nuts and bolts of clinical genomic sequencing thomas stricker md phd vanderbilt university

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Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

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Page 1: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Nuts and Bolts of Clinical Genomic Sequencing

Thomas Stricker MD PhDVanderbilt University

Page 2: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Next Generation SequencingIllumina Seqeuncing TechnologyDNA – the genetic code•DNA is a double stranded polymer of 4 bases (A, T, C,G)

•The order (sequence) of A,T,C,G is the genetic code

•A always pairs with T on the opposite strand, and C always pairs with G

•Enzymes called polymerases make copies of DNA by taking a single strand of DNA, and then adding A,T,C,G according to the base-pairing rules

Sanger (mod by Lee Hood)

•Sequencing by synthesis

•Mix many copies of the same DNA molecule, polymerase, ATCGs, and a small amount of flourescently labeled ATCG that are terminated

•Terminated bases stop extension

•Separate based on size

Page 3: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

1. In vitro amplification, ‘cloning’

2. Flow cell based sequencing by synthesis

3. A draft of the human genome

Illumina Seqeuncing Technology

What Happened?

Page 4: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Illumina Seqeuncing Technology

Page 5: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Single platform – 4 mutation types

Page 6: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

877 Lung Specimens (843 patients) 7/1/2010-2/28/2013 *

No mutation detected

(512)56.1%

EGFR (135)14.8%

BRAF (20)2.2%

AKT1 (2)0.2%

PTEN (2)0.2%

PIK3CA (20)2.2%

NRAS (5)0.5%

MEK1 (8)0.9%

KRAS (198)21.7%

ERBB2 (10)1.1%

* Data courtesy of Dr. William Pao and Dr. Mia Levy

Oncogene Frequency (%)

Treatment

EGFR 10-35 Gefitinib, erlotinib, afatinib

ALK fusion 3-7 Crizotinib

MET amp 2-4 Crizotinib

DDR2 ~4 Dasatinib

HER2 2-4 Afatinib

ROS1 fusion 1 Crizotinib

BRAF Y472C rare Dasatinib

BRAF V600E 1 Vemurafenib, dabrafenib

RET fusion 1 Cabozantinib

NRAS 1 Trametinib (preclinical)

KRAS 15-25 Selumetinib (with chemo)

FGFR1/2 amp

~20 AZD4547

Broad spectrum of mutations gives physicians some information…

…but without well-annotated sequencing reports, physicians struggle to find best therapy

Rare Mutations – Implications for Therapy

Page 7: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

The Long Tail of Cancer mutations

45 Recurrently mutated genes in the TCGA breast cancer data set

Range from over 30% to 2% of cases

Page 8: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Human Genome

3 billion base pairs in the human genome

Roughly 1% is in coding sequence

Page 9: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Target Enrichment = Amplicon-based approach

Page 10: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Target Enrichment = Hybrid capture approach

Page 11: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Fusion Detection = Hybrid Capture

Page 12: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Tumor-Normal Contamination

Page 13: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Tumor-Normal Contamination

Page 14: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Clinical Utility of NGS

Page 15: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Clinical Utility of NGS

Page 16: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Clinical Utility of NGS

Page 17: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Analysis Schematic

Page 18: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

MS Lawrence et al. Nature 000, 1-5 (2013) doi:10.1038/nature12213

.

Somatic mutation frequencies observed in exomes from 3,083tumour–normal pairs

Page 19: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Inherited Variants > Somatic

Synonymous SNVsNon-Synonymous SNV

Page 20: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

Inherited Variants > Somatic

Somatic Coding mutations – 3 to 300

Page 21: Nuts and Bolts of Clinical Genomic Sequencing Thomas Stricker MD PhD Vanderbilt University

IGV – Genotyping