A Rare De Novo Mutation in the TRIM8 Gene in a 17-Year-Old Boy with Steroid-Resistant Nephrotic Syndrome: Case Report.

Idiopathic nephrotic syndrome is the most common chronic glomerular disease in children. Treatment with steroids is usually successful; however, in a small percentage of patients, steroid resistance is observed. The most frequent histologic kidney feature of steroid-resistant nephrotic syndrome (SRNS) is focal segmental glomerulosclerosis (FSGS). Genetic testing has become a valuable diagnostic tool in defining the etiology of SRNS, leading to the identification of a genetic cause. The TRIM8 gene is expressed in various tissues, including kidney cells and the central nervous system (CNS). An association between a mutation in the TRIM8 gene and an early onset of FSGS has been proposed but is not well described. We present a 17-year-old boy with epilepsy, early mild developmental delay, a low IgG serum level, and proteinuria, secondary to FSGS. A Next-Generation Sequencing (NGS)-based analysis revealed a heterozygous de novo pathogenic variant in the TRIM8 gene (c.1200C>G, p.Tyr400Ter). TRIM8 gene sequencing should be considered in individuals with early onset of FSGS, particularly accompanied by symptoms of cortical dysfunction, such as epilepsy and intellectual disability.

Mutations in the NUP93, NUP107 and NUP160 genes cause steroid-resistant nephrotic syndrome in Chinese children.

BACKGROUND: The variants of nucleoporins are extremely rare in hereditary steroid-resistant nephrotic syndrome (SRNS). Most of the patients carrying such variants progress to end stage kidney disease (ESKD) in their childhood. More clinical and genetic data from these patients are needed to characterize their genotype-phenotype relationships and elucidate the role of nucleoporins in SRNS. METHODS: Four patients of SRNS carrying biallelic variants in the NUP93, NUP107 and NUP160 genes were presented. The clinical and molecular genetic characteristics of these patients were summarized, and relevant literature was reviewed. RESULTS: All four patients in this study were female and initially presented with SRNS. The median age at the onset of the disease was 5.08 years, ranging from 1 to 10.5 years. Among the four patients, three progressed to ESKD at a median age of 7 years, ranging from 1.5 to 10.5 years, while one patient reached stage 3 chronic kidney disease (CKD3). Kidney biopsies revealed focal segmental glomerulosclerosis in three patients. Biallelic variants were detected in NUP93 in one patient, NUP107 in two patients, as well as NUP160 in one patient respectively. Among these variants, five yielded single amino acid substitutions, one led to nonsense mutation causing premature termination of NUP107 translation, one caused a single nucleotide deletion resulting in frameshift and truncation of NUP107. Furthermore, one splicing donor mutation was observed in NUP160. None of these variants had been reported previously. CONCLUSION: This report indicates that biallelic variants in NUP93, NUP107 and NUP160 can cause severe early-onset SRNS, which rapidly progresses to ESKD. Moreover, these findings expand the spectrum of phenotypes and genotypes and highlight the importance of next-generation sequencing in elucidating the molecular basis of SRNS and allowing rational treatment for affected individuals.

Idiopathic nephrotic syndrome in Syrian children: clinicopathological spectrum, treatment, and outcomes.

BACKGROUND: Idiopathic nephrotic syndrome (INS) is the most common glomerular disease in children. We performed this study to report histopathological findings, the correlation between clinical and histopathological features, and the response to steroids and other immunosuppressive drugs and outcomes in Syrian children with INS. METHODS: A single-center retrospective observational cohort study was conducted at Children's University Hospital in Damascus, and included all patients aged 1-14 years, admitted from January 2013 to December 2022, with INS and who underwent kidney biopsy. RESULTS: The study included 109 patients, with a male/female ratio of 1.13:1, and a median age of 5 years with interquartile range (2.8-10). The main indication of kidney biopsy was steroid-resistant nephrotic syndrome (SRNS) (57.8%). The main histopathological patterns were minimal change disease (MCD) (45%) and focal segmental glomerulosclerosis (FSGS) (37.6%). FSGS was the most common histopathological pattern in SRNS (44.3%). In SRNS, we used calcineurin inhibitors to induce remission. Tacrolimus was used in 49 patients with response rate (complete remission of proteinuria) of 69.4% and cyclosporine in 20 patients with response rate of 50%. In steroid-dependent nephrotic syndrome (SDNS), we used mycophenolate mofetil (MMF) and cyclophosphamide to prevent relapses; MMF was used in 9 patients with response rate (maintaining sustained remission) of 89% and cyclophosphamide in 3 patients with response rate of 66.7%. Rituximab was used in four patients with FSGS, two SRNS patients and two SDNS patients, with sustained remission rate of 100%. Fifteen patients (13.7%) progressed to chronic kidney disease stage 5. Of them, 7 patients had FSGS and 8 patients had focal and global glomerulosclerosis;14 of them were steroid-resistant and one patient was steroid-dependent with persistent relapses. The most common outcome was sustained remission (47%) in MCD and frequent relapses (31.7%) in FSGS. CONCLUSIONS: FSGS was the most common histopathological pattern in idiopathic SRNS and had the worst prognosis. Calcineurin inhibitors could be an effective therapy to induce complete remission in SRNS. Rituximab may be an effective treatment to achieve sustained remission in SDNS and frequently relapsing NS and may have a potential role in SRNS with further studies required.

