Evaluating the inter and intra batch variability of protein aggregation behaviour using Taylor dispersion analysis and dynamic light scattering

Hulse, W.L., Gray, J., Forbes, Robert T.

January 2013

No / Biosimilar pharmaceuticals are complex biological molecules that have similar physicochemical properties to the originator therapeutic protein. They are produced by complex multi-stage processes and are not truly equivalent. Therefore, for a biosimilar to be approved for market it is important to demonstrate that the biological product is highly similar to a reference product. This includes its primary and higher order structures and its aggregation behaviour. Representative lots of both the proposed biosimilar and the reference product are analysed to understand the lot-to-lot variability of both drug substances in the manufacturing processes. Whilst it is not easy to characterise every variation of a protein structure at present additional analytical technologies need to be utilised to ensure the safety and efficacy of any potential biosimilar product. We have explored the use of Taylor dispersion analysis (TDA) to analyse such batch to batch variations in the model protein, bovine serum albumin (BSA) and compared the results to that obtained by conventional dynamic light scattering analysis (DLS). Inter and intra batch differences were evident in all grades of BSA analysed. However, the reproducibility of the TDA measurements, enabled the stability and reversibility of BSA aggregates to be more readily monitored. This demonstrates that Taylor dispersion analysis is a very sensitive technique to study higher order protein states and aggregation. The results, here, also indicate a correlation between protein purity and the physical behaviour of the samples after heat shocking. Here, the protein with the highest quoted purity resulted in a reduced increase in the measured hydrodynamic radius after heat stressing, indicating that less unfolding/aggregation had occurred. Whilst DLS was also able to observe the presence of aggregates, its bias towards larger aggregates indicated a much larger increase in hydrodynamic radii and is less sensitive to small changes in hydrodynamic radii. TDA was also able to identify low levels of larger aggregates that were not observed by DLS. Therefore, given the potential for immunogenicity effects that may result from such aggregates it is suggested that TDA may be suitable in the evaluating detailed batch to batch variability and process induced physical changes of biopharmaceuticals and biosimilars.

Chemistry techniques

Light

Proteins

Scattering

Serum albumin

Aggregation

Biosimilar

Dynamic light scattering

Hydrodynamic radius

Taylor dispersion analysis

Bovint serum albumin påverkar överlevnad och Aβ-nivåer i Alzheimers sjuka Drosophila flugor. : Bovine serum albumin affects survival and Aβ-levels in Alzheimer's diseased Drosophila flies.

Tani, Milena

January 2024

Alzheimer's disease (AD) was first described more than 100 years ago and is today the most common cause of dementia. It is one of the progressive neurodegenerative diseases that affect 47 million people around the world between the ages of 60 and 90. One of the contributing factors to AD is extracellular amyloid – β (Aβ) plaques that form as a result of protein aggregation. These Aβ proteins are neurotoxic, leading to degeneration of brain neurons and loss of cognitive abilities. Because AD largely affects society, researchers are constantly working to find a cure, which currently does not exist. The purpose of this study was to use Drosophila melanogaster as a living organism model for the expression of two types of Aβ proteins related to AD, Arctic (Glu22Gly) and TandemAβ, and to study the survival of these AD flies when Bovine serum albumin (BSA) was added to the fly food. The hypothesis was that BSA would be effective in slowing down and/or preventing formation of toxic Aβ-aggregates. The focus was therefore to investigate whether the AD flies would live longer if they were allowed to eat Bovine serum albumin and whether the soluble/insoluble Aβ levels in these flies would decrease in comparison to the control AD flies that were not allowed to eat BSA. The effect of BSA on toxicity was evaluated using survival assay on male flies and the levels of soluble/insoluble Aβ were evaluated using Meso Scale Discovery (MSD) on female flies. In both experiments, the following six groups of flies were examined: myow1118 ± BSA; myoArctic ± BSA; myoTandemAβ ± BSA. Conclusions from the studies are that the survival of AD flies could not be extended by adding 0.61 mM BSA to the food, rather the data showed a weak but significant toxic effect in the presence of BSA in the AD flies. However, MSD data showed a reduction of insoluble Aβ aggregates and an equilibrium shift from insoluble Aβ aggregates to soluble Aβ aggregates in the presence of BSA in the AD flies. Equilibrium shifts were particularly detectable in Myo-TandemAβ flies fed with BSA. In Myo-Arctic flies fed with BSA only reduction of insoluble Aβ could be detected. This shows that it is not the amount of Aβ aggregates that is decisive for toxicity, but rather the presence of specific aggregates that have toxic properties. If BSA shows good results in further studies, it could be used in the future to improve AD symptoms in patients.

Drosophila melanogaster

Alzheimer

AD

BSA

Bovine serum albumin

Human serum albumin

HSA

Toxicity

Aβ

survival assay

MSD

Meso Scale Discovery

Arctic (Glu22Gly)

TandemAβ

oligomers

fibrills

GAL4-UAS

TM6B

CyO

enterocytes

Drosophila melanogaster

bananfluga

Alzheimers

BSA

Bovint serum albumin

Aβ

Amyloida plack

Överlevnad

MSD

Meso Scale Discovery

AD

Toxicitet

Arctic (Glu22Gly)

TandemAβ

HSA

Humant serum albumin

GAL4-UAS

TM6B

CyO

fibriller

oligomerer

enterocyter

Natural Sciences

Naturvetenskap

Other Chemistry Topics

Annan kemi

Biochemistry and Molecular Biology

Biokemi och molekylärbiologi

Other Biological Topics

Annan biologi

Genetics

Genetik

The influence of different winemaking techniques on the extraction of grape tannins

