Transcriptome Analyses Reveal Molecular Mechanisms of Novel Compound Heterozygous Variants Causing Infantile Cerebellar Retinal Degeneration

Overview

Journal Front Cell Neurosci

Specialty Cell Biology

Date 2024 Nov 27

PMID 39600307

Authors

Wenke Yang

Shuyue Wang

Ke Yang

Yanjun Li

Zhenglong Guo

Jianmei Huang

Jinming Wang

Shixiu Liao

Affiliations

Soon will be listed here.

Abstract

Background And Purpose: Infantile cerebellar retinal degeneration (ICRD) (OMIM #614559) is a rare autosomal recessive inherited disease associated with mutations in the aconitase 2 (ACO2) gene. We report a Chinese girl with novel compound heterozygous variants in , who presented at 7 months of age with psychomotor retardation, truncal hypotonia, and ophthalmologic abnormalities. This study aims to investigate the potential molecular mechanisms underlying deficiency-induced neuropathy.

Methods: Whole exome sequencing was performed on family members to screen for potential pathogenic mutations, followed by Sanger sequencing for validation. Mitochondrial aconitase activity and mitochondrial DNA (mtDNA) copy number were measured using an aconitase activity detection kit and quantitative PCR, respectively. Transcriptome expression profiles from patient cells, and cerebellar and retinal organoids retrieved from the GEO database were integrated. Functional enrichment analysis and protein-protein interaction networks were used to identify key molecules, and their expression levels were validated using Western blot analysis.

Results: Genetic testing revealed novel compound heterozygous variations in the proband's gene (NM:001098), including c.854A>G (p.Asn285Ser) and c.1183C>T (p.Arg395Cys). Predictive analysis of the tertiary structure of the ACO2 protein suggests that both p.Asn285Ser and p.Arg395Cys affect the binding ability of ACO2 to ligands. The mitochondrial aconitase activity and mtDNA copy number in the proband's leukocytes were significantly reduced. Transcriptomic data analysis identified 80 key candidate genes involved in ACO2-related neuropathy. Among these, and , whose gene expression levels were significantly positively correlated with , were further validated by Western blot analysis.

Conclusions: This study expands the spectrum of pathogenic variants, elucidates the potential molecular mechanisms underlying ACO2-related neuropathy, provides in-depth support for the pathogenicity of genetic variations, and offers new insights into the pathogenesis of ICRD.

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