Desenvolvimento e avaliação de sistemas transdérmicos com a adição de vitamina D3 / Development and evaluation of transdermal delivery system of vitamin D3

Costa, Gabriela Maria D\'Angelo

24 October 2017

A hipovitaminose de vitamina D é um problema global de saúde e a sua deficiência compromete funções importantes ao corpo humano. A suplementação oral, políticas de fortificação em alimentos e mudanças dos hábitos de vida são medidas efetivas para solucionar este problema. Porém, pessoas com doença de Crohn, celíaca, fibrose cística, bypass gástrico e que fazem uso de medicamentos sequestradores de ácido biliares possuem a absorção intestinal de vitamina D comprometida. A via transdérmica pode ser uma alternativa de administração de vitamina D3, porém poucas referências bibliográficas abordam sobre o assunto. A proposta do presente estudo é o desenvolvimento de sistemas transdérmicos com a combinação de promotores de permeação químicos: lecitina de soja, palmitato de isopropila, etoxidiglicol (Transcutol® CG), propilenoglicol e etanol, acrescidos do ingrediente ativo vitamina D3, a validação analítica para quantificação do ativo em Cromatografia Líquida de Alta Eficiência (CLAE), a avaliação da estabilidade, segurança, retenção e permeação cutânea. A validação do método analítico de quantificação da vitamina D3 em CLAE foi considerada específica, linear, precisa e exata. O limite de detecção foi 20 ng/mL e de quantificação 40 ng/mL. Os testes de estabilidade foram realizados (preliminar, acelerado e normal) e a melhor condição de armazenamento foi a geladeira (5,0 ± 2,0 ºC) durante 90 dias. A condição de radiação luminosa foi a menos adequada, o que indica que o armazenamento deve ser realizado em frascos protegidos da luz (âmbar). No teste de segurança de irritação (HET-CAM) as formulações testadas foram consideradas não irritantes. No teste de retenção e permeação cutânea a solubilidade da vitamina D3 foi avaliada para garantir a sink condition do líquido receptor escolhido: Phosfate Buffer Saline (PBS) com etanol a 50% e a integridade da pele foi garantida com o teste de perda de água transepidérmica (TEWL). A formulação desenvolvida com a presença de todos os promotores de permeação avaliados (F1) e o controle, apenas com a presença do etanol e o propilenoglicol, foram avaliados. A F1 permaneceu na superfície da pele, por possuir maior afinidade com a fase oleosa da formulação e houve tendência de hidratação desta formulação. O controle demonstrou uma retenção cutânea em 4 h no estrato córneo e em 24 h na epiderme e derme. Concluiu-se que a formulação desenvolvida é estável, segura e a vitamina D3 ficou retida na pele, o que indica o uso tópico da mesma. A alta lipofilicidade foi a justificativa dos resultados apresentados e futuros estudos podem ser realizados com derivados menos lipofílicos da vitamina D para avaliar a via transdérmica. / Hypovitaminosis D is a global health issue and vitamin D deficiency compromises important functions to the human body. Oral supplementation, fortification food and changes in live style are effective measures to solve this problem. However, people with Crohn\'s disease, celiac disease, cystic fibrosis, gastric bypass and who use bile acid-binding medications have compromised intestinal vitamin D absorption. The transdermal route may be an alternative for vitamin D3 administration, but few references refer to the subject. The purpose of the present study is the development of transdermal systems with the combination of penetrations enhancers (soybean lecithin, isopropyl palmitate, ethoxydiglycol (Transcutol® CG), propylene glycol and ethanol) with vitamin D3, the analytical validation for quantification of the active in High Performance Liquid Chromatography (HPLC), stability assessment, safety, skin retention and permeation. The validation of the analytical method for quantification of vitamin D3 in HPLC was considered specific, linear, precise and accurate. The limit of detection was 20 ng/mL and 40 ng/mL. Stability assessment was performed and the appropriate storage condition was the refrigerator (5.0 ± 2.0 ° C) for 90 days. The indirect solar radiation condition was not adequate, which indicates that the storage should be performed in light-protected bottles (amber). In the irritation safety test (HET-CAM) the formulations tested were considered non-irritant. In the skin permeation and retention test the solubility of vitamin D3 was evaluated to guarantee the sink condition of the receptor fluid: Phosfate Buffer Saline (PBS) with 50% ethanol and skin integrity was guaranteed with Transepidermal Water Loss (TEWL). The developed formulation with the presence of all penetrations enhancers evaluated (F1) and the control formulation with the presence of ethanol and propylene glycol were assessed. F1 remained on the surface of the skin, because it had greater affinity with the oily phase of the formulation and there was tendency of hydration to this formulation. The control formulation demonstrated skin retention in 4 hours in the stratum corneum and in 24 hours in the epidermis and dermis. The study concluded that the formulation developed is stable, safe and vitamin D3 was retained in the skin, which indicates the topical use. High lipophilicity was the explanation of the presented results and future studies can be carried out with less lipophilic derivatives of vitamin D to evaluate the transdermal route.

Penetrations enhancers

Permeação cutânea

Promotores de permeação químicos

Retenção cutânea

Sistemas transdérmicos

Skin permeation

Skin retention

Transdermal Systems

Vitamina D3

vVitamin D3

Avaliação dos óleos essenciais de plantas nativas da Mata Atlântica como promotores de permeação cutânea / Evaluation of essential oils of plants native to the Atlantic Forest as skin permeation enhancers