Nel, Anton Pieter

03 1900

Thesis (MScAgric (Viticulture and Oenology))--University of Stellenbosch, 2011. / Includes bibliography. / ENGLISH ABSTRACT: Grape and wine phenols consist of flavanols which is the building blocks for tannins. These building blocks are called monomers which consist of catechins, epicatechins, epigallocatechins and epicatechin-gallate. Tannin is important in wine as it contributes to bitterness, mouth feel (astringency) and maturation potential of the wine. Futhermore it has a health benefit as an antioxidant. Anthocyanins are responsible for the colour of red wine. The anthocyanins combine with tannins to form stable polymeric pigments. Due to the importance of tannins and anthocyanins in wine, it is imperitative that different winemaking techniques are used to extract as much of these components as possible and that the analysis is done quickly and accurately. The aim of this study was to evaluate different winemaking techniques and their extraction of tannins and anthocyanins into the wine. Too much tannin extraction can have a negative effect on the sensory quality of the wine. Therefore a second aim was to evaluate the mouth feel properties of a Shiraz wine. A third aim was to compare the two tannin precipitation methods in terms of time efficiency, repeatability and the ease of practice. To investigate the amount of tannin concentration extracted by different winemaking techniques, two cultivars (Cabernet Sauvignon and Shiraz) were used. These treatments included the addition of an enzyme during fermentation [E], cold maceration [CM], post maceration [PM] and the combination of cold and post maceration [CM+PM]. The grapes were harvested in two different climatic areas during the 2008 and 2009 vintages. The two climatic areas were classified according to the Winkler scale as a III (Morgenster) and a IV (Plaisir de Merle). The grapes were harvested at two different ripeness levels in order to evaluate the effect of the different winemaking processes on the extraction of tannins and anthocyanins. One harvest was before (LB) and the other after (HB) the commercial harvest. The results of this study showed significant differences in the phenolic composition of the wines. It was found that the warmer area showed higher tannin concentrations than the cooler area for both cultivars. In the 2008 Cabernet Sauvignon the CM extracted higher concentrations of tannin from the cooler area at both ripeness levels. In the warmer area, CM extracted the highest tannin concentration HB, but the CM+PM extracted the highest tannin concentration from Cabernet Sauvignon at the LB and CM at the HB of the warmer area. In 2009 the PM extracted the highest concentration of tannin at the lower ripeness level, while the E treatment extracted the highest concentration from the warmer area. In the cooler area the CM+PM extracted the highest concentration of tannin at a lower ripeness level, while there were no siginicant differences between the different treatments at the higher ripeness level. The highest anthocyanin concentration was found in the cooler area. The CM treatment was found to have no effect on anthocyanin extraction. Different methods are available to quantify the tannin concentration in wine. Two of the most popular tannin analytical methods are the bovine serum albumin (BSA) and the methyl cellulose precipitable tannin (MCP) methods. The BSA method is a very complex method which uses at least 3 times more reagents than the MCP method. The MCP method only analyzes tannins, while the BSA method analyzes tannins, monomeric pigments (MP), small polymeric pigments (SPP) and large polymeric pigments (LPP). In this study a good correlation was found between the two tannin precipitation methods (R2 – 0.88). There is controversy regarding the variability of these methods. Some scientists found that the two methods show a good correlation with HPLC, while others found that there was no such correlation between the precipitation methods and the HPLC. The MCP method had a practical advantage as it could be performed in half the time required for the BSA method. This has a significant impact in scenarios where a high sample throughput is required although it only measures total tannin. The phenolic composition and mouth feel of the wine was strongly influenced by the climatic area. In the warmer area the effect of tannin concentration on mouth feel was much less than in the cooler area. The wine made of riper grapes, was more grippy, bitter