Complete genomic profiles of 1496 Taiwanese reveal curated medical insights

Jacob Shujui Hsu; Dung Chi Wu; Shang Hung Shih; Jen Feng Liu; Ya Chen Tsai; Tung Lin Lee; Wei An Chen; Yi Hsuan Tseng; Yi Chung Lo; Hong Ye Lin; Yi Chieh Chen; Jing Yi Chen; Ting Hsuan Chou; Darby Tien Hao Chang; Ming Wei Su; Wei Hong Guo; Hsin Hsiang Mao; Chien Yu Chen; Pei Lung Chen

doi:10.1016/j.jare.2023.12.018

Complete genomic profiles of 1496 Taiwanese reveal curated medical insights

Jacob Shujui Hsu
, Dung Chi Wu
, Shang Hung Shih
, Jen Feng Liu
, Ya Chen Tsai
, Tung Lin Lee
, Wei An Chen
, Yi Hsuan Tseng
, Yi Chung Lo
, Hong Ye Lin
, Yi Chieh Chen
, Jing Yi Chen
, Ting Hsuan Chou
, Darby Tien Hao Chang
, Ming Wei Su
, Wei Hong Guo
, Hsin Hsiang Mao
, Chien Yu Chen
, Pei Lung Chen

Department of Electrical Engineering

Research output: Contribution to journal › Article › peer-review

6 Citations (Scopus)

Abstract

Introduction: The population of Taiwan has a long history of ethno-cultural evolution. The Taiwanese population was isolated from other large populations such as the European, Han Chinese, and Japanese population. The Taiwan Biobank (TWB) project has built a nationwide database, particularly for personal whole-genome sequence (WGS) to facilitate basic and clinical collaboration nationally and internationally, making it one of the most valuable public datasets of the East Asian population. Objectives: This study provides comprehensive medical genomic findings from TWB WGS data, for better characterization of disease susceptibility and the choice of ideal treatment regimens in Taiwanese population. Methods: We reanalyzed 1496 WGS using a PrecisionFDA Truth challenge winner method Sentieon DNAscope. Single nucleotide variants (SNV) and small insertions/deletions (INDEL) were benchmarked. We also analyzed pharmacogenomic (PGx) drug-associated alleles, and copy number variants (CNV). Multiple practicing clinicians reviewed and curated the clinically significant variants. Variant annotations can be browsed at TaiwanGenomes (https://genomes.tw). Results: We found that each participant had an average of 6,870.7 globally novel variants and 75.3% (831/1103) of the participants harbored at least one PharmGKB-selected high evidence level human leukocyte antigen (HLA) risk allele. 54 PharmGKB-reported high-level instances of evidence of Cytochrome P450 variant-drug pairs, with a population frequency of over 13.2%. We also identified 23 variants in the ACMG secondary finding V3 gene list from 25 participants, suggesting that 1.67% (25/1496) of the population is harboring at least one medical actionable variant. Our carrier status analyses suggest that one in 25 couples (3.94%) would risk having offspring with at least one pathogenic variant, which is in line with rates found in Japan and Singapore. For pathogenic CNV, we detected 6.88% and 2.02% carrier rates for alpha thalassemia and spinal muscular atrophy, respectively. Conclusion: Our study highlights the overall medical insights of a complete Taiwanese genomic profile.

Original language	English
Pages (from-to)	197-207
Number of pages	11
Journal	Journal of Advanced Research
Volume	66
DOIs	https://doi.org/10.1016/j.jare.2023.12.018
Publication status	Published - 2024 Dec

All Science Journal Classification (ASJC) codes

General

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.jare.2023.12.018

Cite this

Hsu, J. S., Wu, D. C., Shih, S. H., Liu, J. F., Tsai, Y. C., Lee, T. L., Chen, W. A., Tseng, Y. H., Lo, Y. C., Lin, H. Y., Chen, Y. C., Chen, J. Y., Chou, T. H., Chang, D. T. H., Su, M. W., Guo, W. H., Mao, H. H., Chen, C. Y., & Chen, P. L. (2024). Complete genomic profiles of 1496 Taiwanese reveal curated medical insights. Journal of Advanced Research, 66, 197-207. https://doi.org/10.1016/j.jare.2023.12.018

