Příprava a charakterizace hydrogelů na bázi kationaktivního biopolymeru / Preparation and characterization of hydrogels based on cationic biopolymer

Tesařová, Barbora

January 2017

Presented thesis deals with the preparation and characterization of hydrogels based on positively-charged biopolymer and negatively-charged tenside. As an appropriate representative of positively-charged polymer was chosen chitosan, because of his biocompatibility and biodegrability, and N,N,N-trimethylchitosan, which was synthetised from chitosan in this diploma thesis. The final product of synthesis was characterised by SEC-MALS, elemental analysis, infrared spectroscopy and nuclear magnetic rezonation. Interactions between these polymers and representatives of negatively-charged tensides, which are sodium dodecylsuphate and sodium tetradecylsulphate, were investigated. The main method used in this thesis was rheology, through it were investigated prepared hydrogels based on chitosan and tensides and also prepared microgels based on N,N,N-trimethylchitosan and tensides. The interactions between polymers and tensides have been proved.

Inkorporace nízkomolekulárních a vysokomolekulárních látek do vezikulárních systémů / Incorporation of low molecular weight and high molecular weight substances into vesicular systems

Geistová, Karolína

January 2021

This master´s thesis deals with the study of the incorporation of low and high molecular weight substances into liposomal systems. The aim of the work was to determine the encapsulation efficiency (EE) of the active substance and the influence of individual components of the liposomal system on EE. Liposomes were prepared from dipalmitoylphosphatidylcholine. They were stabilized by cholesteroland and phosphatidic acid was added to give a negative charge. Stealth properties gain the binding of polyethylene glycol and other trimethyl chitosan we enabled the entry of liposomes into the bloodstream by the paracellular pathway. Vitamin C and the enzyme bromelain were used for incorporation into liposomes. UV-VIS spectrophotometry was used to determine the encapsulation efficiency of liposomes prepared by combining the individual components. It has been suggested that vitamin C and the enzyme can be incorporated into liposomes, but an enzyme with a higher EE. Furthermore, phosphatidic acid and trimethyl chitosan have been found to affect EE, which increases the EE of vitamin C and decreases the EE of the enzyme.

Nanoparticulas de poli (n-butil-cianoacrilato) revestidas com N,N,N,-trimetilquitosana: desenvolvimento, caracterização e estudos de permeabilidade in vitro / N,NN-trimethylchitosan coated poly (n-butyl cyanoacrylate) nanoparticles: development, characterization and in vitro permeability

