Mixture Design Response Surface Methodology Analysis of Seven Natural Bioactive Compounds to Treat Prostate Cancer

Berlin, Ian Geddes

15 December 2021

Natural bioactive compounds have drawn the interest of many researchers worldwide in their effort to find novel treatments, including prostate cancer (PC) treatment which is estimated to be 13.1% of all new cancer cases in the U.S. in 2021. Many of these bioactive compounds have been identified from treatments in traditional Chinese medicine (TCM), that often have multiple bioactive compounds present. However, in vitro studies frequently focus on the compounds in isolation, or in simple combinations of two compounds. We used mixture design response surface methodology (MDRSM) to assess changes in PC cell viability after 48 hours of treatment to identify the optimal mixture of all 35 three-compound combinations of seven bioactive compounds from TCM. We used Berberine, Wogonin, Shikonin, Curcumin, Triptolide, Emodin, and Silybin to treat PC-3, DU145, and LNCaP human PC cells, and a drug-resistant PC-3 cell line. Berberine and Wogonin most frequently contributed to the optimal combination to reduce cell viability in PC-3 and LNCaP cells; DU145 cells more frequently responded best to a single compound.

prostate cancer

berberine

wogonin

shikonin

curcumin

triptolide

emodin

silybin

traditional Chinese medicine (TCM)

Life Sciences

Increasing the Oral Bioaccessibility of Curcumin Using Oleogels Structured by Rice Bran Wax

Hallinan, Robert Michael

January 2020

No description available.

Food Science

Nutrition

food science

lipids

curcumin

bioavailability

bioaccessibility

delivery system

food

oleogel

oil

physical properties

curcuminoids

rice bran wax

in vitro

absorption

gel

edible

food technology

functional food

Co-crystal screening of poorly water-soluble active pharmaceutical ingredients. Application of hot stage microscopy on curcumin-nicotinamide system and construction of ternary phase diagram of fenbufen-nicotinamide-water co-crystal system.

Chan, Hin Chung Stephen

January 2009

Curcumin is the major phenolic diarylheptane derivative in Curcuma longa and has been reported to possess pharmacological activities. Unfortunately this compound suffers from poor bioavailability and rapid neutral-alkaline degradation. Co-crystal of curcumin is one option under exploration, motivated by the fact that a number of active pharmaceutical ingredient (API) co-crystals with improved dissolution have recently been synthesized. Hence, co-crystallization technique highlights an alternative means to improve the performance of curcumin. Within our work evidences for a co-crystal was ascertained from DSC, Kofler hot stage screening and PXRD, and all confirmed a new crystal phase could have been formed between curcumin and a co-crystallizing agent, nicotinamide. We report that re-crystallization step essentially aids the purification of commercial curcumin, a herbal based actives. Otherwise the prevalence of a new crystal phase in solvent-mediated co-crystallization will be significantly reduced. Besides, phase diagram is an effective tool for the study of solubility behaviours in co-crystal system. In order to acquire related techniques, fenbufen, a poorly water soluble drug, was selected. The result showed the huge difference in solubility between fenbufen and nicotinamide lead to difficulty in the construction of phase diagram.

Curcumin

Co-crystal

Nicotinamide

Fenbufen

X-ray powder diffractometry

Kofler hot stage microscopy

Ternary phase diagram

Differential scanning calorimetry

Thermal gravimetric analysis

Nanostructure des particules polymériques : aspects physiques, chimiques et biologiques

