Efeito antimicrobiano residual e citotoxidade in vitro de resina acrílica para base de prótese após imersão prolongada em agentes de limpeza / In vitro residual antimicrobial effect and cytotoxicity of acrylic resin base prosthesis after long-term immersion in cleaning agents

Andréa Lemos Falcão Procópio

15 May 2015

O presente estudo in vitro objetivou avaliar a longo prazo o potencial antimicrobiano residual e a citotoxicidade de soluções químicas de limpeza de prótese quando incorporadas à resina acrílica termopolimerizável após sucessivos ciclos de imersão noturna diária. Discos (10mm x 1mm) de resina acrílica termopolimerizável para base de prótese (Lucitone 550) foram submetidos a três ciclos diários de desinfecção (8h/cada) em hipoclorito de sódio a 1% (NaClO), digluconato de clorexidina a 2% (CLX) ou água destilada (controle) durante 91 (T91) ou 183 dias (T183), simulando o período de 9 meses ou 1,5 ano de imersão noturna diária realizada pelo paciente. Inicialmente, foi utilizado o método de concentração inibitória mínima em caldo para determinar o possível efeito residual (incorporação) das soluções à resina acrílica. Metade dos discos imersos em cada agente de limpeza em um dos tempos de imersão (n=5) foi inoculada (1x107cels/mL) com um dos patógenos associados à estomatite protética: Candida albicans (Ca) e Staphylococcus aureus (Sa). Os discos foram incubados a 37oC para análise em espectrofotômetro após 24h, 7 e 14 dias. Os valores de absorbância foram convertidos em porcentagens de inibição microbiana. Confirmada a ação antimicrobiana residual dos agentes de limpeza incorporados à resina acrílica, foi então analisada sua citotoxicidade in vitro sobre fibroblastos gengivais humanos (L929). Os efeitos citotóxicos foram avaliados por meio do ensaio colorimétrico MTT [brometo de 3-(4,5-dimetiltiazol-2-yl)-2,5-difeniltetrazólio] para a determinação da viabilidade celular, após as células serem expostas por 24h às amostras de cada condição experimentais (n=18) previamente imersas em uma das soluções por um dos períodos avaliados (T91 ou T183). A citotoxicidade foi determinada com base na atividade mitocondrial em relação a corpos de prova não submetidos à imersão nas soluções testadas. Os resultados do ensaio do MTT foram analisados estatisticamente por ANOVA-1 fator seguida pelo teste post-hoc de Tukey HSD (a=0,05). Para os períodos T91 e T183, não houve inibição microbiana com a imersão em água (controle) em até 14 dias de incubação. A CLX inibiu progressivamente o crescimento microbiano ao longo dos 14 dias para ambos os períodos de imersão (Ca: 19 a 73,58%; Sa: 0 a 87,08%), sendo observada maior ação antimicrobiana em T183. O NaClO apresentou discreta inibição microbiana apenas no período de 14 dias tanto em T91 (Ca: 0%; Sa: 2,70%) quanto em T183 (Ca: 8,50%; Sa: 15,08%). De acordo com os resultados do teste de MTT, as soluções químicas de limpeza testadas apresentaram uma redução significativa da viabilidade celular quando comparado às células controles propagadas apenas em meio de cultura (p<0,002). A CLX resultou na menor viabilidade celular em ambos os períodos de imersão (p<0,018). As amostras de resina acrílica imersas em água ou NaClO em T91 e T183 apresentaram viabilidade celular estatisticamente similar às amostras não imersas (p>0,05). Pode-se concluir que a CLX incorporada à resina acrílica para base de prótese apresentou um efeito antimicrobiano residual em ambos os períodos de imersão noturna, o que não foi observado com o NaClO. Por outro lado, a CLX residual resultou em efeito intensamente citotóxico aos fibroblastos gengivais humanos quando comparada ao NaClO e à agua destilada, que se apresentaram discretamente citotóxicos. Esses resultados sugerem precaução na seleção de agentes de limpeza para prótese como meio de prevenção e tratamento adjunto da estomatite protética, pois mesmo em concentrações baixas, recomendadas para imersão noturna, podem apresentar algum grau de toxicidade às mucosas de suporte protético. / This in vitro study aimed to evaluate the long-term residual antimicrobial activity and cytotoxicity of chemical denture cleansers incorporated into a heat-polymerized acrylic resin after successive cycles of daily overnight soaking. Discs (10mm x 1mm) were prepared from heat-polymerized acrylic resin (Lucitone 550) and submitted to three daily immersion (8h/each) in 1% sodium hypochlorite (NaClO), chlorhexidine digluconate 2% (CHX) or distilled water (control) for 91 days (T91) or 183 days (T183), simulating the period of 9 months or 1.5 year of nocturnal immersion performed by the patient. Initially, the method of minimum inhibitory concentration in broth was used to determine the possible residual effect (incorporation) of the acrylic resin solution. Half of the disks immersed in each cleaning agent for one of the period immersion (n=5) was inoculated (1x107cells/mL) with pathogens associated with denture stomatitis: Candida albicans (Ca) or Staphylococcys aureus (Sa). The disks were incubated at 37oC for analysis in a spectrophotometer after 24h, 7 and 14 days. The absorbance values were expressed as percentages of microbial inhibition. Confirmed the residual antimicrobial action of cleaning agents incorporated into the acrylic resin, its cytotoxicity was analyzed in vitro on human gingival fibroblasts (L929). Cytotoxic effects were evaluated by the colorimetric assay MTT [3- (4,5- dimethylthiazol-2-yl) -2,5-diphenyl tetrazolium bromide] to determine cellular viability after the cells were exposed for 24h to the samples of each experimental condition (n=18) previously immersed in one of the solutions for the evaluation periods (T91 or T183). Cytotoxicity was determined based on mitochondrial activity compared to the specimens not subjected to immersion in the solutions. The MTT assay results were 1-way ANOVA followed by Tukey\'s HSD post-hoc test (a=0.05). For the periods T91 and T183, no microbial inhibition was observed with immersion in water (control) for up to 14 days of incubation. The CHX progressively inhibited microbial growth over the 14 days for both immersion times (Ca: 19 to 73.58%, Sa: 0 to 87.08%); with greater antimicrobial activity in T183. The NaClO showed a slight microbial inhibition only in the 14-day period in both T91 (Ca: 0%; Sa: 2.70%) and T183 (Ca: 8.50%; Sa: 15.08%). According to the results of the MTT assay, the chemical cleaning solutions tested showed a significant reduction in cell viability when compared to the control cells propagated in normal culture medium (p<0.002). The CHX resulted in the lowest cell viability in both immersion periods (p<0.018). The acrylic samples immersed in water or NaClO in T91 and T183 showed cell viability statistically similar to nonimmersed samples (p>0.05). CHX incorporated into the acrylic resin denture base had a residual antimicrobial effect on both immersion periods, which was not observed with NaClO. On the other hand, the residual CHX were severely cytotoxic to human gingival fibroblasts compared to NaClO and distilled water which were slightly cytotoxic. These results suggest caution in selecting denture cleaning agents as a method of prevention and adjunct treatment of denture stomatitis because even at low concentrations recommended for overnight immersion, they may exhibit some degree of toxicity to the denture bearing mucosa.