and numbing than the wines made from greener grapes. The E treatment was especially associated with a dry, grippy sensation. / AFRIKAANSE OPSOMMING: Druif en wyn fenole bestaan uit flavanole wat weer die boublokke is van tanniene. Hierdie boublokke, wat bekend staan as monomere, betsaan uit katesjiene, epikatesjiene, epigallokatesjiene an epikatesjien-gallaat. Tanniene is belangrik in wyn aangesien dit bydra tot bitterheid, mondgevoel (vrankheid) asook die verouderingspotensiaal van wyn. As antioksidante hou dit ook gesondheidsvoordele in. Antosianiene dra by tot die kleur van rooiwyn. Antosianiene kombineer met tanniene om meer stabiele polimeriese pigmente te vorm. As gevolg van die belangrikheid van tanniene en antosianiene is dit van uiterse belang dat verskillende wynmaak tegnieke gebruik word om ekstraksie in die wyn te bevoordeel en dat die analitiese metode so vinnig en akkuraat as moontlik gedoen word. Die eerste doel van hierdie studie was om die ekstraksie van tanniene en antosianiene deur middel van verskillende wynmaak tegnieke te evalueer. Te veel tanniene in die wyn kan negatiewe sensoriese kwaliteit tot gevolg het. Daarom is die tweede doel om die sensoriese kwaliteit van Shiraz wyn te evalueer. Die derde doel van hierdie studie was die twee tannien presipitasie metodes met mekaar te vergelyk in terme van die moeilikheidsgraad van die metode, tyd doeltreffendheid en herhaalbaarheid. Verskillende wynmaak tegnieke (ensiem byvoegings [E], koue maserasie [CM], verlengde dopkontak [PM] en ‘n kombinasie van koue maserasie en verlengde dopkontak [CM+PM]) is vergelyk ten opsigte van tannien en antiosianien ekstraksie. In 2008 en 2009 is twee kultivars (Cabernet Sauvignon en Shiraz) in twee verskillende klimatologiese areas gepars. Hierdie areas is geklassifiseer in die Winklerskaal as ‘n IV (Plaisir de Merle) en ‘n III (Morgenster). Om die effek van die verskillende wynmaak tegnieke op die ekstraksie van antosianiene en tanniene te vergelyk, is hierdie twee kultivars by twee verskillende rypheidsgrade geoes. Die eerste oes was net voor kommersiële oes (LB) en die tweede oes het net na kommersiële oes (HB) plaasgevind. Die 2009 Shiraz wyn is organolepties beoordeel om die effek van die verskillende wynmaak tegnieke op die wyn se mondgevoel te vergelyk. Die resultate van hierdie studie toon beduidende verskille in die fenoliese samestelling van die wyne. Dit is gevind dat die warmer area hoër tannien konsentrasies het as die koeler area. In 2008 het die CM+PM die meeste tanniene uit die Cabernet Sauvignon geëkstraheer by LB en die CM by HB in die warmer area. Die CM het in die koeler area meer tanniene geëkstraheer by beide die LB en HB rypheidsgrade. In 2009 het PM die meeste tanniene geëkstraheer by LB terwyl E die meeste tanniene geëkstraheer in die warmer area. In die koeler area het CM+PM die meeste tanniene geëkstraheer, terwyl geen van die behandelings ‘n effek gehad het by HB. Die meeste antosianien konsentrasie was in die koeler area gevind as in die warmer area. In beide 2008 (LB en HB) en 2009 (LB) het CM die meeste antosianiene geëkstraheer, terwyl geen behandeling ‘n effek gehad het by HB. Twee van die mees populêre tannien analitiese metodes is die BSA (bovine serum albumien) en die MCP (metielsellulose presipitasie) metodes. Die BSA metode is ‘n baie meer ingewikkelde metode waarvoor drie keer meer reagense gebruik word as vir die MCP metode. Maar waar die MCP net tanniene ontleed, ontleed die BSA metode tanniene, monomere (MP), klein polimeriese pigmente (SPP) en groot polimeriese pigmente (LPP). Dit help indien daar gekyk wil word na die evolusie van polimeriese pigmente. In hierdie studie is bevind dat daar ‘n redelike korrelasie (R2 – 0.88) tussen die BSA en MCP metode bestaan. Die herhaalbaarheid van die metodes het redelike kontroversie veroorsaak, waar sommige navorsers bevind het dat die BSA metode nie so herhaalbaar is soos eers bevind is nie. Die MCP metode het ’n praktiese voordeel aangesien dit in die helfde van die tyd van die BSA metode uitgevoer kan word. Dit het ‘n groot impak indien ‘n groot hoeveelheid monsters ontleed moet word. Die fenoliese samestelling en mondgevoel word sterk beïnvloed deur die klimatologiese area. In die warmer area was die effek van tannien konsentrasie op mondgevoel kleiner as in die koeler area. Die wyn van ryper druiwe het meer harder, verdowingseffek en bitter nasmaak gehad as by die wyn van groener druiwe. Die ensiem behandeling was meer geassossieerd met droë mond gevoel.