Rabanel, Jean-Michel

04 1900

Les nanotechnologies appliquées aux sciences pharmaceutiques ont pour but d’améliorer l’administration de molécules actives par l’intermédiaire de transporteurs nanométriques. Parmi les différents types de véhicules proposés pour atteindre ce but, on retrouve les nanoparticules polymériques (NP) constituées de copolymères “en bloc”. Ces copolymères permettent à la fois l’encapsulation de molécules actives et confèrent à la particule certaines propriétés de surface (dont l’hydrophilicité) nécessaires à ses interactions avec les milieux biologiques. L’architecture retenue pour ces copolymères est une structure constituée le plus fréquemment de blocs hydrophiles de poly(éthylène glycol) (PEG) associés de façon linéaire à des blocs hydrophobes de type polyesters. Le PEG est le polymère de choix pour conférer une couronne hydrophile aux NPs et son l’efficacité est directement liée à son organisation et sa densité de surface. Néanmoins, malgré les succès limités en clinique de ces copolymères linéaires, peu de travaux se sont attardés à explorer les effets sur la structure des NPs d’architectures alternatives, tels que les copolymères en peigne ou en brosse. Durant ce travail, plusieurs stratégies ont été mises au point pour la synthèse de copolymères en peigne, possédant un squelette polymérique polyesters-co-éther et des chaines de PEG liées sur les groupes pendants disponibles (groupement hydroxyle ou alcyne). Dans la première partie de ce travail, des réactions d’estérification par acylation et de couplage sur des groupes pendants alcool ont permis le greffage de chaîne de PEG. Cette méthode génère des copolymères en peigne (PEG-g-PLA) possédant de 5 à 50% en poids de PEG, en faisant varier le nombre de chaînes branchées sur un squelette de poly(lactique) (PLA). Les propriétés structurales des NPs produites ont été étudiées par DLS, mesure de charge et MET. Une transition critique se situant autour de 15% de PEG (poids/poids) est observée avec un changement de morphologie, d’une particule solide à une particule molle (“nanoagrégat polymére”). La méthode de greffage ainsi que l’addition probable de chaine de PEG en bout de chaîne principale semblent également avoir un rôle dans les changements observés. L’organisation des chaînes de PEG-g-PLA à la surface a été étudiée par RMN et XPS, méthodes permettant de quantifier la densité de surface en chaînes de PEG. Ainsi deux propriétés clés que sont la résistance à l’agrégation en conditions saline ainsi que la résistance à la liaison aux protéines (étudiée par isothermes d’adsorption et microcalorimétrie) ont été reliées à la densité de surface de PEG et à l’architecture des polymères. Dans une seconde partie de ce travail, le greffage des chaînes de PEG a été réalisé de façon directe par cyclo-adition catalysée par le cuivre de mPEG-N3 sur les groupes pendants alcyne. Cette nouvelle stratégie a été pensée dans le but de comprendre la contribution possible des chaines de PEG greffées à l’extrémité de la chaine de PLA. Cette librairie de PEG-g-PLA, en plus d’être composée de PEG-g-PLA avec différentes densités de greffage, comporte des PEG-g-PLA avec des PEG de différent poids moléculaire (750, 2000 et 5000). Les chaines de PEG sont seulement greffées sur les groupes pendants. Les NPs ont été produites par différentes méthodes de nanoprécipitation, incluant la nanoprécipitation « flash » et une méthode en microfluidique. Plusieurs variables de formulation telles que la concentration du polymère et la vitesse de mélange ont été étudiées afin d’observer leur effet sur les caractéristiques structurales et de surface des NPs. Les tailles et les potentiels de charges sont peu affectés par le contenu en PEG (% poids/poids) et la longueur des chaînes de PEG. Les images de MET montrent des objets sphériques solides et l'on n’observe pas d’objets de type agrégat polymériques, malgré des contenus en PEG comparable à la première bibliothèque de polymère. Une explication possible est l’absence sur ces copolymères en peigne de chaine de PEG greffée en bout de la chaîne principale. Comme attendu, les tailles diminuent avec la concentration du polymère dans la phase organique et avec la diminution du temps de mélange des deux phases, pour les différentes méthodes de préparation. Finalement, la densité de surface des chaînes de PEG a été quantifiée par RMN du proton et XPS et ne dépendent pas de la méthode de préparation. Dans la troisième partie de ce travail, nous avons étudié le rôle de l’architecture du polymère sur les propriétés d’encapsulation et de libération de la curcumine. La curcumine a été choisie comme modèle dans le but de développer une plateforme de livraison de molécules actives pour traiter les maladies du système nerveux central impliquant le stress oxydatif. Les NPs chargées en curcumine, montrent la même transition de taille et de morphologie lorsque le contenu en PEG dépasse 15% (poids/poids). Le taux de chargement en molécule active, l’efficacité de changement et les cinétiques de libérations ainsi que les coefficients de diffusion de la curcumine montrent une dépendance à l’architecture des polymères. Les NPs ne présentent pas de toxicité et n’induisent pas de stress oxydatif lorsque testés in vitro sur une lignée cellulaire neuronale. En revanche, les NPs chargées en curcumine préviennent le stress oxydatif induit dans ces cellules neuronales. La magnitude de cet effet est reliée à l’architecture du polymère et à l’organisation de la NP. En résumé, ce travail a permis de mettre en évidence quelques propriétés intéressantes des copolymères en peigne et la relation intime entre l’architecture des polymères et les propriétés physico-chimiques des NPs. De plus les résultats obtenus permettent de proposer de nouvelles approches pour le design des nanotransporteurs polymériques de molécules actives. / The goal set to nanotechnologies applied to pharmaceutical sciences is to improve drug delivery and benefits with the help of nanometer-sized vehicles. At this time different types of drug carriers had been proposed. Amongst