Estudo da gelificação do produto de digestão de ECM descelularizada para uso em engenharia de tecidos / Gelation study of extracellular matrix digestion products for tissue engineering

Os implantes utilizados para regeneração tecidual ainda falham na tentativa de mimetizar as propriedades da matriz extracelular (ECM), o que compromete a viabilidade e aplicabilidade do material. Além disso, permanece o desafio de desenvolver um método de aplicação minimamente invasivo para evitar danos teciduais adicionais (Badylak et al., 2015; Crapo et al., 2011; Xing et al., 2014). Assim, o objetivo do projeto é desenvolver um hidrogel injetável composto de ECM de pericárdio, tendão e osso bovino enzimaticamente digerida e reticulada com glutaraldeído, ésteres ativados de NHS e derivados de polietilenoglicol (PEG). O protocolo de digestão foi modificado de Willians (Williams et al., 2015), utilizando tripsina, pepsina e colagenase. A quantificação de GAGs e peptídeos mostrou que, independentemente do substrato e enzima utilizados, o processo em etapas gerou uma maior concentração de estruturas em relação ao processo contínuo. Adicionalmente, a análise de dicroísmo circular mostrou que o processo em etapas preservou mais estruturas secundárias. O perfil proteico das ECMs foi analisado como descrito em Flores (Flores et al., 2016), e foi verificado que ele é altamente diverso e tecido - específico. A ECM do pericárdio possui 94 tipos diferentes de proteínas, seguidas pela ECM do tendão (48) e pela ECM óssea (35), sendo o colágeno α1 (1) e o colágeno α2 (1) presentes em todas elas. Além disso, os produtos digeridos ECMp aumentaram a proliferação e diferenciação de células-tronco mesenquimais da medula óssea a osteoblastos maduros. A cinética do processo de gelificação, bem como as propriedades mecânicas do gel são dependentes do tipo de agente reticulante, assim como da concentração da gelatina. Este novo material é altamente personalizável e adaptável à aplicação biológica desejada

The implants used for tissue regeneration still fail to mimic properties of extracellular matrix. It compromises the material viability and applicability. Furthermore, the challenge to manufacture a minimally invasive delivery system for it to avoid extra tissue damage still remains (Badylak et al., 2015; Crapo et al., 2011; Xing et al., 2014). Thus, the project goal is to develop an injectable hydrogel composed of pericardium, tendon and bovine bone ECM enzymatically digested and crosslinked with glutaraldehye, activated esters of NHS and polyethylene glycol (PEG) derivatives. The digestion protocol was modified from Willians (Williams et al., 2015), using trypsin, pepsin and collagenase as lytic enzymes. GAGs and peptides quantification showed that regardless of the substrate and enzyme, the stepwise process yields a higher amount of GAGs and peptides in comparison with the continuous process. In addition, circular dicroism analysis showed that the stepwise process preserves more secondary structures of proteins. ECMs protein profile was analyzed as in Flores (Flores et al., 2016) and verified that it is the highly diverse and tissue-specific. Pericardium ECM has 94 different types of proteins, followed by tendon ECM (48) and bones ECM (35), being collagen α1(1) and collagen α2(1) present in all of them. Furthermore, the ECMp digested products enhanced bone marrow mesenchymal stem cells proliferation and differentiation in mature osteoblast. The kinetics of the gelification process, as well as mechanical properties of the gel is dependent of the type of crosslinker and concentration of gelatin. This new material is highly customizable and adaptable to the biological application

Desenvolvimento de biomateriais à base de quitosana: matriz de fibras eletrofiadas para regeneração tecidual e de hidrogel coacervado para entrega controlada de fármaco / Development of chitosan-based biomaterials: electrospun fiber matrix for tissue regeneration and coacervate hydrogel for controlled drug delivery