Tannins

Sensory analysis

MCP

BSA

Phenolic ripeness

Theses -- Viticulture and oenology

Dissertations -- Agriculture

Theses -- Agriculture

Wine and wine making

Bovine serum albumin

Polyphénols d’agrumes (flavanones) : extraction de glycosides de la peau d’orange, synthèse de métabolites chez l’homme (glucuronides) et étude physico-chimique de leur interaction avec la sérum albumine / Citrus polyphenols (flavanones) : extraction of glycosides from orange peel, synthesis of metabolites (glucuronides) found in human and a physico-chemical study to investigate their interaction with human serum albumin

Khan, Muhammad Kamran

15 November 2010

Un groupe d'études épidémiologiques fournit une bonne preuve de la relation inverse associé à la consommation de fruits et légumes et les maladies chroniques important comme maladies cardiovasculaires et certains types de cancers. Après les longues années d'études sur phytomacronutrients, le rôle de phytomicronutrients tels que les polyphénols est désormais très étudiée et appréciée dans le contrôle de ces maladies dégénératives. La présente étude combine les études d'extraction, de synthèse et d'analyse sur les principaux polyphénols des fruits d'agrumes, FLAVANONES. Connaissance de nutritionnels et de santé a augmenté la production d'agrumes en provenance des dernières décennies. Ces productions plus générer des bye-produits. Pour leur utilisation alternative à des antioxydants extraits riches, l'extraction assistée par ultrasons (UAE) des polyphénols en particulier flavanones de l'orange (Citrus sinensis L.) par son peau en utilisant l'éthanol comme solvant de qualité alimentaire a été prouvé son efficacité en comparaison avec la méthode conventionnelle . Un plan composite central (CCD) a révélé que l'approche des conditions optimisées pour UAE ont une température de 40 ° C, une puissance de 150W sonication et un 4:1 (v / v) d'éthanol: ratio de l'eau. En outre, l'activité antioxydante déterminée par les tests DPPH et ORAC a confirmé la pertinence des UAE pour la préparation d'extraits de plantes riches en antioxydants.Les glucuronides de flavanone sont les principaux métabolites phénoliques détectés dans le plasma humain après la consommation d'agrumes. Jusqu'à maintenant, toutes les études sur les cellules liées au cancer ou les maladies cardiovasculaires ont été réalisées soit sur les aglycones ou sur leurs glycosides. Par conséquent, il ya grand besoin de glucuronides flavanone pure pour démontrer le potentiel réel de flavanones dans la prévention de ces maladies. Dans ce travail, glucuronides de naringénine (4'- et 7-O-β-D-glucuronides) et de hespérétine (3'- et 7-O-β-D-glucuronides), les aglycones flavanone majeur dans le pamplemousse et d'orange, respectivement, ont été synthétisés chimiquement par une protection et la déprotection sélective des groupements d'acide glucuronique et de flavanone. La caractérisation structurale complète de composés purifiés a été réalisée par résonance magnétique nucléaire et spectrométrie de masse.L'affinité des quatre glucuronides pour l'albumine sérum d’humaine (HSA) a été testée par leur capacité à éteindre la fluorescence intrinsèque de HSA (Trp, seul résidu de sous-domaine IIA). Leurs constantes de fixation (K) ont été estimées de l'ordre de 30 à 60 × 103 M-1 et comparées à celles de l'aglycones (70 à 90 × 103 M-1). Les enquêtes de la liaison compétitive ou non compétitive de la glucuronides dans la présence de sondes fluorescentes (sarcosine dansyl) nous a permis d'obtenir un aperçu dans les sites de liaison. L'étude a également été étendue aux chalcones hespérétine et naringénine (synthétisés en utilisant des conditions alcalines optimisée), qui sont les précurseurs de biosynthèse des flavanones / A bunch of epidemiological studies provides good evidence on the inverse relationship associated with the consumption of fruits and vegetables and the chronic diseases importantly cardiovascular diseases and some types of cancers. After the long years of study on phytomacronutrients, the role of phytomicronutrients such as polyphenols is now highly studied and appreciated in the control of such degenerative diseases. The present study combines the extraction, synthetic and analytical studies on the major polyphenols of citrus fruits, FLAVANONES.Awareness of nutritional and health facts has increased the production of citrus fruits from last few decades. These higher productions generate higher by-products. For their alternative utilisation to have antioxidants rich extracts, the ultrasound-assisted extraction (UAE) of polyphenols especially flavanones from orange (Citrus sinensis L.) peel by using ethanol as afood grade solvent has been proved its efficiency when compared with the conventional method. A central composite design (CCD) approach revealed that the optimized conditions for UAE were a temperature of 40°C, a sonication power of 150W and a 4:1 (v/v) ethanol:water ratio. Furthermore, the antioxidant activity determined by the DPPH and ORAC tests confirmed the suitability of UAE for the preparation of antioxidant-rich plant extracts. Flavanone glucuronides are the major phenolic metabolites detected in human plasma after consumption of citrus fruits. Up to now all cell studies related to cancer or cardiovascular diseases were conducted either on the aglycones or on their glycosides. Hence, there is great need of pure flavanone glucuronides to demonstrate the real potential of flavanones in the prevention of these diseases. In this work, glucuronides of naringenin (4′- and 7-O-β-D-glucuronides) and hesperetin (3′- and 7-O-β-D-glucuronides), the major flavanone aglycones in grapefruit and orange respectively, have been chemically synthesized by selective protection and deprotection of flavanone and glucuronic acid moieties. The complete structural characterisation of purified compounds were realised by nuclear magnetic resonance and mass spectrometry.The affinity of the four glucuronides for human serum albumin (HSA) was tested via their ability to quench the intrinsic fluorescence of HSA (single Trp residue in sub-domain IIA). Their binding constants (K) were estimated in the range of 30 – 60 × 103 M-1 and compared with those of the aglycones (70 – 90 × 103 M-1). Investigations of competitive or noncompetitive binding of the glucuronides in the presence of fluorescent probes (dansyl sarcosine) allowed us to get some insight in the binding sites. The study was also extended to the hesperetin and naringenin chalcones (synthesised using optimized alkaline conditions), which are the biosynthetic precursors of flavanones

Agrumes

Polyphénols

Flavanone

Extraction assistée par ultrasons

Synthèse

Albumine sérique humaine

Citrus

Polyphenols

Flavanone

Ultrasound-assisted extraction

Synthesis

Human serum albumin

Interakce mezi proteiny a huminovými látkami při koagulaci / Interactions between proteins and humic substances during coagulation

Novotná, Kateřina

January 2015

This diploma thesis is focused on coagulation of humic substances (HS) and BSA (Bovine Serum Albumin) protein which was chosen as a representative of proteins contained in AOM (Algal Organic Matter). Additionally, possible interactions between these compounds were also investigated. It was found that the optimal dosage of coagulant is much higher for HS compared to BSA. The best removal of both HS and BSA was reached in slightly acidic pH range and it is attributed mainly to charge neutralization and adsorption mechanisms. The maximum removal rate was 70 % for humic substances and 80 % for BSA. The results show that BSA has a positive effect on coagulation of HS (resulting in a lower coagulant demand) and vice versa while BSA was removed more efficiently than HS. The existence of interactions between BSA and humic substantces during coagulation was demonstrated in certain pH ranges and it can occur even without the presence of coagulant. These interactions are highly dependent on pH that determines charge properties (and hence reactivity) of organic matters. Finally, the comparison of BSA and cyanobacterial proteins shows that their behavior during coagulation is similar. Consequently, BSA can be used as a model compound representing AOM proteins, especially their high molecular weight fraction....