New insights from the genetic work-up in early onset nephrotic syndrome: report from a registry in western India.

BACKGROUND: Eighty-five percent of infants with congenital nephrotic syndrome (CNS) and 66% with infantile NS (INS) are likely to have a monogenic etiology. There exists a significant genetic variability between different regions and ethnic groups. This study aimed to determine the genetic defects in children with CNS and INS by establishing a registry in western India. METHODS: In this cross-sectional study, pediatric nephrologists from 13 private and government institutions shared relevant clinical data and details of the genetic evaluation of children presenting with NS within the first year of life. RESULTS: The median age at presentation was 9 months (range 1-23, IQR 3-13 months), history of consanguinity between parents existed in 14 patients (34%), family history of similar illness in 6 (15%), and extra-renal manifestations in 17 (41%). Twenty-five (61%) were confirmed to have a monogenic etiology. NPHS1 gene was the most implicated (9/25) followed by PLCE1 (5/25). There were 12 variants of uncertain significance (VUS) involving 10 genes (10/25, 40%), and no definite genetic abnormality was found in 4 (25%). A re-analysis of these VUS attempted 2-3 years later facilitated reclassification of 7/12 (58%); increasing the diagnostic yield from 61 to 68.2%. CONCLUSIONS: Consistent with worldwide data, variants in NPHS1 gene were the most common cause of NS in infancy; however, PLCE1 was implicated more frequently in our cohort. NUP93 and COL4A3 were reported in early onset NS for the first time. Reclassification of VUS should be attempted, if feasible, since it may lead to a useful revision of diagnosis.

Effectiveness of Supramaximal Angiotensin-converting Enzyme Inhibition in Controlling Proteinuria in Congenital Nephrotic Syndrome with Cytomegalovirus Infection and an NPHS1 Mutation.

Congenital nephrotic syndrome (NS) is characterized by early-onset heavy proteinuria. Most cases of congenital NS are associated with genetic mutations in the podocyte proteins. The causal relationship of perinatal infections with congenital NS has not yet been proven. Inadequate response to the treatment of such infections should prompt us to conduct genetic testing for congenital NS. The heavy proteinuria associated with congenital NS is usually difficult to control with conventional treatment. It often results in progressive kidney disease with a high risk of mortality in early life. Here, we describe an infant who developed congenital NS and was found to have a coexisting Cytomegalovirus infection and an underlying NPSH1 mutation. Proteinuria did not respond to a standard dose of enalapril. A supramaximal dose of enalapril was tried and was effective and safe in controlling the proteinuria. It was associated with improved growth, complete resolution of edema, normal serum albumin, and normal renal function beyond 2 years of age.

Identificación de variantes del gen NPHS2 en niños con síndrome nefrótico corticorresistente / NPHS2 Mutation analysis study in children with steroid-resistant nephrotic syndrome

