Post on 10-May-2015
Integrating Large Scale Sequencing into Clinical Practice
Heidi L. Rehm, PhD, FACMGHeidi L. Rehm, PhD, FACMGDirector, Laboratory for Molecular Medicine, PCPGMAssistant Professor of Pathology, BWH, MGH, HMS
Laboratory for Molecular Medicine at PCPGM
15% of testing is from Partners’ patients
85% is from other US and International patients
• CLIA-certified in 2003• LMM offers >150 tests in cardiovascular disease, cancer,
hearing loss, pharmacogenetics and genetic syndromes
• Main focus of testing is large multi-gene panels using sequencing technologies (NGS, Sanger)
• Other technologies include TaqMan, Luminex, allele-specific PCR, MLPA, PNAs, STRs, droplet PCR
• Whole genome sequencing diagnostic service
Ryan Shay
Antonio Puerta
DeCarlo Polk
Joe KennedyJason Collier
HCM SCD in Athletes
d. SCD, 7y
38y
Case Presentation
Cardiac gross exam: asymmetric septal LVHCardiac tissue histology: myofiber disarray
Autopsy
40y
6 y
Normal Deceased
Normal
Deceased
Legend:
MI, 49y MI, 70y
39y
d. SCD, 7y6y 3y
38y
SCD = Sudden Cardiac Death
Case Presentation with Family History
40y
6 y
71y 68y
36y
HCM Family 90
Legend:
= Affected individuals
d. SCD, 49y d. SCD, 70y
39y
d. SCD, 7y6y6y 3y
38yLVHArrhythmia
SCD = Sudden Cardiac Death
LVH = Left Ventricular Hypertrophy
40y
Normal Echo
Normal Echo
Normal Echo
Normal Echo
40y
71y 68y
36y
HCM Family 90
Legend:
= Affected Individuals
+ = E187Q positive genotype
- = E187Q negative genotype
d. SCD, 49y d. SCD, 70y
39y
d. SCD, 7y 7y
Normal ECHO
6y 3y
SCD = Sudden Cardiac Death
LVH = Left Ventricular Hypertrophy
+
+- -
- 38yLVHArrhythmia
E187QTPM1
2004: HCM Panel A (5 genes) $3000
HCM Panel B (3 genes) $1150
PRKAG2 and LAMP2 $1500
GLA $600
2007: HCM CardioChip (11 genes) $3000
2011: Pan Cardiomyopathy Test (51 genes)
HCM (18 genes) $3200
(All Genes $3950)
2013: Genome Sequencing (22,000 genes) $9000
Evolution of Cardiomyopathy Testing at Partners
11 genes$6250
Targeted panels are enlarging and more and more labs are launching exome and genome services.
Genomic testing is improving diagnoses, enabling informed treatments, and defining disease risks.
When do we shift to “genomes for all”?
Genetic Testing is Evolving
Need improved analytical validity of NGS
Improve variant calling accuracy
Indels, CNVs, SVs, repeats
Fill in the holes
Targeted NGS panels miss
a variable amount of content
depending on genes
Exome sequencing misses
5-15% of coding sequence
0
50
100
150 NGS Coverage
Courtesy of Birgit Funke
AGMG NGS Guideline
ACMG (www.acmg.net) > Publications > Laboratory Standards and Guidelines > NGS
A Genetic Sequencing Test is Not One Test
DNA
PCRHundreds of assays per sample
SequencingHundreds of bases per exon
Failed exons/bases
One OtoGenome Test is actually ~380,000 tests with an infinite number of possible results. After the NGS process, Sanger follow-up begins:
Detection of full and partial gene deletions through targeted NGS: VisCap
Lo
g2
ra
tio s
am
ple
/ba
tch
me
dia
nUSH2A heterozygous
exon 10 deletion
All exons, sorted by genome position USH2A exons (3’→5’)
OTOF deletion47 exons
Trevor Pugh
However, deletion analysis is not robust in exome and genome sequencing
WGS Case 1: Nonsyndromic Hearing Loss
• Sept 2010: 2 yr old girl born presents to Genetics
• History of congenital bilateral sensorineural hearing loss
• Mild-moderate “cookie-bite” shaped audiogram
• No other complaints
• Genetic testing for hearing loss (Cx26 and OtoChip): NegativeHowever, >100 loci, many without identified genes, are associated to hereditary hearing loss
WGS Case 1: Nonsyndromic Hearing Loss
• July 2011: Patient enrolled into consented research study
• Obtained blood samples on all 11 family members
• Whole genome sequencing ordered on 3 siblings
WGS on 3 children
Variant Analysis Step 1
• ~4 million sequence variants per child
• ~1,250,000 shared variants among the three siblings
• First considered a recessive model (hom or 2 het variants)
• No cause identified
Variant Analysis Step 2
Genome sequence shared with external company
Proposed otopetrin (OTOP1) as causative gene:
Required for normal formation of otoconia in the inner ear.
