evaluation of in vitro release of the drug by the technique of dialysis bags showed that dried products prepared from nanocapsules were able to promote the control release of the drug, especially the dried products obtained from nanocapsules of PCL by spray-drying, which showed more tioconazole control release at time of 48 hours. / A secagem por aspersão (spray-drying) e a liofilização são técnicas de desidratação que servem como alternativa para aumentar a estabilidade de formulações que se encontram em meio aquoso. Neste sentido, este trabalho objetivou o desenvolvimento de produtos secos redispersíveis preparados a partir de suspensões de nanocápsulas poliméricas e nanoemulsões utilizando o tioconazol, um fármaco antifúngico. As suspensões de nanocápsulas, preparadas com os polímeros poli(-caprolactona) PCL e Eudragit® RS100, e nanoemulsões contendo tioconazol (1,0 mg/mL) foram avaliadas quanto ao diâmetro médio de partículas, teor de fármaco, pH e eficiência de encapsulamento, as quais, após a preparação, apresentaram características físico-químicas adequadas: diâmetro médio de partículas na faixa nanométrica (110 210 nm), índice de polidispersão abaixo de 0,20, teor de fármaco próximo ao teórico e eficiência de encapsulamentro de, aproximadamente, 100 % e 86 % para as nanocápsulas de PCL e Eudragit® RS100, respectivamente. Além disso, as formulações foram estáveis por 30 dias. Após, as formulações líquidas foram submetidas à secagem por aspersão e/ou a liofilização, utilizando a lactose e a trealose como adjuvantes, na proporção de 10 % (m/v). Os produtos secos foram caracterizados em relação ao rendimento, índice de ressuspensão em água, teor de fármaco, umidade e morfologia. Independente do método de desidratação e do adjuvante, os produtos secos apresentaram características físico-químicas satisfatórias: rendimento de 50 100 % (dependendo da técnica de desidratação), teor de fármaco próximo ao teórico, percentual de umidade inferior a 4,2 %, boa redispersão em água, sendo possível verificar a presença de partículas nanométricas e micrométricas (por difração a laser), e a retomada do tamanho nanométrico semelhante à formulação líquida original, após filtração (espectroscopia de correlação de fótons). Na análise morfológica foi observada a presença de partículas arredondadas para os pós obtidos por spray-drying e irregulares para os obtidos por liofilização. Os produtos secos foram estáveis por 30 dias; todavia, os pós obtidos a partir de nanoemulsões e nanocápsulas de Eudragit® RS100, por spray-drying e lactose como adjuvante, apresentaram um decaimento no teor de tioconazol. As suspensões de nanocápsulas e nanoemulsões e seus respectivos produtos secos contendo tioconazol apresentaram atividade antifúngica frente à levedura de C. albicans, demonstrando que os processos de desidratação não afetaram a ação do fármaco. A avaliação de liberação in vitro do fármaco pela técnica de sacos de diálise demonstrou que os produtos secos preparados a partir de nanocápsulas foram capazes de promover o controle de liberação do fármaco, destacando-se os produtos secos obtidos a partir de nanocápsulas de PCL por spray-drying que apresentaram maior controle na liberação do tioconazol no tempo de 48 horas.

Lactose

Liofilização

Nanocápsulas

Spray-drying

Tioconazol

Trealose

Lactose

Freeze-drying

Nanocapsules

Spray-drying

Tioconazole

Trehalose

CNPQ::CIENCIAS BIOLOGICAS::FARMACOLOGIA

A trealase periplasmática e o operon de metabolismo de β-glicosídeos afetam a virulência in vivo na cepa Escherichia coli patogênica extraintestinal MT78

