Genotype–phenotype correlations and clinical outcomes of genetic TRPC6 podocytopathies

Podocytopathy associated with likely pathogenic/pathogenic variants of TRPC6 (TRPC6-AP) has been recognised for about 20 years. As a result of its rarity however, the spectrum of clinical phenotypes and genotype-phenotype correlation of TRPC6-AP remains poorly understood. Here, we characterised clin...

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Published inNephrology, dialysis, transplantation
Main Authors McAnallen, Susan M, Elhassan, Elhussein A E, Stoneman, Sinead, Pinto e Vairo, Filippo, Hogan, Marie C, Hoefele, Julia, Clince, Michelle, Mekraksakit, Poemlarp, Titan, Silvia M, Jorge, Sofia, Calado, Joaquim, Decramer, Stéphane, Colliou, Eloïse, Tellier, Stéphanie, Francisco, Telma, Servais, Aude, Cornet, Joséphine, de Fallois, Jonathan, Dossier, Claire, Fenoglio, Roberta, Renieri, Alessandra, Pinto, Anna Maria, Daga, Sergio, Loberti, Lorenzo, Fila, Marc, Quintana, Luis F, Becherucci, Francesca, Godefroid, Nathalie, Dubrasquet, Astrid, Kálmán, Tory, Dolan, Niamh, Alawi, Bushra Al, Sweeney, Clodagh, Riordan, Michael, Stack, Maria, Awan, Atif, Hui, Ng Kar, McCarthy, Hugh J, Biros, Erik, Harris, Trudie, Kidd, Kendrah, Haeberle, Stefanie, Bleyer, Anthony J, Mallett, Andrew J, Sayer, John A, Schafer, Franz, Benson, Katherine A, McCann, Emma, Conlon, Peter J
Format Journal Article
LanguageEnglish
Published England 19.05.2025
Subjects
FSGS
podocytopathy
TRPC6
steroid-resistant nephrotic syndrome
CKD
Online AccessGet full text
ISSN0931-0509
1460-2385
1460-2385
DOI10.1093/ndt/gfaf086

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Abstract Podocytopathy associated with likely pathogenic/pathogenic variants of TRPC6 (TRPC6-AP) has been recognised for about 20 years. As a result of its rarity however, the spectrum of clinical phenotypes and genotype-phenotype correlation of TRPC6-AP remains poorly understood. Here, we characterised clinical, histological, and genetic correlates of familial and sporadic patients with TRPC6-AP. In this multicentre observational study, an online questionnaire followed by a systematic literature review was performed to create a cohort with comprehensive data on genetic and clinical outcomes (age of onset, clinical presentation, treatment response, kidney biopsy findings, and progression to kidney failure). Logistic regression, Cox proportional hazards model and Kaplan-Meier analyses investigated the associations between genetic variants and disease progression. Among 87 families (96 familial and 45 sporadic cases), 31 distinct missense TRPC6 variants (including 2 novel) were identified, with c.2683C > T p.(Arg895Cys) and c.523C > T p.(Arg175Trp) the commonest variants. Proteinuric kidney disease/nephrotic syndrome was the most common clinical presentation (83.7%), while focal segmental glomerulosclerosis was the most common histological finding (89.4%). By 33 (interquartile range: 17-40) years, 48.9% (69/141) of patients had progressed to kidney failure. Sporadic TRPC6-AP demonstrated an earlier progression to kidney failure than familial cases (P = 0.001) and were more likely to present with nephrotic syndrome (odds ratio: 4.34 (1.85-10.15); P = 0.001). Gain-of-function TRPC6 variants were more frequent in familial than sporadic TRPC6-AP (70.8% vs. 44.4%; P = 0.004). Compared to patients with other TRPC6 variants, patients with TRPC6 p.R175W and p.R895C variants progressed to kidney failure earlier (median kidney survival of 21 years; Hazard ratios (HR): 2.985 [95% CI: 1.40-5.79] and 38 years; HR: 1.65 [95% CI: 1.01-2.81], respectively, log-rank P = 0.005). Our study shows unique clinical and genetic correlations of TRPC6-AP, which may enable personalised care and promising novel therapies.