Resumen: La podocina es una proteína localizada en el diafragma de filtración glomerular donde participa en la regulación de la filtración glomerular. Las mutaciones del gen NPHS2, que codifica a la podocina, son la principal causa de síndrome nefrótico corticorresistente (SNCR) autosómico recesivo en niños. Objetivos: Identificar mutaciones de NPHS2 en niños chilenos con SNCR, y establecer la prevalencia de las variantes más frecuentes en un grupo de adultos sanos. Pacientes y método: Análisis mutacional de NPHS2 en 34 niños chilenos con SNCR. Una vez identificadas las dos variantes de NPHS2 de mayor frecuencia, se realizó un screening de estas mutaciones en 223 adultos sanos. El análisis mutacional se realizó por secuenciación directa de los ocho exones codificantes amplificados por reacción de polimerasa en cadena. La secuenciación del DNA se realizó mediante método fluorométrico y las secuencias fueron evaluadas con el software SeqPilot. La asociación entre la presencia de variantes de NPHS2 y SNCR se calculó comparando las frecuencias alélicas entre los pacientes con SNCR y los voluntarios sanos utilizando prueba exacta de Fisher. Se consideró significativo p < 0,05. Resultados: Se detectaron mutaciones patogénicas de NPHS2 en siete de los 34 pacientes (21%) estudiados, de los cuales seis resultaron heterocigotos para p.R229Q y p.A284 V. En voluntarios sanos la prevalencia de p.R229Q fue de 2,46%. Conclusiones: Este estudio muestra que p.R229Q y p.A284 V son las variantes de NPHS2 más frecuentes en niños chilenos con SNCR. Por primera vez se describe esta asociación en niños chilenos, en base a la cual es posible proponer una estrategia de screening para estudio genético en pacientes con SNCR y sus familias. Se propone una estrategia de búsqueda de p.R229Q y p.A284 V en forma paralela o secuencial en estos pacientes.

Abstract: Podocin is a protein located in the glomerular slit diaphragm where it takes part in the regulation of glomerular filtration. Mutations of the NPHS2 gene that codes podocin are the main cause of autosomal recessive steroid resistant nephrotic syndrome (SRNS). Objectives: To identify the NPHS2 mutations in Chilean children with SRNS, and to determine the prevalence of the most common variants in a group of healthy adults. Patients and methods: Mutation analysis of NPHS2 in 34 Chilean children with SRNS. Once the two most common variants of NPHS2 were identified, screening for these mutations was performed on 233 healthy adults. The mutation analysis was performed by the direct sequencing of the eight coding exons by polymerase chain reaction amplification. The DNA sequencing was performed using a fluorometric method, and then evaluated with SeqPilot™ software. The relationship between the presence of NPHS2 variants and SRNS was calculated by comparing the allele frequency between patients with SRNS and those of the healthy volunteers using the exact Fisher test. A P < .05 was considered significant. Results: Pathogenic NPHS2 mutations were detected in 7 (21%) of the 34 patients studied, of which 6 were heterozygotes for p.R229Q and p.A284 V. The presence of p.R229Q was 2.46% in the healthy volunteers. Conclusions: This study shows that p.R229Q and p.A284 V are the most frequent variants in Chilean children with SRNS. It is the first time that this relationship has been reported in Chilean children. Based on this, a screening strategy is proposed for the genetic study in patients with SRNS and their families. A parallel or sequential search strategy for p.R229Q and p.A284 V in these patients is proposed.

Steroid-resistant idiopathic nephrotic syndrome in children: long-term follow-up and risk factors for end-stage renal disease / Síndrome nefrótica idiopática córtico-resistente na criança: evolução e fatores de risco para falência renal crônica

INTRODUTION: Steroid resistant idiopathic nephrotic syndrome (SRINS) in children is one of the leading causes of progression to chronic kidney disease stage V (CKD V)/end stage renal disease (ESRD). OBJECTIVE: The aim of this retrospective study is to evaluate the efficacy of immunosuppressive drugs (IS) and to identify risk factors for progression to ESRD in this population. METHODS: Clinical and biochemical variables at presentation, early or late steroid resistance, histological pattern and response to cyclosporine A (CsA) and cyclophosfamide (CP) were reviewed in 136 children with SRINS. The analyzed outcome was the progression to ESRD. Univariate as well as multivariate Cox-regression analysis were performed. RESULTS: Median age at onset was 5.54 years (0.67-17.22) and median follow up time was 6.1 years (0.25-30.83). Early steroid-resistance was observed in 114 patients and late resistance in 22. Resistance to CP and CsA was 62.9% and 35% respectively. At last follow-up 57 patients reached ESRD. The renal survival rate was 71.5%, 58.4%, 55.3%, 35.6% and 28.5% at 5, 10, 15, 20 and 25 years respectively. Univariate analysis demonstrated that older age at onset, early steroid-resistance, hematuria, hypertension, focal segmental glomerulosclerosis (FSGS), and resistance to IS were risk factors for ESRD. The Cox proportional-hazards regression identified CsAresistance and FSGS as the only predictors for ESRD. CONCLUSION: Our findings showed that CsA-resistance and FSGS were risk factors for ESRD.

