Clinical and Molecular Findings of Intermediate Allele Carriers in the HTT Gene from the Mexican Mestizo Population

Miguel Ángel Ramírez-García; David José Dávila-Ortiz de Montellano; Leticia Martínez-Ruano; Adriana Ochoa-Morales; Sandra Romero-Hidalgo; Juan Carlos Zenteno; Petra Yescas-Gómez

doi:10.1159/000526260

Clinical and Molecular Findings of Intermediate Allele Carriers in the HTT Gene from the Mexican Mestizo Population

Neurodegener Dis. 2022;22(1):34-42. doi: 10.1159/000526260. Epub 2022 Aug 4.

Authors

Miguel Ángel Ramírez-García^{1

2}, David José Dávila-Ortiz de Montellano¹, Leticia Martínez-Ruano¹, Adriana Ochoa-Morales¹, Sandra Romero-Hidalgo³, Juan Carlos Zenteno^{4

5}, Petra Yescas-Gómez¹

Affiliations

¹ Genetics Department, National Institute of Neurology and Neurosurgery Manuel Velasco Suárez, Mexico City, Mexico.
² Doctoral Program in Medical Sciences, National Autonomous University of Mexico, Mexico City, Mexico.
³ Computational Genetics, National Institute of Genomic Medicine, Mexico City, Mexico.
⁴ Research Unit-Genetics Department, Institute of Ophthalmology, "Conde de Valenciana", Mexico City, Mexico.
⁵ Department of Biochemistry, Faculty of Medicine, National Autonomous University of Mexico, Mexico City, Mexico.

PMID: 35926480
DOI: 10.1159/000526260

Abstract

Introduction: There are reports of different clinical statuses in carriers of intermediate alleles (IAs) of CAG trinucleotide repeats in the HTT gene, from individuals affected by a clinical picture indistinguishable from Huntington's disease (HD) to those without manifestations. Therefore, the possible clinical significance of these alleles has been widely debated.

Objectives: The aim of this study was to describe general and clinical features and discard HD phenocopies by molecular assessment in a case series of IA carriers on the HTT gene of a laboratory sample from a neurological center in Mexico.

Methods: We selected individuals who had previously been tested for the HTT gene expansion, which resulted in IAs. Clinical information was obtained from medical records, and molecular analysis of the JPH3, PRNP, and TBP genes was performed only in IA carriers with clinical manifestations. In addition, two patients with IA and acanthocytes were evaluated by whole-exome sequencing. The scientific and ethical committees of the National Institute of Neurology and Neurosurgery Manuel Velasco Suárez (NINNMVS) approved this study.

Results: From 1994 to 2019, the Genetics Department of the NINNMVS confirmed 34 individuals with IAs, 15 of whom belonged to 11 families with HD (IA-HD) and 19 of whom had no family history of HD (IA-non-HD). We found a high proportion of manifestations of the HD phenotypic spectrum in the IA-non-HD subgroup. In addition, among the 20 samples of IA carriers with manifestations molecularly evaluated, we identified two unrelated subjects with CAG/CTG repeat expansions on the JPH3 gene, confirming HD-like 2 (HDL2), and one patient with the homozygous pathogenic c.3232G>T variant (p.Glu1078Ter) in the VPS13A gene, demonstrating choreoacanthocytosis.

Discussion/conclusion: Our results show the most extensive series of subjects with IAs and clinical manifestations. In addition, we identify three HD phenocopies, two HDL2 cases, and one choreoacanthocytosis case. Therefore, we emphasize evaluating other HD phenocopies in IA carriers with clinical manifestations whose family background is not associated with HD.

Keywords: Choreoacanthocytosis; HTT gene; Huntington’s disease phenocopies; Huntington’s disease-like 2; Intermediate alleles.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Alleles
Humans
Huntingtin Protein / genetics
Huntington Disease* / epidemiology
Huntington Disease* / genetics
Mexico
Neuroacanthocytosis* / genetics
Trinucleotide Repeat Expansion / genetics

Substances

Huntingtin Protein
HTT protein, human

Supplementary concepts

Huntington Disease-Like Syndrome