AbstractList Podocytopathy associated with likely pathogenic/pathogenic variants of TRPC6 (TRPC6-AP) has been recognised for about 20 years. As a result of its rarity however, the spectrum of clinical phenotypes and genotype-phenotype correlation of TRPC6-AP remains poorly understood. Here, we characterised clinical, histological, and genetic correlates of familial and sporadic patients with TRPC6-AP.BACKGROUND AND HYPOTHESISPodocytopathy associated with likely pathogenic/pathogenic variants of TRPC6 (TRPC6-AP) has been recognised for about 20 years. As a result of its rarity however, the spectrum of clinical phenotypes and genotype-phenotype correlation of TRPC6-AP remains poorly understood. Here, we characterised clinical, histological, and genetic correlates of familial and sporadic patients with TRPC6-AP.In this multicentre observational study, an online questionnaire followed by a systematic literature review was performed to create a cohort with comprehensive data on genetic and clinical outcomes (age of onset, clinical presentation, treatment response, kidney biopsy findings, and progression to kidney failure). Logistic regression, Cox proportional hazards model and Kaplan-Meier analyses investigated the associations between genetic variants and disease progression.METHODSIn this multicentre observational study, an online questionnaire followed by a systematic literature review was performed to create a cohort with comprehensive data on genetic and clinical outcomes (age of onset, clinical presentation, treatment response, kidney biopsy findings, and progression to kidney failure). Logistic regression, Cox proportional hazards model and Kaplan-Meier analyses investigated the associations between genetic variants and disease progression.Among 87 families (96 familial and 45 sporadic cases), 31 distinct missense TRPC6 variants (including 2 novel) were identified, with c.2683C > T p.(Arg895Cys) and c.523C > T p.(Arg175Trp) the commonest variants. Proteinuric kidney disease/nephrotic syndrome was the most common clinical presentation (83.7%), while focal segmental glomerulosclerosis was the most common histological finding (89.4%). By 33 (interquartile range: 17-40) years, 48.9% (69/141) of patients had progressed to kidney failure. Sporadic TRPC6-AP demonstrated an earlier progression to kidney failure than familial cases (P = 0.001) and were more likely to present with nephrotic syndrome (odds ratio: 4.34 (1.85-10.15); P = 0.001). Gain-of-function TRPC6 variants were more frequent in familial than sporadic TRPC6-AP (70.8% vs. 44.4%; P = 0.004). Compared to patients with other TRPC6 variants, patients with TRPC6 p.R175W and p.R895C variants progressed to kidney failure earlier (median kidney survival of 21 years; Hazard ratios (HR): 2.985 [95% CI: 1.40-5.79] and 38 years; HR: 1.65 [95% CI: 1.01-2.81], respectively, log-rank P = 0.005).RESULTSAmong 87 families (96 familial and 45 sporadic cases), 31 distinct missense TRPC6 variants (including 2 novel) were identified, with c.2683C > T p.(Arg895Cys) and c.523C > T p.(Arg175Trp) the commonest variants. Proteinuric kidney disease/nephrotic syndrome was the most common clinical presentation (83.7%), while focal segmental glomerulosclerosis was the most common histological finding (89.4%). By 33 (interquartile range: 17-40) years, 48.9% (69/141) of patients had progressed to kidney failure. Sporadic TRPC6-AP demonstrated an earlier progression to kidney failure than familial cases (P = 0.001) and were more likely to present with nephrotic syndrome (odds ratio: 4.34 (1.85-10.15); P = 0.001). Gain-of-function TRPC6 variants were more frequent in familial than sporadic TRPC6-AP (70.8% vs. 44.4%; P = 0.004). Compared to patients with other TRPC6 variants, patients with TRPC6 p.R175W and p.R895C variants progressed to kidney failure earlier (median kidney survival of 21 years; Hazard ratios (HR): 2.985 [95% CI: 1.40-5.79] and 38 years; HR: 1.65 [95% CI: 1.01-2.81], respectively, log-rank P = 0.005).Our study shows unique clinical and genetic correlations of TRPC6-AP, which may enable personalised care and promising novel therapies.CONCLUSIONOur study shows unique clinical and genetic correlations of TRPC6-AP, which may enable personalised care and promising novel therapies.