Lacerda, Aurea Cristina Lemos

09 October 2014

Os óleos essenciais da Pimenta pseudocaryophyllus (Gomes) Landrum de planta de populações naturais de três ecossistemas, localizados na Ilha de Cananéia, região de restinga, no Morro da Cataia, cidade de Cajati, região de encosta, ambas em área de Mata Atlântica, e na Reserva Natural Morro Grande, cidade de Caldas, região de campos montanos, foram avaliados como promotores de permeação cutânea do diclofenaco de potássio. Os óleos essenciais foram extraídos de partes aéreas das plantas e o rendimento do processo foi entre 0,90% (p/p) e 2,7% (p/p). A análise da composição química mostrou diferenças, indicando tratar-se de três quimiotipos diferentes. A interação dos óleos essenciais e dos componentes majoritários com membrana biológica natural foi avaliada por FT-Raman e ATR- FTIR, indicando a interação com as porções lipídicas do tecido. Foram desenvolvidas seis membranas biológicas artificiais, compostas por ceramidas, ácidos graxos e colesterol em proporções equimolares, que foram caracterizadas por espectroscopia Raman confocal e foram consideradas semelhantes. As membranas foram utilizadas no desenvolvimento do sistema PAMPA (Parallel Artificial Membrane Permeability Assay) para avaliar a segurança e eficácia dos óleos essenciais e componentes majoritário como promotores de permeação do diclofenaco de potássio. Os resultados dos ensaios com o sistema PAMPA foram estatisticamente avaliados. A segurança foi avaliada com o critério de permeação mínima dos óleos através das membranas do sistema PAMPA, verificada pela absorbância mínima do eugenol na solução aceptora. Os óleos essenciais e componentes majoritários foram utilizados no pré-tratamento das membranas, nas concentrações de 0,125%, 0,25%, 0,50% e 2,00% (v/v) em etano!. Ensaios de permeação do diclofenaco de potássio no sistema PAMPA indicaram efeito de promoção da permeação para todos os compostos avaliados. O método de doseamento do fármaco por UV foi validado e utilizado para os ensaios de permeação de formulações de gel em base aquosa contendo o diclofenaco de potássio (1,0% p/p). As amostras de gel foram preparadas com o óleo procedente de Morro Grande, selecionado na etapa de avaliação de segurança, a 0,125% (p/v). Adicionalmente, foram preparadas formulações com citronelol e etanol, na mesma concentração. O óleo essencial da Reserva Natural Morro Grande teve efeito de promoção da permeação superior ao do citronelol e etanol, que foram equivalentes. / The essential oils of the species Pimenta pseudocaryophyllus (Gomes) Landrum collected from natural populations of three existing ecosystems in the Cananéia Island, located at sea level, Cajati city, located in hillside region, both in the Atlantic Forest areas, as well as species collected in the Morro Grande Natural Reserve, region of montane fields, were evaluated as skin permeation enhancers of potassium diclofenac. Essential oils were extracted from the aerial parts of the plants and the process yield was between of 0.90% (w/w) and 2.7% (w/w). The chemical composition analysis showed differences between the plants of three origins, indicating that they are different chemotypes. The interaction of the essential oils and their major components with natural biological membrane was evaluated by FT- Raman and ATR-FTIR, indicating interaction with the Iipid portions of the natural membrane. Six artificial biological membranes have been developed, consisting of ceramides, cholesterol and fatty acids in equimolar proportions, which were characterized by confocal Raman spectroscopy and found to be similar. The membranes were used in developing the PAMPA (Parallel Artificial Membrane Permeability Assay) system to evaluate the safety of the potential permeation enhancers. The test results with PAMPA system were statistically evaluated. Safety was evaluated with the criterion of minimum permeation of the essential oil through the membranes, checked by the minimum absorbance of eugenol in the acceptor solution. The essential oils and the major components were used in the pretreatment of the membranes, at concentrations of 0.125%, 0.25%, 0.50% and 2.00% (v/v) in ethanol. Results indicated permeation enhancement effect for ali compounds evaluated. The analytical method for the quantification of potassium diclofenac was validated and used for the evaluation of the permeation of aqueous based gel formulations containing potassium diclofenac (1.0% w/w). The gel samples were prepared with the oil from Morro Grande Natural Reserve, selected in the safety evaluation step, at 0.125% (w/v). In addition, formulations were prepared with citronellol and ethanol at the same concentration. The essential Gil of Morro Grande Natural Reserve was more efficient as permeation enhancer than citronellol and ethanol under the test conditions.

Biophysical methods

Diclofenac potassium

Diclofenaco de potássio

Métodos biofísicos

Oil essential

Óleos essenciais

PAMPA

PAMPA

Pepper pseudocaryophyllus

Permeation enhancers

Pimenta pseudocaryophyllus

Promotores de permeação

Eléments cis-régulateurs du locus IgH et lymphomagenèse B / Cis-regulatory elements of the IgH locus and B cell lymphomagenesis

Ghazzaui, Nour

18 December 2018

Le locus des chaînes lourdes d’immunoglobulines (IgH) subit trois processus de remaniements géniques durant la lymphopoïèse B. Ces événements induisent des cassures de l’ADN potentiellement oncogéniques, d’où la nécessité d’une régulation extrêmement stricte. Ceci est dû aux deux principaux éléments cis-régulateurs du locus IgH. L’enhancer 5’Eµ régule les recombinaisons VHDJH qui établissent un répertoire antigénique fonctionnel lors des phases précoces. La région régulatrice en 3’ (3’RR) est essentielle aux hypermutations somatiques (SHM) et à la recombinaison de classe (CSR) aux stades tardifs, modifiant respectivement, l’affinité et les fonctions effectrices de l’Ig. La plupart des lymphomes B matures portent les stigmates de translocations d’oncogènes au locus IgH. Le but de ma thèse a été de mieux comprendre les interactions transcriptionelles entre les enhancers Eµ et 3’RR et évaluer si le ciblage de cette dernière pourrait se révéler une approche thérapeutique potentielle. Nous avons démontré que la 3’RR est l’élément essentiel qui contrôle la transcription du locus IgH dans les lymphocytes B matures. Elle est dispensable lors des phases initiales (recombinaisons VHDJH), mais agit comme silencer sur l’expression des segments DJH. L’analyse de la lymphomagenèse dans trois modèles murins porteurs d’une insertion de Myc en trois points du locus IgH a montré des différences dans les cinétiques d’émergence des lymphomes, leurs phénotypes et index de prolifération. L’effet de la 3’RR sur l’oncogène est suffisant pour l’émergence de lymphomes B. Son absence ne semble pas être préjudiciable au développement de réactions inflammatoires/immunes. Son ciblage pourrait donc se révéler une approche thérapeutique intéressante pour diminuer son activité transcriptionelle sur l’oncogène transloqué. Un rôle potentiel des inhibiteurs des histones désacétylases est à l’étude. / The immunoglobulin heavy chain locus (IgH) undergoes several changes along B-cell differentiation. VHDJH recombinations during the early stages give the diversity of the antigenic repertoire. Somatic hypermutation (SHM) and class switch recombination (CSR) during late stages allow affinity maturation and the acquisition of new effectors functions. These rearrangements are highly regulated and are under the control of the IgH locus cis-regulatory elements. The 5’ Eµ enhancer is important for VHDJH recombination. The 3’ regulatory region (3’ RR) is essential for both CSR and SHM. These events induce breaks into the IgH locus, making it a hotspot for oncogenic translocations. The aim of my thesis was to understand the transcriptional interactions between Eμ and 3'RR enhancers and to evaluate whether the targeting of the latter could be of a potential therapeutic approach. We have demonstrated that 3'RR is essential to control IgH transcription in mature B cells. It is dispensable during the initial stages of developement (VHDJH recombinations). At the pro-B cell stage, it has a silencer effect rather than a transcriptional one on the DJH segments expression. The analysis of lymphomagenesis in three mice models carrying an insertion of Myc in different locations at the IgH locus showed significant differences in lymphoma kinetics, phenotypes and proliferation index. 3'RR alone, as a major transcriptional activator of the IgH locus, is capable of leading to B-cell lymphomas. Its absence is not detrimental for the development of classical inflammatory/immune reactions. Its targeting may be of a potentially interesting therapeutic approach to decrease its transcriptional activity on the translocated oncogene. A potential role for histone deacetylase inhibitors is under study.

