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HNF1B Alters an Evolutionarily Conserved Nephrogenic Program of Target Genes

Authors :
Grand, Kelli
Stoltz, Martine
Rizzo, Ludovica
Röck, Ruth
Kaminski, Michael M
Salinas, Gabriela
Getwan, Maike
Naert, Thomas
Pichler, Roman
Lienkamp, Soeren Sten
University of Zurich
Source :
JOURNAL OF THE AMERICAN SOCIETY OF NEPHROLOGY
Publication Year :
2023

Abstract

Background Hepatocyte nuclear factor-1 b (HNF1B) is an essential transcription factor during embryogenesis. Mutations in HNF1B are the most common monogenic causes of congenital cystic dysplastic renal malformations. The direct functional consequences of mutations in HNF1B on its transcriptional activity are unknown.Methods Direct reprogramming of mouse fibroblasts to induced renal tubular epithelial cells was conducted both with wild-type HNF1B and with patient mutations. HNF1B was expressed in Xenopus ectodermal explants. Transcriptomic analysis by bulk RNA-Seq identified conserved targets with differentially regulated expression by the wild-type or R295C mutant. CRISPR/Cas9 genome editing in Xenopus embryos evaluated transcriptional targets in vivo.Results HNF1B is essential for reprogramming mouse fibroblasts to induced renal tubular epithelial cells and induces development of ectopic renal organoids from pluripotent Xenopus cells. The mutation R295C retains reprogramming and inductive capacity but alters the expression of specific sets of downstream target genes instead of diminishing overall transcriptional activity of HNF1B. Surprisingly, targets associated with polycystic kidney disease were less affected than genes affected in congenital renal anomalies. Cross-species-conserved transcriptional targets were dysregulated in hnf1b CRISPR-depleted Xenopus embryos, confirming their dependence on hnf1b.Conclusions HNF1B activates an evolutionarily conserved program of target genes that disease-causing mutations selectively disrupt. These findings provide insights into the renal transcriptional network that controls nephrogenesis.

Details

Language :
English
ISSN :
10466673 and 15333450
Database :
OpenAIRE
Journal :
JOURNAL OF THE AMERICAN SOCIETY OF NEPHROLOGY
Accession number :
edsair.doi.dedup.....f060266ce4d8741f941cedddb902bf91