Risk Profiles of Progression in Primary Focal Segmental Glomerulosclerosis

Travis, Lori L., Chan, James C.

01 August 2010

Background: Focal segmental glomerulosclerosis (FSGS) is a component of childhood nephrotic syndrome occurring in 10%-20% of all cases. Over time, 25%-50% of children with FSGS develop kidney failure disease. We followed a cohort of children with FSGS in order to delineate the risk profile of progression to kidney failure (KF). Methods: We evaluated patient data collected from 1977 to 2002 at a regional mid-Atlantic nephrology center in the United States. KF was defined primarily for those patients whose serum creatinine (SCr) value doubled compared with the SCr value from a previous visit. Patients who received dialysis or a kidney transplant were also defined as having KF. We analyzed patient data for those who had at least two visits with SCr values recorded. Various baseline characteristics of patients who had developed KF and those with no kidney failure (NKF) were compared. Hazard ratios and correlation were used to further investigate potential risk factors of the kidney failure. We also compared the inverse SCr trend for KF and NKF patients using weighted linear regression. Results: Thirty-four of 43 FSGS patients had adequate follow-up data. About 60% of the patients developed KF over the study period. The average age of the KF patients at diagnosis of FSGS was 9 years, and that of NKF patients 12 years (P=0.05). FSGS patients with KF had a significantly higher mean diastolic blood pressure (DBP) at baseline, compared to those with NKF (P<0.0001). Other baseline characteristics including race, body mass index (BMI), systolic blood pressure, total cholesterol, urinary protein/creatinine ratio and calculated glomerular filtration rate (cGFR) were not significantly different. Baseline DBP was a significant risk factor in progression to KF (HR: 1.03; 95%CI: 1.01-1.06). Inverse SCr values were significantly decreased over time in KF patients (P=0.01). Conclusions: The data of this study indicate that children diagnosed with FSGS who are younger than 10 years and have elevated baseline DBP are more likely to develop kidney failure. The non-significant hazard ratios for other baseline characteristics including gender, race, and BMI are not instrumental risk factors. These results may help understand what may affect progression towards kidney failure in children with FSGS.

blood pressure

focal segmental glomerulosclerosis

gender

predictors of progression

risk profile

Modeling TRIM8 in cellular and mouse renal systems

Liang, Lorrin

07 February 2023

Nephrotic syndrome (NS) is the second leading cause of chronic kidney disease (CKD) presenting under the age of 30. NS presents in children with edema and severe proteinuria, caused by the effacement of podocyte foot processes within the glomerular filtration barrier. Patients with steroid-resistant NS (SRNS) frequently develop end-stage renal disease (ESRD). Additionally, renal biopsies from these patients often reveal focal segmental glomerulosclerosis (FSGS). Pathogenic mutations in known monogenic disease genes have been found in 11-45% children with FSGS/SRNS. Notably, most Mendelian etiologies exhibit recessive inheritance, while dominant vertical inheritance with incomplete penetrance is observed in the remainder. The role of de novo variants (DNVs) in NS necessitates further investigation. Tripartite motif containing 8, TRIM8, is an E3 ubiquitin ligase. De novo TRIM8 variants were previously implicated in a syndromic disease consisting of neurodevelopmental delay, epilepsy, cerebral atrophy, and nephrotic syndrome. In this study, we recapitulate the patient-specific mutations in inducible overexpression cell lines and in CRISPR/Cas9-generated mouse models. N-terminal MYC or GFP-tagged TRIM8 inducible cell lines were generated and characterized using the pInducer21 system. Western blot and immunofluorescence data show that MYC- and GFP-TRIM8 were induced by doxycycline in immortalized podocyte cell lines. Candidate interactors for TRIM8 from the literature and stratified using kidney single cell mRNA sequencing expression were cloned into mammalian expression vectors. Finally, a Trim8 knockout allele (c. 56_162del; p.H20Qfs*124 and c.367_463+304delins46) was generated and bred to yield an allelic series of wildtype, heterozygous and homozygous animals. These mice exhibited normal survival and did not demonstrate proteinuria through three to four months of life. Overall, further studies are ongoing with regards to the continued monitoring of proteinuria and kidney dysfunction, as well as the potential interactor cloning and cell line characterization. / 2025-02-06T00:00:00Z