INTRODUÇÃO: A síndrome nefrótica idiopática córtico-resistente (SNICR) é uma das principais causas de falência renal crônica (FRC)/doença renal crônica estadio V (DRC V) em crianças. Objetivo: Avaliar a resposta aos imunossupressores e identificar fatores de risco para a FRC. MÉTODOS: Variáveis clínicas e bioquímicas na apresentação, resistência inicial ou tardia aos esteroides, lesão histológica e resposta à ciclosporina A (CsA) e à ciclofosfamida (CF) foram analisados retrospectivamente em 136 crianças com SNICR. O desfecho analisado foi a progressão para FRC e os métodos utilizados foram a análise univariada e a regressão multivariada de Cox. RESULTADOS: A idade mediana do início da doença foi de 5,54 anos (0,67-17,22) e o tempo mediano de seguimento foi de 6,1 anos (0,25-30,83). Resistência inicial aos esteroides ocorreu em 114 pacientes e tardia em 22. Resistência à CF e à CsA ocorreu em 62,9% e 35% dos pacientes, respectivamente. FRC ocorreu em 57 pacientes. A sobrevida renal foi de 71,5%, 58,4%, 55,3%, 35,6% e 28,5% aos 5, 10, 15, 20 e 25 anos, respectivamente. A análise univariada demonstrou que a idade maior ao início da doença, resistência inicial aos esteroides, hematúria, hipertensão, glomeruloesclerose segmentar e focal (GESF) e resistência aos imunossupressores foram fatores de risco para FRC. A regressão de Cox identificou a resistência à CsA e a GESF como os únicos fatores preditores para FRC. CONCLUSÃO: Nossos achados mostraram que a resistência à ciclosporina e a presença de GESF foram fatores de risco para a progressão para DRCV.

Immunosupressive therapy in children with steroid-resistant nephrotic syndrome: single center experience / Tratamento com imunossupressores em crianças com síndrome nefrótica resistente a corticosteróide: experiência de um único centro

INTODUCTION: Nephrotic syndrome is one of the most frequent glomerular diseases among children, and steroid therapy remains as the treatment choice. In spite of this, 10 to 15% of the patients are steroidresistant, and the best therapy for such cases has never been defined. Mycophenolate acid (MA) is one of the treatments used in such situations. OBJECTIVE: To describe the clinical behavior of children diagnosed with steroid-resistant nephrotic syndrome (SRNS) and to assess the therapeutic response to MA. METHODS: This was a retrospective and descriptive study. RESULTS: 26 clinical records of patients with SRNS; 70% male and 30% female. All patients underwent kidney biopsies, which showed a predominance of focal segmental glomerulosclerosis (FSGS). The immunosuppresive drugs used were: Mycophenolate mofetil (MMF) 100%, Cyclosporine 69.2%, Cyclophosphamide 23.1%, and Rituximab 23%. One month after treatment initiation with MMF 61.5% achieved remission. The median of relapses per year for the patients was 3 (p25: 2.75 - p75: 4). This median became 1 (p25: 1 - p75: 3.25) after using this medication (p = 0.08). Furthermore, prior to the start of the MMF treatment, the median of the steroid dose was 1 (p25: 0.5- p75: 1.62) mg/k/day. After using MMF, this median became 0.07 (p25: 0 - p75: 0.55) mg/k/day (p < 0.001), in 8 patients prednisolone was stopped. CONCLUSION: In our experience, treatment with MMF showed positive results such as decrease in the frequency of relapses, less proteinuria, and reduction in the dose of steroids administered without deterioration of glomerular filtration rates. However, more studies are needed to assess efficacy, safety, and optimal dosage.