Clorexidina

Estomatite sob prótese

Higienizadores de dentadura

Hipoclorito de sódio

Prótese total

Teste de biocompatibilidade

Toxicidade

Biocompatibility testing

Chlorhexidine

Complete denture

Denture cleansers

Denture stomatitis

Sodium hypochlorite

Toxicity

Análise da expressão gênica do FOXP3, MIP-3? e Interleucinas 2, 10 e 35 em pacientes com ulceração aftosa recorrente / Analysis of gene expression of FOXP3, MIP-3? and interleukins 2, 10 and 35 in patients with recurrent aphthous ulcers

Érica Fernanda Patricio da Silva

16 November 2015

A ulceração aftosa recorrente (UAR) é considerada a doença ulcerativa mais frequente da cavidade bucal. Sua etiopatogenia ainda não está plenamente esclarecida, embora inúmeros fatores locais e sistêmicos já tenham sido a ela associados. Recentemente, a resposta imune anormal do tipo celular tem sido considerada a responsável pela lesão bucal na UAR, favorecendo uma resposta imunológica pró-inflamatória do tipo Th1, em conjunto com alterações em linfócitos T regulatórios. Sendo assim, o objetivo do presente estudo foi realizar análise da expressão gênica da FOXP3, MIP-3? e Interleucinas 2, 10 e 35 em pacientes com ulceração aftosa recorrente, por meio de estudo caso-controle. Os pacientes do grupo caso apresentavam quadros frequentes de UAR com pelo menos um ano de manifestação de surtos ulcerativos e história negativa de condições sistêmicas ou locais interferentes com a expressão das UAR. Estes foram submetidos a biópsia de lesão ulcerativa recente para a análise molecular. Os pacientes do grupo controle apresentavam história negativa de UAR, mucosa clinicamente saudável, e doaram voluntariamente fragmento de mucosa saudável para análise molecular, quando submetidos a procedimentos cirúrgicos como exodontia de terceiros molares ou biópsias ósseas. Todos os pacientes foram incluídos no grupo de pesquisa apenas após anuência com termo de consentimento livre e esclarecido. Submeteram-se a exame clínico, realizaram exames complementares para controle da saúde geral e suporte diagnóstico. Onze pacientes UAR e três controles voluntários compuseram a casuística estudada, sendo submetidos a biópsia de lesões de UAR ou de mucosa de revestimento sadia. As amostras de tecido bucal foram submetidas aos procedimentos laboratoriais de extração do RNA e análise da expressão gênica da FOXP3, MIP-3? e Interleucinas 2, 10 e 35 por meio da técnica de RT-PCR em tempo real. Não houve diferença significativa na expressão dos genes estudados entre as amostras de portadores de UAR e controles sadios. Concluímos que os genes aqui avaliados não parecem desempenhar papel distintivo na fase ulcerativa inicial das UAR, entretanto estudos adicionais são recomendados a fim de se verificar a real participação desses agentes da inflamação na expressão da doença. / Recurrent aphthous ulcers (RAU) is the most common ulcerative disease of the oral cavity. Its pathogenesis is poorly understood yet, although numerous local and systemic factors have been associated with it. Recently, abnormal immune response of cellular type has been considered responsible for the RAU oral lesions, promoting a pro-inflammatory immune response Th1-type, in conjunction with changes in regulatory T cells. Thus, the aim of this study was to analyze the gene expression of FOXP3, MIP-3? and interleukins 2, 10 and 35 in patients with recurrent aphthous ulceration through a case-control study. The case group of patients presented frequent RAU bouts with at least one year of manifestation of ulcerative outbreaks and negative history of local or systemic conditions interfering with the RAU expression. These patients were submitted to a biopsy procedure of a recent ulcerative lesion for molecular analysis. Patients in the control group presented no history of RAU, and agreed with a donation of a healthy mucosa fragment for molecular analysis when undergoing surgical procedures such as extraction of third molars or bone biopsies. All patients were included in the research group only after agreement with an informed consent. All subjects underwent clinical examination and were submitted to additional lab tests to check overall health and support diagnosis. Eleven RAU patients and three control volunteers composed the sample size and undergone biopsy of RAU lesions or healthy mucosal lining. The oral tissue samples were submitted to the laboratory procedures of RNA extraction and analysis of gene expression of FOXP3, MIP-3? and interleukins 2, 10, 35 by real time RT-PCR. There was no significant difference in gene expression between the studied samples of patients with RAU and healthy controls. It was concluded that the genes evaluated do not seem to play distinctive role in the initial ulcerative phase of RAU, however further studies are recommended in order to verify the actual participation of these inflammation agents in RAU expression.

citocinas

e PCR em tempo real

estomatite aftosa

IL-10

IL-2

interleucinas

quimiocinas

and real time PCR

aphthous stomatitis

chemokines

cytokines

IL-10

IL-2

interleukins

Isolamento de espécies de Candida em pacientes com Candidíase Atrófica Crônica e atividade antimicrobiana de duas espécies de Mikania / Isolation of Candida species from patients with Chronic Atrophic Candidiasis and antimicrobial activity of two species of Mikania

