O volume celular do adipócito contribui para a heterogeneidade funcional do tecido adiposo branco / The adipocyte size contributes to the functional heterogeneity of white adipose tissue

Natalie Carolina de Castro

29 April 2010

O tecido adiposo já foi considerado um tecido metabolicamente pouco ativo, no entanto, os mais recentes avanços mostram que ele desempenha uma função importante no controle da homeostase energética. Baseado neste conceito, este trabalho objetivou caracterizar o perfil morfológico e metabólico de adipócitos isolados de três diferentes coxins adiposos, subcutâneo, peri-epididimal, retro-peritoneal (SC, PE e RP respectivamente). Os adipócitos dos diferentes coxins foram coletados e submetidos a análise morfológica, aos ensaios metabólicos e análise da expressão de enzimas envolvidas no metabolismo lipídico e glicídico. Os resultados mostraram diferença estatisticamente significativa no volume dos adipócitos das três regiões entre si (p<0,05), maior capacidade lipogênica dos adipócitos RP. Paralelamente, o tecido SC, mostrou maior expressão de enzimas envolvidas na via lipogênica (p< 0,05; SC vs PE e RP). / The adipose tissue was considered to be a little active metabolic tissue, however, the most recent advances show that it plays an important function in the control of the energy homostasis. Based on this concept, this work aimed to characterize the morphology and metabolism of isolated adipocytes of three different depots, like: subcutaneous, periepididymal, retroperitoneal (SC, PE and RP) . The adipocytes of the different depots had been collected and submitted to morphologic analysis, metabolic assays and to analysis of the enzymes expressions involved on lipids and glucose metabolism. The results showed statistical significant difference on volume of the adipocytes among the three different depots (p< 0, 05), high lipogenic capacity of RP adipocytes and higher expression of proteins involved in lipogenic patways of SC adipocytes (p<0, 05).

Adipócito

Gordura epididimal

Gordura netro-peitoneal

Gordura sub cutânea

Metabolismo adipócito

Tecido adiposo branco

Adipocyte

Adipocyte metabolism

Epidymal fat

Retroperitoneal fat

Sub-cutaneous fat

White Adipose Tissues

Expressão de Foxp3, IL-17 e IL-23 na Leishmaniose Tegumentar Americana causada por Leishmania (Leishmania) amazonensis e Leishmania (Viannia) braziliensis / Expression of Foxp3, IL-17 and IL-23 in American cutaneous leishmaniasis due Leishmania (Leishmania) amazonensis and Leishmania (Viannia) braziliensis