Os atuais avanços no desenvolvimento de biomateriais caminham para 2 áreas promissoras: a de regeneração tecidual e a de entrega controlada de fármacos. Assim, o presente estudo objetivou a síntese e caracterização de diferentes matrizes (fibras e hidrogel) à base de quitosana, a fim de se obter materiais biomiméticos para atuação em ambas áreas. Para regeneração, delineou-se a síntese de um arcabouço de fibras de quitosana com e sem cristais de nanohidroxiapatita onde, para isso, foram eletrofiadas soluções de quitosana (Ch) e de quitosana com nanohidroxiapatita (ChHa). Os espécimes de Ch apresentaram maior homogeneidade e maior diâmetro médio de fibras (690 ± 102 nm) que ChHa (358 ± 49 nm). No teste de viabilidade celular e na atividade da fosfatase alcalina não houve diferença estatística entre os grupos experimentais (Ch e ChHa), porém ambos diferiram do grupo controle (p < 0,001). Para o âmbito de liberação de fármacos, sintetizou-se, pela técnica de emulsão, dois tipos de hidrogéis: o primeiro, uma mistura da fase aquosa da solução de Ch (1 mL) e da solução de DNA (1 mL) (1:1) e o segundo, mistura da fase aquosa da solução de Ch (1 mL) e solução de Pectina (1 mL) (1:1). Ambas misturas foram realizadas em álcool benzílico (5 mL) com instrumento de dispersão de alto desempenho (31-34000 rpm min-1 por 5 min). Após a obtenção dos géis, 20mg de cada grupo foram imersos em uma solução aquosa de Própolis Verde (PV), na concentração de 70 µg/mL por 2 h e a cinética de liberação do PV foi analisada a 25 e 37oC em água e saliva artificial. Os espécimes obtidos foram liofilizados e depois caracterizados físicoquimicamente. A presença de pectina e de DNA foi comprovada por FTIR. A sorção de PV induziu uma modificação significativa da superfície do gel. Constatou-se uma separação de fases entre a quitosana e o DNA. A eficiência do encapsulamento não mudou significativamente entre 25 e 37oC. A cinética de liberação na água ou na saliva apresentou um mecanismo de duas etapas. E os resultados biológicos exibiram que esses materiais são aceitáveis no ambiente biológico. Assim, conclui-se que a matriz de fibras de quitosana com nHAp é capaz de promover diferenciação celular e a matriz de hidrogel de quitosana com Pectina ou DNA possui potencial para a liberação controlada de fármacos(AU)

Current advances in biomaterial development are moving to 2 promising areas: tissue regeneration and controlled drug delivery. Thus, the present study aimed the synthesis and characterization of different matrices (fibers and hydrogel) based on chitosan, in order to obtain biomimetic materials for performance in both areas. For regeneration, the synthesis of a scaffold of chitosan fibers with and without nanohydroxyapatite crystals was delineated, where chitosan (Ch) and chitosan with hydroxyapatite (ChHa) solutions were electrospun. Ch specimens presented higher homogeneity and larger mean fiber diameter (690±102nm) than ChHa (358 ± 49nm). In the cell viability test and alkaline phosphatase activity there was no statistical difference between the experimental groups. (Ch and ChHa), but both differed from the control group (p < 0,001). For the drug release scope, two types of hydrogels were synthesized by the emulsion technique: the first, a mixture of the aqueous phase of Ch solution (1 mL) and DNA solution (1 mL) (1:1) and the second, mixture of the aqueous phase of the Ch solution (1mL) and Pectin solution (1 mL) (1:1). Both mixtures were performed in benzyl alcohol (5 mL) with high performance dispersion instrument (31-34000 rpm min-1 for 5 min). After obtaining the gels, 20mg from each group were immersed in an aqueous solution of Propolis Green (PV), at a concentration of 70 µg/mL for 2 h and the release kinetics of PV were analyzed at 25 and 37oC in water and artificial saliva. The obtained specimens were lyophilized and then physically-chemically characterized. The presence of pectin and DNA was confirmed by FTIR. PV sorption induced a significant modification of the gel surface. A phase separation was found between chitosan and DNA. Encapsulation efficiency did not change significantly between 25 and 37oC. The release kinetics in water or saliva presented a two-step mechanism. And the biological results showed that these materials are acceptable in the biological environment. Thus, it is concluded that the nHAp chitosan fiber matrix is capable of promoting cell differentiation, whereas the chitosan hydrogel matrix with Pectin or DNA are potential biomaterials for controlled drug release(AU)