Lund, Rafael Guerra

15 May 2008

Made available in DSpace on 2014-08-20T14:30:12Z (GMT). No. of bitstreams: 1 tese_Rafael_Guerra_Lund.pdf: 8802929 bytes, checksum: ef093a1950314ad988093579ba1a09db (MD5) Previous issue date: 2008-05-15 / A great variety of diseases can affect the oral cavity, such as dental caries and candidosis, being the first one considered the most prevalent oral diseases worldwide. The multifactorial and infect-contagious characteristics of dental caries has been established, associated with resident bacterial pathogens of dental biofilm. These microorganisms are responsible by the production of acids and citotoxic products, which could promote the demineralization of dental structure. Currently, Candida infections constitute an important problem in Public Health. Such findings is basically due to the technological advancements of Medicine, increasing in AIDS infection and immune depressed patients in general, using prolonged antimicrobials therapies, which contributes to the microbial disequilibrium. Therefore, the use of efficient antimicrobial agents against pathogenic bacteria and yeasts is an important tool in the control of these infective diseases. Several natural antimicrobial agents are been investigated because of their possible pharmacological properties. Plants of genus Mikania are pointed out as natural products with noticeable antibacterial, antifungicidal, anti-inflammatory and antineoplasic properties. In this study the potential effect of two Mikania species was evaluated (Mikania glomerata Mg e Mikania hirsutissima Mh) using their crude ethanol extracts, based on the ethnobotanics (popular knowledge) and the literature. The test against mutans streptococci was assessed by the determination of Minimum Inhibitory Concentration (MIC), Minimum Bactericidal Concentration (MBC) and inhibition of cell adherence to a glass surface (Adh). Also during a period of one year denture wearer patients with lesions compatible with Chronic Atrophic Candidiasis and assisted in the Center of Diagnosis of Mouth Diseases (CDMD), were investigated. It was applied a questionnaire a questionnaire including the identification of the subject, demographic, medical history and behaviour (oral hygiene and prosthesis wear). It also was carried out a intra-oral exam, where appearance and extension of the stomatitis lesion were evaluated. The microbiological collect was carried out frictioning sterilized swabs in the palate s mucosa, tongue or both of them. The samples were seeded in Agar Sabouraud Dextrose with 100mg/mL of chloramphenicol and they were incubated at 37oC for 24-48h. The presumptive identification of Candida species was based on the morphologic characteristics, Gram colorization of the yeasts, microculture test, hypertonic broth test and it was confirmed by the CHROMagar. The MIC against Streptococcus mutans UA159 was 44.45 Lg/mL (Mg) and 88.90 Lg/mL (Mh), and the MBC was 88.90 Lg/mL (Mh). Against Streptococcus sobrinus 6715, the MIC was 22.23 Lg/mL (Mh) and 88.90 Lg/mL (Mg), and the MBC was 177.80 Lg/mL (Mh). The celular adherence also was inhibited at concentrations of 20 Lg/mL(Mh) and 40 Lg/mL (Mg). These results provide promising baseline information for the potential use of two species of Mikania against mutans streptococci. These findings warrant more-in-depth studies of the active principles of this Mikania ethanol extracts. With regard to Candida isolation with clinical diagnosis of Chronic Atrophic Candidiasis: 1)the results did not confirm a significant difference between patients with clinical diagnosis of denture stomatitis concerning the presence or absence of yeasts; 2) the occurrence of Candida in patients with clinical diagnosis of Chronic Atrophic 6 Candidiasis was negatively related to important factors associated to this opportunistic infection; and 3) mycological findings from the present study do not indicate that the covariates investigated have a significant effect on oral infection by Candida albicans or other species of Candida genus / Uma variedade de doenças envolve a cavidade oral, dentre elas, a cárie dental e a candidíase, sendo que a primeira é considerada a mais prevalente em todo o mundo. Atualmente está bem estabelecido que cárie dental é uma doença multifatorial infecto-contagiosa associada a bactérias patogênicas residentes do biofilme dental. Estes microrganismos são os responsáveis pela produção de ácidos que levam à desmineralização do esmalte dental. As infecções por Candida consistem atualmente num problema de Saúde Pública. Isto se deve ao aumento de casos da Síndrome da Imunodeficiência Adquirida (AIDS) e de hospedeiros imunodeprimidos de modo geral, bem como ao tratamento prolongado com antibacterianos o que contribui para o desequilíbrio da microbiota. Assim, o uso de agentes antimicrobianos eficientes contra bactérias e leveduras é um importante meio de controle destas infecções bucais. Vários agentes antimicrobianos de origem natural estão sendo investigados devido as suas possíveis propriedades farmacológicas. As plantas do gênero Mikania, conhecidas popularmente como guaco , destacam-se entre os produtos naturais com notáveis propriedades antibacterianas, antifúngicas, antiinflamatórias e antineoplásicas. Neste estudo foram avaliados extratos etanólicos brutos de duas espécies de Mikania (Mikania glomerata Mg e Mikania hirsutissima Mh)que foram pré-selecionadas com base na etnobotânica (conhecimento popular) e levantamento bibliográfico sobre as espécies a serem estudadas e suas congêneres. O teste foi realizado em Streptococcus do grupo mutans através da determinação da Concentração Inibitória Mínima (MIC), Concentração Bactericida Mínima (MBC) e inibição da aderência em superfície de vidro (Adh). Durante o período de um ano também foram estudados os pacientes usuários de prótese com lesões compatíveis com Candidíase Atrófica Crônica (CAC) encaminhados ao Centro de Diagnóstico de Doenças da boca. Foi aplicado um questionário para cada paciente, com informações referentes à sua identificação, dados demográficos, história médica e comportamento (hábitos de higiene e uso da prótese). Também foi realizado o exame intra-oral, onde eram avaliadas as variáveis: aparência e extensão da lesão de estomatite. A coleta microbiológica foi realizada com a fricção de swab estéril na mucosa com lesão compatível com CAC. Estas amostras foram semeadas em Agar Sabouraud Dextrose com 100mg/mL de cloranfenicol e incubadas a 37oC por 24-48h. A identificação presuntiva de espécies de Candida foram baseadas nas caracterísiticas macro e micromorfológicas, realização de microcultivo, teste em caldo hipertônico e CHROMagar. A maioria dos casos de CAC apresentou isolamento da levedura. As lesões de CAC foram mais frequentes em mulheres, com prótese total com uso há mais de 10 anos. A CIM frente a Streptococcus mutans UA159 foi 44,45Lg/mL (Mg) e 88,90Lg/mL (Mh), e a CBM foi 88,90Lg/mL (Mh). Frente a Streptococcus sobrinus 6715, a CIM foi 22.23Lg/mL (Mh) e 88,90Lg/mL (Mg), e a CBM foi 177,80 Lg/mL (Mh). A aderência celular também foi inibida em concentrações de 20Lg/mL(Mh) e 40Lg/mL (Mg). Estes resultados são informaçãoes de base para o uso potencial das duas espécies de Mikania contra Streptococcus do grupo mutans, necessitando outros estudos envolvendo os princípios ativos do extrato alcoólico de Mikania. 4 Quanto ao isolamento de Candida em pacientes com diagnóstico clínico de Candidíase Atrófica Crônica: 1) os resultados não confirmam uma diferença significante em pacientes com diagnóstico clínico de estomatite por dentadura com relação à presença ou ausência da levedura; 2) a ocorrência de Candida em pacientes com diagnóstico clínico de Candidíase atrófica Crônica foi negativamente relacionado a importantes fatores associados a esta infecção oportunista; e 3) os achados micológicos do presente estudo não indicaram queas variáveis investigadas tinham um efeito significativo na infecção oral por Candida albicans ou outras espécies do gênero Candida.