them, block copolymer nanoparticles (NP) have been designed to allow, at the same time, efficient drug encapsulation and provide surface properties (hydrophilic layer) to the NP which are necessary for its interactions with biological systems by preventing the opsonisation and the subsequent recognition by the mononuclear macrophage system (MPS) and the rapid elimination of the drug carrier. The most prominent polymer architecture in drug delivery application is the linear di-block copolymer architecture, such as poly(ethylene glycol) blocks (PEG) linked to a polyester hydrophobic chain. PEG is the gold standard to add a hydrophilic corona to drug carrier’s surface, but its efficacy is directly linked to its surface organization and surface densities. In spite of limited success of diblock at the clinical stage, few studies have been devoted to other type of architecture such as comb-like copolymers, either for the exploration of new synthesis routes or for the characterization of particles prepared from alternative architecture polymers. We attempted in preamble of this work to define more closely the conceptual and technical framework allowing quantitative determination of PEG surface densities. This review work has been used in the experimental work to define the characterization methods. Several synthesis strategies have been developed for the preparation of comb copolymers in this work. All strategies are based on random copolymerization of dilactide with small epoxy molecules with a pendant group suitable for subsequent PEG grafting, yielding a polyester-co-ether backbone. In a second step, PEG chains have been grafted on available pendant groups (alcohol groups or alkyne) to produce the final comb copolymers. In the first part of the experimental work, esterification reaction by acylation and coupling (the Steglish reaction) allowed the preparation of a first comb-like copolymer library with PEG content varying from 5 to 50 % (w/w). The number of PEG chains (PEG grafting density) was varying while the lengths of the PEG chains and the hydrophobic PLA backbone were kept constant. The library of comb-like polymers was used to prepare nanocarriers with dense PEG brushes at their surface, stability in suspension, and resistance to protein adsorption. The structural properties of nanoparticles (NPs) produced from these polymers by a surfactant-free method were assessed by DLS, zeta potential, and TEM and were found to be controlled by the amount of PEG present in the polymers. A critical transition from a solid NP structure to a soft particle with either a “micelle-like” or “polymer nano-aggregate” structure was observed when the PEG content was between 15 to 25% w/w. This structural transition was found to have a profound impact on the size of the NPs, their surface charge, their stability in suspension in presence of salts as well as on the binding of proteins to the surface of the NPs. The arrangement of the PEG-g-PLA chains at the surface of the NPs was investigated by 1H NMR and X-ray photoelectron spectroscopy (XPS). NMR results confirmed that the PEG chains were mostly segregated at the NP surface. Moreover, XPS and NMR allowed the quantification of the PEG chain coverage density at the surface of the solid NPs. Concordance of the results between the two methods was found to be remarkable. Physical-chemical properties of the NPs such as resistance to aggregation in saline environment as well as anti-fouling efficacy, assessed by isothermal titration calorimetry (ITC), were related to the PEG surface density and ultimately to polymer architecture. In the second part of this work, grafting of PEG chains on a polyester-co-ether backbone was directly performed using cyclo-addition of PEG azide on pendant alkyne groups. The new strategy was designed to understand the contribution of PEG chains grafted on PLA backbone ends. The new polymer library was composed of PEG-g-PLA with different PEG grafting densities and PEG molecular weights (750, 2000 and 5000 D). PEG chain grafting could only take place on pendant groups with this approach. NPs were produced by different methods of nanoprecipitation, including “flash nanoprecipitation” and microfluidic technology. Some formulation variables such as polymer concentration and speed of mixing were studied in order to observe their effects on NP surface characteristics. Unlike for the first copolymer library, here the NPs size and zeta potential were found to not be much affected by the PEG content (% w/w in polymer). Sizes were also not affected by the PEG chains length. TEM images show round shaped object and as expected sizes were found to decrease with polymer concentration in the organic phase and with a decrease in mixing time of the two phases (for flash nanoprecipitation and microfluidic technology). PEG chain surface densities were assessed by quantitative 1H NMR and XPS. In the third experimental part, we explored the role of polymer architecture on drug encapsulation and release of curcumin from NPs. Curcumin has been chosen as a model with a view to develop a delivery platform to treat diseases involving oxidative stress affecting the CNS. As previously observed with blank NPs, a sharp decrease in curcumin-loaded NP size and morphology change occurred between 15 to 20 % w/w of PEG. Drug loading, Drug loading efficiency and the diffusion coefficients of curcumin in NPs are showing a dependence over the polymer architecture. NPs did not present any significant toxicity when tested in vitro on a neuronal cell line. Moreover, the ability of NPs carrying curcumin to prevent oxidative stress was evidenced and linked to polymer architecture and NPs organization. In a nutshell, our study showed the intimate relationship between the polymer architecture and the biophysical properties of the resulting NPs and sheds light on new approaches to design efficient NP-based drug carriers. The results obtained lead us to propose PEG-g-PLA comb architecture copolymers for nanomedecine development as an alternative to the predominant polyester-PEG diblock polymers.