Locus IgH

3’RR

Myc

Lymphomes B matures

Activateurs transcriptionnels

IgH locus

3’RR

Myc

Mature B-cell lymphomas

Transcriptional enhancers

615.37

Promoter and Enhancer Chromatin Dynamics during Direct Cell Fate Programming

Ibrahim, Mahmoud

09 August 2017

Die Beschreibung genregulatorischer Ereignisse ist entscheidend um Zelldifferenzierung und -entwicklung zu verstehen. Dynamische Vernderungen der Chromatinstruktur, Histonmodifikationen und das Binden von Transkriptionsfaktoren an Enhancer und Promotoren, koennen mit Hilfe von genomweiten Hochdurchsatz-Sequenziertechniken wie ChIP-Seq, DNase-Seq, ATACSeqund RNA-Seq untersucht werden. In dieser Arbeit entwickele ich mehrere probabilistische Modelle fuer die Analyse von genomweiten Sequenzierungsdaten. Diese umfassen 1. einen Peak-Finder fuer ChIP-/DNase-/ATAC-Seq-Daten, der sich Replikate zunutze macht und praezise Peak-Weiten berechnet, 2. eine Pipeline um das Genom in hoher Aufloesung in eindeutige Klassen von Kombinationen von Histonmodifikationen zu segmentieren, 3. ein Bayes-Netzwerk-Modell welches multiple zeitlich aufgelste Histonmodifikations-ChIP-seq-Daten kombinatorisch clustert Klassen von regulatorischen Elementen zu identifizieren. Mit Hilfe dieser Modelle untersuchen wir die Promotorumgeben und zeigen einen Zusammenhang zwischen Chromatinstruktur und Promotordirektionalitaet. Darueber hinaus verwenden wir ein Modell zur direkten Reprogrammierung von Stammzellen in Motorneuronen durch die gezielte Expression von Transkriptionsfaktoren und analysieren die dadurch induzierten zeitlichen Vernderungen der Chromatinstruktur und Transkriptionsfaktorbindedynamik. Wir beobachten, dass Promotoren verschiedenen Chromatin-Dynamiken zur Aktivierung und Repression folgen, die mit den Chromatin-Dynamiken von Enhancer-Elementen korrelieren. Enhancer hingegen werden durch kooperatives Verhalten direkt induzierter Transkriptionsfaktoren und anderen Faktoren, die in den Stammzellen zu Beginn vorhanden waren oder im Verlaufe der Differenzierung aktiviert wurden, kontrolliert. Diese Arbeit zeigt wie wichtig Chromatin-Dynamik und ihre Beziehung zur Logik von Transkriptionsfaktoren ist, um die Veraenderungen der Genexpression zu verstehen. / Delineating transcription regulatory events is crucial to understand cell differentiation and development. Dynamic changes of chromatin structure, histone modifications and transcription factor binding to enhancers and promotors can be investigated with the aid of genome-wide high-throughput sequencing technologies such as ChIP-Seq, DNase-Seq, ATAC Seq and RNA Seq. In this thesis, I develop several probabilistic models for the analysis of genome-wide sequencing data. These include: 1. a peak finder for ChIP-Seq, DNase-Seq and ATAC Seq data, which exploits biological replicates and accurately demarcates peak widths, 2. a pipeline for high-resolution genome segmentation into unique classes of combinations of histone modifications and 3. a Bayesian network model that can co-cluster multiple time-course histone modification ChIP-Seq data sets into distinct classes of regulatory elements. With the aid of these models we investigate the promoter chromatin environment and show a link between chromatin state and transcription initiation directionality. In addition, we use a system for direct reprogramming of stem cells in motor neurons by the targeted expression of transcription factors to analyse changes in chromatin state and transcription factor dynamics during differentiation. We observe that promoters follow different chromatin dynamics for activation and repression that correlate with the chromatin dynamics of enhancer elements. Enhancers are controlled by cooperative behavior of directly induced transcription factors and other factors present in the stem cells initially, or activated in the course of differentiation. Overall, this work demonstrates the importance of understanding chromatin dynamics and their relationship to transcription factors logic in order to better explain changes in gene expression.

Stammzellen

Promoter

Chromatin

Enhancer-Elemente

Stem cells

Promoters

Enhancers

Chromatin

570 Biowissenschaften; Biologie

WE 4500

WE 2200

WC 7700

ddc:570

A influência do D-limoneno como promotor de absorção de ácido 5-aminolevulínico para Terapia Fotodinâmica do câncer de pele: avaliação in vitro e in vivo da permeação e retenção cutâneas / D-limonene influence in the cutaneous penetration enhancer for 5-aminolevulinic acid in photodynamic therapy of skin cancer: in vitro and in vivo skin permeation and retention studies.

Bertolini, Wagner Luiz Heleno Marcus

27 April 2009

BERTOLINI, WAGNER L. H. M. A influência do D-limoneno como promotor de absorção do ácido 5-aminolevulínico para Terapia Fotodinâmica do câncer de pele: avaliação in vitro e in vivo da permeação e retenção cutâneas. 2009 118f. Tese (Doutorado). Faculdade de Ciências Farmacêuticas de Ribeirão Preto Preto Universidade de São Paulo, Ribeirão Preto, 2009. O câncer é a segunda doença principal do planeta, muito próximo de se tornar a mais incidente. Os tratamentos tradicionais do câncer, tais como cirurgia, radioterapia e quimioterapia apresentam severos efeitos colaterais ao paciente devido à citotoxicidade que podem causar às células normais, além das cancerosas. Objetivando minimizar estes efeitos indesejáveis pesquisadores de diversas áreas afins vislumbram novas técnicas, novos tipos e formas de tratamentos que apresentem um melhor perfil terapêutico; que possam agir de forma mais seletiva contra as células cancerosas, minorando os efeitos indesejáveis em relação às células saudáveis. Dentre as técnicas pesquisadas destaca-se a Terapia Fotodinâmica (TFD). Esta é uma técnica de tratamento nova e promissora. A técnica do tratamento consiste em aplicar, no tecido alvo, substâncias fotossensibilizantes, posteriormente ativadas com luz de comprimentos de onda específicos, com a finalidade de produzir destruição celular, por meio da ação de produtos citotóxicos fotoativados. Destaca-se a seletividade apresentada pela técnica, que deve ser reconhecida como uma das vantagens entre as técnicas empregadas no tratamento do câncer. O presente trabalho objetiva verificar a influência do D-limoneno como promotor de permeação do ácido 5-aminolevulínico (5-ALA) em aplicação tópica. Isto visa aumentar a permeação do 5-ALA quando aplicado topicamente. O 5-ALA é convertido a protoporfirina-IX (PpIX) pela via do ciclo Heme. Esta é um potente agente fotossensibilizador endógeno. O interesse no uso deste promotor foi aumentar a taxa de penetração do 5-ALA, possibilitando a permeação de maiores quantidades do fármaco em questão. Para isto foram realizados estudos de permeação in vitro do 5-ALA, em concentração de 1% (p/p) utilizando-se formulações (emulsões O/A) com diferentes concentrações do promotor D-limoneno (0, 5, 10, 20 e 30%), (p/p). Observou-se que o fluxo in vitro do 5-ALA através da pele de orelha de porco aumentou para todas as formulações empregadas quando comparado ao controle, sem D-limoneno, para um período de estudo de 12h. A retenção no estrato córneo e na [epiderme + derme] apresentou aumento significativo, evidenciando, assim, um efeito eficiente do D-limoneno como promotor. Experimentos in vivo foram conduzidos em camundongos objetivando a análise do efeito da formulação na produção e acúmulo de PpIX na pele. Observou-se que o D-limoneno aumentou significantemente a quantidade de PpIX extraída da pele. Os resultados in vitro e in vivo mostraram o potencial do D-limoneno como promotor de absorção cutânea para o 5-ALA para a TFD tópica do cancer de pele. / BERTOLINI, WAGNER L. H. M. D-limonene influence in the cutaneous penetration enhancer for 5-aminolevulinic acid in photodynamic therapy of skin cancer: in vitro and in vivo skin permeation and retention studies. 2009 118f. Thesis (Doctoral). Faculdade de Ciências Farmacêuticas de Ribeirão Preto Preto Universidade de São Paulo, Ribeirão Preto, 2009. The topical administration of 5-ALA has been distinguished on skin cancer photodynamic therapy (PDT) because of its efficiency in the treatment of tumors and the reduced phototoxic collateral effects. However, this effectiveness is limited by its low penetration in the skin. A proposal to optimize the 5-ALA penetration in the skin is the use of cutaneous penetration enhancers, which seek to alter the cutaneous barrier for many bioactive molecules. The aim of this work was the pharmaceutical development of formulations containing D-limonene as a cutaneous penetration enhancer, seeking the increase of the cutaneous penetration of 5-ALA for skin cancer PDT. The in vitro flux of 5-ALA present in 1% (w/w) from different formulations containing D-limonene (20 e 30% w/w) was significantly increased after 12 hours of experiment, in comparison with formulations without D-limonene, mainly for the formulations containing 20% and 30% of D-limonene with 1% of 5-ALA (1,45 and 2,01 times, respectively). The stratum corneum (SC) and [epidermis + dermis] without SC retention were also significantly increased, showing an enhancer effect of the promoter. In addition, in vivo experiments were accomplished in mice, with the purpose of analyzing the formulation effect on the PpIX production and accumulation in the skin. It was observed that the penetration enhancer\'s presence significantly increased the amount of PpIX extracted from the skin. Both in vitro and in vivo results showed the potentiality of the formulations containing D-limonene as a cutaneous penetration enhancer for 5-ALA delivery on the skin cancer PDT.