Acute toxicity study of a polysaccharide based hydrogel from linseed for potential use in drug delivery system

ABSTRACT Linseed hydrogel (LSH) was evaluated by acute toxicity for its potential application in oral drug delivery design. White albino mice and rabbits were divided in four groups (I-IV) and different doses of LSH (1, 2 and 5 g/kg body weight) were given except to the control group (I) that was left untreated. Rabbits were monitored for eye irritation, acute dermal toxicity and primary dermal irritation, whereas, body weight, food and water consumption, hematology and clinical biochemistry, gross necropsy and histopathology of vital organs were scrutinized in mice. LSH was considered safe after eye irritation test as no adverse signs or symptoms were seen in the eye. In dermal toxicity and irritation study, skin of treated rabbits was found normal in color without any edema or erythema. After oral administration, there was no sign of any abnormalities in treated group animals (II-IV). The hematology and clinical biochemistry of treated group animals was comparable with the control group. Histopathology of vital organs has not shown any lesion or abnormalities. In the light of these outcomes, it can be concluded that LSH is not a hazardous biomaterial and could be incorporated as an excipient in oral and dermal preparations.

A step into the RNA world: Conditional analysis of hydrogel formation of adenosine 5'-monophosphate induced by cyanuric acid.

Nucleotide polymerization occurs by the nucleophilic attack of 3'-oxygen of the 3'-terminal nucleotide on the α-phosphorus of the incoming nucleotide 5'-triphosphate. The π-stacking of mononucleotides is an important factor for prebiotic RNA polymerization in terms of attaining the proximity of two reacting moieties. Adenosine and adenosine 5'-monophosphate (AMP) are known to form hydrogel in the presence of cyanuric acid at neutral pH. However, we observed that other canonical ribonucleotides did not gel under the same condition. The π-stacking-induced hydrogel formation of AMP was destroyed at pH 2.0, suggesting that the protonation of N at position 1 of adenine abolished hydrogen bonding with the NH of cyanuric acid and resulted in the deformation of the hexad of adenine and cyanuric acid. A liquid-like gel was formed in the case of adenosine with cyanuric acid and boric acid, whereas AMP caused the formation of a solid gel, implying that the negative charge inherent to AMP prevented the formation of esters of boric acid with the cis-diols of ribose. Cyanuric acid-driven oligomerizations of AMP might have been the first crucial event in the foundation of the RNA world.

Hacking the Matrix.

Recently in Nature, Gjorevski et al. (2016) describe a fully defined synthetic hydrogel that mimics the extracellular matrix to support in vitro growth of intestinal stem cells and organoids. The hydrogel allows exquisite control over the chemical and physical in vitro niche and enables identification of regulatory properties of the matrix.

Improving the controlled delivery formulations of caffeine in alginate hydrogel beads combined with pectin, carrageenan, chitosan and psyllium.

Alginate-based blends consisting of carrageenan, pectin, chitosan or psyllium husk powder were prepared for assessment of the best formulation aimed at encapsulation of caffeine. Alginate-pectin blend exhibited the lowest viscosity and provided the smallest beads. Alginate-psyllium husk blend was characterised with higher viscosity, yielding the largest bead size and the highest caffeine encapsulation efficiency (83.6%). The release kinetics of caffeine indicated that the porosity of alginate hydrogel was not reduced sufficiently to retard the diffusion of caffeine from the beads. Chitosan coated alginate beads provided the most retarded release of caffeine in water. Morphological characteristics of beads encapsulating caffeine were adversely affected by freeze drying. Bitterness intensity of caffeine-containing beads in water was the lowest for alginate-psyllium beads and chitosan coated alginate beads. Higher sodium alginate concentration (3%) for production of hydrogel beads in combination with psyllium or chitosan coating would present the most favourable carrier systems for immobilization of caffeine.