Joyce Prieto Bezerra de Menezes

13 September 2013

A leishmaniose tegumentar americana (LTA) apresenta um amplo espectro de manifestações clínicas e imunopatológicas resultante da interação entre as diferentes espécies de Leishmania e os mecanismos de resposta imune do hospedeiro. Leishmania (Viannia) braziliensis e Leishmania (Leishmania) amazonensis são as espécies de maior potencial patogênico para o homem e de importância médica no Brasil. As células TCD4, quando ativadas por antígenos via MHC II podem se diferenciar em linhagens de células efetoras como Th1, Th2, Th17 e células T reguladoras (Treg). IL-23 é indispensável para as funções efetoras e manutenção de células Th17. O objetivo deste trabalho foi avaliar a expressão de Foxp3, IL-17 e IL-23 em lesões cutâneas de pacientes com diferentes formas clínicas da LTA. Biópsias parafinadas de 44 pacientes foram submetidas à imunoistoquímica, sendo 6 casos de leishmaniose cutânea anérgica difusa (LCADIDRM-) e leishmaniose cutânea disseminada borderline (LCDBIDRM-), ambas causadas por L.(L) amazonensis e 16 casos de leishmaniose cutânea localizada (LCLIDRM+) também causada por L.(L.) amazonensis; 9 casos de LCLIDRM+, 2 casos de LCDBIDRM- e 5 casos de leishmaniose cutâneo-mucosa (LCMIDRM+), todos causados por L.(V.) braziliensis. A densidade de células Tregs Foxp3+ no espectro clínico da LTA mostrou um aumento progressivo partindo das formas centrais LCL causadas por L.(V.) braziliensis (170mm2) e L.(L) amazonensis (140mm2) para as formas polares, LCADIDRM- (289mm2) e LCDBIDRM- (183mm2) causada por L.(L) amazonensis, LCDBIDRM- (189mm2) e LCMIDRM+, causadas por L.(V.) braziliensis (158mm2). A comparação entre as densidades de células IL-17+ nas diferentes formas clínicas da LTA mostrou um perfil semelhante também com um aumento progressivo da expressão de IL-17 partindo das formas centrais LCLIDRM+ causadas por L.(V.) braziliensis (232mm2) e L.(L) amazonensis (197mm2) em direção as formas polares, LCADIDRM- (470mm2) e LCDBIDRM- (340mm2) causada por L.(L.) amazonensis, LCDBIDRM- (431mm2) e LCMIDRM+ (372mm2) causada por L.(V.) braziliensis. A densidade de células IL-23+ mostrou perfil similar ao de IL-17 como no espectro de doença causada por L. (V.) braziliensis ou L. (L.) amazonensis: LCADIDRM- (687mm2), LCDBIDRM- (518mm2) e LCLIDRM+ (348mm2) por L.(L.) amazonensis, LCLIDRM+ (457mm2), LCDBIDRM- (609mm2) e LCMIDRM+ (568mm2) L. (V.) braziliensis. Diante dos nossos achados, observa-se que as células Foxp3+, IL-17+ e IL-23+ desempenham um papel importante na imunopatogênese das diferentes formas clínicas da LTA causadas por L. (V.) braziliensis ou L. (L.) amazonensis, caracterizada por uma resposta imune polarizada de diferente expressão patológica / The American cutaneous leishmaniasis (ACL) presents a wide spectrum of clinical and immunopathological manifestations resulting from the interaction between the different species of Leishmania and the mechanisms of the host immune response. Leishmania (Viannia) braziliensis and Leishmania (Leishmania) amazonensis are the species with the largest pathogenic potential for humans and medical importance in Brazil. The CD4+ T cells can be differentiated into effector cell lines as Th1, Th2, Th17 and regulatory T cells (Treg). IL-23 is essential for effector functions and maintenance of Th17 cells, that produces IL-17. The aim of this study was to evaluate the expression of Foxp3, IL-17 and IL-23 in cutaneous lesions of patients with different clinical forms of ACL. Paraffin embedded biopsies from 44 patients were submitted to immunohistochemistry, there were 6 cases of anergic diffuse cutaneous leishmaniasis (ADCLDTH-) and borderline disseminated cutaneous leishmaniasis (BDCLDTH-) both caused by L. (L.) amazonensis 16 cases of cutaneous leishmaniasis (LCLDTH+) caused by L. (L.) amazonensis, 9 cases of LCLDTH+, 2 cases of BDCLDTH- and 5 cases of mucocutaneous leishmaniasis (MCLDTH+) all caused by L. (V.) braziliensis. The density of Treg Foxp3+ cells in the clinical spectrum of ACL showed a progressive increase starting from the central forms LCLDTH+ caused by L. (V.) braziliensis (170mm2) and L. (L) amazonensis (140mm2) towards the polar forms ADCLDTH- (289mm2). The intermediate clinical forms BDCLDTH- (183mm2) caused by L. (L) amazonensis and BDCLDTH-(189mm2) by L. (V.) braziliensis as well as, MCLDTH+(158mm2) did not present any significant differences. The comparison between the densities of IL-17+ cells in different clinical forms of ACL showed progressive increasing starting from the central forms LCLDTH+ caused by L. (V.) braziliensis (232mm2) and L. (L) amazonensis (197mm2) towards the polar forms, ADCLDTH-(470mm2) and BDCLDTH-(340mm2) caused by L. (L.) amazonensis BDCLDTH- (431mm2) and MCLDTH+ (372mm2) caused by L. (V.) braziliensis. The density of IL-23+ cells showed a similar profile to that of IL-17 at the disease spectrum caused by L. (V.) braziliensis and L. (L.) amazonensis: ADCLDTH-(687mm2) BDCLDTH-(518mm2) and LCLDTH+ (348mm2) by L. (L.) amazonensis; LCLDTH+ (457mm2) LCDBDTH-(609mm2) and MCLDTH+ (568mm2) L. (V.) braziliensis. In view of our findings, we notice that the Foxp3+, IL-17+ and IL-23+ cells play an important role in the immunopathogenesis of different clinical forms of ACL caused by L. (V.) braziliensis and L. (L.) amazonensis, characterized by an immune polarized response with different pathological expression

Foxp3

Interleucina-17

Interleucina-23

L amazonensis

Leishmania braziliensis

Leishmaniose cutânea

Cutaneous leishmaniasis

Foxp3

Interleukin-17

Interleukin-23

Leishmania amazonensis

Leishmania braziliensis

Diagnóstico molecular de Leishmaniose Tegumentar Americana: identificação de espécies de Leishmania por SSUrDNA PCR e G6PD PCR / Molecular diagnosis of American Cutaneous Leishmaniasis: identification of Leishmania species by SSUrDNA PCR and G6PD PCR