5-aminolevulinic acid

Câncer de pele

D-limonene

D-limoneno. 5- Ácido 5-amin

penetration enhancers

Photodynamic therapy

promotor de permeação

Skin

Terapia fotodinâmica

Desenvolvimento e avaliação de sistemas transdérmicos com a adição de vitamina D3 / Development and evaluation of transdermal delivery system of vitamin D3

Gabriela Maria D\'Angelo Costa

24 October 2017

A hipovitaminose de vitamina D é um problema global de saúde e a sua deficiência compromete funções importantes ao corpo humano. A suplementação oral, políticas de fortificação em alimentos e mudanças dos hábitos de vida são medidas efetivas para solucionar este problema. Porém, pessoas com doença de Crohn, celíaca, fibrose cística, bypass gástrico e que fazem uso de medicamentos sequestradores de ácido biliares possuem a absorção intestinal de vitamina D comprometida. A via transdérmica pode ser uma alternativa de administração de vitamina D3, porém poucas referências bibliográficas abordam sobre o assunto. A proposta do presente estudo é o desenvolvimento de sistemas transdérmicos com a combinação de promotores de permeação químicos: lecitina de soja, palmitato de isopropila, etoxidiglicol (Transcutol® CG), propilenoglicol e etanol, acrescidos do ingrediente ativo vitamina D3, a validação analítica para quantificação do ativo em Cromatografia Líquida de Alta Eficiência (CLAE), a avaliação da estabilidade, segurança, retenção e permeação cutânea. A validação do método analítico de quantificação da vitamina D3 em CLAE foi considerada específica, linear, precisa e exata. O limite de detecção foi 20 ng/mL e de quantificação 40 ng/mL. Os testes de estabilidade foram realizados (preliminar, acelerado e normal) e a melhor condição de armazenamento foi a geladeira (5,0 ± 2,0 ºC) durante 90 dias. A condição de radiação luminosa foi a menos adequada, o que indica que o armazenamento deve ser realizado em frascos protegidos da luz (âmbar). No teste de segurança de irritação (HET-CAM) as formulações testadas foram consideradas não irritantes. No teste de retenção e permeação cutânea a solubilidade da vitamina D3 foi avaliada para garantir a sink condition do líquido receptor escolhido: Phosfate Buffer Saline (PBS) com etanol a 50% e a integridade da pele foi garantida com o teste de perda de água transepidérmica (TEWL). A formulação desenvolvida com a presença de todos os promotores de permeação avaliados (F1) e o controle, apenas com a presença do etanol e o propilenoglicol, foram avaliados. A F1 permaneceu na superfície da pele, por possuir maior afinidade com a fase oleosa da formulação e houve tendência de hidratação desta formulação. O controle demonstrou uma retenção cutânea em 4 h no estrato córneo e em 24 h na epiderme e derme. Concluiu-se que a formulação desenvolvida é estável, segura e a vitamina D3 ficou retida na pele, o que indica o uso tópico da mesma. A alta lipofilicidade foi a justificativa dos resultados apresentados e futuros estudos podem ser realizados com derivados menos lipofílicos da vitamina D para avaliar a via transdérmica. / Hypovitaminosis D is a global health issue and vitamin D deficiency compromises important functions to the human body. Oral supplementation, fortification food and changes in live style are effective measures to solve this problem. However, people with Crohn\'s disease, celiac disease, cystic fibrosis, gastric bypass and who use bile acid-binding medications have compromised intestinal vitamin D absorption. The transdermal route may be an alternative for vitamin D3 administration, but few references refer to the subject. The purpose of the present study is the development of transdermal systems with the combination of penetrations enhancers (soybean lecithin, isopropyl palmitate, ethoxydiglycol (Transcutol® CG), propylene glycol and ethanol) with vitamin D3, the analytical validation for quantification of the active in High Performance Liquid Chromatography (HPLC), stability assessment, safety, skin retention and permeation. The validation of the analytical method for quantification of vitamin D3 in HPLC was considered specific, linear, precise and accurate. The limit of detection was 20 ng/mL and 40 ng/mL. Stability assessment was performed and the appropriate storage condition was the refrigerator (5.0 ± 2.0 ° C) for 90 days. The indirect solar radiation condition was not adequate, which indicates that the storage should be performed in light-protected bottles (amber). In the irritation safety test (HET-CAM) the formulations tested were considered non-irritant. In the skin permeation and retention test the solubility of vitamin D3 was evaluated to guarantee the sink condition of the receptor fluid: Phosfate Buffer Saline (PBS) with 50% ethanol and skin integrity was guaranteed with Transepidermal Water Loss (TEWL). The developed formulation with the presence of all penetrations enhancers evaluated (F1) and the control formulation with the presence of ethanol and propylene glycol were assessed. F1 remained on the surface of the skin, because it had greater affinity with the oily phase of the formulation and there was tendency of hydration to this formulation. The control formulation demonstrated skin retention in 4 hours in the stratum corneum and in 24 hours in the epidermis and dermis. The study concluded that the formulation developed is stable, safe and vitamin D3 was retained in the skin, which indicates the topical use. High lipophilicity was the explanation of the presented results and future studies can be carried out with less lipophilic derivatives of vitamin D to evaluate the transdermal route.