Tavares, Guilherme Diniz

22 March 2013

A via oral é considerada preferencial para a administração de fármacos, sobretudo no tratamento de doenças crônicas. Entretanto, princípios ativos administrados por essa via podem apresentar biodisponibilidade variável e/ou limitada. Diversos tipos de sistemas de liberação vêm sendo desenvolvidos com o objetivo de melhorar esse parâmetro, dentre os quais se destacam as nanopartículas de poli (alquil-cianoacrilato) (PACA). Pelo exposto, no presente trabalho foram desenvolvidas nanopartículas de poli(n-butilcianoacrilato) (PBCA) contendo aciclovir (ACV), revestidas por N,N,N-trimetilquitosana (TMQ), um promissor promotor de absorção. A TMQ foi sintetizada com elevado rendimento e grau de quaternização de aproximadamente 73%. As nanopartículas de PBCA foram obtidas com rendimento adequado e apresentaram características físico-químicas semelhantes às descritas na literatura. Após o revestimento, foi observado um aumento no diâmetro médio, bem com uma inversão nos valores de potencial zeta. Essas observações podem indicar a ocorrência do revestimento. A partir das análises de DSC, pôde-se comprovar a eficiência do revestimento das nanopartículas pelo derivado sintetizado, já que o comportamento das nanopartículas de PBCA-TMQ foi diferente daquele obtido para a mistura física entre os constituintes da formulação. Nessa mesma perspectiva, análises de FTIR foram conduzidas e a ocorrência do revestimento foi corroborada. Além disso, as análises morfológicas por Microscopia de Força Atômica (AFM) revelaram que as nanopartículas revestidas apresentam baixa tendência à agregação, o que pode ser um indicativo de estabilidade para a formulação desenvolvida. Em relação aos ensaios de citotoxicidade, foi evidenciado que as nanopartículas de PBCA não apresentaram toxicidade significativa frente às células Caco-2, ao passo que a formulação revestida mostrou um efeito tóxico dose-dependente influenciado pelo grau de quaternização. Além disso, as nanopartículas desenvolvidas foram capazes de diminuir, reversivelmente, a Resistência Elétrica Transepitelial (RET) da monocamada de células. A fim de quantificar o fármaco associado às nanopartículas, foi desenvolvido e validado método analítico por espectrofotometria derivada com detecção no UV. Tal método mostrou-se capaz de eliminar a interferência dos excipientes, permitindo a quantificação do ACV na formulação de nanopartículas com precisão e exatidão adequadas. Assim, a porcentagem de fármaco associado às nanoestruturas pode ser calculada, obtendo-se um valor satisfatório. De maneira semelhante, foi desenvolvido e validado método por CLAE para a quantificação do fármaco nos ensaios de permeação. A metodologia proposta mostrou-se adequada considerando-se as recomendações da RE 899/03. Por meio dos ensaios de permeabilidade em células Caco-2, foi constatado que a formulação desenvolvida aumentou em 3 vezes o valor de Permeabilidade aparente (Papp) do fármaco em estudo. Além disso, as nanopartículas revestidas foram capazes de propiciar a liberação controlada do ACV nos ensaios de liberação in vitro utilizando meios com diferentes valores de pH (1,2; 6,8 e 7,4). / The oral route is considered for the administration of drugs, especially in the treatment of chronic diseases. However, drugs administered by this route may have variable and/or limited bioavailability. Various types of delivery systems have been developed with the goal of improving this parameter, among which stand out the nanoparticles of poly (alkylcyanoacrylate) (PACA).Such nanomaterials have been coated to improve stability in the gastrointestinal tract, promote greater solubility or enhance permeation. Therefore, in this work were developed nanoparticles of poly (n-butilcianoacrilato) (PBCA) containing acyclovir (ACV), coated with N,N,N-trimethylchitosan (TMC), a promising absorption promoter. The TMC was synthesized with high-yield and approximately 73% of quaternization. The PBCA nanoparticles presented physico-chemical characteristics similar to those described in the literature. After the coating, it was observed an increase in the average diameter, and a inversion on the values of zeta potential. These observations may indicate the occurrence of coating. DSC analysis could proved the efficiency of the coating of nanoparticles, since the behavior of nanoparticles of PBCA-TMC was different from those obtained for the physical mixture between the constituents of the formulation. In this same perspective, FTIR analyses were conducted and the occurrence of coating was corroborated. In addition, morphological analyses by Atomic Force Microscopy (AFM) showed that nanoparticles coated presented low tendency to aggregate, which can be an indication of stability for the formulation developed. In relation to cytotoxicity assays, it was evidenced that the PBCA nanoparticles showed no significant toxicity against the Caco-2 cells, whereas the coated formulation showed a dose-dependent toxic effect influenced by the degree of quaternization. In addition, the nanoparticles developed were able to decrease, reversibly, Transepitelial Electric Resistance (TEER) of the monolayer. In order to quantify the drug associated with nanoparticles, was developed and validated analytical method by derivative spectrophotometry with UV detection. This method was able to eliminate the interference of excipients, allowing the quantification of ACV in the formulation of nanoparticles with appropriate precision and accuracy. Thus, the percentage of drug associated with nanostructures can be calculated, obtaining a satisfactory value. Similarly, has been developed and validated HPLC method for the quantification of drug permeation tests. The proposed methodology was appropriate considering the recommendations of the RE 899/03. Through the permeability assays in Caco-2 cells, it has been found that the formulation developed increased by 3 times the value os Apparent Permeability (Papp) of ACV. In addition, the nanoparticles were able to provide controlled release of ACV in vitro using media with different pH values (1.2; 6.8 and 7.4).