Ana Carolina Stocco de Lima

17 August 2010

A Leishmaniose Tegumentar Americana (LTA) representa um sério problema de saúde pública. No Brasil muitas espécies são reconhecidas como patogênicas para o homem, portanto o diagnóstico diferencial é necessário para compreender o perfil epimemiológico da LTA em áreas endêmicas. Com o objetivo de identificar espécies de Leishmania utilizando ferramentas moleculares, cinquenta e três biópsias de pele de pacientes com LTA, fixadas em formalina e incluídas em parafina dos Estados do Pará (N=33) e Maranhão (20) foram submetidos a diferentes protocolos da Reação em Cadeia da Polimerase (PCR) para a identificação dos agentes causadores. Biopsias foram desparafinizadas e o DNA foi extraído usando o protocolo de fenol-clorofórmio, quantificado e submetido a reações de PCR, com base na sequência de nucleotídeos codificadora do RNA que compõe a subunidade menor do ribossomo (SSUrDNA) e da enzima Glicose 6-Fosfato Desidrogenase (G6PD). O alvo G6PD foi utilizado tanto em reações de PCR convencional (cPCR), como de PCR quantitativo (qPCR). As reações de cPCR e Nested PCR SSUrDNA apresentaram resultado positivo para o gênero Leishmania em 40 (83,3%) das amostras submetidas. Vinte e sete desses produtos de PCR foram sequenciados, sendo 17 identificados como L.(L.) amazonensis e 10 como L.(Viannia) sp. A cPCR G6PD identificou 9 amostras como L.(V.) braziliensis , sendo 7 do Maranhão (36%) e 2 do Pará (6%). O DNA de L.(Viannia) sp. foi quantificado em quatro amostras do Maranhão através da reação de qPCR G6PD, mesmo esse alvo sendo de cópia única. Esses resultados indicam que sequências especificas de Leishmania sp. presentes em múltiplas cópias devem ser escolhidas para a aplicação de cPCR em DNA provindo de amostras parafinadas,uma vez que é freqüente casos de LTA com baixo parasitismo e consequentemente, pequenas concentrações de DNA. E ainda a cPCR SSUrDNA pode ser um bom alvo para estudos diagnósticos e epidemiológicos.A qPCR G6PD permitiu a detecção, identificação e quantificação de L. (Viannia) sp. em uma única etapa de amplificação em quatro amostras que presentaram resultados positivos somente na Nested ou Semi-Nested PCR, demonstrando uma maior sensibilidade oferecida pela q PCR / American Cutaneous Leishmaniasis (ACL) presents a serious problem of public healthy. In Brazil many species are recognized as pathogenic to humans, therefore differential diagnostic is necessary to understand the epidemiological profile of ACL in endemic areas. Fifty-three paraffinembedded skin biopsies of ACL patients from Pará (N=33) and Maranhão (20) States, were submitted to different protocols of polymerase chain reaction (PCR) for identification of their causative agents. Biopsies were deparaffinized and DNA were extracted using phenol-chloroform, quantified and submitted to PCR reaction, using small subunit coding sequence (SSUrDNA) and enzyme glucose-6-phosphate dehydrogenase (G6PD). The target of G6PD was used both in conventional PCR reactions (cPCR) and quantitative PCR (qPCR). The reactions of cPCR and Nested PCR SSUrDNA showed positive result for the genus Leishmania in 40 (83.3%) of the samples. Twenty-seven positive samples were submitted to sequencing and 10 were identified as L. (Viannia) sp. and 17 as L. (L.) amazonensis. The G6PD PCR identified 9 samples as L. (V.) braziliensis, 2 from Pará (6%) and 7 from Maranhão (35%).Four samples were quantified in G6PD qPCR, even this is a single copy. These results indicate that specific sequences from Leishmania sp. present in multiple copies should be chosen in relation to those from unique copies in paraffin-embedded tissues, once is frequent cases of ACL with low parasitism, consequently small DNA concentrations and that SSUrDNA can be a good target to diagnostic and epidemiologic studies of ACL. The qPCR allowed the detection and identification of L. (Viannia) sp. in a single round of amplification in four samples that when showed positive results only in the Nested or Semi Nested cPCR suggesting a higher sensitivity offered by qPCR

Diagnóstico

Leishmania (Leishmania) amazonensis

Leishmania (Viannia) braziliensis

Leishmaniose cutânea

Reação em cadeia da polimerase

Cutaneous leishmaniasis

Diagnosis

Leishmania (Leishmania) amazonensis

Leishmania (Viannia) braziliensis

polimerase chain reaction

Avaliação da sensibilidade cutânea em pacientes com lesões agudas de nervos periféricos de membros superiores / Assessment the cutaneous sensibility in acute peripheral upper limb nerve trauma