@article{b705fd2390404ea8ad842706c8e8fe15,

title = "Complete genomic profiles of 1496 Taiwanese reveal curated medical insights",

abstract = "Introduction: The population of Taiwan has a long history of ethno-cultural evolution. The Taiwanese population was isolated from other large populations such as the European, Han Chinese, and Japanese population. The Taiwan Biobank (TWB) project has built a nationwide database, particularly for personal whole-genome sequence (WGS) to facilitate basic and clinical collaboration nationally and internationally, making it one of the most valuable public datasets of the East Asian population. Objectives: This study provides comprehensive medical genomic findings from TWB WGS data, for better characterization of disease susceptibility and the choice of ideal treatment regimens in Taiwanese population. Methods: We reanalyzed 1496 WGS using a PrecisionFDA Truth challenge winner method Sentieon DNAscope. Single nucleotide variants (SNV) and small insertions/deletions (INDEL) were benchmarked. We also analyzed pharmacogenomic (PGx) drug-associated alleles, and copy number variants (CNV). Multiple practicing clinicians reviewed and curated the clinically significant variants. Variant annotations can be browsed at TaiwanGenomes (https://genomes.tw). Results: We found that each participant had an average of 6,870.7 globally novel variants and 75.3\% (831/1103) of the participants harbored at least one PharmGKB-selected high evidence level human leukocyte antigen (HLA) risk allele. 54 PharmGKB-reported high-level instances of evidence of Cytochrome P450 variant-drug pairs, with a population frequency of over 13.2\%. We also identified 23 variants in the ACMG secondary finding V3 gene list from 25 participants, suggesting that 1.67\% (25/1496) of the population is harboring at least one medical actionable variant. Our carrier status analyses suggest that one in 25 couples (3.94\%) would risk having offspring with at least one pathogenic variant, which is in line with rates found in Japan and Singapore. For pathogenic CNV, we detected 6.88\% and 2.02\% carrier rates for alpha thalassemia and spinal muscular atrophy, respectively. Conclusion: Our study highlights the overall medical insights of a complete Taiwanese genomic profile.",

author = "Hsu, \{Jacob Shujui\} and Wu, \{Dung Chi\} and Shih, \{Shang Hung\} and Liu, \{Jen Feng\} and Tsai, \{Ya Chen\} and Lee, \{Tung Lin\} and Chen, \{Wei An\} and Tseng, \{Yi Hsuan\} and Lo, \{Yi Chung\} and Lin, \{Hong Ye\} and Chen, \{Yi Chieh\} and Chen, \{Jing Yi\} and Chou, \{Ting Hsuan\} and Chang, \{Darby Tien Hao\} and Su, \{Ming Wei\} and Guo, \{Wei Hong\} and Mao, \{Hsin Hsiang\} and Chen, \{Chien Yu\} and Chen, \{Pei Lung\}",