Vliv složek synoviální kapaliny na mazání náhrad kyčelního kloubu / The Effect of Synovial Fluid Constituents on Lubrication of Hip Joint Replacements

Nečas, David

January 2016

Dizertační práce se zabývá mechanismy mazání v náhradách kyčelního kloubu. Byla provedena systematická studie formování proteinového filmu při zahrnutí různých materiálů a provozních podmínek. Hlavní pozornost je přitom věnována roli jednotlivých proteinů obsažených v synoviální kapalině při současné přítomnosti dalších proteinů. Jelikož metody aplikované v předchozích studiích neumožňovaly separovat jednotlivé složky maziva, byla vyvinuta optická měřící metoda na principu fluorescenční mikroskopie. Z důvodu verifikace metody byly provedeny dvě nezávislé studie zaměřené na měření tloušťky mazacího filmu a dělení maziva na výstupu mazaného kontaktu. Z důvodu určitých limitací fluorescenční mikroskopie byla dále využita i metoda optické interferometrie, jejíž využití je ilustrováno ve studii zabývající se formováním mazacího filmu v náhradách kyčelního klubu při uvažování reálné konformity třecích povrchů. Závěrečná část práce představuje nový metodologický přístup založený na in situ pozorování kontaktní oblasti umožňující popsat roli jednotlivých proteinů ve vztahu k vývoji tloušťky mazacího filmu. Práce obsahuje originální výsledky, které přináší nové poznání v oblasti biotribologie náhrad kyčelního kloubu vedoucí k dalšímu vývoji implantátů při snaze zabránit jejich selhání v důsledku omezené životnosti.

Mousses rigides et élastiques à base de tannins et d'albumine : préparation, caractérisation et modification / Rigid and elastic tannin and albumin foams : Preparation, characterization and modification

Li, Xinjun

12 June 2013

Du fait de leur faible coût, de leur bonne résistance à la compression, de leur fort pouvoir isolant et de leur résistance au feu, les mousses tannin/furanique constituent une alternative très intéressante aux mousses phénoliques et aux polyuréthanes dans diverses applications. Par ailleurs elles sont constituées à 95 % de matériaux naturels. Cependant, les mousses tannin/furanique sont : a) moins résistantes mécaniquement que les mousses synthétiques telles que phénoliques et polyuréthanes; b) potentiellement toxiques si le formaldéhyde utilisé pour les formuler est libéré dans l'environnement ; c) par ailleurs, des mousses légèrement élastiques seraient un plus. Dans cette thèse, des modifications et les caractérisations associées des mousses tannin/furaniques sont apportées pour résoudre ces défauts. Ce travail a été réalisé en quatre étapes principales :1) Étude et compréhension de la relation structure - propriétés des mousses. Dans ce but, les agents gonflants tels que le diéthyléther, le pentane, et des isocyanates et des polyuréthanes ont été particulièrement étudiés.2) Du noir de carbone, des nanotubes de carbone, de l'argile micronisé, des oligomères d'un polymère hyperramifié (ester-amine), des isocyanates et des polyuréthanes ont été ajoutés dans les formulations des mousses pour tenter d'améliorer leurs propriétés mécaniques et modifier leurs structures cellulaires.3) Le glutaraldéhyde et le glyoxal ont été essayés pour remplacer le formaldéhyde et préparer ainsi des mousses exemptes de formaldéhyde.4) Une nouvelle mousse, la mousse d'albumine, a été préparée, caractérisée et optimisée / The solid foams, because of their low density and cell structure, are commercial products with more and more interest. In recent decades, various methods for making foams based on bio-based materials have been prepared and characterized, such as lignin, starch and tannins. Because of their low cost, their resistance to compression, their high insulation and resistance to fire, tannin/furanic foams are supposed to be alternatives of phenolic foams and polyurethane in various applications. However, tannin/furanic foams are: a) lower mechanical resistant than synthetic foams such as polyurethane and phenolic foams b) potentially toxic because of formaldehyde, c) it is also interesting to prepare a foam more elastic. In this thesis, These works were carried out by four main steps: 1) Study and understanding the relationship of structure and properties of the foams. So different blowing agents, such as diethyl ether, pentane, and isocyanates and polyurethanes, were studied. 2) Carbon black, carbon nanotubes, nano clay, oligomers of hyperbranched poly (ester-amine) and pMDI were added to the formulations to improve their mechanical properties and change their cellular structures. 3) Glyoxal and glutaraldehyde have been tried to replace and prepare formaldehyde-free formaldehyde foams. 4) A new foam, albumin foam was prepared, characterized and optimized

Mousses de tanin/ furane

Mousses élastiques

Mousses d'albumine

Résine de tanin/ furane

Mousses de carbone

Tannin/furanic foams

Elastic foams

Albumin foams

Tannin/furanic resin

Carbon foams

620.116

541.345 1

Complexos híbridos de polieletrólitos e magnetita para liberação controlada de amoxicilina / Hybrid complexes of polyelectrolytes and magnetite for controlled release of Amoxicillin