Nelio Watanabe Aguilera

10 November 2010

A mão humana desempenha a função de um órgão sensorial de percepção, localização e discriminação `a estimulação cutânea. A injúria de nervos periféricos em membros superiores é uma condição com repercurssões funcionais e sociais graves pois, uma mão sem sensibilidade é usualmente uma mão sem função. O objetivo deste estudo é descrever a utilização do PSSD (Pressure- specified sensory device ) como auxiliar ao seguimento dos índices de recuperação da sensibilidade cutânea em pacientes submetidos a reconstruções microcirúrgicas de lesões traumáticas de nervos periféricos de membros superiores. O PSSD consiste de um aparelho que incorpora um transdutor de pressão com duas extremidades rombas e com regulagem de distância entre elas, acoplado a um computador capaz de determinar os limiares cutâneos de pressão para os parâmetros de 1 ponto estático, 1 ponto dinâmico e respectivos 2 pontos. No estudo, os pacientes foram divididos em três grupos: pacientes com lesões de n. mediano e/ou n. ulnar em nível do antebraço, punho e dedos. O teste estatístico utilizado para análise das comparações, tanto entre os grupos quanto para os diferentes momentos considerados de 1, 3, 6 e 12 meses foi a Análise de Variância (ANOVA) com Medidas Repetidas. Os resultados demonstraram haver interação entre os grupos onde, em média, houve diferença estatística (p<0,05) para os parâmetros considerados, a medida que, se aumenta o tempo de avaliação. As lesões digitais, para todos os parâmetros avaliados, apresentaram menores valores dos limiares cutâneos de pressão seguidos do punho e antebraço e não se evidenciou diferença estatística (p>0,05) entre os resultados dos limiares cutâneos de pressão nos nervos mediano e ulnar / The human hand has an important sensorial capacity to perceive, to localize and to distinguish simultaneously, in the act of touch. Peripheral nerve injury at upper limb have seriously functional and social disabilities: a hand without sensibility is usually a hand without function. This study has the purpose to use the PSSD (Pressure-specified sensory device) in patients submitted to microsurgical reconstructions of peripheral upper limb nerves to evaluate the cutaneous sensibility recovery. The PSSD is a tool that incorporates a pressure transducer with two prongs, linked to a computer capable of measuring the cutaneous pressure thresholds referred by the patient. In this study, the patients were divided in three groups: patients with median or ulnar nerve trauma at forearm, wrist or digital levels. The statistical analysis method used to compare the groups and considering different moments in the study of 1, 3, 6 and 12 months was the analysis of variance (ANOVA). The results demonstrate interaction between groups where the generalized mean showed statistical relevance for the parameters of the study as well as the time grows. The digital nerve injuries considering all parameters evaluated revealed the smaller values of cutaneous pressure thresholds followed by the results of the wrist and in the last the forearm cutaneous pressure thresholds values. There were no statistical significance between the median and the ulnar nerves considering the values of the cutaneous sensibility thresholds

Nervo mediano

Nervo ulnar

Nervos periféricos/lesões

Prognóstico

Sensibilidade cutânea/diagnóstico

Cutaneous sensibility/diagnosis

Median nerve

Peripheral nerves/Injuries

Prognosis

Ulnar nerve

Estudos in vitro, in vivo e in silico da atividade de derivados aminoquinolínicos em espécies de Leishmania relacionadas à Leishmaniose tegumentar americana