Medicine

Focal segmental glomerulosclerosis

Nephrology

Nephrotic syndrome

Pediatrics

Renal

TRIM8

Estudo de aspectos moleculares podocitários nas variantes histológicas da glomerulosclerose segmentar e focal / Podocytes molecular expression in the variants of focal segmental glomerulosclerosis

Testagrossa, Leonardo de Abreu

15 August 2011

INTRODUÇÃO: A Glomerulosclerose Segmentar e Focal (GESF) é a glomerulopatia primária mais prevalente no Brasil e sua incidência vem aumentando no mundo inteiro. Na sua forma primária, caracteriza-se clinicamente por acometer pessoas jovens e causar proteinúria acentuada, geralmente acompanhada de síndrome nefrótica. O mecanismo patogênico tem como evento principal a lesão ao podócito, desencadeado por fatores de natureza variada: vírus, drogas/medicamentos, imunológicos, etc. Em 2004, foi publicada a classificação de Columbia, propondo 5 variantes morfológicas distintas na GESF: colapsante (COL), usual (NOS), apical ou tip lesion (TIP), perihilar (PHI) e variante celular (CEL). Diversos estudos comprovam alterações moleculares em podócitos na GESF. Essas alterações são observadas em diversos sítios podocitários: em moléculas envolvidas na fenda de filtração (slit diaphragm), por exemplo, nefrina, podocina e CD2AP; em moléculas do citoesqueleto podocitário, como a -actinina-4 e sinaptopodina; em moléculas marcadoras de diferenciação dos podócitos, como CD10 e WT-1; e ainda em marcadores de divisão celular como Ki-67 e PCNA. Os objetivos desse estudo foram: 1-) classificar as lesões morfológicas de GESF em biópsia renais nas 5 variantes da GESF propostas na Classificação de Columbia; e 2-) analisar a ocorrência de alterações moleculares podocitárias nestes casos. MÉTODOS: Foram selecionados 131 casos de biópsias renais com diagnóstico de GESF primária no período de 1996 a 2006. Os casos foram classificados de acordo com os critérios de Columbia e posteriormente submetidos a reações imuno-histoquímicas para os marcadores CD10, WT-1, vimentina, sinaptopodina, -actinina-4, GLEPP-1, citoqueratina 8/18, citoqueratina 19 e Ki-67. Os resultados foram submetidos à análise estatística através do teste qui-quadrado. RESULTADOS: A classificação das variantes da GESF se distribuiu da seguinte forma: 38,2% de variante NOS, 36,6% de variante COL, 14,5% de variante TIP, 6,9% de variante PHI e 3,8% de variante CEL. Os casos da variante COL se destacaram das demais variantes pela perda de expressão de marcadores de diferenciação celular, como o CD10 e o WT-1 (p<0,01), perda da molécula do citoesqueleto -actinina-4 (p<0,01) e neo-expressão de citoqueratinas 8-18 (p<0,05) e 19 (p<0,01). Adicionalmente, os casos das variantes COL e CEL se destacam das outras variantes pela expressão do marcador de divisão celular Ki-67 (p<0,05). CONCLUSÃO: a variante COL destacou-se das demais em relação às alterações moleculares observadas na análise imuno-histoquímica. O diagnóstico diferencial desta forma de GESF tem importância clínica por ela estar associada a pior evolução e prognóstico em relação às demais variantes. A integração destes marcadores na rotina diagnóstica pode auxiliar no diagnóstico diferencial da GESF COL / INTRODUCTION: Focal segmental glomerulosclerosis (FSGS) is the most prevalent primary glomerulopathy in Brazil and its incidence is increasing worldwide. Primary FSGS is characterized clinically by affecting young people and causing severe proteinuria, often accompanied by nephrotic syndrome. The pathogenesis is related to podocyte injury, which may be due to several factors: viruses, drugs, immunological, etc. In 2004, the Columbia classification of FSGS identified five histological variants of the disease: collapsing (COL), usual (NOS), tip lesion (TIP), perihilar (PHI) and cellular variant (CEL). Several studies have demonstrated molecular changes in podocytes of FSGS patients, which were observed in molecules involved in the filtering function of these cells (nephrin, podocina and CD2AP), in podocyte cytoskeleton molecules (-actinin-4, and synaptopodin), as well as in molecular markers of podocyte differentiation (CD10 and WT-1) and of cell division (Ki-67 and PCNA). The aim of this study was to classify the FSGS biopsies according to the Columbia classification and to analyze the occurrence of molecular changes in the five morphological variants. METHODS: 131 cases of renal biopsies with a diagnosis of primary FSGS in the period 1996 to 2006 were classified according to the criteria of Columbia and then submitted to immunohistochemical reactions with the following antibodies: CD10, WT-1, Vimentin, Synaptopodin, -actinin-4, GLEPP-1, cytokeratin 8-18, cytokeratin 19, and Ki-67. RESULTS: FSGS cases were classified into five variants as follows: 38.2% of NOS variant, 36.6% COL, 14.5% TIP, 6.9% PHI and 3.8% CEL. The COL variant cases distinguished themselves among the other for having lost the expression of CD10 and WT-1 (p <0.01), and also of -actinin-4 (p <0, 01). Furthermore, they gained expression of the cytokeratin 8-18 (p <0.05) and 19 (p <0.01). The group of CEL and COL variants together differed from the other variants regarding the expression of cell division marker Ki-67 (p <0.05). CONCLUSION: COL variant of FSGS presents molecular changes that differs from others and can be demonstrated by immunohistochemistry. The differential diagnosis of this variant is important because of the worse clinical outcome and prognosis it presents in comparison with other variants. The identification of these markers by immunohistochemical on the routine practice may be useful in the diagnosis of COL FSGS

