Network-Based Assessment of Minimal Change Disease Identifies Glomerular Response to IL-7 and IL-12 Pathways Activation as Innovative Treatment Target

Øystein Eikrem; Bjørnar Lillefosse; Nicolas Delaleu; Philipp Strauss; Tarig Osman; Bjørn Egil Vikse; Hanna Debiec; Pierre Ronco; Miroslav Sekulic; Even Koch; Jessica Furriol; Sabine Maria Leh; Hans-Peter Marti

doi:10.3390/biomedicines11010226

Network-Based Assessment of Minimal Change Disease Identifies Glomerular Response to IL-7 and IL-12 Pathways Activation as Innovative Treatment Target

Biomedicines. 2023 Jan 16;11(1):226. doi: 10.3390/biomedicines11010226.

Authors

Affiliations

¹ Department of Clinical Medicine, University of Bergen, 5020 Bergen, Norway.
² Department of Medicine, Haukeland University Hospital, 5021 Bergen, Norway.
³ 2cSysBioMed, 6646 Contra, Switzerland.
⁴ INSERM UMRS 1155, Hôpital Tenon, 75020 Paris, France.
⁵ Department of Pathology and Cell Biology, Columbia University, New York, NY 10032, USA.
⁶ Department of Pathology, Haukeland University Hospital, 5021 Bergen, Norway.

Abstract

Background: Minimal change disease (MCD), a major cause of nephrotic syndrome, is usually treated by corticosteroid administration. MCD unresponsiveness to therapy and recurrences are nonetheless frequently observed, particularly in adults. To explore MCD-related pathogenetic mechanisms and to identify novel drug targets ultimately contributing to novel therapeutic avenues with a certain specificity for MCD, we compared glomerular transcriptomes from MCD with membranous nephropathy (MN) patients and healthy controls. Methods: Renal biopsies from adult patients with MCD (n = 14) or MN (n = 12), and non-diseased controls (n = 8) were selected from the Norwegian Kidney Biopsy Registry. RNA for 75 base-pair paired-end RNASeq were obtained from laser capture micro-dissected (LCM) glomeruli from FFPE sections. Transcriptional landscapes were computed by combining pathway-centered analyses and network science methodologies that integrate multiple bioinformatics resources. Results: Compared to normal glomeruli, cells from MCD displayed an inflammatory signature apparently governed by the IL1 and IL7 systems. While enrichment of IL1 production and secretion was a shared feature of MCD and MN compared to normal tissue, responses involving IL7 pathway activation were unique to MCD. Indeed, IL7R expressed by glomeruli was the most upregulated gene of the interleukin family in MCD versus normal controls. IL7 pathway activation was paralleled by significant enrichment in adaptive immune system processes and transcriptional regulation and depletion in pathways related to energy metabolism and transcription. Downregulation of these organ function-related themes again occurred predominately in MCD and was significantly less pronounced in MN. Immunofluorescence and immunohistochemistry, respectively, confirmed the expression of phosphorylated IL-7 receptor alpha (IL7RA, CD127) and IL12 receptor beta 1 (IL12RB1) proteins. Conclusions: Gene expression profiling of archival FFPE-biopsies identifies MCD-specific signatures with IL7RA and IL12RB1 as novel targets for MCD treatment.

Keywords: IL-12; IL-7; membranous nephropathy; minimal change disease; transcriptome.

Abstract

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