Antinarelli, Luciana Maria Ribeiro

15 February 2017

Submitted by isabela.moljf@hotmail.com (isabela.moljf@hotmail.com) on 2017-08-17T11:16:52Z No. of bitstreams: 1 lucianamariaribeiroantinarelli.pdf: 16756474 bytes, checksum: 2304892df326fd4997c78bc7f0870bae (MD5) / Approved for entry into archive by Adriana Oliveira (adriana.oliveira@ufjf.edu.br) on 2017-08-17T11:34:54Z (GMT) No. of bitstreams: 1 lucianamariaribeiroantinarelli.pdf: 16756474 bytes, checksum: 2304892df326fd4997c78bc7f0870bae (MD5) / Made available in DSpace on 2017-08-17T11:34:54Z (GMT). No. of bitstreams: 1 lucianamariaribeiroantinarelli.pdf: 16756474 bytes, checksum: 2304892df326fd4997c78bc7f0870bae (MD5) Previous issue date: 2017-02-15 / As leishmanioses representam um grande problema de saúde pública mundial com sérias limitações na quimioterapia atual, como: número limitado de fármacos, baixa eficácia, custo elevado, crescente resistência parasitária e toxicidade. O objetivo do presente trabalho foi avaliar a atividade de uma série de dez derivados de 4- aminoquinolinas em espécies de Leishmania relacionadas a leishmaniose tegumentar. Avaliar os possíveis mecanismos de ação do composto com atividade antileishmanial promissora, identificando as organelas alvo e os processos de morte celular desencadeados no parasito, bem como a sua eficácia in vivo. Dentre os compostos avaliados, o derivado AMQ-j foi o mais ativo, com atividade expressiva em L. amazonensis e L. braziliensis (CI50 menor que 6.0 μg/mL e 2,5 μg/mL em promastigotas e amastigotas intracelulares, respectivamente) para ambas as espécies avaliadas. O composto AMQ-j apresentou baixa toxicidade para macrófagos murinos (CC50> 40.0 μg/mL), sendo mais tóxico para amastigotas intracelulares (Índice de Seletividade>12,0). Os resultados preliminares acerca do modo de ação apontam que o composto AMQ-j induziu drásticos efeitos na mitocôndria do parasito e caracterizado pelo colapso do potencial de membrana mitocondrial (ΔΨm), inchaço da organela, aumento na produção de Espécies Reativas do Oxigênio (EROS) e acúmulo de corpúsculos lipídicos (CLs) no citoplasma. O tratamento com AMQ-j induziu nas formas promastigotas uma série de alterações bioquímicas e celulares sugestivas de morte por apoptose-like como redução do volume celular, exposição de fosfatidilserina no folheto externo da membrana plasmática, manutenção da integridade da membrana plasmática e alterações drásticas no núcleo celular evidenciadas por meio da desorganização da cromatina e fragmentação do DNA. O efeito do composto em promastigotas está também associado à indução de morte por autofagia evidenciada pelo aumento de vacúolos autofágicos, presença de corpos multivesiculares dentro de vacúolos, vesículas citoplasmáticas e acúmulo de compartimentos acídicos no citoplasma dos promastigotas. O composto também induziu fragmentação do DNA dos amastigotas intracelulares de modo seletivo, sem induzir fragmentação da célula hospedeira. Estudos in silico sugerem que AMQ-j é um potencial inibidor da tripanotiona redutase (TryR), enzima fundamental na defesa antioxidante do parasito. Estudos in vivo em modelo murino de infecção com L. amazonensis demonstraram a eficácia do AMQ-j pela via intralesional na redução do tamanho da lesão e da carga parasitária, sem indução de toxicidade hepática, cardíaca e renal. Os estudos de predição in silico relacionados a propriedades farmacocinéticas (ADMET) e características físico-químicas (regra de Lipinsky) sugerem que AMQ-j pode ser utilizado pela via oral. O efeito leishmanicida do composto está associado a múltiplos alvos, desencadeando a morte do parasito por diferentes vias, como apoptose e autofagia. O efeito in vivo do composto aponta para a necessidade da continuidade dos estudos no intuito de melhor estabelecer o seu efeito leishmanicida. / Leishmaniasis represents a major global public health problem with serious limitations in current chemotherapy, such as limited number of drugs, low efficacy, high cost, increasing parasitic resistance and toxicity. The objective of the present study was to evaluate a series of ten 4-aminoquinolines derivatives (AMQs) on Leishmania species related to tegumentary leishmaniasis. It was also evaluated the possible mechanisms of action of a compound with promising leishmanicidal activity, identifying the target organelles and the type of death triggered in the parasite, as well as to its leishmanicidal effect in vivo. Among the evaluated compounds, the AMQ-j derivative was the most active, with expressive activity on L. amazonensis and L. braziliensis (IC50 less than 6.0 μg/mL and 2.5 μg/mL against intracellular promastigotes and amastigotes, respectively) for both evaluated species. Furthermore, AMQ-j showed low toxicity for murine macrophages (CC50> 40.0 μg/mL) being more destructive to the intracellular parasites (selectivity index > 12.0). Preliminary studies about the mode of action showed that AMQ-j compound induced marked effects on the parasite mitochondria, characterized by mitochondrial membrane potential collapse (ΔΨm), organelle swelling, increased of Reactive Oxygen Species (ROS) production and lipidic bodies accumulation in the cytoplasm. The treatment with AMQ-j induced in the promastigote forms a series of biochemical and cellular alterations which suggest apoptosis-like death, including reduction of cellular volume, phosphatidylserine exposure on the outer leaflet of the plasma membrane, maintenance of plasma membrane integrity and drastic changes in the cell nucleus evidenced by chromatin disorganization and DNA fragmentation. The effect of AMQ-j in promastigote forms is also associated with the induction of death by autophagy evidenced by the increase of autophagic vacuoles, presence of multivesicular bodies inside vacuoles, cytoplasmic vesicles and accumulation of acidic compartments in the promastigote cytoplasm. The compound also induced DNA fragmentation of intracellular amastigotes selectively, without inducing host cell fragmentation. In silico studies suggest that this compound is a potential inhibitor of key redox enzyme trypanothione reductase (TryR). In vivo studies in murine infection model of L. amazonensis demonstrated the efficacy of AMQ-j by the intralesional route, reducing lesion size and parasite load, without induction of hepatic, cardiac and renal toxicity. The in silico prediction studies on pharmacokinetic properties (ADMET) and physico-chemical characteristics (Lipinsky's rule) suggest that AMQ-j can be used orally. Taken together, the results suggest that the leishmanicidal effect of the compound is associated with multiple targets and triggers parasite death through different pathways, including apoptosis and autophagy. The in vivo effect indicates that studies with this compound should be continued in order to better establish its leishmanicidal effect.