INTRODUÇÃO: A síndrome nefrótica é uma das mais frequentes doenças glomerulares em crianças e o tratamento com corticosteróides ainda é o tratamento de escolha. Apesar disso, 10 a 15% dos pacientes são resistentes a corticosteróides, e o melhor tratamento para tais casos ainda não foi definido. O ácido micofenólico (AM) é um dos tratamentos usados em tais situações. OBJETIVO: Descrever o comportamento clínico de crianças diagnosticadas com síndrome nefrótica resistente a corticosteróide (SNRC) e avaliar a resposta terapêutica ao AM. MÉTODOS: Esse foi um estudo retrospectivo e descritivo. RESULTADOS: 26 registros de pacientes com SNRC; 70% homens e 30% mulheres. Todos os pacientes foram submetidos a biópsias renais, o que mostrou predominância de glomeruloesclerose segmentar focal (GESF). Os medicamentos imunossupressores utilizados foram: Mofetil Micofenolato (MMF) 100%; Ciclosporina 69,2%; Ciclosfosfamida 23,1%; e Rituximabe 23%. Um mês após início do tratamento com MMF, 61,5% tiveram remissão. A mediana das recidivas por ano para os pacientes foi de 3 (p25: 2,75 - p75: 4). Essa mediana se tornou 1 (p25: 1 - p75: 3,25) após o uso da medicação (p = 0,08). Além disso, antes do início do tratamento com MMF, a mediana da dose de corticosteróide foi de 1 (p25: 0.5 - p75: 1.62) mg/k/ dia. Após a utilização do MMF, essa mediana se tornou 0,07 (p25: 0 - p75: 0,55) mg/k/dia (p < 0,001), em 8 pacientes a prednisolona foi interrompida. CONCLUSÃO: em nossa casuística, o tratamento com MMF mostrou resultados positivos, tais como a redução na frequência de recidivas, menos proteinúria, e redução da dose de corticosteróide administrada sem deterioração nas taxas de filtração glomerular. Entretanto, mais estudos são necessários para se avaliar a eficácia, segurança e otimização da dosagem.

Tacrolimo para o tratamento da síndrome nefrótica primária em crianças e adolescentes / Tacrolimus for the treatment of primary nephrotic syndrome in children and adolescents

A síndrome nefrótica (SN) é caracterizada por proteinúria maciça, hipoalbuminemia, edema e hiperlipidemia e ocorre pelo aumento da permeabilidade da membrana basal glomerular. Pode ser dividida em secundária, quando causada por alguma outra doença, ou idiopática. Em crianças, a síndrome nefrótica idiopática (SNI) representa 90% dos casos diagnosticados antes dos 10 anos de idade e 50% dos que se apresentam após essa idade. Apesar de menos frequente, a avaliação inicial deve afastar a presença de causas secundárias, como doenças sistêmicas, infecções, neoplasias e uso de medicamentos. O diagnóstico de SNI em crianças e adolescentes é baseado nos seguintes critérios clínicos e laboratoriais. O paciente deverá apresentar todos os critérios abaixo: -edema; e -proteinúria nefrótica ­ proteinúria acima de 50 mg/kg/dia ou acima de 40 mg/m2/h ou acima de 3,5 g/24 h/1,73 m2 ou índice proteinúria/creatininúria (IPC) acima de 2,0; e -hipoalbuminemia ­ albumina sérica abaixo de 2,5 g/dl; e -hiperlipidemia (colesterol total igual ou acima de 240 mg/dl ou triglicerídios igual ou acima 200 mg/dl. Os pacientes são classificados de acordo com a resposta ao tratamento nas seguintes categorias: -em remissão completa; -em remissão parcial; -com resistência ao glicocorticoide; -com recidiva; -com recidivas frequentes; -com dependência ao corticosteroide; -com resistência ao corticosteroide; com resistência ao corticosteroide. Esquematicamente, o tratamento pode ser dividido em: -tratamento inicial (primeiro episódio); -síndrome nefrótica sensível ao corticosteroide; -síndrome nefrótica resistente ao corticosteroide. O tacrolimo (TAC) é um inibidor da calcineurina largamente utilizado na prevenção da rejeição aguda no transplante de órgãos. Trata-se de um antibiótico macrolídeo, que inibe a ativação de um fator de transcrição essencial para a produção de citocinas pelo linfócito CD4, resultando em diminuição de produção de interleucina-2 (IL-2) e interferon-gama. A CONITEC, na 4ª reunião ordinária realizada no dia 10/05/2012, decidiu recomendar a ampliação de uso no SUS do medicamento tacrolimo para tratamento da síndrome nefrótica primária em crianças e adolescentes. O medicamento será utilizado como alternativa terapêutica à ciclosporina quando ocorrerem efeitos adversos associados ao seu uso­hiperplasia gengival e hipertricose­, e conforme PCDT a ser elaborado pelo Ministério da Saúde. A Portaria SCTIE/MS Nº 35, de 27 de setembro de 2012 - Torna pública a decisão de incorporar o medicamento tacrolimo para o tratamento da Síndrome Nefrótica Primária no Sistema Único de Saúde (SUS).