Nanoparticules

Nanoparticle

Poly(lactique)

Poly(lactic)

Poly(éthylène glycol)

Poly(ethylene glycol)

XPS

RMN

NMR

Micelle-like

Microcalorimétrie

Chimie clic

Click chemsitry

Curcumin

Curcumine

Microcalorimetry

Nano-agrégat polymère

Caracterização química e atividade biológica de extratos etanólicos de Curcuma longa e Bixa orellana /

Guedes, Juliana Campos Diniz

January 2019

Orientador: Elisa Helena Giglio Ponsano / Resumo: O objetivo deste estudo foi investigar a composição química e as atividades antimicrobiana e antioxidante dos extratos etanólicos de Curcuma longa e Bixa orellana, na busca por substituintes aos aditivos sintéticos utilizados na indústria de alimentos. Pela espectrometria de massa (GC-MS) foram identificados bisdemetoxicurcumina, demetoxicurcumina e curcumina no extrato de C. longa e prunina e naringenina no extrato de B. orellana. C. longa apresentou atividade antimicrobiana frente a Clostridium sporogenes e Staphylococcus aureus, com concentração bactericida mínima (CBM) de 25 mg/mL e 156 µg/mL, respectivamente. O extrato de B. orellana apresentou CBM de 50 mg/mL para C. sporogenes e 625 µg/mL para S. aureus. Nenhum dos extratos apresentou atividade bactericida para Escherichia coli e Salmonella Typhimurium. A atividade antioxidante dos extratos foi evidenciada pelos métodos Poder Antioxidante por Redução Férrica (FRAP) e Capacidade de Absorção do Radical Oxigênio (ORAC). O extrato de B. orellana apresentou maior atividade antioxidante pelos métodos FRAP e ORAC (277,70 e 455,17 mM trolox equivalente/g, respectivamente) do que o extrato de C. longa (129,74 e 217,98 mM trolox equivalente/g, respectivamente). Os efeitos biológicos dos extratos etanólicos de C. longa e B. orellana revelados no presente estudo apontaram seu potencial para a utilização na indústria de alimentos como uma alternativa aos aditivos sintéticos. / Abstract: The objective of this study was to investigate the chemical composition and the antimicrobial and antioxidant activities of Curcuma longa and Bixa orellana ethanolic extracts, in the search for alternatives to the synthetic additives used in the food industry. Mass spectrometry (GC-MS), identified bisdemethoxycurcumin, demethoxycurcumin and curcumin in the extract of C. longa and prunin and naringenin in the extract of B. orellana. C. long showed antimicrobial activity against Clostridium sporogenes and Staphylococcus aureus, with a minimum bactericidal concentration (MBC) of 25 mg/mL and 156 μg/mL, respectively. MBC of B. orellana extract was 50 mg/mL for C. sporogenes and 625 μg/mL for S. aureus. None of the extracts showed bactericidal activity against Escherichia coli and Salmonella Typhimurium. The antioxidant activity of the extracts was evidenced by the methods Iron Reduction Antioxidant Power (FRAP) and Oxygen Radical Absorption Capacity (ORAC). B. orellana extract had higher antioxidant activity by FRAP and ORAC (277.70 and 455.17 mM trolox equivalent/g, respectively) than C. longa extract (129.74 and 217.98 mM trolox equivalent/g, respectively). The biological effects of C. longa and B. orellana ethanolic extracts revealed in this study indicated their potential as an alternative to synthetic additives used in the food industry. / Mestre

Antibacterianos.