4-aminoquinolinas

Mitocôndria

Apoptose-like

Autofagia

Leishmaniose cutânea murina

4-aminoquinolines

Mitochondria

Apoptosis-like

Autophagy

Murine cutaneous leishmaniasis

Avaliação da sobrevida e de marcadores histomorfológicos como potenciais fatores prognósticos para carcinoma de células escamosas em cães e gatos / Evaluation of survival and histomorphological markers as potential prognostic factors for squamous cell carcinoma in dogs and cats

Guim, Tainã Normanton

26 February 2010

Made available in DSpace on 2014-08-20T14:38:00Z (GMT). No. of bitstreams: 1 dissertacao_taina_guim.pdf: 1081277 bytes, checksum: 7c03f9dccecf657fea6e60fa6a359381 (MD5) Previous issue date: 2010-02-26 / Squamous cell carcinoma (SCC) is a cutaneous malignant neoplasm commonly observed in dog and cat. Especially in our country, the SCC represents a serious problem, since chronic exposure to ultraviolet radiation is one of the important factors for the development of the disease. In this way, the objective of this study was establish histomorphological markers as prognostic factors and determine the time and the estimated survival of dogs and cats carriers of SCCs. A survey of cases of SCCs in dog and cat diagnosed at the Regional Diagnostic Laboratory from the Federal University of Pelotas, was performed during the period of 1999 to 2009. Fifty samples were obtained from biopsies and/or necropsies. From the studied cases, 24 animals with the disease were followed for a period of one year. In this study, we used the histological grade and survival time of animals as a criterion to prognostic evaluation. The histological parameters evaluated as peritumoral lymphoplasmacytic infiltration, tissue eosinophilia associated with tumor, mitotic index, arrangement, invasion to adjacent tissues, emboli vascular blood and/or lymphatic, desmoplastic reaction and quantification of AgNORs were confronted with the histological grade and the survival time of affected animals. When the histological parameters were compared with survival, a significant relation was observed with the intensity of invasion to adjacent tissues (p <0.05). When confronted with the histological grade, the invasion show significant results only to poorly differentiated SCCs and desmoplasia were statistically significant (p <0.05). In this study, the estimate of survival was 23.4% in one year to animals with or without treatment. From the results obtained, it was concluded that the intensity of invasion is an important predictive prognostic factor for cutaneous SCCs in dogs and cats. Other parameters showed no relation with the histological grade and/or survival, thus, are not considered prognostic factors predictive. The time and the estimate of survival were low and therefore the prognosis for dogs and cats carrier of cutaneous SCCs is unfavorable. / Carcinoma de células escamosas (CCE) é um neoplasma cutâneo maligno comumente observado no cão e no gato. Especialmente em nosso país, o CCE representa um problema sério, uma vez que a exposição crônica à radiação ultravioleta é um dos fatores importantes para o desenvolvimento da doença. Neste sentido, o presente estudo teve como objetivo estabelecer marcadores histomorfológicos como fatores prognósticos e determinar o tempo e a estimativa de sobrevida de cães e gatos portadores de CCEs cutâneos. Foi realizado um levantamento dos casos de CCEs em cães e gatos diagnosticados no Laboratório Regional de Diagnóstico da Universidade Federal de Pelotas, durante o período de 1999 a 2009. Foram recuperadas 50 amostras provenientes de biópsias e/ou necropsias. Do total de casos estudados, 24 animais portadores da doença foram acompanhados durante um período de um ano. Neste estudo, utilizou-se o grau histológico e o tempo de sobrevida como critério de avaliação prognóstica. Os parâmetros histológicos avaliados como: infiltrado linfoplasmacítico peritumoral, eosinofilia tecidual associada a tumores, índice mitótico, arranjo, invasão para tecidos adjacentes, êmbolo vascular sanguíneo e/ou linfático, desmoplasia e quantificação das AgNORs, foram confrontados com o grau histológico e com a sobrevida dos animais acometidos. Quando os parâmetros histológicos foram confrontados com a sobrevida, observou-se relação estatística significativa com a intensidade de invasão para tecidos adjacentes (p<0,05) e, quando confrontados com o grau histológico, a invasão somente para CCEs pouco diferenciados e a desmoplasia foram estatisticamente significativos (p<0,05). No presente estudo, a estimativa de sobrevida para animais portadores de CCEs cutâneos foi 23,4% em um ano, independentemente de terem sido tratados ou não. A partir dos resultados obtidos, concluiu-se que a intensidade de invasão é um fator prognóstico preditivo importante para CCEs cutâneos em cães e gatos. Os demais parâmetros avaliados não mostraram relação com o grau histológico e/ou com a sobrevida, dessa forma, não são considerados fatores prognósticos preditivos. O tempo e a estimativa de sobrevida foram baixos e, portanto, o prognóstico para cães e gatos portadores de CCEs cutâneos é, de um modo geral, desfavorável.

neoplasmas cutâneos

carcinoma de células escamosas

fatores prognósticos

cães

gatos

cutaneous neoplasms

squamous cell carcinoma

prognostic factors

dogs

cats

Hedgehog signaling in cutaneous squamous cell carcinoma

Pyczek, Joanna

30 May 2017

No description available.

