Biblioteca Digital de Teses e Dissertações PÓS-GRADUAÇÃO SCTRICTO SENSU Programa de Pós-Graduação em Ciências da Saúde
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dc.creatorMONTEIRO, Maria Luiza Gonçalves dos Reis-
dc.creator.ID08730813662por
dc.creator.Latteshttp://lattes.cnpq.br/6872717162309834por
dc.contributor.advisor1REIS, Marlene Antônia-
dc.contributor.advisor1ID51733277668por
dc.contributor.advisor1Latteshttp://lattes.cnpq.br/3194932402580523por
dc.contributor.advisor-co1MACHADO, Juliana Reis-
dc.contributor.advisor-co1ID06911408636por
dc.contributor.advisor-co1Latteshttp://lattes.cnpq.br/5289363102869037por
dc.date.accessioned2020-09-24T11:57:49Z-
dc.date.issued2019-12-12-
dc.identifier.citationMONTEIRO, Maria Luiza Gonçalves dos Reis. Nefropatia por IgA primária: relação entre dados clínicos e parâmetros morfológicos, papel dos subtipos de glomeruloesclerose segmentar e das alterações ultraestruturais podocitárias. 2019. 81f . Tese (Doutorado em Ciências da Saúde) - Programa de Pós-Graduação em Ciências da Saúde, Universidade Federal do Triângulo Mineiro, Uberaba, 2019 .por
dc.identifier.urihttp://bdtd.uftm.edu.br/handle/tede/982-
dc.description.resumoIntrodução: Nefropatia por IgA (NIgA) é a glomerulonefrite primária mais comum, apresenta ampla variação de manifestações clínicas e histológicas. Este estudo objetivou avaliar a sensibilidade, especificidade e acurácia dos dados clínicos no momento da biópsia na previsão dos parâmetros da classificação de Oxford e investigar a influência na apresentação clínica dos subtipos de esclerose segmentar (GESF), lesão podocitária, apagamento dos pedicelos (AP) e evidências de morte podocitária. Material e métodos: Estudo transversal com biópsias de 103 pacientes com NIgA, que foram submetidas a microscopia de luz, imunofluorescência, imuno-histoquímica para WT1 e microscopia eletrônica de transmissão (MET). A classificação de Oxford foi atualizada e as lesões de GESF foram subclassificadas. Foram utilizadas curvas ROC, regressão logística univariada e multivariada. Células marcadas com WT1 em alças glomerulares foram contadas como podócitos e a área glomerular foi medida para obter a densidade de podócitos (DP). O número de diafragmas de filtração (DF) foi dividido pelo comprimento (μm) da alça, resultando em densidade de DF/μm. O perímetro da alça coberto por AP ou áreas desnudas foi dividido pelo perímetro total, resultando em Índice de Apagamento (IA). Resultados: Na classificação de Oxford, a maioria dos pacientes apresentava M0, E0, S1, T2 e C0. A hipertensão aumenta a chance de M1 em 2,54x (p=0,02). Para cada unidade de aumento de creatinina, 2,6x mais chances de E1 (p = 0,001). S1 é previsto pela proteinúria com sensibilidade de 75% e especificidade de 90,9% (p<0,0001). Para cada unidade de aumento da TFG, há redução de 6% na chance de T2 em relação a T0 (p=0,0001). Se houver hipertensão, há 5 vezes mais chances de T2 do que T0 (p=0,01). Para cada unidade de aumento de creatinina, há 2,8 vezes mais chances de C (p=0,003). A creatinina também apresentou sensibilidade de 75,8% e especificidade de 75% para predição de C (p=0,002). Inversamente, para cada unidade de TFG, a chance de C é reduzida em 4% (p=0,007). A proteinúria foi o único parâmetro clínico com diferença significativa entre os grupos S0 e S1 (p<0,0001). Os subtipos de GESF relacionados à proteinúria foram celular (p=0,03) e peri-hilar (p=0,02). A DP foi menor nos casos com proteinúria nefrótica (p=0,03; r=-0,22). Podócitos destacados foram encontrados em todos os grupos de morte de podócitos, com proporção significativamente menor nos casos de autofagia (p=0,03). Na maioria dos casos com podócitos destacados, houve morte de podócitos, especialmente autofagia e necrose. Nenhum podócito apoptótico foi encontrado. Os pseudocistos não se correlacionaram com o destacamento de podócitos (p=0,49). Os casos com autofagia apresentaram frequência significativamente menor de hematúria (p=0,03). A densidade de DF e o IA não se correlacionaram com dados clínicos ou morfológicos. Conclusão: Os parâmetros de classificação de Oxford corresponderam a alguns dados clínicos, o que abre a possibilidade de no futuro predizer-se os dados morfológicos a partir dos dados clínicos. Lesões de GESF não especificamente relacionadas a podocitopatias podem influenciar os parâmetros clínicos. A proteinúria correlacionou-se com a DP e não com o AP, o que reforça a teoria de que o apagamento é um mecanismo adaptativo. Os podócitos destacados estão relacionados à lesão podocitária e não aos pseudocistos, o que reforça a hipótese de que, na NIgA, a perda de podócitos está relacionada à lesão celular e não apenas a fatores mecânicos. Autofagia parece ser um mecanismo de proteção com menor proporção de podócitos destacados e menos casos de hematúria. Essas características podem auxiliar na avaliação da gravidade na rotina diagnóstica.por