Podocytopathy associated with likely pathogenic/pathogenic variants of TRPC6 (TRPC6-AP) has been recognised for about 20 years. As a result of its rarity however, the spectrum of clinical phenotypes and genotype-phenotype correlation of TRPC6-AP remains poorly understood. Here, we characterised clinical, histological, and genetic correlates of familial and sporadic patients with TRPC6-AP. In this multicentre observational study, an online questionnaire followed by a systematic literature review was performed to create a cohort with comprehensive data on genetic and clinical outcomes (age of onset, clinical presentation, treatment response, kidney biopsy findings, and progression to kidney failure). Logistic regression, Cox proportional hazards model and Kaplan-Meier analyses investigated the associations between genetic variants and disease progression. Among 87 families (96 familial and 45 sporadic cases), 31 distinct missense TRPC6 variants (including 2 novel) were identified, with c.2683C > T p.(Arg895Cys) and c.523C > T p.(Arg175Trp) the commonest variants. Proteinuric kidney disease/nephrotic syndrome was the most common clinical presentation (83.7%), while focal segmental glomerulosclerosis was the most common histological finding (89.4%). By 33 (interquartile range: 17-40) years, 48.9% (69/141) of patients had progressed to kidney failure. Sporadic TRPC6-AP demonstrated an earlier progression to kidney failure than familial cases (P = 0.001) and were more likely to present with nephrotic syndrome (odds ratio: 4.34 (1.85-10.15); P = 0.001). Gain-of-function TRPC6 variants were more frequent in familial than sporadic TRPC6-AP (70.8% vs. 44.4%; P = 0.004). Compared to patients with other TRPC6 variants, patients with TRPC6 p.R175W and p.R895C variants progressed to kidney failure earlier (median kidney survival of 21 years; Hazard ratios (HR): 2.985 [95% CI: 1.40-5.79] and 38 years; HR: 1.65 [95% CI: 1.01-2.81], respectively, log-rank P = 0.005). Our study shows unique clinical and genetic correlations of TRPC6-AP, which may enable personalised care and promising novel therapies.
Author Stoneman, Sinead
Hui, Ng Kar
Daga, Sergio
Kidd, Kendrah
Dolan, Niamh
Quintana, Luis F
Pinto e Vairo, Filippo
Tellier, Stéphanie
Haeberle, Stefanie
de Fallois, Jonathan
Fenoglio, Roberta
Harris, Trudie
Titan, Silvia M
Mekraksakit, Poemlarp
Pinto, Anna Maria
Decramer, Stéphane
Cornet, Joséphine
Godefroid, Nathalie
Servais, Aude
Mallett, Andrew J
Fila, Marc
Becherucci, Francesca
Elhassan, Elhussein A E
McCarthy, Hugh J
Benson, Katherine A
Stack, Maria
Dossier, Claire
Awan, Atif
Conlon, Peter J
Alawi, Bushra Al
Riordan, Michael
Calado, Joaquim
Dubrasquet, Astrid
Francisco, Telma
Hogan, Marie C
Clince, Michelle
Renieri, Alessandra
Sayer, John A
Hoefele, Julia
Bleyer, Anthony J
Biros, Erik
Jorge, Sofia
McCann, Emma
Colliou, Eloïse
Schafer, Franz
Sweeney, Clodagh
McAnallen, Susan M
Kálmán, Tory
Loberti, Lorenzo
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Keywords FSGS
podocytopathy
TRPC6
steroid-resistant nephrotic syndrome
CKD
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The Author(s) 2025. Published by Oxford University Press on behalf of the ERA.
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PublicationTitle Nephrology, dialysis, transplantation
PublicationTitleAlternate Nephrol Dial Transplant
PublicationYear 2025
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Snippet Podocytopathy associated with likely pathogenic/pathogenic variants of TRPC6 (TRPC6-AP) has been recognised for about 20 years. As a result of its rarity...
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Title Genotype–phenotype correlations and clinical outcomes of genetic TRPC6 podocytopathies
URI https://www.ncbi.nlm.nih.gov/pubmed/40388293
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