Fitoterapia

Agentes antimicrobianos

Candidíase oral

Estomatite por dentadura

Candida

Cárie

Phytoterapy

Antimicrobial agents

Oral candidiasis

Denture stomatitis

Candida sp

Caries

CNPQ::CIENCIAS DA SAUDE

TARGETING DNA DAMAGE AND REPAIR TO OVERCOME THERAPY MEDIATED TUMOR IMMUNE EVASION AND HETEROGENEITY IN THE CONTEXT OF ONCOLYTIC VIRUS VACCINATION

Kesavan, Sreedevi

January 2021

Due to the inevitable reality that most patients diagnosed with cancer will eventually relapse, modern oncology research has been forced to tackle this outcome primitively using combination therapies. Adoptive T-cell transfer with Oncolytic Virus Vaccination represents a new class of combination therapies that can facilitate the crosstalk of multiple aspects of the immune system such that they work in concert to prevent this outcome for many types of cancer. Despite this, immunosuppressive systems like those characterized in the B16F10-gp33 melanoma model pose a new problem for this approach. Typically, this model has total regression but is subsequently followed by relapse. Previous work from the Wan lab has suggested that this may be an outcome of total target gene deletion. Here we present two approaches to tackle this through the targeting of DNA repair pathways of the host cell. Our data can show that both VSV and Vaccinia infection/ propagation does lead to the generation of DNA damage but in the case of VSV this leads to incomplete cell lysis, and ultimately target gene loss via double-stranded DNA repair mechanisms. We were able to tackle the phenomenon following VSV administration by adding DNA repair inhibitors to the mix and showed that the proportion of cells that escaped after the loss of the target antigen was decreased by half when compared to the standard procedures. Additionally, this work also gave a preliminary understanding of how Vaccinia may achieve a similar outcome to this via its unique cytoplasmic replication mechanisms. / Thesis / Master of Science (MSc)

VSV

Vaccinia

DNA Damage

DNA Repair

ACT

OV

Combination Therapy

Oncolytic Virus Vaccines

Mirin

AZD7648

B16F10

Vesicular Stomatitis Virus

Melanoma

DNA Repair Inhibition

MS-275 (ENTINOSTAT) PROMOTES SUSTAINED TUMOR REGRESSION IN THE CONTEXT OF BOOSTING ONCOLYTIC IMMUNOTHERAPY

Nguyen, Andrew

10 1900

<p>We showed previously that histone deacetylase (HDAC) inhibition with MS-275 in the context of boosting oncolytic immunotherapy can drive heightened antitumor responses, leading to increased survival in mouse intracranial melanoma models. However, it is currently unclear how the co-administration of MS-275 directly impacts tumor growth. Here, we investigated the role of MS-275 in preventing the outgrowth of antigen-deficient tumor variants as a result of suboptimal treatment protocols. By adoptively transferring tumor antigen-specific memory T cells (Tm) that were expanded <em>in vivo</em> with recombinant Vesicular Stomatitis Virus (VSV-gp33), we observed complete regression of 5-day old, intradermal B16-gp33 tumors (B16-F10 overexpressing the LCMV GP33-41 epitope); however, the tumors relapsed within a month of treatment. Relapsing tumor explants were able to grow in mice that were prophylactically immunized with recombinant Adenovirus (Ad-gp33), indicating that the tumor could no longer be recognized. Strikingly however, there was zero tumor recurrence if MS-275 was co-administered with Tm and VSV-gp33, suggesting that MS-275 may prevent the emergence and/or escape of antigen loss variants. Such a benefit is lost if the administration of the drug is delayed as little as five days post VSV treatment, suggesting that its synergistic effects coincide with early immune responses and oncolytic activity. Furthermore, transplantation studies of relapsing tumor explants showed that combination treatment was unable to provide tumor protection, confirming that the mechanisms by which MS-275 prevents tumor recurrence are unlikely through direct up-regulation of antigen presentation in low- or non-antigen-expressing variants <em>in vivo</em>. Indeed, CD4 depletion in the absence of MS-275 resulted in sustained tumor regression, implying that immunoregulatory cells such as CD4+ Treg play a prominent role in sustaining tumor regression. Moreover, MS-275 modulates the phenotypic status of tumor-infiltrating MDSCs toward the differentiation of inflammatory macrophages. Taken together, the data suggests that combination therapy with HDACi with oncolytic immunotherapy mediates a synergized immune attack against the tumor through subversion of immunomodulatory mechanisms.</p> / Master of Science in Medical Sciences (MSMS)

oncolytic immunotherapy

vesicular stomatitis virus (VSV)

adoptive transfer therapy

histone deacetylase inhibitor (MS-275)

regulatory T cells (Tregs)

myeloid-derived suppressor cells (MDSCs)

Medical Immunology

Medical Immunology

L'étude des effets des estrogènes sur la virothérapie du cancer du sein

Paradisis, Stamatios

08 1900

Le cancer est une maladie qui touche des millions de personnes et ne discrimine pas. La forme de cancer la plus répandue chez les femmes au Canada est le cancer du sein et la deuxième cause de décès par le cancer chez cette population. Les traitements dépendent de plusieurs facteurs dont le stade du cancer, la ménopause, le statut des récepteurs hormonaux et du récepteur HER2 du cancer, etc. Les traitements qui existent sont la chirurgie suivie par la radio- et/ou chimiothérapie et l’hormonothérapie. Malgré les nombreuses études et les avancées dans les traitements pour différents cancers, plusieurs patients ont des cancers du sein qui sont réfractaires aux traitements disponibles. Une alternative naissante est l’utilisation de virus oncolytiques, c’est-à-dire des virus qui ciblent spécifiquement les cellules cancéreuses et laissent intact les cellules saines. Malheureusement, certains cancers demeurent réfractaires aux traitements avec virus oncolytiques. Ceci nous amène donc à regarder plus en détail des facteurs de l’environnement tumoral qui pourraient prédire la susceptibilité virale et engendrer des résultats positifs. C’est dans cette perspective que nous avons découvert que l'estrogène, précisément l’estradiol, rend les cellules cancéreuses qui en expriment le récepteur plus sensible au virus oncolytique VSV (virus de la stomatite vésiculaire). Cependant, nous ignorons toujours si d’autres hormones peuvent également moduler l’action de VOs. Nous émettons donc l’hypothèse que, comme l’estrogène, d’autres hormones vont affecter l’efficacité des VOs et qu’il serait possible de manipuler ces interactions pour améliorer la réponse au traitement. Notre étude nous permettra de concevoir des stratégies thérapeutiques améliorées pour les patients atteints du cancer du sein. L’importance de cette étude est que jusqu’à présent l’impact des hormones sur l’efficacité des virus oncolytiques reste un sujet inexploré. Nous allons déterminer l’effet de différents niveaux d’hormones sur la réplication et l’effet oncolytique de VSV. Ceci nous donnera ainsi la possibilité et les connaissances d’améliorer la sélection des patients pour le traitement et la conception d’une nouvelle génération de virus oncolytiques perfectionnés. / Cancer is a disease that affects millions of people across the world. The most common cancer in Canadian women is breast cancer and it also represents the second cause of death by cancer in this same group. The treatment depends on multiple factors including the stage of the cancer, menopause status, hormone receptor status, HER2 receptor status, etc. The available treatments for breast cancer are surgery followed by either radiation or chemotherapy as well as endocrine therapy. Despite numerous studies and advances in the treatment of different cancers, many patients’ cancer still remains refractory to these treatments. An exciting new alternative treatment is the use of oncolytic viruses. An oncolytic virus is a virus that can specifically target cancer cells all while leaving healthy normal cells intact. However, many cancers remain refractory to treatment with oncolytic viruses. There was thus a need to investigate different factors or the tumor microenvironment that may predict viral susceptibility and obtain positive outcomes. In this vein, it was found that estrogen (specifically estradiol), a hormone found in the body, can render cancer cells that express its receptor more sensitive to oncolytic virus infection by VSV (vesicular stomatitis virus). In spite of that, we are unaware if there are other hormones capable of modulating the actions of oncolytic viruses. Our hypothesis is that, like estrogen, other hormones will affect the efficacy of oncolytic viruses and that it will be possible to manipulate these interactions with the goal to improve treatment response. Our research will allow the conception of enhanced therapeutic strategies for patients with breast cancer. The importance of this study is that as of now the interplay between hormones and oncolytic viruses remains unexplored. We will determine the effects of hormone levels on viral replication and oncolytic ability of VSV. This knowledge will allow for a greater selection of patients for which oncolytic virus treatment will have a positive outcome. Additionally, it will allow for the development of a new generation of perfected oncolytic virus platforms.