dc.description.abstractIntroduction: IgA nephropathy (IgAN) is the most common primary glomerulonephritis, has a broad range of histological and clinical manifestations. This study aims to assess sensitivity, specificity and accuracy of clinical data at the time of biopsy in predicting Oxford classification parameters and investigate if subtypes of segmental sclerosis (FSGS), podocyte injury, foot process effacement (FPE) and evidences of cell death influence clinical presentation. Material and methods: Transversal study with 103 IgAN patients. Renal samples underwent light microscopy, immunofluorescence, immunohistochemistry for WT1 and transmission electron microscopy (TEM). Oxford classification was updated and FSGS lesions were subclassified. ROC curves, univariate and multivariate logistic regression were used. WT1-labeled cells in glomerular loops were counted as podocytes and glomerular area was measured to get podocyte density (PD). The length (μm) of the loop divided the number of slit diaphragms (SD), resulting in density of SD/μm. The perimeter of the loop covered by FPE or denuded areas were divided by total perimeter, resulting in Effacement Index (EI). Results: In Oxford classification, the majority of patients had M0, E0, S1, T2 and C0. Hypertension increases the chance of M1 in 2.54x (p=0.02). For each unit of increased creatinine, 2.6x more chances of E1 (p=0.001). S1 is predicted by proteinuria with 75% sensitivity and 90.9% specificity (p < 0.0001). For each unit of increase in GFR, there is a reduction of 6% in the chance of T2 in relation to T0 (p=0.0001). If hypertension, there is 5x more chances of T2 than T0 (p=0.01). For each unit of increase in creatinine, there are 2.8x more chances of C (p=0.003). Creatinine also showed 75.8% sensitivity and 75% specificity for prediction of C (p=0.002). Inversely, for each unit of GFR, the chance of C is reduced by 4% (p=0.007). Proteinuria was the only clinical parameter with significative difference, between S0 and S1 groups (p < 0.0001). FSGS subtypes related to proteinuria were cellular (p=0.03) and peri-hilar (p=0.02). PD was lower in cases with nephrotic proteinuria (p= 0.03; r=-0.22). Detached podocytes were found in all groups of podocyte death, with significantly lower proportion in cases with autophagy (p=0.03). In most cases with detached podocytes, there were podocyte death, specially autophagy and necrosis. No apoptotic podocyte was found. Pseudocysts were not correlated with podocyte detachment (p=0.49). Cases with autophagy, had significantly lower frequency of hematuria (p=0.03). SD density and EI did not correlate with clinical or morphological data. Conclusion: Oxford classification parameters corresponded to some clinical data, making it possible to predict, in the future, morphological data from clinical parameters. FSGS lesions not specifically related to podocytopathies may also influence clinical parameters. Proteinuria correlated with PD and not with FPE, which reinforces the theory that this FP change is an adaptive mechanism. Detached podocytes were related to podocyte injury and not with pseudocysts, which reinforces the hypothesis that in IgAN, podocyte loss is related to cell injury and not just mechanical factors. Autophagy seems to be a protection mechanism with a smaller proportion of detached podocytes and fewer cases with hematuria. These characteristics may add to severity assessment in diagnostic routine.eng
dc.description.sponsorshipCoordenação de Aperfeiçoamento de Pessoal de Nível Superiorpor
dc.description.sponsorshipFundação de Amparo à Pesquisa do Estado de Minas Geraispor
dc.description.sponsorshipConselho Nacional de Desenvolvimento Científico e Tecnológicopor
dc.description.sponsorshipEmpresa Brasileira de Serviços Hospitalarespor
dc.description.sponsorshipUniversidade Federal do Triângulo Mineiropor
dc.formatapplication/pdf*
dc.thumbnail.urlhttp://bdtd.uftm.edu.br/retrieve/6646/Tese%20Maria%20L%20G%20R%20Monteiro.pdf.jpg*
dc.languageporpor
dc.publisherUniversidade Federal do Triângulo Mineiropor
dc.publisher.departmentInstituto de Ciências da Saúde - ICS::Programa de Pós-Graduação em Ciências da Saúdepor
dc.publisher.countryBrasilpor
dc.publisher.initialsUFTMpor
dc.publisher.programPrograma de Pós-Graduação em Ciências da Saúdepor
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dc.rightsAcesso Abertopor
dc.rights.urihttp://creativecommons.org/licenses/by-nc-nd/4.0/-
dc.subjectNefropatia por IgA.por
dc.subjectGlomeruloesclerose segmentar.por
dc.subjectPodócitos.por
dc.subjectMorte celular.por
dc.subjectAutofagia.por
dc.subjectMicroscopia eletrônica de transmissão.por
dc.subjectProteinúria.por
dc.subjectIgA nephropathy.eng
dc.subjectSegmental glomerulosclerosis.eng
dc.subjectPodocytes.eng
dc.subjectCell death.eng
dc.subjectAutophagy.eng
dc.subjectTransmission electron microscopy.eng
dc.subjectProteinuria.eng
dc.subject.cnpqMedicinapor
dc.titleNefropatia por IgA primária: relação entre dados clínicos e parâmetros morfológicos, papel dos subtipos de glomeruloesclerose segmentar e das alterações ultraestruturais podocitáriaspor
dc.typeTesepor
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