Population-specific genetic modification of Huntington's disease in Venezuela.

Authors

Michael J Chao
Kyung-Hee Kim
Jun Wan Shin
Diane Lucente
Vanessa C Wheeler
Hong Li, Institute for Systems Biology, Seattle
Jared C Roach, Institute for Systems Biology, Seattle
Leroy Hood, Institute for Systems Biology, Seattle
Nancy S Wexler
Laura B Jardim
Peter Holmans
Lesley Jones
Michael Orth
Seung Kwak
Marcy E MacDonald
James F Gusella
Jong-Min Lee

Document Type

Article

Publication Date

5-1-2018

Publication Title

PLoS Genet

Keywords

Age of Onset; Family Health; Female; Gene-Environment Interaction; Genes, Modifier; Genetics, Population; Genome-Wide Association Study; Haplotypes; Humans; Huntingtin Protein; Huntington Disease; Male; Polymorphism, Single Nucleotide; Proteins; Venezuela; Whole Genome Sequencing

Abstract

Modifiers of Mendelian disorders can provide insights into disease mechanisms and guide therapeutic strategies. A recent genome-wide association (GWA) study discovered genetic modifiers of Huntington's disease (HD) onset in Europeans. Here, we performed whole genome sequencing and GWA analysis of a Venezuelan HD cluster whose families were crucial for the original mapping of the HD gene defect. The Venezuelan HD subjects develop motor symptoms earlier than their European counterparts, implying the potential for population-specific modifiers. The main Venezuelan HD family inherits HTT haplotype hap.03, which differs subtly at the sequence level from European HD hap.03, suggesting a different ancestral origin but not explaining the earlier age at onset in these Venezuelans. GWA analysis of the Venezuelan HD cluster suggests both population-specific and population-shared genetic modifiers. Genome-wide significant signals at 7p21.2-21.1 and suggestive association signals at 4p14 and 17q21.2 are evident only in Venezuelan HD, but genome-wide significant association signals at the established European chromosome 15 modifier locus are improved when Venezuelan HD data are included in the meta-analysis. Venezuelan-specific association signals on chromosome 7 center on SOSTDC1, which encodes a bone morphogenetic protein antagonist. The corresponding SNPs are associated with reduced expression of SOSTDC1 in non-Venezuelan tissue samples, suggesting that interaction of reduced SOSTDC1 expression with a population-specific genetic or environmental factor may be responsible for modification of HD onset in Venezuela. Detection of population-specific modification in Venezuelan HD supports the value of distinct disease populations in revealing novel aspects of a disease and population-relevant therapeutic strategies.

Clinical Institute

Neurosciences (Brain & Spine)

Department

Neurosciences

Recommended Citation

Chao, Michael J; Kim, Kyung-Hee; Shin, Jun Wan; Lucente, Diane; Wheeler, Vanessa C; Li, Hong; Roach, Jared C; Hood, Leroy; Wexler, Nancy S; Jardim, Laura B; Holmans, Peter; Jones, Lesley; Orth, Michael; Kwak, Seung; MacDonald, Marcy E; Gusella, James F; and Lee, Jong-Min, "Population-specific genetic modification of Huntington's disease in Venezuela." (2018). Articles, Abstracts, and Reports. 415.
https://digitalcommons.providence.org/publications/415