Focal segmental glomerulosclerosis

Glomerulosclerose segmentar e focal

Glomerulosclerose/classificação

Glomerulosclerosis/classification

Immunohistochemistry

Imunoistoquímica

Podócitos

Podocytes

Estudo de aspectos moleculares podocitários nas variantes histológicas da glomerulosclerose segmentar e focal / Podocytes molecular expression in the variants of focal segmental glomerulosclerosis

Leonardo de Abreu Testagrossa

15 August 2011

INTRODUÇÃO: A Glomerulosclerose Segmentar e Focal (GESF) é a glomerulopatia primária mais prevalente no Brasil e sua incidência vem aumentando no mundo inteiro. Na sua forma primária, caracteriza-se clinicamente por acometer pessoas jovens e causar proteinúria acentuada, geralmente acompanhada de síndrome nefrótica. O mecanismo patogênico tem como evento principal a lesão ao podócito, desencadeado por fatores de natureza variada: vírus, drogas/medicamentos, imunológicos, etc. Em 2004, foi publicada a classificação de Columbia, propondo 5 variantes morfológicas distintas na GESF: colapsante (COL), usual (NOS), apical ou tip lesion (TIP), perihilar (PHI) e variante celular (CEL). Diversos estudos comprovam alterações moleculares em podócitos na GESF. Essas alterações são observadas em diversos sítios podocitários: em moléculas envolvidas na fenda de filtração (slit diaphragm), por exemplo, nefrina, podocina e CD2AP; em moléculas do citoesqueleto podocitário, como a -actinina-4 e sinaptopodina; em moléculas marcadoras de diferenciação dos podócitos, como CD10 e WT-1; e ainda em marcadores de divisão celular como Ki-67 e PCNA. Os objetivos desse estudo foram: 1-) classificar as lesões morfológicas de GESF em biópsia renais nas 5 variantes da GESF propostas na Classificação de Columbia; e 2-) analisar a ocorrência de alterações moleculares podocitárias nestes casos. MÉTODOS: Foram selecionados 131 casos de biópsias renais com diagnóstico de GESF primária no período de 1996 a 2006. Os casos foram classificados de acordo com os critérios de Columbia e posteriormente submetidos a reações imuno-histoquímicas para os marcadores CD10, WT-1, vimentina, sinaptopodina, -actinina-4, GLEPP-1, citoqueratina 8/18, citoqueratina 19 e Ki-67. Os resultados foram submetidos à análise estatística através do teste qui-quadrado. RESULTADOS: A classificação das variantes da GESF se distribuiu da seguinte forma: 38,2% de variante NOS, 36,6% de variante COL, 14,5% de variante TIP, 6,9% de variante PHI e 3,8% de variante CEL. Os casos da variante COL se destacaram das demais variantes pela perda de expressão de marcadores de diferenciação celular, como o CD10 e o WT-1 (p<0,01), perda da molécula do citoesqueleto -actinina-4 (p<0,01) e neo-expressão de citoqueratinas 8-18 (p<0,05) e 19 (p<0,01). Adicionalmente, os casos das variantes COL e CEL se destacam das outras variantes pela expressão do marcador de divisão celular Ki-67 (p<0,05). CONCLUSÃO: a variante COL destacou-se das demais em relação às alterações moleculares observadas na análise imuno-histoquímica. O diagnóstico diferencial desta forma de GESF tem importância clínica por ela estar associada a pior evolução e prognóstico em relação às demais variantes. A integração destes marcadores na rotina diagnóstica pode auxiliar no diagnóstico diferencial da GESF COL / INTRODUCTION: Focal segmental glomerulosclerosis (FSGS) is the most prevalent primary glomerulopathy in Brazil and its incidence is increasing worldwide. Primary FSGS is characterized clinically by affecting young people and causing severe proteinuria, often accompanied by nephrotic syndrome. The pathogenesis is related to podocyte injury, which may be due to several factors: viruses, drugs, immunological, etc. In 2004, the Columbia classification of FSGS identified five histological variants of the disease: collapsing (COL), usual (NOS), tip lesion (TIP), perihilar (PHI) and cellular variant (CEL). Several studies have demonstrated molecular changes in podocytes of FSGS patients, which were observed in molecules involved in the filtering function of these cells (nephrin, podocina and CD2AP), in podocyte cytoskeleton molecules (-actinin-4, and synaptopodin), as well as in molecular markers of podocyte differentiation (CD10 and WT-1) and of cell division (Ki-67 and PCNA). The aim of this study was to classify the FSGS biopsies according to the Columbia classification and to analyze the occurrence of molecular changes in the five morphological variants. METHODS: 131 cases of renal biopsies with a diagnosis of primary FSGS in the period 1996 to 2006 were classified according to the criteria of Columbia and then submitted to immunohistochemical reactions with the following antibodies: CD10, WT-1, Vimentin, Synaptopodin, -actinin-4, GLEPP-1, cytokeratin 8-18, cytokeratin 19, and Ki-67. RESULTS: FSGS cases were classified into five variants as follows: 38.2% of NOS variant, 36.6% COL, 14.5% TIP, 6.9% PHI and 3.8% CEL. The COL variant cases distinguished themselves among the other for having lost the expression of CD10 and WT-1 (p <0.01), and also of -actinin-4 (p <0, 01). Furthermore, they gained expression of the cytokeratin 8-18 (p <0.05) and 19 (p <0.01). The group of CEL and COL variants together differed from the other variants regarding the expression of cell division marker Ki-67 (p <0.05). CONCLUSION: COL variant of FSGS presents molecular changes that differs from others and can be demonstrated by immunohistochemistry. The differential diagnosis of this variant is important because of the worse clinical outcome and prognosis it presents in comparison with other variants. The identification of these markers by immunohistochemical on the routine practice may be useful in the diagnosis of COL FSGS