note = "Publisher Copyright: {\textcopyright} 2023",

year = "2024",

month = dec,

doi = "10.1016/j.jare.2023.12.018",

language = "English",

volume = "66",

pages = "197--207",

journal = "Journal of Advanced Research",

issn = "2090-1232",

publisher = "Elsevier BV",

}

TY - JOUR

T1 - Complete genomic profiles of 1496 Taiwanese reveal curated medical insights

AU - Hsu, Jacob Shujui

AU - Wu, Dung Chi

AU - Shih, Shang Hung

AU - Liu, Jen Feng

AU - Tsai, Ya Chen

AU - Lee, Tung Lin

AU - Chen, Wei An

AU - Tseng, Yi Hsuan

AU - Lo, Yi Chung

AU - Lin, Hong Ye

AU - Chen, Yi Chieh

AU - Chen, Jing Yi

AU - Chou, Ting Hsuan

AU - Chang, Darby Tien Hao

AU - Su, Ming Wei

AU - Guo, Wei Hong

AU - Mao, Hsin Hsiang

AU - Chen, Chien Yu

AU - Chen, Pei Lung

PY - 2024/12

Y1 - 2024/12

N2 - Introduction: The population of Taiwan has a long history of ethno-cultural evolution. The Taiwanese population was isolated from other large populations such as the European, Han Chinese, and Japanese population. The Taiwan Biobank (TWB) project has built a nationwide database, particularly for personal whole-genome sequence (WGS) to facilitate basic and clinical collaboration nationally and internationally, making it one of the most valuable public datasets of the East Asian population. Objectives: This study provides comprehensive medical genomic findings from TWB WGS data, for better characterization of disease susceptibility and the choice of ideal treatment regimens in Taiwanese population. Methods: We reanalyzed 1496 WGS using a PrecisionFDA Truth challenge winner method Sentieon DNAscope. Single nucleotide variants (SNV) and small insertions/deletions (INDEL) were benchmarked. We also analyzed pharmacogenomic (PGx) drug-associated alleles, and copy number variants (CNV). Multiple practicing clinicians reviewed and curated the clinically significant variants. Variant annotations can be browsed at TaiwanGenomes (https://genomes.tw). Results: We found that each participant had an average of 6,870.7 globally novel variants and 75.3% (831/1103) of the participants harbored at least one PharmGKB-selected high evidence level human leukocyte antigen (HLA) risk allele. 54 PharmGKB-reported high-level instances of evidence of Cytochrome P450 variant-drug pairs, with a population frequency of over 13.2%. We also identified 23 variants in the ACMG secondary finding V3 gene list from 25 participants, suggesting that 1.67% (25/1496) of the population is harboring at least one medical actionable variant. Our carrier status analyses suggest that one in 25 couples (3.94%) would risk having offspring with at least one pathogenic variant, which is in line with rates found in Japan and Singapore. For pathogenic CNV, we detected 6.88% and 2.02% carrier rates for alpha thalassemia and spinal muscular atrophy, respectively. Conclusion: Our study highlights the overall medical insights of a complete Taiwanese genomic profile.

AB - Introduction: The population of Taiwan has a long history of ethno-cultural evolution. The Taiwanese population was isolated from other large populations such as the European, Han Chinese, and Japanese population. The Taiwan Biobank (TWB) project has built a nationwide database, particularly for personal whole-genome sequence (WGS) to facilitate basic and clinical collaboration nationally and internationally, making it one of the most valuable public datasets of the East Asian population. Objectives: This study provides comprehensive medical genomic findings from TWB WGS data, for better characterization of disease susceptibility and the choice of ideal treatment regimens in Taiwanese population. Methods: We reanalyzed 1496 WGS using a PrecisionFDA Truth challenge winner method Sentieon DNAscope. Single nucleotide variants (SNV) and small insertions/deletions (INDEL) were benchmarked. We also analyzed pharmacogenomic (PGx) drug-associated alleles, and copy number variants (CNV). Multiple practicing clinicians reviewed and curated the clinically significant variants. Variant annotations can be browsed at TaiwanGenomes (https://genomes.tw). Results: We found that each participant had an average of 6,870.7 globally novel variants and 75.3% (831/1103) of the participants harbored at least one PharmGKB-selected high evidence level human leukocyte antigen (HLA) risk allele. 54 PharmGKB-reported high-level instances of evidence of Cytochrome P450 variant-drug pairs, with a population frequency of over 13.2%. We also identified 23 variants in the ACMG secondary finding V3 gene list from 25 participants, suggesting that 1.67% (25/1496) of the population is harboring at least one medical actionable variant. Our carrier status analyses suggest that one in 25 couples (3.94%) would risk having offspring with at least one pathogenic variant, which is in line with rates found in Japan and Singapore. For pathogenic CNV, we detected 6.88% and 2.02% carrier rates for alpha thalassemia and spinal muscular atrophy, respectively. Conclusion: Our study highlights the overall medical insights of a complete Taiwanese genomic profile.

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UR - https://www.scopus.com/pages/publications/85184723886#tab=citedBy

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DO - 10.1016/j.jare.2023.12.018

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AN - SCOPUS:85184723886

SN - 2090-1232

VL - 66

SP - 197

EP - 207

JO - Journal of Advanced Research

JF - Journal of Advanced Research

ER -

Complete genomic profiles of 1496 Taiwanese reveal curated medical insights

Abstract

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