AI Article Synopsis
- The study highlights the existence of "dark" and "camouflaged" regions in the human genome that standard short-read sequencing cannot effectively analyze, impacting the identification of disease-related mutations.
- Researchers discovered 36,794 dark regions across important gene pathways, with varying degrees of darkness, and employed linked-read and long-read sequencing technologies to significantly reduce the number of unresolved regions.
- The study suggests that long-read sequencing can uncover significant genetic information, like a rare mutation in a gene associated with Alzheimer's, underscoring the need for further investigation in larger samples to understand its implications.
Article Abstract
Background: The human genome contains "dark" gene regions that cannot be adequately assembled or aligned using standard short-read sequencing technologies, preventing researchers from identifying mutations within these gene regions that may be relevant to human disease. Here, we identify regions with few mappable reads that we call dark by depth, and others that have ambiguous alignment, called camouflaged. We assess how well long-read or linked-read technologies resolve these regions.
Results: Based on standard whole-genome Illumina sequencing data, we identify 36,794 dark regions in 6054 gene bodies from pathways important to human health, development, and reproduction. Of these gene bodies, 8.7% are completely dark and 35.2% are ≥ 5% dark. We identify dark regions that are present in protein-coding exons across 748 genes. Linked-read or long-read sequencing technologies from 10x Genomics, PacBio, and Oxford Nanopore Technologies reduce dark protein-coding regions to approximately 50.5%, 35.6%, and 9.6%, respectively. We present an algorithm to resolve most camouflaged regions and apply it to the Alzheimer's Disease Sequencing Project. We rescue a rare ten-nucleotide frameshift deletion in CR1, a top Alzheimer's disease gene, found in disease cases but not in controls.
Conclusions: While we could not formally assess the association of the CR1 frameshift mutation with Alzheimer's disease due to insufficient sample-size, we believe it merits investigating in a larger cohort. There remain thousands of potentially important genomic regions overlooked by short-read sequencing that are largely resolved by long-read technologies.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6526621 | PMC |
| http://dx.doi.org/10.1186/s13059-019-1707-2 | DOI Listing |
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