Bueno, Pedro Vinicius de Assis

10 August 2018

Novos sistemas biocompatíveis para aplicações biotecnológicas são relevantes não só do ponto de vista tecnológico, mas também para avanços científicos. A presente dissertação visou à criação e caracterização de filmes finos (espessura de até 100 nm) ou micrométricos (espessura de 50 µm a 100 µm) formados por goma xantana (GXT), poli(cloreto de dimetil dialil amônio), (PDDA), albumina bovina sérica (BSA), e nanopartículas de magnetita (NPM). A incorporação de amoxicilina (Amox), um antibiótico amplamente utilizado contra muitas infecções, nos filmes foi realizada durante a formação dos sistemas. Os filmes finos foram caracterizados através de elipsometria e microscopia de força atômica. Em solução, as interações favoráveis entre o Amox e a BSA foram evidenciadas por mudanças substanciais na estrutura secundária da BSA, como revelado pelo dicroísmo circular. Os filmes micrométricos (patches) de GXT e GXT/NPM/BSA foram imersos em Amox 2 g/L, levando a incorporação de 10 ± 3 e 17 ± 4 µg/cm³ de Amox, respectivamente. Sua caracterização compreendeu espectroscopia vibracional no infravermelho por transformada de Fourier no modo de refletância total atenuada (FTIR-ATR), microscopia eletrônica de varredura (MEV), medidas de sorção e espectrometria de emissão óptica com plasma indutivamente acoplado (ICP-OES). A incorporação de 0,2% em massa de Fe3O4 nos \"patches\" e sua exposição a um campo magnético externo, viabilizou a liberação total in vitro de Amox, em pH 5,5 e em 0,02 mol/L de NaCl, seguindo o comportamento quasi-Fickiano. A difusão da Amox dos \"patches\" de GXT/NPM/BSA em ágar contendo Staphylococcus aureus e Escherichia coli, levou halos de inibição consideráveis. A inibição do crescimento de E. coli foi particularmente eficiente sob efeito de campo magnético externo. / New biocompatible systems for biotech applications are relevant not only from a technological point of view, but also for scientific advances. The present project aimed at the creation and characterization of thin films (thickness up to 100 nm) or micrometric patches (thickness of 50 µm to 100 µm) formed by the deposition of xanthan gum (GXT), poly (dimethyl diallyl ammonium chloride) (PDDA), bovine serum albumin (BSA), and magnetite nanoparticles (NPM). The incorporation of amoxicillin (Amox), a widely used antibiotic against many infections, in the films was performed during the formation of the systems. Thin films were characterized by means of ellipsometry and atomic force microscopy. In solution, favorable interactions between Amox and BSA were evidenced by substantial changes in the secondary structure of BSA, as revealed by circular dichroism spectra. Patches of GXT and GXT/NPM/BSA were immersed into Amox solution at 2 g/L, leading to the Amox incorporation of 10 ± 3 and 17 ± 4 µg/cm3, respectively. The patches characterization included Fourier Transform Infrared vibration spectroscopy in the attenuated total reflectance mode (FTIR-ATR), scanning electron microscopy (MEV), sorption measurements and inductively coupled plasma optical emission spectrometry (ICP-OES). The incorporation of 0.2 wt% of Fe3O4 in the patches and their exposure to an external magnetic field, allowed the total in vitro release of Amox, at pH 5.5 and 0.02 mol/L NaCl, following the behavior quasi-Fickian. Amox diffusion from GXT/NPM/BSA patches in agar containing Staphylococcus aureus and Escherichia coli led to a considerable zone of inhibition. Inhibition of E. coli growth was particularly efficient under the effect of external magnetic field.

Albumin

Albumina

Amoxicilina

Amoxicillin

Escherichia coli

Escherichia coli

Goma xantana

Inhibition of microbial growth

Inibição do crescimento microbiano

Staphylococcus aureus

Staphylococcus aureus

Xanthan gum

Aterogênese induzida por albumina modificada por glicação avançada em camundongos dislipidêmicos é previnida pelo tratamento com losartana / Atherogenesis induced by advanced glycated albumin in dyslipidemic mice is prevented by losartan