Cancer du sein

Estrogène

Virus oncolytique

VSV

Estradiol

Hormones

Microenvironnement tumoral

Breast cancer

Estrogen

Oncolytic virus

Vesicular stomatitis virus

Estradiol

Immunology / Immunologie (UMI : 0982)

A randomized follow-up study of the general health and quality of life of an elderly edentulous population wearing either mandibular two-implant overdentures or conventional dentures

Emami, Elham

12 1900

L’augmentation de la population âgée dans la société indique que les systèmes de soins de la santé font face à de nouveaux défis. Les hauts niveaux d’incapacité qui en résultent peuvent être réduits par les nouvelles technologies, la promotion de la santé ainsi que des stratégies de prévention. Les écrits scientifiques récents soulignent la supériorité des prothèses dentaires implanto-portées par rapport aux prothèses conventionnelles en termes de satisfaction et de qualité de la vie des patients. Cependant, il n'est toujours pas clair si ces avantages ont des effets positifs à long terme sur la santé orale et générale ainsi que sur la qualité de vie des populations âgées. Objectifs, Hypothèses : Notre but était de mesurer l’impact des prothèses mandibulaires retenues par 2 implants sur la qualité de vie associée à la santé bucco-dentaire et générale ainsi que sur la santé orale et la qualité du sommeil des aînés édentés. Nous avons évalué les hypothèses nulles suivantes : il n'y a aucune différence entre les individus portants des prothèses mandibulaires retenues par 2 implants (IODs) et ceux qui portent des prothèses conventionnelles (CDs), par rapport à la qualité de vie reliée à la santé bucco-dentaire et générale, la santé orale et la qualité du sommeil, un an après avoir reçu leurs nouvelles prothèses. Méthodes : Dans cette étude randomisée contrôlée, 255 aînés ont reçu au hasard IODs ou les CDs, les deux types de prothèses étant opposés à des prothèses maxillaires conventionnelles. La qualité de la vie reliée à la santé bucco-dentaire (OHRQoL) et la santé générale subjective ont été mesurées avec les questionnaires Oral Health Impact Profile (OHIP-20) et Short Form-36 (SF-36) en condition pré-traitement et après un an. La qualité du sommeil et la somnolence diurne ont été mesurées à l’aide du questionnaire Qualité de Sommeil de Pittsburg et de l'Échelle de Somnolence Epworth. La santé orale a été évaluée par un examen clinique. Les variables indépendantes étaient le sens de cohérence et le type de prosthèse, ainsi que des variables socio-démographiques. En utilisant des analyses statistiques bi et multi-factorielles, des comparaisons à l’intérieur d’un même groupe et entre deux groupes ont été effectuées. Résultats : Les différences pré et post traitement pour les cotes OHIP étaient significativement plus grandes pour le groupe IOD que le groupe CD (p<0.05). Le type de traitement et la cote pré-traitement étaient des facteurs significatifs à OHRQoL (p < 0.0001). Dans le groupe CD, il y avait une diminution significative par rapport aux cotes de «Physical Component Scores (PCS)», le fonctionnement physique, le rôle physique et la douleur physique entre les données pré-traitement et un an après le traitement, ce qui indique une diminution au niveau de la santé générale subjective. Dans le groupe IOD, une diminution statistiquement non significative a été remarquée par rapport à toutes les cotes des sous-échelles de SF-36, sauf pour la douleur physique. Le modèle final de régression a démontré qu’après ajustement pour les variables âge, sexe, statut marital et type de traitement, la cote totale finale d’OHIP et les données de bases de PCS prédisaient la cote finale de PCS (p < 0.0001). Aucune corrélation significative entre sens de cohérence et OHRQoL n'a été détectée (r =-0.1; p > 0.05). Les aînés porteurs des prothèses conventionnelles avaient presque 5 fois plus de chance d’avoir une stomatite prothétique que ceux portant des prothèses mandibulaires hybrides retenues par 2 implants (p < 0.0001). Les aînés ayant subjectivement une mauvaise santé générale avaient une qualité de sommeil moins bonne que ceux avec une meilleure santé générale subjective (p < 0.05). Les personnes qui avaient une OHRQoL moins bonne étaient presque 4 fois plus somnolentes pendant le jour que celles avec une meilleure OHRQoL (p=0.003, χ2; OR =3.8 CI 1.5 to 9.8). L'analyse de régression a montré que la santé générale subjective et OHRQoL prévoient la qualité du sommeil (p=0.022 et p=0.001, respectivement) et la somnolence diurne (p=0.017 et p=0.005, respectivement). Conclusions: Les résultats de cette étude suggèrent que, chez les aînés édentés, des prothèses mandibulaires hybrides retenues par deux implants amènent une amélioration significative de la qualité de vie reliée à la santé bucco-dentaire et maintiennent la sensation d’une meilleure santé physique. Des prothèses hybrides implanto-portées peuvent contribuer à la santé orale en réduisant les traumatismes infligés à la muqueuse orale et en contrôlant la stomatite prothétique. Les aînés édentés dont le niveau de qualité de vie reliée à la santé bucco-dentaire est bas, peuvent aussi avoir des troubles de qualité du sommeil. / The global greying of society indicates that health care systems face new challenges. High levels of disability can be reduced through new technologies, health promotion and preventive strategies. Recent literature has underlined the superiority of mandibular implant overdentures over conventional dentures for patient satisfaction and quality of life. However, it is still not clear whether this benefit has any long-term positive effects on oral and general health, as well as on the quality of life of elderly populations. Objectives, Hypotheses: We aimed to measure the impact of mandibular two-implant overdentures on the general and oral health quality of life, as well as on oral health and sleep quality of edentulous elders. We tested the null hypothesis that there is no difference in the general and oral health quality of life, as well as, on oral health and sleep quality of those wearing mandibular two-implant overdentures (IODs) and those who wear conventional dentures (CDs), one year following prosthesis delivery. Methods: In this randomized controlled trial, 255 elders randomly received IODs or CDs, both opposed by conventional maxillary dentures. OHRQoL and perceived general health were measured with the Oral Health Impact Profile (OHIP-20) and the Short Form-36 (SF-36) at baseline and after one year. Sleep quality and daytime sleepiness were measured with the Pittsburg Sleep Quality global score and the Epworth Sleepiness Scale. Clinical exams were conducted to evaluate oral health. Independent variables included sense of coherence and prosthesis type, as well as socio-demographic variables. Between and within group comparisons were performed using bivariate and multivariate statistical tests. Results: Pre/post treatment differences in OHIP scores were significantly greater for the IOD than the CD group (p<0.05). Type of treatment and pre-treatment scores were significant contributors to OHRQoL (p<0.0001). In the CD group, there was a statistically significant decrease in physical component scores (PCS), physical functioning, role physical and bodily pain from baseline to one year follow up, indicating decreased perceived general health. In the IOD group, no statistically significant decrease was seen in SF-36 subscale scores from baseline to one year, except for bodily pain. The final regression model demonstrated that, after controlling for age, sex, marital status and type of treatment, the OHIP total final and the PCS baseline scores predict PCS final scores (p<0.0001). No significant correlation between sense of coherence and OHRQoL was detected (r= -0.1; p> 0.05). Elders wearing conventional dentures were almost 5 times more likely to have denture stomatitis than those wearing mandibular two-implant retained overdentures (p < 0.0001). Elders with low perceived general health had poorer sleep than those with high perceived general health (p<0.05). Those with low oral health related quality of life were almost 4 times sleepier during the day than those with high OHRQoL (p=0.003, χ2; OR =3.8 CI 1.5 to 9.8). Regression analysis showed that perceived general health and OHRQoL predict sleep quality (p=0.022 and p=0.001, respectively) and daytime sleepiness (p=0.017 and p=0.005, respectively). Conclusions: The results of this study suggest that, in edentulous elders, mandibular two-implant overdentures provide significant improvement in oral health related quality of life and maintain perceived physical health. Implant overdentures may contribute to oral health by reducing oral mucosa trauma and control denture stomatitis. Edentulous elders whose oral health related quality of life is low may also have poor sleep quality.