Administração oral

Controlled release

Liberação controlada

N,N,N-trimethylchitosan

N,N,N-trimetilquitosana

Nanopartículas poliméricas

Nanotechnology

Nanotecnologia

Oral administration

Permeabilidade in vitro

Permeability in vitro

Polymeric nanoparticles

Nanoparticulas de poli (n-butil-cianoacrilato) revestidas com N,N,N,-trimetilquitosana: desenvolvimento, caracterização e estudos de permeabilidade in vitro / N,NN-trimethylchitosan coated poly (n-butyl cyanoacrylate) nanoparticles: development, characterization and in vitro permeability

Guilherme Diniz Tavares

22 March 2013

A via oral é considerada preferencial para a administração de fármacos, sobretudo no tratamento de doenças crônicas. Entretanto, princípios ativos administrados por essa via podem apresentar biodisponibilidade variável e/ou limitada. Diversos tipos de sistemas de liberação vêm sendo desenvolvidos com o objetivo de melhorar esse parâmetro, dentre os quais se destacam as nanopartículas de poli (alquil-cianoacrilato) (PACA). Pelo exposto, no presente trabalho foram desenvolvidas nanopartículas de poli(n-butilcianoacrilato) (PBCA) contendo aciclovir (ACV), revestidas por N,N,N-trimetilquitosana (TMQ), um promissor promotor de absorção. A TMQ foi sintetizada com elevado rendimento e grau de quaternização de aproximadamente 73%. As nanopartículas de PBCA foram obtidas com rendimento adequado e apresentaram características físico-químicas semelhantes às descritas na literatura. Após o revestimento, foi observado um aumento no diâmetro médio, bem com uma inversão nos valores de potencial zeta. Essas observações podem indicar a ocorrência do revestimento. A partir das análises de DSC, pôde-se comprovar a eficiência do revestimento das nanopartículas pelo derivado sintetizado, já que o comportamento das nanopartículas de PBCA-TMQ foi diferente daquele obtido para a mistura física entre os constituintes da formulação. Nessa mesma perspectiva, análises de FTIR foram conduzidas e a ocorrência do revestimento foi corroborada. Além disso, as análises morfológicas por Microscopia de Força Atômica (AFM) revelaram que as nanopartículas revestidas apresentam baixa tendência à agregação, o que pode ser um indicativo de estabilidade para a formulação desenvolvida. Em relação aos ensaios de citotoxicidade, foi evidenciado que as nanopartículas de PBCA não apresentaram toxicidade significativa frente às células Caco-2, ao passo que a formulação revestida mostrou um efeito tóxico dose-dependente influenciado pelo grau de quaternização. Além disso, as nanopartículas desenvolvidas foram capazes de diminuir, reversivelmente, a Resistência Elétrica Transepitelial (RET) da monocamada de células. A fim de quantificar o fármaco associado às nanopartículas, foi desenvolvido e validado método analítico por espectrofotometria derivada com detecção no UV. Tal método mostrou-se capaz de eliminar a interferência dos excipientes, permitindo a quantificação do ACV na formulação de nanopartículas com precisão e exatidão adequadas. Assim, a porcentagem de fármaco associado às nanoestruturas pode ser calculada, obtendo-se um valor satisfatório. De maneira semelhante, foi desenvolvido e validado método por CLAE para a quantificação do fármaco nos ensaios de permeação. A metodologia proposta mostrou-se adequada considerando-se as recomendações da RE 899/03. Por meio dos ensaios de permeabilidade em células Caco-2, foi constatado que a formulação desenvolvida aumentou em 3 vezes o valor de Permeabilidade aparente (Papp) do fármaco em estudo. Além disso, as nanopartículas revestidas foram capazes de propiciar a liberação controlada do ACV nos ensaios de liberação in vitro utilizando meios com diferentes valores de pH (1,2; 6,8 e 7,4). / The oral route is considered for the administration of drugs, especially in the treatment of chronic diseases. However, drugs administered by this route may have variable and/or limited bioavailability. Various types of delivery systems have been developed with the goal of improving this parameter, among which stand out the nanoparticles of poly (alkylcyanoacrylate) (PACA).Such nanomaterials have been coated to improve stability in the gastrointestinal tract, promote greater solubility or enhance permeation. Therefore, in this work were developed nanoparticles of poly (n-butilcianoacrilato) (PBCA) containing acyclovir (ACV), coated with N,N,N-trimethylchitosan (TMC), a promising absorption promoter. The TMC was synthesized with high-yield and approximately 73% of quaternization. The PBCA nanoparticles presented physico-chemical characteristics similar to those described in the literature. After the coating, it was observed an increase in the average diameter, and a inversion on the values of zeta potential. These observations may indicate the occurrence of coating. DSC analysis could proved the efficiency of the coating of nanoparticles, since the behavior of nanoparticles of PBCA-TMC was different from those obtained for the physical mixture between the constituents of the formulation. In this same perspective, FTIR analyses were conducted and the occurrence of coating was corroborated. In addition, morphological analyses by Atomic Force Microscopy (AFM) showed that nanoparticles coated presented low tendency to aggregate, which can be an indication of stability for the formulation developed. In relation to cytotoxicity assays, it was evidenced that the PBCA nanoparticles showed no significant toxicity against the Caco-2 cells, whereas the coated formulation showed a dose-dependent toxic effect influenced by the degree of quaternization. In addition, the nanoparticles developed were able to decrease, reversibly, Transepitelial Electric Resistance (TEER) of the monolayer. In order to quantify the drug associated with nanoparticles, was developed and validated analytical method by derivative spectrophotometry with UV detection. This method was able to eliminate the interference of excipients, allowing the quantification of ACV in the formulation of nanoparticles with appropriate precision and accuracy. Thus, the percentage of drug associated with nanostructures can be calculated, obtaining a satisfactory value. Similarly, has been developed and validated HPLC method for the quantification of drug permeation tests. The proposed methodology was appropriate considering the recommendations of the RE 899/03. Through the permeability assays in Caco-2 cells, it has been found that the formulation developed increased by 3 times the value os Apparent Permeability (Papp) of ACV. In addition, the nanoparticles were able to provide controlled release of ACV in vitro using media with different pH values (1.2; 6.8 and 7.4).

