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Abstract

Aims:

Genomic studies play a major role in variant observations between and within populations and in identifying causal relationships between genotypes and phenotypes. Analyses using databases such as gnomAD can provide insight into the frequencies of alleles in large populations. There have been reports that detail such frequencies for several countries and ethnic groups, but as yet, there are no such datasets for the Czech population.

Patients and Methods:

Whole-exome sequencing (WES) data from 222 individuals from the Czech Republic were analyzed by The Genome Analysis Toolkit best practices pipeline. These data were annotated with the ANNOVAR tool, and the allele frequencies were computed.

Results:

We developed a database that contains 300,111 variants in 17,512 genes. It is accessible through a simple web query available at prot2hg.com/variantbrowser. Gene-based analyses identified those genes that are most tolerant to variants in our population. Second, allele frequencies in our population were compared to the gnomAD database and groups of variants frequent in our population, but ultra-rare in gnomAD as a whole were identified.

Conclusion:

This tool should be useful for detecting local variants in the Czech population of patients with neurogenetic diseases.

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References

1000. Genomes Project Consortium, Auton

, Brooks

, et al. (2015) A global reference for human genetic variation. Nature, 526:68-74.

Ahmed

, More

, Viswanath

, et al. (2019) INDEX-db: the Indian Exome Reference Database (phase I). J Comput Biol, 26:225-234.

Clark

, Stark

, Farnaes

, et al. (2018) Meta-analysis of the diagnostic and clinical utility of genome and exome sequencing and chromosomal microarray in children with suspected genetic diseases. NPJ Genom Med, 3:16.

Helbig

, Farwell Hagman

, et al. (2016) Diagnostic exome sequencing provides a molecular diagnosis for a significant proportion of patients with epilepsy. Genet Med, 18:898-905.

Karczewski

, Francioli

, Tiao

(2019) Variation across 141,456 human exomes and genomes reveals the spectrum of loss-of-function intolerance across human protein-coding genes. BioRxiv 531210.

Lassuthova

, Safka Brozkova

, Krutova

(2016) Severe axonal Charcot-Marie-Tooth disease with proximal weakness caused by de novo mutation in the MORC2 gene. Brain, 139:e26.

MacDonald

, Ziman

, Yuen

(2013) The Database of Genomic Variants: a curated collection of structural variation in the human genome. Nucleic Acids Res, 42:D986-D992.

Mashima

, Kodama

, Kosuge

, et al. (2015) DNA data bank of Japan (DDBJ) progress report. Nucleic Acids Res, 44:D51-D57.

Nutile

, Ruggiero

, Herzig

, et al. (2019) Whole-exome sequencing in the Isolated populations of Cilento from South Italy. Sci Rep, 9:4059.

10.

Safka Brozkova

, Deconinck

, Griffin

, et al. (2015) Loss of function mutations in HARS cause a spectrum of inherited peripheral neuropathies. Brain, 138:2161-2172.

11.

Sedlackova

, Lassuthova

, Sterbova

, et al. (2019) UBTF Mutation Causes Complex Phenotype of Neurodegeneration and Severe Epilepsy in Childhood. Neuropediatrics, 50:57-60.

12.

, Dou

, Chai

, et al. (2019) Large-scale whole-genome sequencing of three diverse Asian populations in Singapore. Cell, 179:736-749.e15.

Supplementary Material

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