Glomerulosclerose segmentar e focal

Glomerulosclerose/classificação

Imunoistoquímica

Podócitos

Focal segmental glomerulosclerosis

Glomerulosclerosis/classification

Immunohistochemistry

Podocytes

Elucidation of TRPC channel regulation mechanism and its contribution to kidney channelopathy． / TRPCチャネル制御機構とその腎臓チャネロパチーに対する関与の解明

Polat, Onur Kerem

25 November 2019

京都大学 / 0048 / 新制・課程博士 / 博士(工学) / 甲第22124号 / 工博第4654号 / 新制||工||1726(附属図書館) / 京都大学大学院工学研究科合成・生物化学専攻 / (主査)教授 森 泰生, 教授 跡見 晴幸, 教授 浜地 格 / 学位規則第4条第1項該当 / Doctor of Philosophy (Engineering) / Kyoto University / DGAM

Molecular Biochemistry

Electrophysiology

Calcium-dependent inactivation

Focal Segmental Glomerulosclerosis

TRPC channels

500

Oxidative Injury in Focal Segmental Glomerulosclerosis

Chan, James

01 February 2008

Background and objective: By reviewing our current understanding of oxidative injury as a cause of focal segmental glomerulosclerosis (FSGS), we hope to advance the use of antioxidants as a promising treatment in addition to the other therapeutic modalities to slow the rate of progression. Methods: Key references from the past concerning oxidative injury and FSGS were analyzed, together with those from a PubMed search of the literature from 1997 to 2007, to form the basis of this commentary. Results: In animal studies in FSGS produced by subtotal nephrectomy or puromycin injections, evidence of oxidant injury provided the rationale for disease reversal with an antioxidant such as high dose vitamin E. Clinical trial in children with FSGS using vitamin E resulted in significant reduction in proteinuria. Other treatment modalities in children with FSGS over the past four decades were reviewed. These consisted of one or more of the following medications: oral prednisone, angiotensin converting enzyme inhibitors, angiotensin receptor blockers, and intravenous methylprednisolone with and without cyclophosphamide or cyclosporine. The prognosis with these recent therapeutic interventions improved the outcome of children with FSGS compared to no treatment as advocated earlier. However, when the current regimen of combined treatment was compared with the regimen of prednisone plus cyclophosphamide, there was no difference in Kaplan-Meier kidney survival rate at a mean follow-up of 12 to 16 years. Conclusion: In reviewing current concepts of oxidant injury and other mechanisms of injury in the development of FSGS and the available modalities of treatment, we call into question, whether the cost and side effects of intravenous methylprednisolone is justifiable on the basis of unchanged kidney survival rates with continuing this particular mode of intervention.

Africa-American

combined therapy

focal segmental glomerulosclerosis

long-term outcome

oxidative injury

EXPRESSION MICROARRAY ANALYSIS OF RENAL DEVELOPMENT AND HUMAN RENAL DISEASE

SCHWAB, KRISTOPHER R.

January 2006

No description available.

microarray

Wnt signaling

metanephros

kidney development

focal segmental glomerulosclerosis

Hox genes

gene knockout mice

Mutační analýza genu TRPC6 u pacientů s nefrotickým syndromem / Mutational analysis of the TRPC6 gene in patients with nephrotic syndrome

Obeidová, Lena

January 2011

Focal segmental glomerulosclerosis is one of the commonest cause of the nephrotic syndrome in adults patients. It is a damage of glomerulus characterized by leakage of proteins to urine and oedemas which usually develops into the end-stage renal disease within 10 years. Recently have been described familial forms of this disease which arise from injury to proteins making up filtration barrier of kidney. In 2005 non-selective ion channel TRPC6 was assigned among these proteins. In this thesis I focused on summarizing existing knowledge of the nephrotic syndrome, focal segmental glomerulosclerosis and involvement of TRPC6 in their origin. Second part of this work is devoted to the screening analysis of TRPC6 gene to discover possible mutations and polymorfisms in 47 patients with histologically proven focal segmental glomerulosclerosis or minimal change disease. The used methods were high resolution melting and direct sequencing. In the group of patients was detected no pathogenic mutation, only 2 known polymorfisms P15S and A404V and few changes which do not result in alteration of amino acid. So it seems TRPC6 gene mutations are a rare cause of the focal segmental glomerulosclerosis in adult patients in the Czech Republic.

