The future of CNVs: sequence based resolution and links to human disease 2

Eichler, Evan

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View the Talks
32 min
1. Gene copy number variation in human and primate evolution
- Prof. James Sikela
43 min
2. Quantitative CNV testing in molecular diagnostics
- Prof. Dimitri J. Stavropoulos
21 min
3. Ethical considerations in dealing with CNV information
- Dr. Holly Tabor
38 min
4. The future of CNVs: sequence based resolution and links to human disease 1
- Prof. Evan Eichler
31 min
5. The future of CNVs: sequence based resolution and links to human disease 2
- Prof. Evan Eichler
Archived Lectures *These may not cover the latest advances in the field
26 min
6. Population genetics of structural variation
- Dr. Don Conrad
47 min
7. Databases for CNV in control and disease populations
- Dr. Lars Feuk
45 min
8. Copy number variation in mental retardation
- Dr. Joris Veltman
35 min
9. The case for offering all women amniocentesis and chromosomal microarray analysis
- Prof. Arthur Beaudet
34 min
10. Structural variants and susceptibility to common human disorders
- Prof. Xavier Estivill
40 min
11. Indels, CNVs and the spectrum of human genome variation
- Prof. Samuel Levy
36 min
12. Genome structure and expression
- Prof. Alexandre Reymond
39 min
13. Quantitative CNV testing in molecular diagnostics
- Prof. Martin Somerville
40 min
14. Copy number variation in neuropsychiatric disorders
- Dr. Christian Marshall
41 min
15. Copy number variation in association studies of human disease
- Dr. Steven McCarroll
31 min
16. Williams-Beuren syndrome locus: a model of CNV affecting gene dosage and phenotypes
- Dr. Lucy Osborne
32 min
17. CNVs in human genomes
- Prof. Chris Ponting
64 min
18. Genomic disorders: mechanisms for copy number variation and clinical implementation of high-resolution genome analysis
- Prof. James Lupski
37 min
19. Copy number variation
- Prof. Steve Scherer
17 min
20. Array comparative genomic hybridization to characterize copy number variation in the human genome
- Dr. Nigel Carter
33 min
21. Mendelian CNV mutations
- Prof. Joris Vermeesch
44 min
22. CNVs and clinical diagnosis
- Dr. Brynn Levy

Printable Handouts

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Introduction
Future discovery of CNVs
Probe coverage for deletion intervals
Genotyping: targeted design
Recurrent and large events flanked by duplications
Microdeletions vs. inversion polymorphisms
A common inversion under selection in Europeans
17q21.31 microdeletion syndrome
Inversion and deletion
17q21.31 targeted sequencing
Duplication architecture of H2 vs. H1 haplotype
Application of next-gen. sequencing technology
Detecting smaller structural variants with next-gen
Paired-end mapping reveals structural variation
Detecting large CNVs based on WGS
Personalized duplication or CNV maps
Summary
Impacts
Addendum (2017): Long read sequencing
PacBio whole genome sequencing
Structural variation detection using PacBio
Summary of results
Increased resolution of structural variation
Increased sensitivity for structural variation
Acknowledgements

Topics Covered

Future discovery of CNVs
Genotyping
Inversion and deletion
17q21.31 targeted sequencing
Application of next-generation sequencing technology
Personalized duplication or CNV map
Long read sequencing technology
Single-molecule, real-time detection of structural variation (SMRT-SV)
Full-spectrum of human genetic variation

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Genetics & Epigenetics

Talk Citation

Eichler, E. (2017, March 29). The future of CNVs: sequence based resolution and links to human disease 2 [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved October 31, 2025, from https://doi.org/10.69645/UQEM6461.
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Publication History

Published on August 30, 2009
Updated on March 29, 2017

Financial Disclosures

Prof. Evan Eichler, Other: Scientific advisory board of DNAnexus, Inc. with stock options.

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The future of CNVs: sequence based resolution and links to human disease 2

Prof. Evan Eichler – University of Washington, USA

Published on August 30, 2009 Updated on March 29, 2017 31 min

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Transcript

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0:04

So what I would like to do is really kind of focus on where I think the field is heading with respect to copy number variation research and genome structure variation and highlight some of the limitations and excitement in the field with respect to future discovery. So the number of unanswered questions I think the most important is how we're going to actually activate genotype copy number variation particularly within these difficult duplicated regions and there is a need to develop new technologies specifically for that purpose. I and other labs really have argued that sequence resolution is the key for understanding the genetic basis of disease. I will highlight an example of this. And finally, I want to share with you some of the excitement really with respect to more complete ascertainment in terms of discovery of smaller variation using next generation sequencing technology and really the promise, potential promise of developing personalized CNV maps for individual genomes.

0:55

This slide actually highlights one of the limitations of many of the commercial SNP microarrays that are commonly used to detect copy number variation. So what I'm showing you are two histograms of both the Illumina and Affymetrix SNP platforms various versions, and the number of probes that are placed with insights that we've actually sequenced and confirmed with the base pair level as copy number polymorphic. Most groups would agree that you need at least two probes to accurately genotype copy number variation, preferably more than two probes to accurately genotype copy number variation once you know where it exists. So these two histograms actually show you that there is in fact a deficit of probes in regions of copy number polymorphism owing largely to the fact that they map to complex regions of genome and where there has been fewer probes laid down than the average. So typically, in these roughly 500 regions that we've sequenced, there is only about 60% of the sites that could be in principle adequately genotyped, and in fact, the actual number is much less than that. If you then looked at, for example, new insertion sequences or duplication intervals as opposed to deletion intervals, the number gets in fact considerably worse. In those cases, less than 20% of the existing or known sequence resolved duplications and new insertion sequences could be adequately resolved using these types of platforms.

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The future of CNVs: sequence based resolution and links to human disease 2

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A selection of talks on Genetics & Epigenetics

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The future of CNVs: sequence based resolution and links to human disease 2