Permeação cutânea

Promotores de permeação químicos

Retenção cutânea

Sistemas transdérmicos

Vitamina D3

Penetrations enhancers

Skin permeation

Skin retention

Transdermal Systems

vVitamin D3

Epigenetic regulation by estrogen receptor in breast cancer cells / Régulation de l'épigénome par le récepteur des oestrogènes dans le cancer du sein

Sklias, Athéna

06 September 2019

Les travaux épidémiologiques et expérimentaux effectués à ce jour sur le cancer du sein ont montré que les oestrogènes - comme l’eostradiole (E2) - et leur récépteur (ER) - un facteur de transcription les liants - sont fortement impliqués dans au moins 70% des cas de cancer du sein. Cette implication est d’autant plus visible que les patients, suite à une thérapie anti-oestrogénique, ont tendance à développer une résistance endocrinienne au traitement. Pendant longtemps, l’ER a été étudié en tant que facteur indépendant liant directement une séquence ADN spécifique sur le génome. Aujourd’hui le paradigme a profondément changé. Il est bien connu que ER s’associe avec de nombreux autres facteurs de transcription et protéines régulant la chromatine afin de réguler l’expression des gènes. Cependant, nos connaissances concernant la fonction de modifications épigénétiques suite à l’activation de ER - notamment la méthylation de l’ADN et l’acétylation des histones - sont encore limitées. Dans cette étude, j’ai mis en place un protocole de culture cellulaire adapté à l’étude de la privation et à la re-stimulation d’E2 stricto sensu. Dans un premier temps, ce protocole a été évalué à l’aide de la toute dernière technologie de puce permettant la lecture du méthylome et couvrant la liste complète des éléments amplificateurs. Dans un deuxième temps, j’ai mesuré le transcriptome et les profiles d’acétylation de l’histone H3 (H3K27ac) afin de déterminer la capacité de ER à réguler l’expression des gènes J’ai découvert que, suite à la privation de E2, les niveaux de méthylation de l’ADN et de H3K27ac changent et que ces changements s’accentuent avec le temps, en particulier au niveau des éléments amplificateurs. Une analyse d’enrichissement des facteurs de transcription et des séquences de liaison spécifiques a révélé que les facteurs de transcriptions des familles AP-1 et FOX sont des intermédiaires favorisants la liaison de ER aux éléments amplificateurs. Finalement, la re-stimulation des cellules par de l’E2 a montré que la majorité des changements épigénétiques observé sont réversibles mais que certains éléments amplificateurs restent hyperméthylés et déacétylés. Ceci pourrait indiquer que les traitements anti-oestrogéniques sont efficaces mais pourrait également indiquer un marqueur de résistance endocrinienne. Cette étude apporte des informations nouvelles quant aux effets de l’inhibition et l’activation de ER sur la méthylation de l’ADN et l’acétylation de l’histone H3 à l’échelle du génome et renforce l’importance du rôle d’autres facteurs au niveau des amplificateurs / Previous epidemiological and experimental studies have strongly implicated estrogens in breast cancer risk and Estrogen Receptor (ER), the transcription factor to which estrogen binds, is considered as the major molecular driver of around 70% breast cancers. The importance of the deregulated estrogen signalling is further highlighted by increasing evidence that current chemopreventive and therapeutic strategies that target hormonally responsive breast cancers frequently result in the development of resistance to anti-estrogens and metastatic progression, highlighting the need for understanding the molecular underlying mechanisms. While until recently, ER was believed to act as a stand-alone transcription factor, which can directly bind its motifs in DNA, it is now accepted that ER activity is a complex and dynamic process that requires highly concerted actions of a dozen transcriptional cofactors and various chromatin regulators at DNA. Recent studies focused on characterising ER-associated cofactors and their role in opening the chromatin provided a remarkable insight into transcriptional regulation mediated by ER. However DNA methylation and histone acetylation are poorly understood in the context of ER’s dynamic binding. In this thesis, I combined a cell culture protocol adapted for studying estradiol (E2) deprivation and re-stimulation in stricto sensu in ER-positive breast cancer cells with the latest methylation array, that allowed a genome-wide interrogation of DNA methylation (including a comprehensive panel of enhancers). I further investigated histone acetylation (ChIP-seq) and transcriptome (RNA-seq) after E2 deprivation and re-stimulation to better characterise the ability of ER to coordinate gene regulation. I found that E2 deprivation and re-stimulation result in time-dependent DNA methylation changes and in histone acetylation across diverse genomic regions, many of which overlap with enhancers. Further enrichment analysis of transcription factor (TF) binding and motif occurrence highlights the importance of ER tethering mainly through two partner TF families, AP-1 and FOX, in the proximity of enhancers that are differentially methylated and acetylated. This is the first study that comprehensively characterized DNA methylation at enhancers in response to inhibition and activation of ER signalling. The transcriptome and genome occupancy data further reinforced the notion that ER activity may orchestrate a broad transcriptional programme through regulating a limited panel of critical enhancers. Finally, the E2 re-stimulation experiments revealed that although the majority of the observed epigenetic changes induced by E2 deprivation could be largely reversed when the cells were re-stimulated we show that DNA hypermethylation and H3K27 acetylation at enhancers as well as several gene expression changes are selectively retained. The partial reversibility can be interpreted as a sign of treatment efficiency but also as a mechanism by which ER activity may contribute to endocrine resistance. This study provides entirely new information that constitutes a major advance in our understanding of the events by which ER and its cofactors mediate changes in DNA methylation and chromatin states at enhancers. These findings should open new avenues for studying role of the deregulated estrogen signalling in the mechanism underlying the “roots” of endocrine resistance that commonly develops in response to anti-estrogen therapy

Récepteur aux oestrogènes

Méthylation de l'ADN

H3K27ac

Éléments amplificateurs

Cancer du sein

Complexe AP-1

Estrogen Receptor

DNA methylation

H3k27ac

Enhancers

Breast cancer

AP-1 complex

570

Optimalios gelio su kaštonų sėklų ekstraktu sudėties paieška, technologija ir vertinimas / The search of optimal composition of gel with chestnut seeds extract, its technology and evaluation