610

cutaneous squamous cell carcinoma

Hedghehog signaling

GLI

EGF/EGFR

MEK/ERK

Medizin (PPN619874732)

Biologie (PPN619875151)

1-How in vivo cutaneous biometrology could demonstrate skin modifications induced by various methods. 2-In vitro evaluation of phenytoin on the morphology and activity of human primary melanocytes and in vivo repigmentation effect of topical phenytoin / 1-Comment la biométrologie cutanée in vivo peut démontrer les modifications de la peau induites par diverses méthodes d'évaluation. 2-Evaluation d'effet de la phénytoïne sur la morphologie et l'activité des mélannocytes primaires humaines in vitro et l'effet de repigmentation in vivo de la phénytoïne topique

Fanian, Ferial

14 December 2016

La Biometrogie cutanée est un nouveau spectre de différentes méthodes d'évaluation qui permettent de mesurer les différents paramètres de la peau même en cas des petites modifications. Dans la première partie de nos travaux, nous avons étudié différentes capacités de ces méthodes afin de les corréler avec d'autres données cliniques et histologiques. Ces données nous ont encouragés à découvrir de plus en plus la pigmentation de la peau qui est un peu plus compliquée que les autres paramètres. Par conséquent, sur la deuxième partie, nous nous sommes concentrés sur la biologie cutanée en particulier sur la morphologie et l'activité des mélanocytes. Les travaux de cette thèse ont porté sur les effets de la phénytoïne sur les mélanocytes humains afin de savoir si cette molécule peut être un traitement efficace pour le vitiligo. Dans un premier temps, nous avons évalué deux concepts : tout d'abord et pour la première fois, les effets in vitro des différentes concentrations de phénytoïne sur la morphologie et l'activité des mélanocytes humains, et parallèlement, nous avons mis en place la méthode du transfert de mélanosomes sur les mélanocytes et des kératinocytes humains. Dans un deuxième temps, nous avons procédé à l'évaluation in vivo de la forme topique à différentes concentrations à l'aide d'une étude in vivo sur des cochons d'Inde noirs. Notre travail constitue une étape clé dans la compréhension des mécanismes d'action de la phénytoïne sur les mélanocytes humains qui contribuerait à l'amélioration des pratiques cliniques et donc à la qualité de vie des patients souffrant de troubles pigmentaire. / Cutaneaous Biometrogy is a new vast spectrum of measuring methods wich provide the possibility to measure the différents parameteres of the skin even in the case of small changes. In the first part of this work, we studied various capabilities of these methods in order to correlates them with other clinical and histological data. These data encouraged us to discover more and more the skin pigmentation which is a little more complicated than the other parameters.So, on the second part, we concentrated more on cutaneaous biology particularily on the melanocytes morphology and activity.The work of this thesis focused on the effects of phenytoin on human melanocytes in order to know if this molecule can be eventually an available treatment for vitiligo.Fisrt, we evaluated two concepts : for the first time we evaluated the in vitro effects of the different concentrations of phenytoin on the morphology and activity of human melanocytes and, in parallel, we implemented the method of transfert of melanosomes on human melanocytes and keratinocytes.In a second step, the topical form of phenytoin at different concentrations was evaluated through an in vivo study on black ginea pigs.Our work is a key step on understanding the mechanisms of avtion of phenytoin on human melanocytes which would contribute to the improvement of clinical practices and therefore to the quality of life of patients suffering from depilatory disorders.

Biométrologie

Mélanocytes primares d'humains

Phénytoïne topique

Cochon d'inde noir

Repigmentation

Cutaneous biometrology

Primary human melanocytes

Topical phenytoin

Black guinea pigs

Repigmentation

616.5

Nanoparticules en réseau pour la protection cutanée / Nanoparticular network for the skin protection

Bignon, Cécile

10 November 2015

Les agents chimiques de guerre et leurs dérivés pesticides sont des molécules toxiques qui provoquent une incapacité temporaire ou des dommages permanents allant jusqu’à la mort de l’individu. Une des voies majeures de la contamination est la pénétration cutanée. La protection de la peau semble donc importante pour prévenir de ces dangers. Cette thèse concerne l’élaboration de nouveaux topiques protecteurs cutanés contenant des polymères HASE fluorés greffés avec des nanoparticules de silice, cérine ou titane. Dans un premier temps les actifs ont été synthétisés en grosse quantité et leurs propriétés de mouillabilité améliorées. Les tests toxicologiques ont montré que les actifs n’étaient pas irritants pour la peau et non toxiques pour l’environnement. La formulation de ces polymères a permis le développement de deux nouvelles crèmes barrières contre la pénétration du paraoxon dont l’efficacité est dépendante de la présence des nanoparticules. Le greffage des nanoparticules à un polymère HASE fluoré et leur formulation a donc permis le développement de nouveaux topiques efficaces. L’évaluation de l’efficacité a été réalisée sur membranes artificielles et confirmée sur explants de peaux humaines. Enfin, le peu de disponibilité des explants de peaux humaines a motivé le développement d’un modèle d’efficacité utilisant des épidermes humains reconstruits. / Chemical warfare agents and pesticides are toxic molecules causing temporary incapacitation or permanent harms leading to the death of people. One of the major routes of contamination is the percutaneous penetration. Skin protection is important to prevent these dangers. The aim of this thesis is to develop new active topical skin protectants based on nanoparticular networks containing fluorinated HASE polymers grafting with silica, cerium or titanium nanoparticles. First, polymers were synthesized in larger quantity and their wettability properties improved. Toxicological studies have showed that these compounds are non-irritant and non-toxic for the environment. The formulation of these polymers has led to the elaboration of two new barrier creams against paraoxon penetration whose efficiency is dependent on the presence of nanoparticles. Therefore, the grafting of nanoparticles to fluorinated HASE polymer and their formulation have enabled the development of new active topical skin protectant. Efficiency evaluation was done using artificial membranes and was confirmed on ex vivo human skin. The limited availability of human skin explants has motivated the development of a new efficiency model using reconstructed human epidermis.