Gomes, Diego Juvenal

02 September 2015

INTRODUÇÃO: Produtos de glicação avançada (AGE) encontram-se aumentados no diabete melito e contribuem independentemente para o risco cardiovascular. O reconhecimento dos AGE pelo receptor para produtos de glicação avançada (RAGE) potencializa vias de sinalização pró-aterogênicas. Antagonistas do receptor de angiotensina II (ANGII) do tipo 1 (AT-1) diminuem a expressão de RAGE em área de lesão aterosclerótica. No presente projeto, avaliou-se, na aorta de camundongos dislipidêmicos (knockout para apoE) tratados ou não com inibidor do receptor AT-1 (losartana, LOS), o efeito do tratamento crônico com albumina-AGE sobre o infiltrado de lípides, a expressão de mRNA e proteínas envolvidas no eixo AGE/RAGE, ANGII/AT-1, modulação da resposta inflamatória e fluxo de lípides, além da secreção de citocinas inflamatórias por macrófagos tratados com albumina controle ou AGE, concomitantemente ou não a losartana, isolados da cavidade peritoneal de camundongos apoE knockout. MÉTODOS: Camundongos machos knockout para apoE de 12 semanas de idade foram mantidos em dieta padrão e divididos, aleatoriamente, em quatro grupos experimentais (n = 20/grupo): grupo Controle (C), C+LOS, albumina-AGE (AGE) e AGE+LOS. Os animais receberam injeção intraperitoneal diária, durante 30 dias, de 2 mg de albumina controle (grupos C e C+LOS) ou albumina AGE (AGE e AGE+LOS). Os animais C+LOS e AGE+LOS foram tratados durante todo o período experimental com losartana (100 mg/L água). Secções do arco aórtico foram utilizadas para imunofluorescência para RAGE, carboximetil-lisina (CML), AT-1 e 4-hidroxinonenal (4-HNE) e determinação infiltrado lipídico por coloração com Oil Red-O. Análise do mRNA de Ager (RAGE), Agtr1a (AT-1), Orl1 (LOX-1), Msr1 (MCP-1), Ccl2 (SR-A), Cybb (Nox2), Nfkb (NF-kB), Tnf (TNF-alfa), Abca1 (ABCA-1), Abcg1 (ABCG-1) e Agt (angiotensinogênio) foi realizada por de qRT-PCR. Ensaio in vitro para secreção de IL-6 por ELISA e expressão de Il1b (IL-1beta) e Il18 (IL-18) por alfaRT-PCR, foi realizado com macrófagos peritoneais isolados camundongos apoE knockout incubados com albumina C ou AGE (2 mg/mL), concomitante ou não ao tratamento com losartana (1 uM). RESULTADOS: Não houve diferença entre os grupos em relação ao peso corporal, colesterol total, triglicérides e glicose plasmáticos, no período basal e final. A pressão arterial sistólica foi reduzida nos animais tratados com losartana quando comparados aos não tratados (p < 0,05). Não foi detectada a presença de infiltrado macrofágico na aorta por meio de ensaios de imunofluorescência para CD-68 e pela análise de coloração com hematoxilina-eosina. Todavia, o infiltrado de lípides foi 5,3 e 2 vezes maior no grupo AGE quando comparado, respectivamente, ao grupo C e AGE+LOS (p < 0,05). O conteúdo proteico de RAGE e CML, assim como do marcador de peroxidação lipídica (4-HNE) foi maior no grupo AGE em comparação aos demais grupos, o que não prevenido no grupo AGE+LOS (p < 0,05). A expressão do mRNA de Ager, Orl1 e Tnf foi maior no grupo AGE em comparação ao C, ao passo que o tratamento com losartana impediu o aumento da expressão destes genes (p < 0,05). Isto não foi observado para aumento de Cybb estimulado por albumina-AGE. A losartana diminuiu o mRNA de Agtr1a (AT-1) em ambos os grupos tratados. Não foram observadas diferenças na expressão do mRNA de Msr1, Ccl2, Abca1, Abcg1, Agt e Nfkb. Macrófagos tratados com albumina-AGE apresentaram secreção de IL-6 aumentada em 1,4 vezes em comparação ao grupo C, o que foi prevenido pela losartana (p < 0,05). Nestas mesmas células, a albumina-AGE aumentou a expressão de Il1b e Il18, em comparação à albumina-C, o que não foi prevenido pela losartana. CONCLUSÃO: A administração crônica de albumina-AGE em modelo animal de dislipidemia isento de DM, aumentou o infiltrado de lípides no aorco aórtico, independentemente de variação na pressão arterial, lípides plasmáticos e da modulação local de componentes do sistema renina-angiotensina. A ação da albumina-AGE foi consequente ao maior insulto oxidativo e inflamatório associado ao maior conteúdo de RAGE e CML. A losartana, por reduzir o insulto oxidativo e inflamatório contrapõe-se à albumina-AGE, contribuindo para prevenção da aterogênese / INTRODUCTION: Advanced glycated end-products (AGE) elevated in diabetes mellitus and independently contribute to cardiovascular risk. The AGE binding to the receptor for AGE (RAGE) potentializes pro-atherogenic signaling pathways. Antagonists of angiotensin II receptor type 1 (AT-1) diminish RAGE expression in atherosclerotic plaques. In this study, we evaluated in the aortic arch of dyslipidemic mice (apoE knockout), treated or not with AT-1 blocker losartan (LOS), the effect of chronic treatment with AGE-albumin in aortic root lipid infiltration, mRNA expression and protein content of components of AGE/RAGE, ANGII/AT-1 axes and modulators of lipid flux and inflammation, and also the secretion of inflammatory cytokines by peritoneal macrophages treated either with control (C) or AGE-albumin, together with or not by losartan treatment,. METHODS: 12-week old male apoE knockout mice were fed chow diet and ramdomly assigned into four groups (n = 20/group): Control (C), C+LOS, AGE-albumin (AGE) and AGE+LOS. Animals received daily intraperitoneal injection of 2 mg of C- albumin (C and C+LOS) or AGE-albumin (AGE and AGE+LOS) during 30 days. LOS groups were treated with losartan (100 mg/L water). Immufluorescence for RAGE, AT-1, carboxymethyllysine (CML) and 4-hydroxynonenal (4-HNE), and Oil red-O staining for lipid infiltration was performed in sections from the aortic arch. mRNA expression of Ager (RAGE), Agtr1a (AT-1), Orl1 (LOX-1), Msr1 (MCP-1), Ccl2 (SR-A), Cybb (Nox2), Nfkb (NF-kB), Tnf (TNF-alfa), Abca1 (ABCA-1), Abcg1 (ABCG-1) e Agt (angiotensinogen) was evaluated by qRT-PCR. In vitro assay for IL-6 secretion was performed by ELISA and Il1b (IL-1beta) and Il18 (IL-18) mRNA expression was performed by qRT-PCR in peritoneal macrophages from of apoE knockout mice after treatment with C or AGE-albumin (2 mg/mL), with or without losartan (1 ?M). RESULTS: No differences among groups were observed in body weight, plasma total cholesterol, triglycerides and glucose in basal and final periods. Sistolic blood pressure was reduced in both LOS groups when compared to non-treated groups (p < 0.05). It was not observed CD-68 infiltration in the arterial wall. However, lipid infiltration was, respectively, 5.3 and 2 times greater in AGE group in comparison to C and AGE+LOS groups (p < 0.05). RAGE and CML protein and the lipid peroxidation marker (4-HNE) were greater in AGE group when compared to other groups, which was prevented in AGE+LOS (p < 0.05). Ager, Orl1 and Tnf mRNA expression was increased in AGE group when compared to C, and losartan was able to prevent this event (p < 0.05), except for Cybb. Losartan decreased Agtr1a mRNA expression in both groups (p < 0.05). No differences were observed among groups for Msr1, Ccl2, Abca1, Abcg1, Agt and Nfkb mRNA expression. Macrophages treated with AGE-albumin presented 1.4 times great IL-6 secretion, which was prevented by losartan (p < 0.05). In these cells, AGE-albumin increased Il1b and Il18 mRNA expression in AGE group, but this was not prevent by losartan. CONCLUSION: Chronic administration of AGE-albumin in non diabetic dyslipidemic mice increased aortic lipid infiltration, independently of changes in blood pressutre, plasma lipids and local modulation of renin angiotensin system components. The role of AGE-albumin was consequent to the enhanced inflammatory and oxidative insult associated to the higher content of CML and RAGE. Losartan by reducing oxidation and inflammation counteracts the effects of AGE-albumin contributing to prevent atherogenesis