Essai randomisé contrôlé

Randomized clinical trial

Prothèse implanto-portée hybride

Implant overdenture

Santé générale

General health

Qualité de vie

Qulity of life

Stomatite prothétique

Denture stomatitis

Sommeil

Sleep

Sens de cohérence

Sense of coherence

Stomatite prothétique, candidose orale et leur évolution dans le temps

Savignac, Katia

07 1900

Objectifs: Observer l’évolution de la stomatite prothétique dans le temps quant à la fréquence et la sévérité ainsi que son association avec de potentiels facteurs de risque au cours d’un suivi longitudinal de 2 ans. Matériels et méthodes : Cent trente-cinq patients âgés complètement édentés et en bonne santé ont été sélectionnés pour participer à cette étude et ont été divisés de façon randomisée en deux groupes. Ils ont tous reçu une prothèse dentaire amovible totale conventionnelle au maxillaire supérieur. La moitié d’entre eux a reçu une prothèse totale mandibulaire implanto-portée retenue par deux attachements boule et l’autre moitié une prothèse conventionnelle. Ils ont été suivis sur une période de deux ans. Les données sociodémographiques, d’habitudes de vie, d’hygiène et de satisfaction des prothèses ont été amassées à l’aide de questionnaires. Les patients ont aussi subi un examen oral complet lors duquel une évaluation de la stomatite prothétique, basée sur la classification de Newton, a été effectuée ainsi qu’un prélèvement de la plaque prothétique. Les analyses microbiologiques pertinentes afin de détecter la présence de Candida ont ensuite été effectuées. Des tests Chi-carré de Pearson et McNemar ont été utilisés pour analyser la fréquence de la stomatite, son association avec de possibles facteurs de risque ainsi que son évolution dans le temps. Des rapports de cotes (odds ratio) et leurs intervalles de confiance (95%) ont été effectués afin de déterminer la force d’association entre les facteurs de risque et la stomatite prothétique. Résultats : La prévalence de la stomatite a augmenté entre la première (63,6%) et la deuxième année de suivi (88,7%) avec une incidence de 78,8%. Les patients souffrant d’une stomatite de type 2 ou 3 et qui brossent leur palais ont environ 6 fois plus de chance de voir la sévérité de leur stomatite diminuer [p = 0,04 OR 5,88 CI (1,1-32,2)]. Il n’y a pas d’association statistiquement significative entre la fréquence de la stomatite et les facteurs de risque investigués. La prévalence de la candidose est demeurée stable dans le temps (45,8% et 49,2% à la première et deuxième année de suivi respectivement, p > 0,05). Il n’y a pas d’association entre la présence d’une candidose orale, la stomatite prothétique et les facteurs de risque étudiés. Conclusion : Les résultats de cette étude suggèrent que la stomatite prothétique progresse dans le temps indépendamment de la présence d’une candidose. Le brossage du palais pourrait être une approche simple à conseiller aux patients souffrant d’une stomatite prothétique de type 2 ou 3. / Objectives: To assess the evolution of denture stomatitis in term of frequency and severity and its association with potential risk factors over a two-year period. Methods: One hundred thirty five healthy edentulous elders who were randomly rehabilitated with a maxillary complete denture opposed by a conventional denture or an implant-supported overdenture retained by two ball attachments were followed over two years. Demographic and clinical data concerning oral and general health, smoking, denture status and hygienic habits were obtained from oral examination and standard questionnaires. Denture stomatitis was evaluated according to Newton’s classification. Microbiological analyses consist of detection of Candida species in denture plaque and inoculation in selective growth medium. Pearson Chi-square and McNemar tests were used to analyse the frequency of denture stomatitis, its association with potential risk factors and it’s evolution over time. Odds ratios and their 95% confidence intervals were calculated to determine the strength of association between risk factors and denture stomatitis. Results: The prevalence of denture stomatitis increased between the first (63.6%) and second year follow-up (88.7%) with an incidence rate of 78.8%. Those individuals suffering from type 2 or type 3 denture stomatitis and who brushed their palate had approximately 6 times more chance of observing a decrease in the severity of their condition [p=0.04 OR 5.88 CI (1.1-32.2)]. There was no statistically significant association between the frequency of denture stomatitis and classical risk factors at both follow-ups. The carriage rate of Candida species remained stable over time (45.8% and 49.2% first and second year of follow-up consecutively, p > 0.05). There was no association between the presence of oral candidiosis and denture stomatitis or its potential risk factors. Conclusion: The results of this study suggest that denture stomatitis progresses overtime independent of Candida carriage. Palatal brushing could be a preventive approach to minimise the inflammation in individuals suffering from type 2 or type 3 denture stomatitis.