Antioxidantes.

aditivos alimentares

bactérias anaeróbias

bactérias aeróbias

Bactérias gram-negativas.

Bactérias gram-positivas.

espectrometria de massas

Curcumina.

flavononas

antibacterials

antioxidants

food additives

anaerobic bacteria

Bactérias aeróbicas.

gram-negative bacteria

gram-positive bacteria

mass spectrometry

curcumin

flavonones

Tierexperimentelle Behandlungsversuche der Charcot-Marie-Tooth-Erkrankung 1A / Experimental therapy trials of the Carcot-Marie-Tooth Disease 1A in vivo

Weiss, Bernhard G.

03 March 2014

No description available.

610

Carcot-Marie-Tooth Disease 1A

Peripheral myelin protein 22

PMP22

experimental therapy trial

Curcumin

progesterone antagonist

CMT rat

CMT1A

acetylsalicylic acid

erythropoietin

liver x receptor agonist

in vivo

Medizin (PPN619874732)

A curcumina previne os efeitos da exposição à fumaça do cigarro sistema purinérgico, sistema colinérgico e memória / Curcumin prevents against the effects of cigarette smoke exposure purinergic system, cholinergic system and memory

Jaques, Jeandre Augusto dos Santos

09 May 2013

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / Cigarette smoke exposure is a major risk factor to the development of cardiovascular diseases, neurocognitive and neurobiological deficits. Nowadays, phytotherapy is widely employed in the treatment of many illnesses. Curcumin, a polyphenol obtained from the rhizomes of Curcuma longa and commonly used in the oriental culinary and traditional medicine, has several pharmacological properties such as antioxidant, antiaggregant and neuroprotective. Despite its wide-ranging spectrum of pharmacological properties, curcumin possess potential to prevent the noxious effects caused by cigarette smoke exposure. In this context, the purpose of this study was to evaluate the effect of curcumin on memory and parameters involved in the homeostasis of central nervous system (CNS) in rats passively exposed to cigarette smoke. The experiments were performed in two different stages, being the first divided in two sets. In the first set, animals were randomly assigned into four groups: vehicle; curcumin 12.5 mg/kg; curcumin 25 mg/kg; and curcumin 50 mg/kg. In the second set, animals were randomly assigned into five groups: vehicle, cigarette smoke; curcumin 12.5 mg/kg along with cigarette smoke; curcumin 25 mg/kg along with cigarette smoke; and curcumin 50 mg/kg along with cigarette smoke. In the second experimental stage, animals were randomly divided into ten groups: vehicle; curcumin 12.5 mg/kg; curcumin 25 mg/kg; curcumin 50 mg/kg; nanoencapsulated curcumin 4 mg/kg; cigarette smoke; curcumin 12.5 mg/kg along with cigarette smoke; curcumin 25 mg/kg along with cigarette smoke; curcumin 50 mg/kg along with cigarette smoke; and nanoencapsulated curcumin 4 mg/kg along with cigarette smoke. The treatment with curcumin and cigarette smoke was carried out once a day, 5 days each week, during 30 days. Curcumin was administered orally and, approximately 10 minutes later, the smoking groups were exposed to the sidestream smoke of four commercial cigarettes (nicotine 0.9 mg, tar 10 mg each) inside a whole-body smoke exposure chamber. After thirty days, the animals were euthanized, the blood collected and the brain dissected in cerebral cortex, hippocampus, hypothalamus, striatum and cerebellum. The group of rats exposed to cigarette smoke showed an increase in the activity of the enzymes E-NTPDase (ATP as substrate) and E-5 -NT, and a reduction in the activity of the enzyme E-NTPDase (ADP as substrate) in platelets; an increase in the activities of the enzymes E-NTPDase, E-5 -NT and AChE in synaptosomes from the cerebral cortex; an increase in the activity of AChE in cerebellum, cerebral cortex, hippocampus, striatum, hypothalamus and peripheral blood; a decrease in the activities of the enzymes Na+,K+-ATPase and Ca2+-ATPase and a redox imbalance. Furthermore, in the same group of animals, it was observed a cognitive impairment