Meet Me Halfway: When Genomics Meets Structural Bioinformatics

被引:0
|
作者
Sungsam Gong
Catherine L. Worth
Tammy M. K. Cheng
Tom L. Blundell
机构
[1] University of Cambridge,Biocomputing Group, Department of Biochemistry
[2] Cardiovascular Biomedical Research Unit,undefined
[3] Royal Brompton Hospital,undefined
[4] Charité Universitätsmedizin Berlin,undefined
[5] Cancer Research UK London Research Institute,undefined
关键词
Next-generation sequencing; Genotype–phenotype relationship; Single nucleotide polymorphism; Computational algorithm; Database;
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中图分类号
学科分类号
摘要
The DNA sequencing technology developed by Frederick Sanger in the 1970s established genomics as the basis of comparative genetics. The recent invention of next-generation sequencing (NGS) platform has added a new dimension to genome research by generating ultra-fast and high-throughput sequencing data in an unprecedented manner. The advent of NGS technology also provides the opportunity to study genetic diseases where sequence variants or mutations are sought to establish a causal relationship with disease phenotypes. However, it is not a trivial task to seek genetic variants responsible for genetic diseases and even harder for complex diseases such as diabetes and cancers. In such polygenic diseases, multiple genes and alleles, which can exist in healthy individuals, come together to contribute to common disease phenotypes in a complex manner. Hence, it is desirable to have an approach that integrates omics data with both knowledge of protein structure and function and an understanding of networks/pathways, i.e. functional genomics and systems biology; in this way, genotype–phenotype relationships can be better understood. In this review, we bring this ‘bottom-up’ approach alongside the current NGS-driven genetic study of genetic variations and disease aetiology. We describe experimental and computational techniques for assessing genetic variants and their deleterious effects on protein structure and function.
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页码:281 / 303
页数:22
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