Estudo das doenças glomerulares na Zona da Mata Mineira

Carmo, Priscylla Aparecida Vieira do

15 February 2008

Submitted by Renata Lopes (renatasil82@gmail.com) on 2016-10-18T11:17:00Z No. of bitstreams: 1 priscyllaaparecidavieiradocarmo.pdf: 1470676 bytes, checksum: fd5e83ad78ccfe4675fb74294a6ad3a6 (MD5) / Approved for entry into archive by Adriana Oliveira (adriana.oliveira@ufjf.edu.br) on 2016-10-25T12:06:50Z (GMT) No. of bitstreams: 1 priscyllaaparecidavieiradocarmo.pdf: 1470676 bytes, checksum: fd5e83ad78ccfe4675fb74294a6ad3a6 (MD5) / Made available in DSpace on 2016-10-25T12:06:50Z (GMT). No. of bitstreams: 1 priscyllaaparecidavieiradocarmo.pdf: 1470676 bytes, checksum: fd5e83ad78ccfe4675fb74294a6ad3a6 (MD5) Previous issue date: 2008-02-15 / CAPES - Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / As glomerulopatias persistem entre as principais causas de doença renal crônica dialítica em nosso país. Traçar um perfil destas doenças assume importância não só como fonte para investigações clínicas e epidemiológicas, como também constitui-se em importante passo para o conhecimento da história natural das doenças glomerulares. O presente estudo avaliou o perfil das doenças glomerulares na Zona da Mata Mineira, estabelecendo a distribuição e freqüência dos tipos histológicos das glomerulopatias primárias e secundárias, relacionando-os com os achados clínico laboratoriais. Foram realizadas 261 biópsias, sendo que 126 delas correspondiam a rins nativos de adultos e foram consideradas para análise. A síndrome glomerular mais freqüente foi a nefrótica (55,2%), seguida da síndrome de anormalidades urinárias (28,8%). As glomerulopatias primárias e secundárias predominantes foram a glomeruloesclerose segmentar e focal (40,8%) e a nefrite lúpica (80,7%), respectivamente. Considerando-se toda a população, a GESF foi a glomerulopatia predominante (n=31; 24,6%), seguida pela nefrite lúpica (n=21; 16,6%) e pela nefropatia por IgA (n=16; 12,6%). Dentre as principais causas de síndrome nefrótica, a 10 GESF foi a glomerulopatia mais freqüentemente encontrada (27,5%), seguida pela nefrite lúpica (23,1%). Na síndrome de anormalidades urinárias, os diagnósticos mais freqüentes foram o rim normal (27,7%) e a nefropatia por IgA (22,2%). A maioria dos pacientes avaliados apresentavam algum grau de cronicidade à biópsia renal (56,3%), que se relacionou com menores valores de filtração glomerular. Este estudo forneceu informações importantes sobre as glomerulopatias na nossa região, contribuindo não só para uma adequada documentação da distribuição destas doenças entre nós, mas sobretudo para definição de melhores condutas visando terapêuticas cada vez mais específicas para diferentes tipos histológicos. / Glomerulopathies are still among the main causes of chronic kidney diseases requiring dialysis in our country. It is important to establish a profile of these diseases not only as a source for clinical and epidemiological investigations, but also because this is an important step for the knowledge of the natural history of glomerular diseases. This study assessed the profile of glomerular diseases in the Zona da Mata region of Minas Gerais, and established the distribution and frequency of the histological types of primary and secondary glomerulopathies, comparing them to clinical-laboratorial results. 