evaluated through the inhibitory avoidance test and the object recognition test. We conclude that the use of both formulations of curcumin, free and nanostructured, prevents the effects observed in the purinergic and cholinergic system, in the enzymes involved in the ion homeostasis and in the oxidative stress parameters. Finally, the results obtained in this study indicate that curcumin administration as lipid-core nanocapsules may be an alternative to increase its efficacy, probably by the increase of its bioavailability when administered orally. / A exposição à fumaça do cigarro é um fator de risco para o desenvolvimento de doenças cardiovasculares, déficits neurocognitivos e neurobiológicos. Atualmente, o emprego de fitoterápicos é uma das alternativas para o tratamento de diversas doenças. A curcumina, um polifenol obtido a partir de rizomas de Curcuma longa e amplamente utilizado na culinária e na medicina tradicional oriental, possui diversas propriedades farmacológicas como antioxidante, anti-agregante e neuroprotetora. Em virtude de seu amplo espectro de propriedades farmacológicas a curcumina possui potencial para a prevenção dos efeitos causados pela exposição à fumaça do cigarro. Neste contexto, o objetivo deste estudo foi avaliar o efeito da curcumina sobre a memória e parâmetros envolvidos na homeostase do sistema nervoso central (SNC) em ratos expostos de forma passiva à fumaça do cigarro. Os experimentos foram realizados em duas etapas, sendo a primeira delas dividida em duas fases. Na primeira fase, os animais foram divididos aleatoreamente em quatro grupos, denominados: veículo; curcumina 12,5 mg/kg; curcumina 25 mg/kg; e curcumina 50 mg/kg. Na segunda fase, os animais foram divididos aleatoreamente em cinco grupos, denominados: veículo; cigarro; cigarro + curcumina 12,5 mg/kg; cigarro + curcumina 25 mg/kg; e cigarro + curcumina 50 mg/kg. Na segunda etapa experimental, os animais foram divididos aleatoreamente em dez grupos, denominados: veículo; curcumina 12,5 mg/kg; curcumina 25 mg/kg; curcumina 50 mg/kg; curcumina nanoencapsulada 4 mg/kg; cigarro; cigarro + curcumina 12,5 mg/kg; cigarro + curcumina 25 mg/kg; cigarro + curcumina 50 mg/kg; cigarro + curcumina nanoencapsulada 4 mg/kg. O tratamento com a curcumina e com a fumaça do cigarro foi realizada uma vez por dia, cinco dias por semana, durante trinta dias. A curcumina foi administrada de forma oral e, após aproximadamente dez minutos, os grupos fumantes eram expostos à fumaça de quatro cigarros comerciais (0,9 mg de nicotina, 10 mg de alcatrão cada) dentro de uma câmara de exposição. Após trinta dias, os animais foram eutanasiados, o sangue coletado e o encéfalo dissecado em córtex cerebral, hipocampo, hipotálamo, estriado e cerebelo. O grupo de ratos expostos à fumaça do cigarro apresentou um aumento na atividade das enzimas E-NTPDase (ATP como substrato) e E-5 -NT, e uma redução na atividade da enzima E-NTPDase (ADP como substrato) em plaquetas; um aumento nas atividades das enzimas E-NTPDase, E-5 -NT e AChE em sinaptossomas de córtex cerebral; um aumento na atividade da enzima AChE em cerebelo, córtex cerebral, hipocampo, estriado, hipotálamo e sangue periférico; uma redução nas atividades das enzimas Na+,K+-ATPase e Ca2+-ATPase e um desequilíbrio no balanço redox. Além disso, neste mesmo grupo de animais observou-se um déficit cognitivo avaliado através dos testes da esquiva inibitória e do reconhecimento de objetos. Concluimos que o uso de ambas as formulações de curcumina livre e nanoestruturada previne os efeitos observados nas atividades das enzimas do sistema purinérgico, colinérgico, nas enzimas envolvidas na formação do gradiente iônico e nos parâmetros de estresse oxidativo. Por fim, os resultados obtidos neste estudo indicam que a administração da curcumina através de nanocápsulas de núcleo lipídico possa ser uma alternativa para o aumento de sua eficácia, provavelmente pelo aumento da biodisponibilidade da curcumina administrada de forma oral.