Two mutations identified:
p.Arg232Trp
4 bp insertion leading to frameshift
Upon manual examination of read data, frameshift variant was deemed a false positive
Copyright 2013 – Partners HealthCare Incorporated – All Rights Reserved
Validation of WGS Alignment and Variant Calling
Variant type1000G
Variants SensitivityWith concordant
zygosity
SNVs 2762933 2735592 (99.0%) 2730826 (98.8%)
Indels 327474 299300 (91.4%) 285401 (87.2%)
Total 3090407 3034892 (98.2%) 3016227 (97.6%)
Concordance with 1000 Genomes Data
Courtesy of Matt Lebo
Copyright 2013 – Partners HealthCare Incorporated – All Rights Reserved
Validation of WGS Alignment and Variant Calling
Variant Type FP (before thresholds) FP (after thresholds)*
SNVs 20 1
Indels 1 0
Variant Type # FN Sensitivity 95% CI
SNVs 410 0 100% 99.1%-100%
Indels 15 0 100% 79.6%-100%
Specificity
Sensitivity
425 Sanger confirmed variants in 195 genes across 700kb of sequence
*Fisher Strand (FS) < 30 and Quality by Depth (QD) >= 4
Courtesy of Matt Lebo
WGS Case 1: Nonsyndromic Hearing Loss
• January 2012: Mother called to say that the 4 oldest children with hearing loss were now complaining of headaches – could this be related?
• Also relayed that a paternal grandfather was reported to have hearing loss detected at age 19 - described inability to hear fire alarm but the clicking of an automatic seat belt annoyed him
Variant Analysis Step 3
• Consider dominant inheritance with reduced penetrance
• Examined known hearing loss genes (~70) for any single variant
• 32 rare/novel variants found across 31 different genes
• All missense variants with no strong data to support a deleterious
impact
Variant Analysis Step 4: Segregation
• Cost to develop Sanger assays for all 32 variants and test
for presence in 11 family members = $5428
• Examined cost to perform linkage analysis by SNP array:
$386.00 per sample x 11 samples = $4246
• Requested additional sample from grandfather
D3S1278 to D3S2453 = chr3:115,124,154-136,278,257 (3q13.31-22.3, 21 Mb)
Courtesy of Jun Shen
Some genes fail analysis by genome/exome sequencing
STRC
Exome Coverage of 73 Hearing Loss Genes
Analyzed case by new OtoGenome Test
STRC pSTRC
STRC pSTRC
Hom deletion of STRC
pSTRC
pSTRCSTRC Gene
100 kb deletion (43.89 Mb to 43.99 Mb)
STRCPseudogene
STRC
100,000 Base Deletion Identified
WGS Case 1: Nonsyndromic? Hearing Loss
• Called family to return cause of hearing loss
• Mother relayed that headaches in 4 affected children had resolved once it was discovered that all 4 needed glasses
• Question: Could STRC mutations cause vision problems?
WGS Case 1: Deafness Infertility Syndrome
Males with this deletion will be infertile due to deletion of the adjacent CATSPER gene
Males can father children through intracytoplasmic sperm injection (ICSI)
WGS Case 2: Distal Arthrogryposis Type 5
Disease is known to be AD and to occur de novo
No known genes for DA5
Skeletal Spine stiffness, Hunched anteverted shoulders, Pectus excavatum, Limited forearm rotation and
wrist extension, Bilateral club feet, Congenital finger contractures, Long fingers, Absent phalangeal
creases, Poorly formed palmar creases, Camptodactyly, Dimples over large joints
Muscle Decreased muscle mass (especially in lower limbs), Firm muscles
Face Triangular face, Decreased facial expression
Ears Prominent ears
Eyes Ophthalmoplegia, Deep-set eyes, Epicanthal folds, Ptosis, Duane anomaly, Keratoglobus,
Keratoconus, Macular retinal folds, Strabismus, Astigmatism, Abnormal electroretinogram, Abnormal
retinal pigmentation
Clinical features:
Case from of Michael Murray, MD
Case 2: Distal Arthrogryposis Type 5
Two de novo mutations in exonic sequence:
ACSM4 – acyl-CoA synthetase medium-chain family member 4
5 nonsense variants identified in ESP; 1 with 6.4% MAF; 4 occur once
PIEZO2: mechanosensitive ion channel
Great candidate, but how to we prove causality for a novel gene-disease association?
Collaboration with Shamil Sunyeav
Matchmaker System for Exomes/Genomes
o Collaboration with Ada Hamosh (OMIM/Hopkins)
o Enhance PhenoDB to become a matchmaker system for unsolved exomes and genomes
o Entry of structured phenotypes
o Ability to upload candidate genes/variants and vcf files
o Matches require data entry and dual notification of both parties
o Build algorithm to prioritize matches based upon phenotype match strength and phenotype/gene/variant prior likelihood parameters
o Goal to also interface with other systems (e.g. Decipher, LOVD, etc)
A New Paradigm in Clinical Genomics
Traditional Paradigm
New Paradigm
What is the biggest bottleneck in clinical
sequencing?