261 biopsies were carried out, 126 of which were native adult kidneys and which were submitted to analysis. The most common glomerular syndrome was nephrotic syndrome (55.2%), followed by urinary abnormality syndrome (28.8%). The predominant primary and secondary glomerulopathies were focal segmental glomerulosclerosis (40.8%) and lupus nephritis (80.7%), respectively. Considering the whole population, FSGS was the predominant glomerulopathy (n=31; 24.6%), followed by lupus nephritis (n=21; 16.6%) and IgA nephropathy (n=16; 12.6%). Among the main causes of nephrotic syndrome, FSGS was the most frequently found glomerulopathy (27.5%), followed by lupus nephritis (23.1%). In the urinary abnormality syndrome, the most common diagnoses 12 were normal kidney (27.7%) and IgA nephropathy (22.2%). The majority of the patients presented some degree of chronicity at the renal biopsy (56,3%), which correlated with lower values of glomerular filtration rate. This study supplied important information about glomerulopathies in our region, contributing not only to suitable documentation on the distribution of these diseases among us, but particularly to a definition of more appropriate conduct, aiming at therapies that are more and more specific for different histological types.

CNPQ::CIENCIAS DA SAUDE::MEDICINA

Glomerulopatias

Biópsia renal

Glomeruloesclerose segmentar e focal

Nefrite lúpica

Síndrome nefrótica

Anormalidades urinárias

Glomerulopathies

Renal biopsy

Focal segmental glomerulosclerosis

Lupus nephritis

Nephrotic syndrome

Urinary abnormalities

Genetické faktory ovlivňující průběh vybraných forem nefrotického syndromu / Genetic factors affecting course of selected forms of nephrotic syndrome

Šafaříková, Markéta

January 2011

Nephrotic syndrome (NS) is characterized by proteinuria, hypalbuminemia and edemas. It occurs during first and second glomerulopathies. This disease can be divided into two groups: primary (idiopathic) and secondary. The heredity of the familial nephrotic syndrome is autosomal dominant and autosomal recessive. There are four most important genes that condition the formation of hereditary nephrotic syndrome in adult patienst. These genes are ACTN4, CD2AP, NPHS2 and TRPC6. The gene ACTN4, which encodes protein α-actinin 4, is responsible for the autosomal dominant form of focal segmental glomerulosclerosis (FSGS). FSGS is included in first glomerulopathies. α-Actinin 4 was also researched for some types of carcinomas. There was performed the mutational analysis of the gene ACTN4 on the set of 48 patients with nephrotic syndrome in this diploma thesis. High resolution melting (HRM) analysis and sequencing selected samples were used during this mutation detection. During this process many published and unpublished SNPs and one unpublished candidate mutation that could have causal associations with FSGS were found.