Zubrickaitė, Rasa

28 June 2011

Lėtinis venų nepakankamumas (LVN) apibūdinamas kaip būklė, apimanti galūnių venas, sukeldama veninę hipertenziją, kuri savo ruožtu sąlygoja kitų patologijų – skausmo, tinimo, edemos, odos pokyčių ir opų, atsiradimą. Paprastojo kaštono sėklų ekstrakto saponinai yra viena iš keturių venas veikiančių grupių, kuri buvo įvertinta LVN gydyme, nes lengvina simptomus ir apsaugo venas nuo antrinių komplikacijų vystymosi bei ligos progreso. Šis tyrimas apima: 1) polifenolinių junginių skvarbos in vitro pro pusiau laidžią membraną iš dvidešimties skirtingų gelių su kaštonų sėklų ekstraktu, 1 proc. polimerinio pagrindo (Carbopol Ultrez 10, Carbopol Ultrez 20, Carbopol 980 ir Carbopol 940), propilenglikoliu, izopropilo alkoholiu, trietanolaminu analizę; 2) visų gelių klampos ir jos įtakos polifenolinių junginių skvarbai in vitro vertinimą. Rezultatai: Geliai be eterinio aliejaus buvo naudojami kaip standartiniai pavyzdžiai, vertinant skirtingų karbomerinių pagrindų įtaką skvarbai in vitro. Carbopol Ultrez 20 polimero geliai pasižymėjo mažiausia, o Carbopol 980 – didžiausia dinamine klampa. Didinant eterinio aliejaus koncentraciją, gelių klampa mažėja, o skirtumai tarp 0 proc. ir 1,5 proc. eterinio aliejaus buvo statistiškai patikimi (p<0,05). Polifenolinių junginių kiekis, prasiskverbęs iš gelių, tam tikrais laiko tarpais buvo nustatomas spektrofotometriniu metodu. Nustatyta, kad gelio su Carbopol Ultrez 20 polimeru (0 proc. eterinio aliejaus) srautas per pirmąjį pusvalandį (1,655 mg/cm... [toliau žr. visą tekstą] / Chronic venous insufficiency (CVI) describes a condition that affects the venous system of the lower extremities with venous hypertension causing various pathologies including pain, swelling, edema, skin changes, and ulcerations. Saponosides from horse chestnut extract are one of four groups of venoactive drugs, that have been evaluated in the treatment of CVI to reduce symptoms and help prevent the development of secondary complications and the progression of disease. This study assessed the following: (1) the permeability in vitro through cellulose membranes of polyphenolic compounds in twenty different horse chestnut seed extract (0,5% w/w) gel formulations (Ultrez 10, Ultrez 20, Carbopol 980 and Carbopol 940 gels (1%) with different peppermint oil concentrations (0; 0,1; 0,5; 1; 1,5%), propylenglycol, isopropyl alcohol, TEA, water); (2) the viscosity of all gels and its influence for in vitro permeation. Results: As the base-gels to investigate the effect of the in vitro penetration from different carbomers was formultions without peppermint oil. Gels with Ultrez 20 had the lowest and with Carbopol 980 the highest viscosity. By increasing concentration of peppermint oil, viscosity decreased and the difference between 0% and 1,5% in all carbomers was statistically significant (p<0,05). The quantity of the released polyphenols in time function was determined by spectrophotometric method. Ultrez 20 gel (0% peppermint oil) showed the highest flux during the first half hour (... [to full text]

Pharmacy

Hidrogeliai

Kaštonų sėklų ekstraktas

Skvarbos stiprikliai

Carbopol Ultrez 20

Carbopol 940

Hydrogels

Horse chestnut seeds extract

Permeation enhancers

Carbopol Ultrez 20

Carbopol 940

Διαδερμική χορήγηση φαρμάκων : I) Σύγκριση διαφόρων τύπων ελαστικών λιποσωμάτων και μελέτη μηχανισμού αύξησης διαπερατότητας υδατοδιαλυτών φαρμάκων με τη χρήση τους. ΙΙ) Αύξηση διαπερατότητας αντιϋπερτασικών φαρμάκων με συστήματα ενισχυτών διαπέρασης