Curcumina

Curcuma longa

Fumaça do cigarro

Sistema purinérgico

Sistema colinérgico

Memória

Estresse oxidativo

Nanocápsulas

Curcumin

Curcuma longa

Cigarette smoke

Purinergic system

Cholinergic system

Memory

Oxidative stress

Nanocapsules

CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA

Studium nitrobuněčných signálních molekul oxidu uhelnatého a oxidu dusnatého v hepatocytech v souvislosti s hepatotoxickými a hepatoprotektivními účinky vybraných látek / Study on intracellular signal molecules of carbon monoxide and nitric oxide related to hepatotoxic and hepatoprotective effects of selected substances

Černý, Dalibor

January 2012

Background and aims: Treatment of acute fulminant liver damage arising as a result of various origins (ischemia-reperfusion injury, toxic shock, an infectious cause or cholestasis) still remains a major clinical problem. We currently do not have available clinically proven, pharmacologically effective and universal compound for the treatment of acute liver injury. The main aim of my research work was, therefore, to test the potential hepatoprotective effect of selected cytoprotective drugs and try to find out or suggest their mechanism of action, which we have examined in the systems for the intracellular gaseous signaling molecules NO and CO, where the key enzymes for their formation are NOS / HO respectively. My PhD study had two main directions: 1) Experimental study of the relationship between HO / CO and NOS / NO systems in the environment of hepatotoxic substances on isolated primary rat hepatocytes and in rat model, 2) Evaluation of ameliorative effect of selected substances in the hepatotoxicity models and to test the relationship of this effect on changes in some parameters of cytotoxicity / cytoprotection, antioxidant parameters, gene expression of mRNA for selected genes and histological changes in the state of cells / tissues / organs. Methods: We measured urea, bilirubin and liver...

Elaboration des nanocristaux de cellulose fonctionnalisés pour la vectorisation d’agents anticancéreux et pour la transfection de gènes / Development of cellulose nanocrystals for the vectorization of anticancer drugs and for genes transf

Ndong ntoutoume, Gautier mark arthur

14 December 2015

La vectorisation et le ciblage d’agents anticancéreux représentent des axes de recherche majeurs au sein du LCSN. En effet, la plupart des molécules actives utilisées en thérapie anticancéreuse sont peu sélectives des tumeurs et sont toxiques pour les cellules saines. L’élaboration de nanobiomatériaux aptes à cibler spécifiquement les tumeurs par effet EPR mais également capables de les détruire par l’action de la drogue transportée s’avère capital. Le nanovecteur utilisé est élaboré à partir des nanocristaux de cellulose (CNCx) issus de l’hydrolyse acide du coton. Une première approche a consisté à élaborer la nanoplateforme thérapeutique suivant la technique. / Targeting and drug delivery are major areas of research within the LCSN. Indeed, most of the active molecules used in cancer therapy are not very selective against tumors and are toxic to healthy cells. The development of nanobiomaterials able to specifically target tumors by EPR effect but also capable of destroying them by the action of the drug transported turns capital. In this work we achieved the binding of triphenylphosphonium cation (to target the mitochondria), hydrophobic active ingredients and a nucleic acid on cellulose nanocrystals issued from the acid hydrolysis of cotton. The first therapeutic platform synthesized according to the technique.

Cancer

Vectorisation

Curcumine

Piperlogumine

Protoporphyrine IX

SiRNA

Nanoparticules

Nanocristaux de cellulose

Plateformes thérapeutiques

Cyclodextrine

Complexation

Polyéthylèneimine

Cancer

Vectorization

Curcumin

Piperlogumine

Protoporphyrin IX

SiRNA

Nanoparticles

Cellulose nanocrystals

Therapeutics plateforms

Cyclodextrin

Complexation

Polyethyleneimine

616.994 061

Platinum(II) Complexes as Dual Action DNA Crosslinking & Photochemotherapeutic Agents

