A likely HOXC4 predisposition variant for Chiari malformations

Douglas L Brockmeyer; Samuel H Cheshier; Jeff Stevens; Julio C Facelli; Kerry Rowe; John D Heiss; Anthony Musolf; David H Viskochil; Kristina L Allen-Brady; Lisa A Cannon-Albright

doi:10.3171/2022.10.JNS22956

A likely HOXC4 predisposition variant for Chiari malformations

J Neurosurg. 2022 Nov 25;139(1):266-274. doi: 10.3171/2022.10.JNS22956. Print 2023 Jul 1.

Authors

Douglas L Brockmeyer^{1

2}, Samuel H Cheshier^{1

2

3}, Jeff Stevens⁴, Julio C Facelli⁵, Kerry Rowe², John D Heiss⁶, Anthony Musolf⁷, David H Viskochil^{2

8}, Kristina L Allen-Brady⁴, Lisa A Cannon-Albright^{3

4}

Affiliations

¹ 1Division of Pediatric Neurosurgery, Department of Neurosurgery, University of Utah, Salt Lake City, Utah.
² 2Intermountain Healthcare, Salt Lake City, Utah.
³ 3Huntsman Cancer Institute, Salt Lake City, Utah.
⁴ 4Genetic Epidemiology, Department of Internal Medicine, University of Utah, Salt Lake City, Utah.
⁵ Departments of5Biomedical Informatics and.
⁶ 6Surgical Neurology Branch, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland; and.
⁷ 7Statistical Genetics Section, Computational and Statistical Genomics Branch, National Human Genome Research Institute, National Institutes of Health, Bethesda, Maryland.
⁸ 8Pediatrics, University of Utah, Salt Lake City, Utah.

Abstract

Objective: Inherited variants predisposing patients to type 1 or 1.5 Chiari malformation (CM) have been hypothesized but have proven difficult to confirm. The authors used a unique high-risk pedigree population resource and approach to identify rare candidate variants that likely predispose individuals to CM and protein structure prediction tools to identify pathogenicity mechanisms.

Methods: By using the Utah Population Database, the authors identified pedigrees with significantly increased numbers of members with CM diagnosis. From a separate DNA biorepository of 451 samples from CM patients and families, 32 CM patients belonging to 1 or more of 24 high-risk Chiari pedigrees were identified. Two high-risk pedigrees had 3 CM-affected relatives, and 22 pedigrees had 2 CM-affected relatives. To identify rare candidate predisposition gene variants, whole-exome sequence data from these 32 CM patients belonging to 24 CM-affected related pairs from high-risk pedigrees were analyzed. The I-TASSER package for protein structure prediction was used to predict the structures of both the wild-type and mutant proteins found here.

Results: Sequence analysis of the 24 affected relative pairs identified 38 rare candidate Chiari predisposition gene variants that were shared by at least 1 CM-affected pair from a high-risk pedigree. The authors found a candidate variant in HOXC4 that was shared by 2 CM-affected patients in 2 independent pedigrees. All 4 of these CM cases, 2 in each pedigree, exhibited a specific craniocervical bony phenotype defined by a clivoaxial angle less than 125°. The protein structure prediction results suggested that the mutation considered here may reduce the binding affinity of HOXC4 to DNA.

Conclusions: Analysis of unique and powerful Utah genetic resources allowed identification of 38 strong candidate CM predisposition gene variants. These variants should be pursued in independent populations. One of the candidates, a rare HOXC4 variant, was identified in 2 high-risk CM pedigrees, with this variant possibly predisposing patients to a Chiari phenotype with craniocervical kyphosis.

Keywords: Chiari malformation; Utah Population Database; craniocervical kyphosis; high-risk pedigree; predisposition; protein prediction modeling.

MeSH terms

Brain* / abnormalities
Genetic Predisposition to Disease* / genetics
Genotype
Homeodomain Proteins* / genetics
Humans
Mutation
Pedigree
Phenotype
Risk Factors

Substances

Homeodomain Proteins
HOXC4 protein, human

Grants and funding

UL1 TR002538/TR/NCATS NIH HHS/United States