Evolutionary coupling analysis identifies the impact of disease-associated variants at less-conserved sites

Author:

Kim Donghyo1,Han Seong Kyu1,Lee Kwanghwan1,Kim Inhae1,Kong JungHo1,Kim Sanguk1

Affiliation:

1. Department of Life Sciences, Pohang University of Science and Technology, Pohang 790-784, Korea

Abstract

Abstract Genome-wide association studies have discovered a large number of genetic variants in human patients with the disease. Thus, predicting the impact of these variants is important for sorting disease-associated variants (DVs) from neutral variants. Current methods to predict the mutational impacts depend on evolutionary conservation at the mutation site, which is determined using homologous sequences and based on the assumption that variants at well-conserved sites have high impacts. However, many DVs at less-conserved but functionally important sites cannot be predicted by the current methods. Here, we present a method to find DVs at less-conserved sites by predicting the mutational impacts using evolutionary coupling analysis. Functionally important and evolutionarily coupled sites often have compensatory variants on cooperative sites to avoid loss of function. We found that our method identified known intolerant variants in a diverse group of proteins. Furthermore, at less-conserved sites, we identified DVs that were not identified using conservation-based methods. These newly identified DVs were frequently found at protein interaction interfaces, where species-specific mutations often alter interaction specificity. This work presents a means to identify less-conserved DVs and provides insight into the relationship between evolutionarily coupled sites and human DVs.

Funder

Korean National Research Foundation

Korea Institute of Marine Science & Technology

Publisher

Oxford University Press (OUP)

Subject

Genetics

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