Síndrome nefrótico congénito por mutación del gen de la nefrina: caso clínico / Congenital nephrotic syndrome due to mutation of nephrine gene: clinical case

Congenital Nephrotic Syndrome (CNS) is defined as a corticoresistant nephrotic syndrome which appears in the first 90 days of life. NPHS1 gene mutations, codifying nephrine cause nearly 40 percent of the cases. Such a clinical case has not yet been described in Chile. Objective: Describe a patient with CNS and his genetic study. Clinical case: Full-term 38 week male newborn, birth weight 2620 gr, height 48,5 cm, ALPGAR 9/10. Head circumf: 33 cm. First child, well controlled pregnancy. 16 days after birth, he develops edema, massive proteinuria (3,2 gr/ dl), hypoalbuminemia (0,79 mg/dl) and hypercholesterolemia ( total cholesterol: 318 mg/dl). Renal sonogram showed increase in size and echogenicity in both kidneys, and loss of corticomedullar differentiation. Renal biopsy showed diffuse mesangial glomeruloesclerosis. Genetic study for NPHS1 was performed through direct sequencing of 29 exons and adjacent regions of introns chromosome 19q13.1. Analysis disclosed C567X, ho-mozygote mutation. Conclusions: The first case of Nephrine mutation causing CNSis described in Chile. The importance of genetic studies in these patients is highlighted for clinical decision making.

El síndrome nefrótico congénito (SNC) se define como un síndrome nefrótico córticoresistente que aparece en los primeros 90 días de vida. Mutaciones en el gen NPHS1 que codifica a la nefrina son causantes de aproximadamente del 40 por ciento de los niños con SNC. En Chile no se ha descrito hasta ahora esta mutación asociada al cuadro clínico. Objetivo: Describir el caso de un paciente con SNC y su estudio genético. Caso clínico: Paciente de sexo masculino, RNT 38 semanas, PRN 2620 gr, TN 48,5 cm APGAR 9/10. CC: 33 cm. Embarazo controlado primer hijo. A los 16 días comienza con edema, proteinuria masiva (3,2 gr/dl), hipoalbuminemia (0,79 mg/dl) e hipercolesterolemia (colesterol total: 318 mg/dl). Se descarta TORCH (-). La ecografía renal mostró un aumento de tamaño y de ecogenicidad de ambos riñones, pérdida de diferenciación corticomedular. La biopsia renal se informó como glomeruloesclerosis mesangial difusa. El estudio genético para NPHS1 se realizó por secuenciación directa de los 29 exones y las regiones adyacentes de los intrones en el cromosoma 19q13.1 El análisis demostró una mutación C567X, homocigoto. Conclusiones: Se describe el primer caso de mutación para Nefrina en un SNC chileno. Se destaca la importancia del estudio genético en estos pacientes debido a las implicancias en las decisiones clínicas y terapéuticas.

Síndrome de Denys-Drash: presentación de un caso / Denys-Drash's syndrome: a case report

El síndrome de Denys-Drash se caracteriza por pseudohemafroditismo masculino, tumor de Wilms y glomerulopatía con rápida progresión a la insuficiencia renal terminal, es producido por una mutación en el gen supresor TW1 localizado en el cromosoma 11p 13. La lesión glomerular se caracteriza por una esclerosis mesangial difusa. Reportamos un caso con genitales ambiguos, cariotipo 46 XY, síndrome nefrótico congénito a los 7 días de nacido, con rápida progresión a la insuficiencia renal terminal. Se hizo necesaria la diálisis peritoneal, y murió al mes de edad por sepsis generalizada. En el análisis del tejido renal se demuestra la esclerosis mesangial difusa

Síndrome nefrótica: relato de um caso de esclerose mesangial difusa / Nephrotic syndrome: report of a case of diffuse mesangial sclerosis

Habib & Bois descreveram seis casos de um tipo específico de síndrome nefrótica infantil e designaram a entidade esclerose mesangial difusa, baseados em lesöes características. Relatamos o curso clínico e achados histopatológicos de biópsia renal, com estudo a microscopia eletrônica, em paciente com síndrome nefrótica congênita