What question did this study set out to answer?

To characterize clinical and molecular aspects of a case of giant axonal neuropathy caused by a homozygous GAN variant.

March 26, 2026Open Access

Clinical and molecular characteriz ation of giant axonal neuropathy due to a homozygous c.851+1G>A variant in GAN: a case report and literature review

Key Points

To characterize clinical and molecular aspects of a case of giant axonal neuropathy caused by a homozygous GAN variant.
Clinical evaluation of symptoms and physical features in a 7-year-old girl.
Sanger sequencing for PTPN11 and RASopathy gene panel testing.
Whole-exome sequencing to identify genetic variants.
Neuroimaging via brain MRI for structural analysis.
Haplotype analysis to explore parental consanguinity and genetic inheritance.
Identified a homozygous c.851+1 G>A variant in the GAN gene.
Clinical features included global developmental delay and kinky hair.
Neuroimaging showed peridentate hyperintensities.
Variant classified as pathogenic following ACMG/AMP guidelines.
Evidence of a possible founder effect in the Mexican population.

Abstract

Background Giant Axonal Neuropathy (GAN) is a rare autosomal recessive neurodegenerative disorder caused by biallelic pathogenic variants in the GAN gene, which encodes gigaxonin. The disease typically begins in childhood and is characterized by muscle weakness, gait disturbances, peripheral neuropathy, and distinctive kinky hair. Case description We report the clinical, radiological, and molecular findings of a 7-year-old Mexican girl from Jalisco, Mexico, born to consanguineous parents, who presented with global developmental delay and absence of independent ambulation by age of five. Additional features included kinky hair, broad forehead, blepharoptosis, depressed nasal bridge with a bulbous tip, high-arched palate, micrognathia, and generalized joint hyperlaxity. Given the phenotypic overlap with Noonan syndrome, PTPN11 Sanger sequencing was initially performed, followed by a RASopathy gene panel; both analyses yielded negative results. Results Whole-exome sequencing identified a homozygous splice-site variant in GAN c.851+1 G>A, which was confirmed by Sanger sequencing. Both parents were heterozygous carriers, consistent with parental consanguinity. According to ACMG/AMP guidelines (PVS1, PM2, PM3), the variant was classified as pathogenic. Additional studies, including brain magnetic resonance imaging, revealed peridentate hyperintensities compatible with gliosis or hypomyelination. Conclusion The integration of clinical features, neuroimaging findings, and molecular analysis confirmed the diagnosis of giant axonal neuropathy type 1. This case underscores the clinical relevance of whole-exome sequencing in patients with overlapping syndromic features. Notably, the GAN c.851+1 G>A variant has previously been reported in at least five homozygous patients of Mexican ancestry, supporting a possible founder effect in this population. • Homozygous GAN c.851+1 G>A variant identified in a Mexican patient • Noonan syndrome was initially suspected due to overlapping clinical features with GAN. • Whole-exome sequencing enabled a definitive molecular diagnosis • Haplotype analysis supports a possible founder effect

Clinical and molecular characteriz ation of giant axonal neuropathy due to a homozygous c.851+1G>A variant in GAN: a case report and literature review

Key Points

Abstract

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