Polymère HASE

Nanoparticules

CeO2

SiO2

TiO2

Toxicité

Paraoxon

Pénétration cutanée

Agent chimique de guerre

Thickening polymers

Nanoparticles

CeO2

SiO2

TiO2

Toxicity

Paraoxon

Cutaneous penetration

Chemical warfare agent

Identification des régulateurs de l’expression transcriptionnelle de TSPAN8 impliqués dans l’invasion précoce du mélanome cutané / Identification of the transcriptional expression regulators of TSPAN8 implicated in the early invasion of cutaneous melanoma

Agaësse, Gweltaz

15 December 2016

Le mélanome cutané est l’affection de la peau la plus meurtrière. Afin de pouvoir être traité efficacement, ce cancer nécessite un diagnostic et une exérèse chirurgicale précoce des lésions primitives non-invasives. En effet, les patients atteints de métastases ont peu de chance de survivre car les lésions de mélanome développent rapidement des résistances aux thérapies et possèdent une forte propension à disséminer des métastases dans de nombreux organes. Le franchissement de la lame basale de la peau appelée jonction dermo épidermique est la première étape cruciale dans l’invasion précoce du mélanome cutané. Notre équipe étudie cette étape depuis plusieurs années et a démontré que l’expression de la tétraspanine 8 (TSPAN8) apparait lors de la progression de ce cancer et permet l’acquisition d’un phénotype invasif par les cellules tumorales. Plusieurs membres de la famille des protéines tétraspanines sont connus pour leurs implications dans divers cancers, mais notre connaissance de leurs régulations transcriptionnelles est encore assez réduite. Les travaux présentés dans cette thèse ont permis d’identifier les premiers régulateurs transcriptionnels connus de TSPAN8, et également de commencer l’étude fonctionnelle de ces régulations sur l’invasion dépendante de TSPAN8 par le mélanome cutané. En particulier, nous montrons que l’invasion dépendante de TSPAN8 est entre autres régulée par le membre du complexe Mediator LCMR1/MED19 et par le suppresseur de tumeur p53. Ainsi, ces travaux apportent une meilleure compréhension de l’invasion précoce du mélanome cutané, ce qui devrait permettre une meilleure prise en charge des patients à l’avenir / Cutaneous melanoma is the deadliest skin condition. Curing this cancer requires an early diagnosis and surgical excision of the non-invasive primary lesions. Indeed, patients with metastasis have few chances to survive this cancer since the melanoma lesions rapidly develop treatment resistances, and can disseminate metastasis in numerous organs. Crossing the skin basal membrane called the dermal epidermal junction is the first crucial step of early melanoma invasion. Our team has studied the early invasion of melanoma for many years, and demonstrated for the first time the implication of Tetraspanin (TSPAN8) in melanoma early invasion. Indeed, the expression of this gene and the protein that it codes appears with the progression of melanoma and confers the tumor cells an invasive phenotype. Several members of the tetraspanin protein family are known for their implication in various cancers, yet their transcriptional regulation remains poorly understood. In the case of TSPAN8, nothing was known regarding its transcriptional regulation in melanoma. The experiments presented in this thesis allowed us to identify the first known regulators of TSPAN8 transcriptional expression, and also to begin the functional study of the regulators impact on TSPAN8 dependent invasion of human cutaneous melanoma. Amongst these regulators are the member of the Mediator Complex MED19/LCMR1 and the tumor suppressor p53. The results presented in the present manuscript allow a better understanding of cutaneous melanoma early invasion and should help improving the treatments against this cancer in the future

Cancer

Mélanome cutané

Invasion

TSPAN8

Tétraspanine

Régulation transcriptionnelle

Criblage haut débit

Biologie moléculaire

Cancer

Cutaneous melanoma

Invasion

TSPAN8

Tetraspanin

Transcriptional regulation

High throughput screening

Molecular biology

571.6