Albumina sérica

Aterosclerose

Atherosclerosis

Camundongos

Cholesterol

Colesterol

Estresse oxidativo

Glycosylation end products advanced

Inflamação

Inflammation

losartan

losartan

Mice

Oxidative stress

Produtos finais de glicação avançada

Serum albumin

Estudo da interação de metalofármacos de dirutênio-anti-inflamatórios com as proteínas séricas transferrina e albumina / Study on the interaction of diruthenium-antiinflamatory metallodrugs with albumin and transferrin serum proteins

Sanches, Rute Nazaré Fernandes

26 April 2016

Metalofármacos baseados em rutênio têm se mostrado promissores com relação à atividade anticancerígena frente a diversos tipos de tumores. Nosso grupo de pesquisa dedica-se ao estudo de compostos contendo o centro dimetálico de valência mista Ru2(II,III) coordenado a ligantes derivados de Faines (Fármacos anti-inflamatórios não esteroides), tendo demostrando o potencial desses complexos frente a glioma. O entendimento do modo de ação destes complexos requer o estudo de suas interações com biomoléculas presentes no meio biológico. Neste cenário, o presente trabalho teve por objetivo investigar a interação de três complexos de dirutênio-Faines, ou RuFaines, [Ru2(ibp)4Cl], [Ru2(ceto)4Cl] e [Ru2(npx)4(H2O)2]PF6 (ibp = ibuprofenato, ceto = cetoprofenato e npx = naproxenato), e também do precursor [Ru2(O2CCH3)4Cl], RuAc, com as principais proteínas presentes no soro humano, transferrina e albumina. Os complexos foram sintetizados e caracterizados conforme metodologias desenvolvidas no grupo. A interação destes complexos com a transferrina, em suas formas apo e holo, e com a albumina foi avaliada por técnicas como espectroscopia eletrônica, dicroísmo circular, fluorescência, e realizaram-se estudos de ultrafiltração com análise do aduto formado por ICP-OES e espectrometria de massas. Além disso, fez-se um estudo de captação celular dos complexos RuFaines por células de glioma humano da linhagem U-87. Os resultados demonstraram que os complexos de dirutênio-Faines interagem com ambas as proteínas séricas (transferrina (apo e holo) e albumina), de modo semelhante, mas que é distinto daquele observado para o complexo RuAc. A presença de íons Fe(III) nos sítios específicos da transferrina não afetou a interação dos complexos RuFaines, enquanto que um comportamento diferente foi observado para o RuAc. Verificou-se que todas as proteínas avaliadas (albumina, apo-transferrina e holo-transferrina) apresentam capacidades similares de retenção dos complexos (~ 70% da quantidade de Ru adicionada inicialmente), independentemente da natureza do ligante carboxilato coordenado. Estudos de captação celular mostraram que a interação dos complexos RuFaines com a transferrina não contribuiu para modificar a capacidade de entrada desses complexos na célula, em comparação com os metalofármacos livres. Em alguns casos, inclusive, a formação de aduto com a apo-transferrina teve um efeito contrário, diminuindo a captação de rutênio. Dessa forma, concluiu-se que o ciclo da transferrina provavelmente não é a principal rota de entrada nas células para os complexos estudados. / Ruthenium metallodrugs have shown promising antitumor activity against to several tumor types. Our research group is dedicated to study compounds containing the mixed-valence Ru2(II,III) dimetallic center coordinated to NSAIDs (nonsteroidal anti-inflammatory drugs) derived ligands, and have demonstrated the potential of these complexes against glioma. The understanding of the mode of action of these complexes requires the study of their interactions with biomolecules present in biological environment. In this scenario, the present work aimed to investigate the interaction of three complexes of diruthenium-NSAIDs, or RuNSAIDs, [Ru2(ibp)4Cl], [Ru2(ceto)4Cl] and [Ru2(npx)4(H2O)2]PF6 (ibp = ibuprofenate, ceto = ketoprofenate, npx = naproxenate), and also of the precursor [Ru2(O2CCH3)4Cl], RuAc, with the major proteins present in the human serum, transferrin and albumin. The complexes were synthesized and characterized according to methods developed in our group. The interaction of these complexes with transferrin, in the two forms apo and holo, and with albumin was evaluated by techniques as electronic spectroscopy, circular dichroism, fluorescence, and ultrafiltration studies accompanied by analysis of adducts by ICP-OES and mass spectrometry. Moreover, cellular uptake studies of the RuNSAIDs complexes by U-87 human glioma cells line were performed. The results demonstrated that the diruthenium-NSAIDs complexes interact with both proteins (transferrin (apo and holo) and albumin), in a similar way, but that is distinct of that observed for the RuAc complex. The presence of Fe(III) ions in transferrin specific binding sites did not affect the interaction of the RuNSAID complexes with the protein, while a different behavior was shown by RuAc. All the proteins studied here (albumin, apo-transferrin and holo-transferrin) showed similar capabilities for retention of the complexes (~ 70 % of the initial amount of Ru added), independently of the nature of the coordinated carboxylate ligand. Cellular uptake studies showed that the interaction of the RuNSAIDs complexes with transferrin did not contribute to modify the internalization capacity of these complexes, in comparison with the free metallodrugs. In some cases, the adduct formation with apo-transferrin showed an opposite effect, leading to the decrease of ruthenium uptake. The findings led to the conclusion that transferrin cycle probably is not the main entry way to the cells for the studied complexes.

Albumin

Albumina

Anti-inflamatórios não esteroides

Captação celular

Cellular uptake

Glioma

Glioma

Metallodrugs

Metalofármaco

Nonsteroidal anti-inflammatory drug

Rutênio

Ruthenium

Transferrin

Transferrina