Study of free volumes of polymer hydrogel and -silicone-hydrogel contact lenses by means of the positron annihilation lifetime spectroscopy method.

BACKGROUND: Polymer materials based on hydrogel and silicone-hydrogel materials are commonly used in ophthalmology. It is important to research the structure of these materials, mainly the prevalence of free volumes. OBJECTIVES: The study has been conducted in order to determine the presence of free volume gaps in the structure of polymer hydrogel and silicone-hydrogel contact lenses. In addition, to demonstrate differences in the occurrence of free volumes between types of represented contact lenses. MATERIAL AND METHODS: Three different hydrogel and three different silicone-hydrogel polymer contact lenses were used as research material. The study was done by means of positron annihilation lifetime spectroscopy (PALS). RESULTS: As a result of the performed measurements, a graphical curve resulted which describes the relationship between the number of the annihilation acts in the time function. The study revealed the existence of three τ1, τ2 and τ3 components. Significant changes were observed in the ortho-positronium long life component τ3 and their intensities between the examined polymer contact lenses. CONCLUSIONS: The conducted study using the Tao-Eldrup model indicates the presence of free volume holes in all research materials. The results lead to the following connection: contact lenses of higher oxygen permeability coefficient (silicone-hydrogel contact lenses) have more and larger free volumes than contact lenses of less oxygen permeability coefficient (hydrogel contact lenses).

Structural studies of polymer hydrogel and silicone hydrogel contact lenses by means of positron lifetime spectroscopy methods.

UNLABELLED: PURPOSE OF JOB: Currently, there isa need to increase comfort and visual acuity man. Simultaneously improving biocompatibility and minimizing the impact of the material on the physiology of the cornea is the primary driving force behind the evolution of materials used in the manufacture of contact lenses. Despite progressive development of modern materials science, there is still the problem of reducing the level of oxygen available to the cornea resulting in pathological changes in the cornea. Therefore, structural studies increases interesting in relating to the amorphous contact lenses polymeric materials. MATERIALS AND METHODS: The aim of this work is structural investigation of polymer hydrogel and silicone hydrogel contact lenses made in the technology of PC (Phosphoryl Choline). The study method was used positron lifetime spectroscopy PALS. RESULTS: As a result of the measurements obtained curve describing the dependence of the number of counts of acts of annihilation as a function of time. CONCLUSIONS: The study of PALS showed the existence of three components. Component tau1 is responsible for the annihilation of free positrons and the annihilation of electrons vacancy-type point defects. Component tau2 is associated with defects in the volume of grain boundaries formed, dislocations or clusters of vacancies. The results of calculations of mean values positron lifetime samples, showed longtime component tau3 in the spectrum of positron lifetime. Component tau3 is assigned to pick-off annihilation of ortho-positronium o-Ps trapping by free volume and providing information on the geometric parameters of the volume.

Preparation and characterisation of Dextran-70 hydrogel for controlled release of praziquantel

A hydrogel was developed from 70 kDa dextran (DEX-70) and praziquantel (PZQ) incorporated as a model drug. Biopharmaceutical properties, such as solubility and dissolution rate, were analysed in the design of the hydrogel. Furthermore, the hydrogel was also characterized by IR spectroscopy and DSC. Tests of the swelling rate showed that the hydrogel swelled slowly, albeit faster than the rate for the free polymer. In dissolution tests, the hydrogel released the drug slowly and continuously. This slow release was similar to that observed in the swelling tests and resulted in controlled release of the drug. Thus, this dextran is a suitable polymer for the development of hydrogels as vehicles for the controlled release of drugs.