Ντυμένου, Βασιλική

15 October 2012

Στην παρούσα διατριβή, μελετήθηκε η χρήση ελαστικών λιποσωμάτων στη διαδερμική χορήγηση υδατοδιαλυτών ουσιών και πραγματοποιήθηκαν επίσης μελέτες προ-μορφοποίησης αντιϋπερτασικών βιοδραστικών ενώσεων για διαδερμική χορήγηση. Αρχικά, πραγματοποιήθηκαν μελέτες της φυσιολογίας του δέρματος με τεχνικές μικροσκοπίας και μέτρησης της απώλειας ύδατος μέσω της επιδερμίδας (TEWL) με σκοπό να διαπιστωθεί η λειτουργία του φραγμού της κεράτινης στοιβάδας, καθώς και η ορθότητα χρήσης των σχετικών τεχνικών προετοιμασίας των δειγμάτων δέρματος που χρησιμοποιήθηκαν. Η οπτική μικροσκοπία ειδικά μας έδωσε πληροφορίες ως προς τη δομή της επιδερμίδας και ως προς τον πιθανό μηχανισμό μεταφοράς ουσιών μέσω της χρήσης λιποσωμάτων. Στη συνέχεια πραγματοποιήθηκε μελέτη και σύγκριση των διαφόρων φυσικοχημικών χαρακτηριστικών ελαστικών λιποσωμάτων που μπορεί να χρησιμοποιηθούν ως πρώτοι δείκτες για πρόγνωση της διαδερμικής απορρόφησης (in vivo) των υδρόφιλων βιοδραστικών ενώσεων. Ως μοντέλα υδρόφιλων βιοδραστικών ενώσεων χρησιμοποιήθηκαν οι φθορίζουσες χρωστικές καλσεΐνη και καρβοξυφλουορεσκεΐνη. Όλες οι λιποσωμικές διασπορές (τόσο τα συμβατικά λιποσώματα-CLs, όσο και τα ελαστικά λιποσώματα τύπου transfersome-TRs και τύπου invasomes-INVs) χαρακτηρίστηκαν ως προς τα εξής φυσικοχημικά χαρακτηριστικά: Την κατανομή μεγέθους, το ζ-δυναμικό, το σφαιρικό σχήμα και τη μορφολογία τους, την ικανότητα εγκλωβισμού υδρόφιλων ουσιών, τη σταθερότητά τους (ως προς τα μορφολογικά χαρακτηριστικά, τη διασπορά μεγέθους και το φορτίο επιφανείας, και τη συγκράτηση της εγκλωβισμένης σε αυτά ουσίας) σε σχέση με το χρόνο, την ελαστικότητα και τέλος ως προς τη δυνατότητα διαπέρασης εγκλωβισμένων σε αυτές υδρόφιλων ουσιών μέσω ανθρώπινου δέρματος in vitro. Το μέγεθος των λιποσωμάτων ήταν παρόμοιο και αρκετά ομοιογενές, ενώ η προσθήκη διαφορετικών τύπων ενισχυτικών διαπέρασης στα ελαστικά λιποσώματα, στα συνήθη εύρη συγκεντρώσεων που χρησιμοποιούνται, δεν επηρεάζει καθόλου το επιφανειακό φορτίο των παραχθέντων λιποσωμάτων. Αύξηση του μεγέθους και αστάθεια ως προς τη συγκράτηση της εγκλωβισμένης ουσίας παρατηρήθηκε στην περίπτωση προσθήκης μεγαλύτερης ποσότητας ενισχυτικού διαπέρασης, η οποία αλλάζει και τα φυσικοχημικά χαρακτηριστικά των λιποσωμάτων. Τα TRs που περιείχαν χολικό νάτριο ήταν πιο ελαστικά από τα αντίστοιχα με Tween 80, τα οποία είχαν συγκριτικά χαμηλές τιμές ελαστικότητας (<40mg/s∙cm2). Οι υψηλότερες τιμές ελαστικότητας από όλους τους τύπους ελαστικών λιποσωμάτων που παρασκευάστηκαν στα πλαίσια αυτής της διατριβής, παρατηρήθηκε στην περίπτωση των INVs με 1% w/w PE και 1% w/w LIM. Επιπλέον, τα περισσότερα λιποσώματα τύπου INVs είχαν υψηλότερες τιμές ελαστικότητας σε σχέση με τα αντίστοιχα χωρίς τερπένια (INVs αναφοράς), εκτός από την περίπτωση των INVs με citral και cineol, όπου η ελαστικότητα σημείωσε μείωση σε σχέση με τα INVs χωρίς τερπένια. Οι διάφοροι τύποι λιποσωμάτων φαίνεται να μεταβάλλουν τη διαπέραση της χρωστικής με την εξής σειρά: Διάλυμα<CLs<TRs<<INVs. H διαπερατότητα (permeability), η ροή (flux) και ο λόγος προσαύξησης (ER) δείχνουν ότι τα συμβατικά λιποσώματα αύξησαν ελάχιστα τη ροή της καλσεΐνης, ενώ τα TRs και INVs κατά 1.8 και 7.2 φορές, αντίστοιχα. Τα αποτελέσματα αυτά επιβεβαιώνουν το γεγονός ότι τα συμβατικά λιποσώματα είναι ανεπαρκή συστήματα μεταφοράς υδρόφιλων μορίων μέσω του δέρματος, ενώ παράλληλα δείχνουν ότι τα ελαστικά λιποσώματα με τη μεγαλύτερη τιμή ελαστικότητας είναι πιο αποτελεσματικά στη μεταφορά της ουσίας μέσω του δέρματος. Σε επόμενα πειράματα μελετήθηκε η δυνατότητα διείσδυσης τόσο υδρόφιλων όσο και λιπόφιλων μορίων στις στοιβάδες του δέρματος, σε μια προσπάθεια να διερευνηθεί ο μηχανισμός αύξησης της διαδερμικής διαπέρασης των υδρόφιλων χρωστικών από τους διάφορους τύπους ελαστικών λιποσωμάτων. Ως μοντέλο υδρόφιλης ουσίας χρησιμοποιήθηκε η φθορίζουσα χρωστική καλσεΐνη, ενώ η λιπιδική ροδαμίνη χρησιμοποιήθηκε ως μοντέλο λιπόφιλης ουσίας (που δεν φεύγει από τα λιποσώματα και ουσιαστικά μας δείχνει το βάθος εις το οποίο εισχωρούν μέσα στο δέρμα τα αντίστοιχα είδη λιποσωμάτων). Τα λιποσώματα τύπου TR φαίνεται ότι επάγουν τη διαπέραση με το να βοηθούν τη χρωστική να προχωρά (υπό μορφή λιποσωμάτων που την εγκλωβίζουν) σε βαθύτερα στρώματα της κεράτινης στιβάδας σε σχέση με τα συμβατικά λιποσώματα όπου σε μεγάλο ποσοστό διαρρηγνύονται και απελευθερώνουν την υδρόφιλη ουσία η οποία στη συνέχεια διέρχεται μόνη της, ως ελεύθερο μόριο, στις στιβάδες του χορίου. Αντίθετα, τα λιποσώματα τύπου INV αποδείχτηκε ότι εισδύουν σε βαθύτερες στιβάδες της επιδερμίδας, φθάνοντας σε αρκετά υψηλά ποσοστά σε στιβάδες του χορίου, παρασύροντας μαζί τους και τα μόρια του εγκλωβισμένου σε αυτά υδρόφιλου φαρμάκου. Τέλος, μελετήθηκε η δυνατότητα μορφοποίησης ενός πειραματικού φαρμάκου με ανάλογη δομή γνωστού φαρμάκου προκειμένου για διαδερμική αντιϋπερτασική θεραπεία. Αρχικά, μελετήσαμε το πειραματικό φάρμακο ως προς τις φυσικοχημικές του ιδιότητες (διαλυτότητα σε διάφορα μέσα, σύνδεση με πρωτεΐνες) και στη συνέχεια μελετήσαμε τη δυνατότητα χορήγησης μιας φαρμακοτεχνικής μορφής μέσω του δέρματος σε κατάλληλο σύστημα διαλυτών. Αφού βρέθηκαν οι κατάλληλες συνθήκες, χρησιμοποιήθηκαν ενισχυτικά διαπέρασης στη φαρμακοτεχνική μορφή για να επιταχυνθεί η διαδερμική απορρόφηση του φαρμάκου, όσο είναι δυνατόν, και να ευρεθεί η βέλτιστη φαρμακοτεχνική μορφή. Τέλος, πραγματοποιήθηκαν πειράματα σύγκρισης μεταξύ του πειραματικού φαρμάκου και γνωστού αντιϋπερτασικού (Los) ως προς τις φυσικοχημικές ιδιότητες και την ικανότητα μεταφοράς τους διαδερμικά. Τα αποτελέσματα έδειξαν ότι το ΠΦ παρουσίασε μεγαλύτερη διαπέραση υπό μορφή ουδέτερου μορίου (σε σχέση με την αντίστοιχη του άλατος με TFA (όπως φάνηκε από τα αρχικά πειράματα αυτής της σειράς) ή του μετά Καλίου άλατος (όπως προκύπτει μετά από σύγκριση των σχετικών τιμών Ροής και Συντελεστή Διαπερατότητας (P). Συγκρίνοντας λοιπόν τις τιμές διαπερατότητα και ροής διαμέσου ανθρώπινης επιδερμίδας με τις αντίστοιχες τιμές του φαρμάκου Los θα πρέπει να λάβουμε υπ’ όψη και τις τιμές για το ουδέτερο μόριο. Η διαπέραση του ουδέτερου μορίου του ΠΦ είναι σημαντικά χαμηλότερη από την αντίστοιχη του μετά καλίου άλατος της los. / In this study, we investigated the use of elastic liposomes in transdermal delivery of hydrophilic substances and we studied the possibility of formulating a new antihypertensive drug for transdermal delivery. Primarily, morphological studies of human skin were conducted by the use of optical microscopy and transepidermal water loss measurements (TEWL), in order to assess the barrier function of stratum corneum (SC), and the integrity of the techniques used in this study. By optical microscopy, in particular, data concerning the skin structure and the possible mechanism by which substances can be delivered through / into the skin, were obtained. Secondly, we studied and compared various physicochemical characteristics of two different types of elastic liposomes, which could help us predict the transdermal absorption (in vivo) of hydrophilic molecules. Fluorescent markers calcein and carboxyfluorescein were used as hydrophilic model drugs. All liposomal dispersions (conventional liposomes CLs, and elastic liposomes i.e. transfersomes TRs and invasomes INVs) were evaluated in means the following physicochemical properties: size distribution, z-potential, stability upon storage, morphology by cryo-electron microscopy and membrane elasticity. Moreover, their ability to encapsulate and also to retain aqueous soluble markers, was investigated. Finally, the permeation of calcein through human skin was tested and compared by use of elastic and conventional rigid liposomes. The mean diameter was found relatively homogenous, similar for most liposomal dispersions, while the addition of different penetration enhancers during the preparation did not influence z-potential. Increase of size average and instability – as far as the retention of the encapsulated substance is concerned – was observed at higher concentrations of penetration enhancers used. Sodium cholate containing TRs were found more elastic compared to Tween 80 containing TRs, which showed relatively low elasticity values (<40mg/s∙cm2). The highest elasticity values among all types of elastic liposomes prepared, were found in the case of INVs with 1%w/w PE and 1% w/w LIM. Furthermore, most INVs showed higher elasticity values compared to the ones without terpenes (control INVs), except from citral and cineol INVs, where elasticity decreased compared to the control ones. It appears that different types of liposomes can alter fluorescent permeation in the following order: Solution<CLs<TRs<<INVs. Permeability, flux and enhancement ratio (ER) show that conventional liposomes increased slightly calcein flux, while TRs and INVs 1.8 and 7.2 times respectively. These findings confirm the fact that CLs are inefficient drug delivery systems for water soluble molecules through human skin, and show that elastic liposomes having the highest elasticity value are more efficient in delivering CF transdermally. In further experiments, the penetration of both hydrophilic and lipophilic molecules in human skin was studied, in order to investigate the mechanism of action by which liposomes could enhance the drug delivery in skin. Fluorescent marker calcein was used as a hydrophilic drug model, while lipid rhodamine-PE was used as a lipophilic model (it shows us how deeply the liposomes penetrate into the skin). Liposomes TRs seem to enhance skin permeation by helping the marker to penetrate (through liposomes) in deeper stratum corneum layers while conventional liposomes the hydrophilic substance which penetrates the skin layers as a free molecule. In contrast, INV liposomes were proved to be able to penetrate in deeper skin layers, and deliver relatively high amounts of the encapsulated substance. In the end, experiments with a new molecule with similar structure to losartan were conducted. This study aimed at discovering a new formulation for this experimental drug in order to be used as a transdermal antihypertensive. First, we studied the physicochemical properties (solubility in PBS, BSA etc, and protein binding). Secondly, we investigated the possibility of preparing a formulation to be used transdermally. After establishing the techniques and drug properties we used penetration enhancers in order to increase the transdermal absorption as possible and help find the right skin formulation. Last, we compared the experimental drug and losartan in terms of physicochemical properties and their ability to be transported through human skin. The results showed that the experimental drug had better permeation rate as a neutral molecule compared to TFA salt, (as shown in preliminary experiments) or K+ (as shown after comparing P and flux values). Therefore, the values given for the neutral molecule should be taken into consideration when comparing the two drugs. (losartan and experimental drug). The permeation of the neutral molecule nevertheless is significantly lower than the one for losartan.

