Functional analysis of promoter mutations in the ACTN4 and SYNPO genes in focal segmental glomerulosclerosis

doi:10.1093/ndt/gfp394

NDT Advance Access published online on August 7, 2009
Nephrology Dialysis Transplantation, doi:10.1093/ndt/gfp394

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Functional analysis of promoter mutations in the ACTN4 and SYNPO genes in focal segmental glomerulosclerosis

Shengchuan Dai¹^,*, Zhaohui Wang¹^,*, Xiaoxia Pan¹, Weiming Wang¹, Xiaonong Chen¹, Hong Ren¹, Cuilan Hao¹, Bin Han² and Nan Chen¹

¹ Department of Nephrology, Ruijin Hospital, School of Medicine, Shanghai Jiaotong University ² National Center for Gene Research, Shanghai Institutes for Biological Sciences, Chinese Academy of Sciences, Shanghai, China

Correspondence and offprint requests to: Nan Chen; E-mail: chen-nan{at}medmail.com.cn

Abstract

Background. To investigate the promoter mutations of ACTN4 andSYNPO genes in patients with idiopathic focal segmental glomerulosclerosis(FSGS), and to provide functional analysis of these mutationsin the role of FSGS occurrence.

Methods. The study consisted of 82 Chinese idiopathic FSGS patients(55 patients had nephrotic syndrome: NS) and 90 healthy individuals.Genomic DNA extracted from peripheral leukocytes of patientsof healthy individuals were used to analyse the ACTN4 and SYNPOgene promoter mutations by polymerase chain reaction (PCR) anddirect sequencing. Mutations were matched with GenBank and TRANSFACsoftware database (www.genometix.de; www.gene-regulation.com).A dual luciferase assay system was used to analyse the effectsof mutations based on PGL3-Basic vector, pRL-SV40 vector, aPC12 cell line and podocytes in vitro. Kidney alpha-actinin-4and synaptopodin expression of mutated patients and genomicDNA of their parents were investigated.

Results. The study detected the ACTN4 gene promoter 1–34C>T,1–590delA and (1–1044delT)+(1–797T>C)+(1–769A>G)heterozygous mutations in three patients, respectively, andthe SYNPO gene promoter 1–24G>A and 1–851C>Theterozygous mutations in two patients, respectively (with adenineof translation start site ATG naming +1). The same mutationswere not found in the control group of 90 healthy people. Exceptingone patient with an ACTN4 gene promoter mutation who inheritedher parents’ 1–1044delT and 1–797T>C mutatedchromosome, respectively, the same mutations were not foundin patients’ parents. Alpha-actinin-4 and synaptopodinprotein expression are reduced in mutated patients’ kidneys.Dual luciferase assays show that compared to the normal group(with the exception of the 1–1044delT group), luciferaseactivity in mutated groups decreased for the most part. (1–1044delT)+(1–797T>C)+(1–769A>G)mutations are associated with poor clinical outcomes, and patientswith these mutations progress to end-stage renal failure.

Conclusion. The study detected heterozygous mutations in thepromoters of the ACTN4 and SYNPO genes in patients with idiopathicFSGS. These mutations affected gene transcription in vitro andmay affect protein translation in vivo. So we presumed thatthe ACTN4 and SYNPO promoter mutations might also contributeto pathophysiology of idiopathic FSGS.

Keywords: ACTN4; focal segmental glomerulosclerosis; mutation; promoter; SYNPO

^* The first two authors contributed equally to this work.

Received for publication: 26. 9.08
Accepted in revised form: 13. 7.09

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