Prothèse implanto-portée

Prothèses dentaires

Stomatite prothétique

Étude prospective randomisée

Santé buccale

Implant overdenture

Dental protheses

Denture stomatitis

Randomised controlled trial

Oral health

DESENVOLVIMENTO DE UM ADESIVO PARA PRÓTESES REMOVÍVEIS CONTENDO MICROPARTÍCULAS POLIMÉRICAS DE NITRATO DE MICONAZOL: SÍNTESE E CARACTERIZAÇÃO / DEVELOPMENT OF REMOVABLE DENTURE ADHESIVE CONTAINING MICONAZOLE NITRATE-POLYMERIC MICROPARTICLES: SYNTHESIS AND CHARACTERIZATION

Molina, Andrés Felipe Cartagena

05 February 2016

Made available in DSpace on 2017-07-24T19:21:59Z (GMT). No. of bitstreams: 1 Andres Felipe.pdf: 3893759 bytes, checksum: fd56d743b750b678334823fb1406f10a (MD5) Previous issue date: 2016-02-05 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / The combination of well-fitting dentures with topical antifungals is appropriate therapeutic approach for denture stomatitis (EP). It was developed and evaluated an adhesive for removable dentures containing miconazole nitrate (NM) incorporated into mucoadhesive and/or pH dependent polymer microparticles aiming at increasing bioavailability. Initially, microparticles have been developed containing 10% and 20% of NM, spray-drying, using Gantrez MS-955 polymer (G10, G20), Eudragit L-100 (E10, E20) or both (EG10, EG20). An analytical method by high-performance liquid chromatography (HPLC) to quantify NM of the microparticles was validated. Microparticles were characterized by scanning electron microscopy (SEM), x-ray diffraction, Fourier-transformed infrared spectrometry (FTIR), differential scanning calorimetry (DSC), in-vitro release studies (percentage of dissolution / time, and release profiles) and antifungal activity. An experimental denture adhesive formulation (ACT) was developed containing 10% by weight of the microparticles (AE1, AG1, AEG1, AE2, AG2, AEG2) or 2% of pure drug (ANM). For all adhesives it was determined: minimum inhibitory concentration (MIC) for Candida albicans (microdilution and agar dilution); adhesive force (FA among acrylic surfaces after 0.5, 1, 3, or 6 h immersion in water); and toxicity to brine shrimp (24 h and 48 h) by calculating lethal concentration 50 (LC50). The HPLC method was proven specific, linear (r = 0.9992), precise, accurate and robust in the range 5-90 μg.mL-1, with running and retention times of 10.0 and 5.58 minutes, respectively. All microparticles showed acceptable performance (37.22% - 55.36%) and encapsulation (over 89%) values. E10 and E20 microparticles showed spherical and smooth surface, while EG20 had similar shape, but rough surface. G10, G20 and EG20 had depressed craters and morphology. The diameters of the microparticles ranged from 1.9 to 4.3 micrometers. No chemical bond was observed between the MN and the polymers through the FTIR spectra. Microencapsulation contributed to the drug amorphization, according to thermal analysis and X-ray diffraction, reducing the release time. NM and the G10, G20 and EG20 microparticles fitted the biexponential release kinetic model and the microparticles E10, E20 and EG10 fitted to mono-exponential model. The microparticles showed antifungal efficiency similar to pure drug. Extracts of the adhesives containing the microparticles and ANM showed MIC of 1.25 to 5 μg.mL-1 (comparable to Daktarin®, 2.5 μg.mL-1). Significant differences in AF for adhesive formulations evaluated as a function of immersion time in water were observed (p <0.001), with an upward trend between 1 h and 3 h, followed by reduction or stabilization up to 6 h. The incorporation of NM and polymeric microparticles did not affect the FA of the experimental adhesive and AEG20 showed the best results, with high initial values, and holding them for 6 h. All adhesive formulations showed low or no toxicity (LC50 349.53 to 931.00 μg.mL-1). The proposed denture adhesive formulation was proven compatible with the incorporation of polymeric microparticles containing NM. / A associação de próteses bem adaptadas com a presença tópica de antifúngicos é adequada abordagem terapêutica para estomatite protética (EP). Foi desenvolvido e avaliado um adesivo para prótese removível contendo nitrato de miconazol (NM) incorporado a micropartículas poliméricas muco-adesivas e/ou pH dependentes visando aumento de biodisponibilidade. Inicialmente, foram desenvolvidas micropartículas contendo 10% e 20% de NM, por spray-drying, utilizando os polímeros Gantrez MS-955 (G10, G20), Eudragit L-100 (E10, E20) ou ambos (EG10, EG20). Foi validado um método analítico por cromatografia líquida de alta eficiência (CLAE) para se quantificar NM das micropartículas. Estas foram caracterizadas por microscopia eletrônica de varredura (MEV), difração de raios x, espectrometria de infravermelho por transformada em Fourier (FTIR), calorimetria exploratória diferencial (CED), estudos de liberação in-vitro (porcentagem de dissolução/tempo e perfis de liberação) e atividade antifúngica. A seguir foram desenvolvidas formulações de um adesivo experimental para prótese (ACT) acrescido de 10% em peso das micropartículas (AE1, AG1, AEG1, AE2, AG2, AEG2) ou 2% do fármaco puro (AMN). Para todos adesivos determinou-se: concentração inibitória mínima (CMI) em Candida albicans (microdiluição em caldo e diluição em ágar); força adesiva (FA, entre superfícies acrílicas após 0,5, 1, 3, ou 6 h de imersão em água); e toxicidade em Artemia salina (24 h e 48 h), calculando-se concentração letal 50 (CL50). O método de CLAE apresentou-se específico, linear (r = 0,9992), preciso, exato e robusto na faixa de 5 a 90 μg.mL-1, com tempos de corrida e de retenção de 10,0 e 5,58 minutos, respectivamente. Todas as micropartículas mostraram aceitáveis valores de rendimento (37,22% – 55,36%) e de encapsulação (superiores a 89%). As micropartículas E10 e E20 apresentaram forma esférica e superfície lisa, enquanto EG20 possuíam a mesma forma, porém superfície rugosa. As micropartículas G10, G20 e EG20 apresentaram morfologia deprimida e crateras. Os diâmetros das micropartículas variaram entre 1,9 a 4,3 μm. Nenhuma ligação química foi observada entre o NM e os polímeros, através dos espectros de FTIR. A microencapsulação contribuiu para amorfizar o fármaco, segundo as análises térmicas e difração de raios X, reduzindo seu tempo de liberação. Ajustaram-se ao modelo cinético de liberação biexponencial o NM e as micropartículas G10, G20 e EG20, e ao modelo monoexponencial, as micropartículas E10, E20 e EG10. As micropartículas apresentaram eficiência antifúngica similar ao fármaco puro. Extratos dos adesivos contendo micropartículas e a formulação AMN apresentaram CMI entre 1,25 a 5 μg.mL-1 (comparável a Daktarin®, 2,5 μg.mL-1). Foram verificadas diferenças significativas na FA para as formulações de adesivos avaliadas em função do tempo de imersão na água (p<0,001), com tendência de aumento entre 1 h e 3 h, seguido de decréscimo ou estabilização até 6 h. A incorporação do NM e de micropartículas poliméricas não prejudicou a FA do adesivo experimental e AEG20 exibiu os melhores resultados, apresentando elevados valores iniciais, e mantendo-os por 6 h. Todas as formulações de adesivos apresentaram baixa ou nenhuma toxicidade (CL50 de 349,53 a 931,00 μg.mL-1). A formulação de adesivo para prótese removível proposta foi compatível com a incorporação de micropartículas poliméricas contendo NM.