Mitra, Koushambi

January 2016

The thesis work delineates the rational design and successful syntheses of platinum (II) complexes for achieving light promoted dual action anticancer properties. The research work focuses on the syntheses, elaborate characterization including crystallization and mechanistic aspects of photodegradation processes. Theoretical studies were done to elucidate the properties of the excited states. The interaction of active Pt (II) species with DNA is also explored. The cellular studies include evaluation of the photo-induced cytotoxicities, mode of cell death, nature of reactive oxygen species (ROS), quantification of cellular Pt content and cellular and sub-cellular localization of the complexes. Chapter I provides an overview of the hallmarks of cancer and the current anticancer treatment modalities. It outlines the evolution of platinum based chemotherapeutic drugs, their mechanism of action and associated disadvantages. It also depicts the resurgence of metal complexes as photosensitizers for photoactivated chemotherapy, a selective tripartite strategy which permits light induced tumor destruction. Detailed literature reports of potential transition metal complexes showing light induced generation of ROS and controlled delivery of multiple drugs in tumor microenvironment are presented. The key challenges are the delivery and controlled activation of the clinically approved platinum (II) drugs. These prime objectives of the present investigation are depicted as a concluding segment of this introductory chapter. Chapter II includes the syntheses, characterization, evaluation of visible light induced cytotoxicity and interaction with DNA of novel ferrocenyl terpyridine appended platinum (II) complexes. Detailed mechanistic investigations revealed the important role of ferrocene in light triggered generation of reactive oxygen species. The effect of extensive conjugation on the photophysical properties of the complexes were also rationalized from theoretical calculations. The alteration in DNA binding affinities of the complexes on incorporation of a ferrocene unit in the platinum (II)terpyridines is also reflected. The work is the first report of the remarkable photocytotoxicity of platinum(II) complexes in visible light with nominal dark toxicity. Chapter III deals with novel ferrocenyl terpyridyl platinum(II) complexes having tumor targeting biotinylated acetylides which were synthesized for achieving selective photocytotoxicity only in cancer cells. An interesting observation was the red light promoted release of biotinylated acetylide ligands from platinum centre thereby generating mono-functional Pt(II) species. The possible covalent interactions of these platinum(II) species with DNA were also explored. These biotin complexes exhibit preferential cellular uptake in BT474 breast cancer cells over HBL-100 breast normal cells resulting in targeted photocytotoxicity in visible light. Chapter IV rationalizes design, syntheses and extensive characterization of 2-(phenylazo)pyridine based platinum(II) catecholates containing photosensitizers. The O^O donor ligand was chosen to release the more cytotoxic bi-functional platinum(II) species based on the prior knowledge of the labile Pt-O bonds. Interestingly, we observed glutathione triggered release of the catecholates imparting dual action anticancer properties to the molecules. Detailed mechanistic aspects indicated a possible reduction of the metal coordinated azo bond by cellular glutathione. The excellent photocytotoxicity in HaCaT and MCF-7 cells, cellular ROS generation and apoptosis, cellular Pt content and localization of these complexes are discussed. Chapter V addresses the advantages of navigating the platinum(II) complexes to mitochondrial DNA instead of genomic DNA. BODIPY appended platinum(II) catecholates were synthesized and the BODIPY core was modified to fine-tune the photophysical properties. The visible light induced growth inhibitory effects of the complexes and the mechanism of cell death in light exposed cells are explored. The novelty of this work is the mitochondria targeted remarkable photocytotoxicity as well as cellular imaging properties of the complexes making them ideal candidates for developing platinum based theranostic agents. Chapter VI presents the syntheses, characterization of unprecedented platinum(II) complexes of curcumin for dual action DNA crosslinking and photochemotherapeutic activities. The important feature of these Pt(II) prodrugs is the photorelease of curcumin from Pt(II) centre which results in controlled delivery of two potential anticancer agents. The visible light induced cytotoxicities of the complexes in HaCaT, BT474, T47D, Hep3B and HPL1D cells, their effect on the various cellular events, the interaction of the complexes with DNA and their cellular distribution in light and dark are explored. The appropriate references are provided at the end of each chapter and allocated as superscripts in the main text. The synthesized complexes are denoted by bold-faced numbers. Crystallography data of the complexes that are structurally characterized by single crystal X-ray crystallography are given in CIF format in the enclosed CD (Appendix-I). Due acknowledgements are provided for mentioned literature reports. Any omission is purely unintentional and is deeply regretted. INDEX WORDS: Platinum(II) complexes • Crystal structure • Visible light induced cytotoxicity • Cellular imaging • Photochemotherapeutic agents • DNA crosslink.

Photochemotherapeutic Agents

DNA Crosslinking

Platinum(II) Complexes

Anticancer Properties

Photocytotoxicity

Curcumin

cis‐Diammineplatinum(II) Complex

Inorganic and Physical Chemistry