Um hidrogel foi desenvolvido a partir de dextrano 70 kDa (DEX-70) e praziquantel incorporado (PZQ) como fármaco modelo. Propriedades biofarmacêuticas, como solubilidade e velocidade de dissolução, foram analisadas no desenvolvimento do hidrogel. Além disso, o hidrogel também foi caracterizado por espectroscopia na região do infravermelho e calorimetria diferencial exploratória (DSC). Testes da taxa de intumescimento mostraram que o hidrogel intumesce lentamente, embora tenha sido mais rápido do que a taxa do polímero livre. Nos testes de dissolução, o hidrogel liberou o fármaco lenta e continuamente. Esta liberação lenta foi semelhante a observada nos testes de intumescimento e resultou em uma liberação controlada do fármaco. Assim, o dextrano 70 kDa é um polímero adequado para o desenvolvimento de hidrogéis como veículos para a liberação controlada de fármacos.

Formulation of a novel oxybenzone-loaded nanostructured lipid carriers (NLCs).

The objective of the current study was to formulate oxybenzone into nanostructured lipid carriers (NLCs) to enhance its sunscreening efficacy and safety. NLCs of oxybenzone were prepared by the solvent diffusion method. A complete 2(3) factorial design was used for the evaluation of the prepared oxybenzone NLCs. The study design involves the investigation of the effect of three independent variables namely liquid lipid type (Miglyol 812 and oleic acid), liquid lipid concentration (15% and 30%), and oxybenzone concentration (5% and 10% with respect to total lipids) on the particle size (p.s.) , the entrapment efficiency (EE%) and the in vitro drug release after 8 h. The prepared NLCs were spherical in overall shape and were below 0.8 microm. Miglyol 812 and 30% liquid lipid were found to significantly decrease the p.s. and increase the EE% when compared to oleic acid and 15% liquid lipid. Increasing oxybenzone concentration increased significantly the p.s. but did not affect the EE%. NLCs prepared using Miglyol 812, 15% liquid lipid, and 10% oxybenzone showed slower drug release when compared to those prepared using oleic acid, 30% liquid lipid, and 5% oxybenzone, respectively. The candidate oxybenzone-loaded NLC dispersion was then formulated into gel. The incorporation of oxybenzone into NLCs greatly increased the in vitro sun protection factor and erythemal UVA protection factor of oxybenzone more than six- and eightfold, respectively, while providing the advantage of overcoming side effects of free oxybenzone as evidenced by very low irritation potential.

A three-phase in-vitro system for studying Pseudomonas aeruginosa adhesion and biofilm formation upon hydrogel contact lenses.

BACKGROUND: Pseudomonas aeruginosa is commonly associated with contact lens (CL) -related eye infections, for which bacterial adhesion and biofilm formation upon hydrogel CLs is a specific risk factor. Whilst P. aeruginosa has been widely used as a model organism for initial biofilm formation on CLs, in-vitro models that closely reproduce in-vivo conditions have rarely been presented. RESULTS: In the current investigation, a novel in-vitro biofilm model for studying the adherence of P. aeruginosa to hydrogel CLs was established. Nutritional and interfacial conditions similar to those in the eye of a CL wearer were created through the involvement of a solid:liquid and a solid:air interface, shear forces and a complex artificial tear fluid. Bioburdens varied depending on the CL material and biofilm maturation occurred after 72 h incubation. Whilst a range of biofilm morphologies were visualised including dispersed and adherent bacterial cells, aggregates and colonies embedded in extracellular polymer substances (EPS), EPS fibres, mushroom-like formations, and crystalline structures, a compact and heterogeneous biofilm morphology predominated on all CL materials. CONCLUSIONS: In order to better understand the process of biofilm formation on CLs and to test the efficacy of CL care solutions, representative in-vitro biofilm models are required. Here, we present a three-phase biofilm model that simulates the environment in the eye of a CL wearer and thus generates biofilms which resemble those commonly observed in-situ.

Enhanced Overhauser contrast in proton-electron double-resonance imaging of the formation of an alginate hydrogel.