nitrato de miconazol

liberação controlada de fármacos

adesivos a tecidos

estomatite sob prótese

Candida albicans

miconazole nitrate

drug liberation

dental pharmaceutical-preparations

tissue adhesives

denture stomatitis

Candida albicans

CNPQ::CIENCIAS DA SAUDE::ODONTOLOGIA

EFEITO DA INCORPORAÇÃO DE FÁRMACOS ANTIFÚNGICOS SOBRE A MORFOLOGIA DE SUPERFÍCIE E A LIBERAÇÃO IN VITRO DE MATERIAIS MACIOS TEMPORÁRIOS PARA BASE DE PRÓTESE / Effect of the addition of antifungals on the surface morphology and the in vitro leaching from temporary soft denture materials

Aliaga, Adelaida Sánchez

21 February 2014

Made available in DSpace on 2017-07-24T19:22:34Z (GMT). No. of bitstreams: 1 Adelaida S Aliaga.pdf: 5670394 bytes, checksum: 9cdda52bc2a6b833409747ce8d7cf507 (MD5) Previous issue date: 2014-02-21 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / Purpose: The purpose of this study was to evaluate the surface morphology and roughness and the in vitro leachability of temporary soft liners modified by the incorporation of antifungals, generally used for the denture stomatitis treatment, in their minimum inhibitory concentrations (MIC) for the biofilm of Candida albicans. Material and methods: The surface analyses of the tissue conditioner Softone (S) and the resilient liner Trusoft (T) modified or not by the addition of nystatin (Ny), miconazole (Mc), ketoconazole (Ke), chlorhexidine diacetate (Chx), and itraconazole (It) were made by using scanning electron microscopy and confocal laser microscopy. In vitro leachability of Ny and Chx was measured using Ultraviolet visible spectroscopy. Additional analyses of the modified materials containing Ny and Chx were made using differential scanning calorimetry (DSC). The antifungals were incorporated at their previously determined MIC for the biofilm of C. albicans (Ny = 0.032 g; Mc = 0.256 g; Ke = 0.128 g; Chx = 0.064 g; and It = 0.256 g/g of material). The specimens were stored in distilled water at 37ºC for up to 14 days previously to the analyses. Results: Softone had more irregular surface morphology than Trusoft did. Morphological changes were noted in both materials with increasing immersion time, particularly in those containing drugs. Ny and Ke showed the smallest particle sizes, while Chx and It showed the largest ones. Groups containing Chx and It presented extremely porous and irregular surface. Modified specimens had superior roughness (Ra) values in comparison with the control specimens. There was a trend towards an increase in Ra parameter after 7 days, followed by a decrease to values lower than the initial ones after 14 days, in the control and specimens with Ny, Mc, and Ke. Both materials had biexponential kinetics of release: a rapid initial release followed by a slower leaching. Softone leached more concentration of the antifungals than Trusoft and chlorhexidine was released at higher concentration than nystatin. DSC analysis revealed low Tg for Softone and that the fusion temperature of the drugs changed little after they had been added to the materials. Conclusion: The addition of Chx or It changed more significantly the surface of the materials. Softone was able to release more drug concentration and it was noted a weak chemical bond between the drugs and the evaluated materials. / Objetivo: A proposta deste estudo foi avaliar a morfologia e a rugosidade de superfície e a liberação in vitro de materiais macios temporários com incorporação de fármacos antifúngicos, comumente utilizados para o tratamento da estomatite protética, em suas concentrações mínimas inibitórias (CMI) ao biofilme de Candida albicans. Material e métodos: As análises de superfície do condicionador de tecido Softone (S) e do reembasador resiliente Trusoft (T) tanto controles como modificados pela incorporação de nistatina (Ni), miconazol (Mc), cetoconazol (Ce), diacetato de clorexidina (Clx) e itraconazol (It) foram feitas por meio de microscopia eletrônica de varredura e microscopia confocal laser. A liberação in vitro dos fármacos Ni e Clx foi quantificada utilizando espectrofotometria na região do Ultravioleta visível. Análises adicionais dos materiais contendo Ni e Clx foram feitas utilizando calorimetria exploratória diferencial (DSC). Os antifúngicos foram incorporados em suas CMI ao biofilme de C. albicans determinadas em estudo prévio (Ni = 0,032 g; Mc = 0,256 g; Ce = 0,128 g; Clx = 0,064 g e It = 0,256 g/g do material). Os corpos de prova foram armazenados em água destilada a 37ºC por até 14 dias previamente às análises. Resultados: O Softone apresentou morfologia mais irregular que o Trusoft. Foi notada alteração de superfície em ambos os materiais, principalmente naqueles contendo fármacos, com o aumento do tempo de imersão. Os maiores e os menores tamanhos de partículas foram dos fármacos Clx e It e Ni e Ce, respectivamente. Os grupos contendo Clx e It demonstraram superfícies extremamente porosas e irregulares. Os espécimes modificados apresentaram valores superiores de rugosidade média (Ra) em relação aos controles. Houve uma tendência de aumento de Ra após 7 dias, seguida por uma diminuição a valores inferiores aos iniciais após 14 dias para o grupo controle e aqueles contendo Ni, Mc e Ce. Ambos os materiais apresentaram cinética de liberação biexponencial: rápida liberação inicial seguida por uma liberação mais lenta. O Softone liberou maior concentração dos fármacos que o Trusoft e a clorexidina foi liberada em maior quantidade que a nistatina. As análises em DSC revelaram Tg mais baixa para o Softone e que a temperatura de fusão dos fármacos pouco alterou após terem sido incorporados aos materiais. Conclusão: A incorporação de Clx ou It alterou mais significativamente a superfície dos materiais. O Softone foi capaz de liberar maior concentração dos fármacos Clx e Ni e foi detectada uma fraca ligação química entre estes fármacos e os materiais avaliados.

sstomatite sob prótese

microscopia eletrônica de varredura

microscopia confocal

espectrofotometria ultravioleta

calorimetria diferencial de varredura.

denture stomatitis

denture liners

anti-infective agents

scanning electron microscopy

confocal microscopy

ultraviolet spectrophotometry

differential scanning calorimetry

CNPQ::CIENCIAS DA SAUDE::ODONTOLOGIA