Λιποσώματα

Διαδερμική χορήγηση

Χολικό νάτριο

Τερπένια

Ελαστικά λιποσώματα

615.6

Liposomes

Transdermal/dermal delivery

Sodium cholate

Terpenes

Elastic liposomes

Penetration enhancers

Transfersomes

Invasomes

Avaliação dos óleos essenciais de plantas nativas da Mata Atlântica como promotores de permeação cutânea / Evaluation of essential oils of plants native to the Atlantic Forest as skin permeation enhancers

Aurea Cristina Lemos Lacerda

09 October 2014

Os óleos essenciais da Pimenta pseudocaryophyllus (Gomes) Landrum de planta de populações naturais de três ecossistemas, localizados na Ilha de Cananéia, região de restinga, no Morro da Cataia, cidade de Cajati, região de encosta, ambas em área de Mata Atlântica, e na Reserva Natural Morro Grande, cidade de Caldas, região de campos montanos, foram avaliados como promotores de permeação cutânea do diclofenaco de potássio. Os óleos essenciais foram extraídos de partes aéreas das plantas e o rendimento do processo foi entre 0,90% (p/p) e 2,7% (p/p). A análise da composição química mostrou diferenças, indicando tratar-se de três quimiotipos diferentes. A interação dos óleos essenciais e dos componentes majoritários com membrana biológica natural foi avaliada por FT-Raman e ATR- FTIR, indicando a interação com as porções lipídicas do tecido. Foram desenvolvidas seis membranas biológicas artificiais, compostas por ceramidas, ácidos graxos e colesterol em proporções equimolares, que foram caracterizadas por espectroscopia Raman confocal e foram consideradas semelhantes. As membranas foram utilizadas no desenvolvimento do sistema PAMPA (Parallel Artificial Membrane Permeability Assay) para avaliar a segurança e eficácia dos óleos essenciais e componentes majoritário como promotores de permeação do diclofenaco de potássio. Os resultados dos ensaios com o sistema PAMPA foram estatisticamente avaliados. A segurança foi avaliada com o critério de permeação mínima dos óleos através das membranas do sistema PAMPA, verificada pela absorbância mínima do eugenol na solução aceptora. Os óleos essenciais e componentes majoritários foram utilizados no pré-tratamento das membranas, nas concentrações de 0,125%, 0,25%, 0,50% e 2,00% (v/v) em etano!. Ensaios de permeação do diclofenaco de potássio no sistema PAMPA indicaram efeito de promoção da permeação para todos os compostos avaliados. O método de doseamento do fármaco por UV foi validado e utilizado para os ensaios de permeação de formulações de gel em base aquosa contendo o diclofenaco de potássio (1,0% p/p). As amostras de gel foram preparadas com o óleo procedente de Morro Grande, selecionado na etapa de avaliação de segurança, a 0,125% (p/v). Adicionalmente, foram preparadas formulações com citronelol e etanol, na mesma concentração. O óleo essencial da Reserva Natural Morro Grande teve efeito de promoção da permeação superior ao do citronelol e etanol, que foram equivalentes. / The essential oils of the species Pimenta pseudocaryophyllus (Gomes) Landrum collected from natural populations of three existing ecosystems in the Cananéia Island, located at sea level, Cajati city, located in hillside region, both in the Atlantic Forest areas, as well as species collected in the Morro Grande Natural Reserve, region of montane fields, were evaluated as skin permeation enhancers of potassium diclofenac. Essential oils were extracted from the aerial parts of the plants and the process yield was between of 0.90% (w/w) and 2.7% (w/w). The chemical composition analysis showed differences between the plants of three origins, indicating that they are different chemotypes. The interaction of the essential oils and their major components with natural biological membrane was evaluated by FT- Raman and ATR-FTIR, indicating interaction with the Iipid portions of the natural membrane. Six artificial biological membranes have been developed, consisting of ceramides, cholesterol and fatty acids in equimolar proportions, which were characterized by confocal Raman spectroscopy and found to be similar. The membranes were used in developing the PAMPA (Parallel Artificial Membrane Permeability Assay) system to evaluate the safety of the potential permeation enhancers. The test results with PAMPA system were statistically evaluated. Safety was evaluated with the criterion of minimum permeation of the essential oil through the membranes, checked by the minimum absorbance of eugenol in the acceptor solution. The essential oils and the major components were used in the pretreatment of the membranes, at concentrations of 0.125%, 0.25%, 0.50% and 2.00% (v/v) in ethanol. Results indicated permeation enhancement effect for ali compounds evaluated. The analytical method for the quantification of potassium diclofenac was validated and used for the evaluation of the permeation of aqueous based gel formulations containing potassium diclofenac (1.0% w/w). The gel samples were prepared with the oil from Morro Grande Natural Reserve, selected in the safety evaluation step, at 0.125% (w/v). In addition, formulations were prepared with citronellol and ethanol at the same concentration. The essential Gil of Morro Grande Natural Reserve was more efficient as permeation enhancer than citronellol and ethanol under the test conditions.

Diclofenaco de potássio

Métodos biofísicos

Óleos essenciais

PAMPA

Pimenta pseudocaryophyllus

Promotores de permeação

Biophysical methods

Diclofenac potassium

Oil essential

PAMPA

Pepper pseudocaryophyllus

Permeation enhancers