Proton-electron double-resonance imaging (PEDRI) was recently employed to monitor the process of formation of a calcium alginate hydrogel at a field of 16mT. Here, under the same experimental conditions, images obtained through this technique are compared to images obtained by conventional T(2)-weighted method. The results confirm that the image contrast obtained using PEDRI, thanks to the Overhauser effect, exhibits an improved sensitivity with respect to changes in water mobility as previously suggested in the literature. Furthermore, by increasing the echo time interval for the T(2)-weighted images, important features of the gelling dynamics obtained via PEDRI could not be reproduced.

Characterisation of the internal and external surfaces of four types of Foley catheter using SEM and profilometry.

Unfortunately the use of Foley catheters for long-term catheterisation is frequently associated with complications such as infection and encrustation. This study investigated whether a link could exist between the surface properties of the catheters and the problems that can develop. The internal and external surfaces of four different types of urinary catheter were examined. Three latex devices coated with either PTFE or hydrogel or surface treated with silicone were investigated. In addition, an all-silicone device was examined. The surfaces of the all-silicone catheters were relatively smooth and featureless. In contrast, the external surfaces of each of the latex devices were 'paved' in nature. The internal surfaces of latex based devices produced by different manufacturers showed distinct differences with evidence of inorganic inclusions on the internal surfaces of two of the catheter types. These findings may be significant in the context of catheter infection and encrustation.

How does the type of vehicle influence the in vitro skin absorption and elimination kinetics of terpenes?

Terpenes are widely used in the topical dermal preparations, cosmetics and toiletries and also in the experimental dermopharmacy, as penetration enhancers. Terpenes do not need to penetrate into viable skin tissue and this event is not even desired. The aim of this study was to investigate skin absorption and elimination kinetics of two terpenes, namely linalool and terpinen-4-ol, incorporated in three different dermatological vehicles: oily solution, hydrogel and o/w emulsion. The preparations were applied onto the human skin in vitro, and after 1-4 h the content of terpenes in the stratum corneum layers and in the epidermis/dermis was determined using GC. Similarly, the amounts of terpenes in the skin were analysed during 4 h elimination process following 1 h absorption. The highest skin absorption was observed when terpenes were applied in hydrogel--their total content in the skin after 4 h was 385 and 705 microg/cm2 for linalool and terpinen-4-ol, respectively. After 1 h of the elimination process about 10-20% drop of the total content of both terpenes in the skin was noted for all formulations. The skin penetration of both terpenes from the vehicles is increasing in the following order: emulsion < oily solution < hydrogel, while the elimination phase is relatively slower for terpenes applied in hydrogel.

Autonomic neuropathy may be associated with delayed orocaecal transit time in patients with cirrhosis.

UNLABELLED: Orocaecal transit (OCT) time is delayed in patients with cirrhosis, but the reasons for this remain unclear. We hypothesized that autonomic neuropathy (AN) may explain the delay in OCT. METHODS: We determined OCT and autonomic function tests (AFT) in 48 patients (Child A-15, B-27, C-6) with cirrhosis of various aetiologies. AFT were categorized as normal, borderline, or abnormal. OCT was measured using the lactulose hydrogen (H2) breath test. OCT was defined as the time from baseline when there was a rise in H2 levels of >20 ppm over baseline or >10 ppm over baseline sustained over 2 consecutive time points. RESULTS: Based on OCT, patients were separated into those with delayed OCT (>90 min, group I) and normal OCT (< or = 90 min, group II). Mean OCT time of patients in group I was 169.7+/-49.7 min vs. 84.4+/-12.1 min in group II. Baseline clinical characteristics of patients with and without AN, and those with normal and delayed OCT were similar. Presence of mild encephalopathy did not have an effect on OCT. AN was seen more frequently in group I than group II [16/32 (50%) vs. 3/16 (19%), p=0.03]. Logistic regression analysis showed that the presence of AN was the only independent variable associated with delayed OCT (OR 7.3, CI 1.3-39.4, p=0.02). CONCLUSION: Our study showed that the presence of AN was associated with delayed OCT in patients with cirrhosis.