Pavanelo, Daniel Brisotto

January 2017

Escherichia coli patogênicas extraintestinais (ExPEC) causam colibacilose aviária, infecções do trato urinário e meningite neonatal em humanos. A cepa ExPEC MT78 é virulenta in vitro e in vivo, e possui a habilidade de invadir células eucarióticas. Para melhor entender o fenótipo invasivo dessa cepa, foi criada uma biblioteca de mutantes aleatórios pela técnica de mutagênese marcada com assinatura, e os mutantes foram selecionados negativamente em ensaio de invasão a fibroblastos aviários. Mutantes atenuados apresentaram mutação em genes do operon da fímbria do tipo 1 e nos genes de metabolismo de açúcares treA e bglB. Foram feitos mutantes específicos para o gene que codifica a enzima trealase periplasmática (TreA) e para o operon de metabolismo de β-glicosídeos (bgl). O mutante MT78ΔtreA apresentou, frente à cepa selvagem, diminuição na capacidade de adesão e invasão a fibroblastos aviários, na expressão da fímbria do tipo 1 e na capacidade de colonizar a bexiga de camundongos em modelo de infecção urinária. O mutante MT78Δbgl também apresentou, frente à cepa selvagem, diminuição na capacidade de adesão e invasão a fibroblastos aviários e na capacidade de colonizar a bexiga de camundongos em modelo de infecção urinária, mas não mostrou alteração na expressão da fímbria do tipo 1, medida por aglutinação de leveduras. Os resultados deste trabalho mostraram que a trealase periplasmática afeta a expressão da fímbria do tipo 1 e a virulência in vivo da cepa ExPEC MT78, enquanto o operon do metabolismo de β-glicosídeos afeta a virulência in vivo da cepa ExPEC MT78 por um mecanismo ainda não-elucidado. / Extraintestinal pathogenic E. coli (ExPEC) cause colibacillosis in birds, urinary tract infections and neonatal meningitis in humans. The ExPEC strain MT78 is virulent in vitro and in vivo, and is able to invade eukaryotic cells. In order to better understand the invasive phenotype of this strain, a library of random mutants was made using the signature-tagged mutagenesis approach. The mutants were negatively selected in invasion assays of avian fibroblasts. Attenuated mutants presented mutation in the type 1 fimbria operon and in the genes of sugar metabolism treA and bglB. Specific mutants were created for the periplasmic trehalase (TreA) gene and for the β-glycosides metabolism operon (bgl). The MT78ΔtreA mutant displayed, in comparison with the wild type strain, a reduction on the capacity of adhesion and invasion to avian fibroblastos, on type 1 fimbriae expression and on the capacity to colonize the bladder in a murine model of urinary tract infection. The MT78Δbgl mutant, compared to the wild type strain, also displayed a reduction on the capacity of adhesion and invasion to avian fibroblastos and on the capacity to colonize the bladder in a murine model of urinary tract infection, but did not show any difference on type 1 fimbriae expression as detected by yeast agglutination. Taken together, our results show that the periplasmic trehalase affects type 1 expression and in vivo virulence of the ExPEC strain MT78, and the operon for β-glycosides metabolism affects in vivo virulence by an as yet unidentified mechanism.

Escherichia coli

Mutagenese

Trealase

β-glycosides

Trehalose

Type 1 fimbriae

Signature-tagged mutagenesis

A trealase periplasmática e o operon de metabolismo de β-glicosídeos afetam a virulência in vivo na cepa Escherichia coli patogênica extraintestinal MT78

Pavanelo, Daniel Brisotto

January 2017

Escherichia coli patogênicas extraintestinais (ExPEC) causam colibacilose aviária, infecções do trato urinário e meningite neonatal em humanos. A cepa ExPEC MT78 é virulenta in vitro e in vivo, e possui a habilidade de invadir células eucarióticas. Para melhor entender o fenótipo invasivo dessa cepa, foi criada uma biblioteca de mutantes aleatórios pela técnica de mutagênese marcada com assinatura, e os mutantes foram selecionados negativamente em ensaio de invasão a fibroblastos aviários. Mutantes atenuados apresentaram mutação em genes do operon da fímbria do tipo 1 e nos genes de metabolismo de açúcares treA e bglB. Foram feitos mutantes específicos para o gene que codifica a enzima trealase periplasmática (TreA) e para o operon de metabolismo de β-glicosídeos (bgl). O mutante MT78ΔtreA apresentou, frente à cepa selvagem, diminuição na capacidade de adesão e invasão a fibroblastos aviários, na expressão da fímbria do tipo 1 e na capacidade de colonizar a bexiga de camundongos em modelo de infecção urinária. O mutante MT78Δbgl também apresentou, frente à cepa selvagem, diminuição na capacidade de adesão e invasão a fibroblastos aviários e na capacidade de colonizar a bexiga de camundongos em modelo de infecção urinária, mas não mostrou alteração na expressão da fímbria do tipo 1, medida por aglutinação de leveduras. Os resultados deste trabalho mostraram que a trealase periplasmática afeta a expressão da fímbria do tipo 1 e a virulência in vivo da cepa ExPEC MT78, enquanto o operon do metabolismo de β-glicosídeos afeta a virulência in vivo da cepa ExPEC MT78 por um mecanismo ainda não-elucidado. / Extraintestinal pathogenic E. coli (ExPEC) cause colibacillosis in birds, urinary tract infections and neonatal meningitis in humans. The ExPEC strain MT78 is virulent in vitro and in vivo, and is able to invade eukaryotic cells. In order to better understand the invasive phenotype of this strain, a library of random mutants was made using the signature-tagged mutagenesis approach. The mutants were negatively selected in invasion assays of avian fibroblasts. Attenuated mutants presented mutation in the type 1 fimbria operon and in the genes of sugar metabolism treA and bglB. Specific mutants were created for the periplasmic trehalase (TreA) gene and for the β-glycosides metabolism operon (bgl). The MT78ΔtreA mutant displayed, in comparison with the wild type strain, a reduction on the capacity of adhesion and invasion to avian fibroblastos, on type 1 fimbriae expression and on the capacity to colonize the bladder in a murine model of urinary tract infection. The MT78Δbgl mutant, compared to the wild type strain, also displayed a reduction on the capacity of adhesion and invasion to avian fibroblastos and on the capacity to colonize the bladder in a murine model of urinary tract infection, but did not show any difference on type 1 fimbriae expression as detected by yeast agglutination. Taken together, our results show that the periplasmic trehalase affects type 1 expression and in vivo virulence of the ExPEC strain MT78, and the operon for β-glycosides metabolism affects in vivo virulence by an as yet unidentified mechanism.

Escherichia coli

Mutagenese

Trealase

β-glycosides

Trehalose

Type 1 fimbriae

Signature-tagged mutagenesis