Administração oral

Liberação controlada

N,N,N-trimetilquitosana

Nanopartículas poliméricas

Nanotecnologia

Permeabilidade in vitro

Controlled release

N,N,N-trimethylchitosan

Nanotechnology

Oral administration

Permeability in vitro

Polymeric nanoparticles

Studium interakce záporně nabitých vezikulárních systémů s polykationty / Study of interaction of negatively charged vesicular systems with polycations

Repová, Romana

January 2020

This diploma thesis deals with the preparation and characterization of negatively charged catanionic vesicular systems and their combination with selected polycations. The catanionic vesicular system was prepared by mixing of two oppositely charged surfactants SDS and CTAB. The negative charge as well as the stability of the vesicular system was provided by the incorporation of phosphatidic acid. Polycations, DEAE and TMC, have been selected for use in a pharmaceutical applications. Characterization of the prepared systems was performed by measuring DLS and ELS. The results indicate that we were able to prepare stable negatively charged vesicles that were eligible to non-covalently interact with selected polycations.

Studium membránových vlastností liposomálních systémů pomocí fluorescenční spektroskopie / Study of membrane properties of liposomal systems using fluorescence spectroscopy

Zbořilová, Hana

January 2021

The presented diploma thesis is focused on the preparation, characterization and study of membrane properties of liposomal systems which were composed of the neutral phosphatidylcholine (DPPC), cholesterol, negatively charged phosphatidylglycerol (DPPG), polyethylenglycol bounded to phosphatidylethanolamine (PEG5000–PE) and polycation N,N,N-trimethylchitosan (TMC). The influence of individual components and their concentrations on the average particle size, zeta potential and changes in the outer and inner part of the bilayer was investigated. In this matter, methods of dynamic and electrophoretic light scattering and fluorescence spectroscopy with the application of laurdan and DPH probes were used. Based on the above-mentioned parameters, concentrations of components that most suitably influence properties of liposomes in terms of the intended application were selected for the definite complex. It was managed to prepare a liposomal complex stealth liposome–N,N,N-trimethylchitosan, which, due to the optimized composition, could have suitable attributes as a drug delivery system for inhalation administration of biologically active substances.

Příprava a charakterizace komplexních liposomálních systémů pro distribuci léčiv / Preparation and characterization of complex liposomal for drug delivery systems

Szabová, Jana

January 2019

This diploma thesis deals with the preparation and characterization of stealth liposomes and their combination with trimethylchitosan (TMC). This complex could find application in the field of inhalation administration. Stealth liposomes were prepared from neutral phophatidylcholine, negatively charged fosfatidic acid and polyethyleneglycol bounded to phosphatidylethanolamine. We have managed to prepare stealth liposomes with suitable properties that should guarantee passive targeting without evocation an immune response, despite the content of the negative component. We also found a suitable method of preparation for stealth liposome–TMC complex, where the change of size and zeta potential confirmed the non–covalent bound between two components despite the content of the polyethyleneglycol.