Expression profiling of cultured podocytes exposed to nephrotic plasma reveals intrinsic molecular signatures of nephrotic syndrome

Stuti Panigrahi; Varsha Chhotusing Pardeshi; Karthikeyan Chandrasekaran; Karthik Neelakandan; Hari PS; Anil Vasudevan

doi:10.3345/cep.2020.00619

Clinical and Experimental Pediatrics (Jul 2021)

Expression profiling of cultured podocytes exposed to nephrotic plasma reveals intrinsic molecular signatures of nephrotic syndrome

Stuti Panigrahi,
Varsha Chhotusing Pardeshi,
Karthikeyan Chandrasekaran,
Karthik Neelakandan,
Hari PS,
Anil Vasudevan

Affiliations

Stuti Panigrahi: Division of Molecular Medicine, St. John’s Research Institute, St. John’s Medical College, Bangalore, India
Varsha Chhotusing Pardeshi: Division of Molecular Medicine, St. John’s Research Institute, St. John’s Medical College, Bangalore, India
Karthikeyan Chandrasekaran: Division of Molecular Medicine, St. John’s Research Institute, St. John’s Medical College, Bangalore, India
Karthik Neelakandan: Division of Molecular Medicine, St. John’s Research Institute, St. John’s Medical College, Bangalore, India
Hari PS: Division of Molecular Medicine, St. John’s Research Institute, St. John’s Medical College, Bangalore, India
Anil Vasudevan: Division of Molecular Medicine, St. John’s Research Institute, St. John’s Medical College, Bangalore, India

DOI: https://doi.org/10.3345/cep.2020.00619
Journal volume & issue: Vol. 64, no. 7
pp. 355 – 363

Abstract

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Background Nephrotic syndrome (NS) is a common renal disorder in children attributed to podocyte injury. However, children with the same diagnosis have markedly variable treatment responses, clinical courses, and outcomes, suggesting molecular heterogeneity. Purpose This study aimed to explore the molecular responses of podocytes to nephrotic plasma to identify specific genes and signaling pathways differentiating various clinical NS groups as well as biological processes that drive injury in normal podocytes. Methods Transcriptome profiles from immortalized human podocyte cell line exposed to the plasma of 8 subjects (steroid-sensitive nephrotic syndrome [SSNS], n=4; steroid-resistant nephrotic syndrome [SRNS], n=2; and healthy adult individuals [control], n=2) were generated using microarray analysis. Results Unsupervised hierarchical clustering of global gene expression data was broadly correlated with the clinical classification of NS. Differential gene expression (DGE) analysis of diseased groups (SSNS or SRNS) versus healthy controls identified 105 genes (58 up-regulated, 47 down-regulated) in SSNS and 139 genes (78 up-regulated, 61 down-regulated) in SRNS with 55 common to SSNS and SRNS, while the rest were unique (50 in SSNS, 84 genes in SRNS). Pathway analysis of the significant (P≤0.05, -1≤ log2 FC ≥1) differentially expressed genes identified the transforming growth factor-β and Janus kinase-signal transducer and activator of transcription pathways to be involved in both SSNS and SRNS. DGE analysis of SSNS versus SRNS identified 2,350 genes with values of P≤0.05, and a heatmap of corresponding expression values of these genes in each subject showed clear differences in SSNS and SRNS. Conclusion Our study observations indicate that, although podocyte injury follows similar pathways in different clinical subgroups, the pathways are modulated differently as evidenced by the heatmap. Such transcriptome profiling with a larger cohort can stratify patients into intrinsic subtypes and provide insight into the molecular mechanisms of podocyte injury.

Published in Clinical and Experimental Pediatrics

ISSN: 2713-4148 (Online)
Publisher: The Korean Pediatric Society
Country of publisher: Korea, Republic of
LCC subjects: Medicine: Pediatrics
Website: http://www.e-cep.org

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