Variant Assessment and Reporting
Somatic Cancer
~15,000 variants interpreted in patient reports to date
Average22 min25 min120 min
Variant Assessment TypeVariant with no dataVariant with dbSNP/ESP data onlyVariant with publications
HCM Gene Mutations – 3000 cases tested
>500 clinically significant mutations identified
66% of clinically significant mutations are seen in only one family
Number of probands
Nu
mb
er
of v
ari
ants
MYBPC3E258K
MYBPC3MYH7R502WW792fsR663H
Hearing Loss Gene Mutations – 2000 Cases Tested
Number of probands
Nu
mb
er
of v
ari
ants
GJB2
35delG
GJB2
V37IGJB2
M34T
USH2A
2299delG
SLC26A4
81% (423/523) of clinically significant variants have been seen in only one family
Variant Analysis for General Genome Report
3,227,455 Substitutions and 418,331 Indels3,227,455 Substitutions and 418,331 Indels
20,240 CDS/Splice Variants20,240 CDS/Splice Variants
25 “Pathogenic” Variants
25 “Pathogenic” Variants
Published as Disease-Causing
Genes
5 PGx Class 1
5 Variants5 Variants
PharmGKB
2 Pathogenic0 Likely Pathogenic6 VUS4 Likely Benign13 Benign
<1%
616 Rare CDS/Splice Variants616 Rare CDS/Splice Variants
LOF in Disease Associated Genes
2 Pathogenic9 VUS
11 Variants11 Variants
~2 CNVs >1kb~2 CNVs >1kb
0 PathogenicReview evidence for gene-disease association and LOF role
Review evidence for variant pathogenicity
Fetus with US finding: ↑NT
PTPN11 p.Ile309ValPublished as “pathogenic” for
Noonan syndrome
Patient contacted author of paper who said he later found the variant in 7% of AJ controls; now feels the variant is benign
Courtesy Sherri Bale
Noonan Syndrome Case
?
LMMCase
To improve our knowledge of DNA variation will require a massive effort in data sharing
U41 Genomic Resource Grant: A Unified Clinical Genomics
DatabaseTo raise the quality of patient care by:
• Standardizing the annotation and interpretation of genomic variants
• Sharing variant and case level data through a centralized database for clinical and research use
• Implementing an evidence-based expert consensus process for curating variant interpretations
We will work jointly with the recipients of the Clinically Relevant Variant Resource awards.
Sequencing Laboratories Which Have Agreed to Share Data
www.ncbi.nlm.nih.gov/clinvar
NIH NCBI ClinVar
ClinVar Contributors (>40)
Group Submissions
OMIM 22954
Partners Healthcare’s Laboratory for Molecular Medicine 7127
International Standards For Cytogenomic Arrays (ISCA) 4557
GeneReviews 2264
ARUP 1415
LabCorp (Correlagen) 1391
Sharing Clinical Report Project – BRCA1/BRCA2 902
GeneDx 589
NHGRI (ClinSeq) 423
Leiden Muscular Dystrophy 114
Emory 43
Total = 41923
LMM’s Disease Area Submissions to ClinVar
Phenotypes Probands Genes Unique Variants
Cardiomyopathy 5485 51 3929
Somatic Cancer 3421 21 178
RASopathies 2781 12 376
Hearing Loss and Related Syndromes 2048 65 2218
Connective Tissue Disorders 915 3 227
Hereditary Cancer 665 9 81
Congenital Heart Defects 91 4 43
Ectodermal Dysplasia 81 1 36
Other 867
Documenting arguments will improve the evidence-based assessment of variants
Current Limitations of ClinVar
Many labs have limited and/or non-
standardized infrastructure to house their
data which limits the quantity, quality and
efficiency of data sharing
GeneInsight LabGeneInsight Lab
Reporting EngineReporting Engine
Laboratory KnowledgebaseLaboratory Knowledgebase
Case RepositoryCase Repository
The GeneInsight Suite
• In clinical use since 2005; over 28,000 cases reported• Commercialized and used by >10 clinical labs/research
consortia to date
Current Limitations of ClinVar
o Genomic data and other case-level data is difficult to share in meaningful ways in the public domain
My lab has 25,000 cases with phenotypic data that I am willing but unable to share through ClinVar right now
o We are gathering stakeholders at NIH in September to discuss policies surrounding case-level data submission and access for NCBI databases including ClinVar and dbGaP
GeneInsight Data Sharing Networks
NetworkedStandaloneDatabases
Bioreference Lab-MGH PathologyGeneInsight Clinical Lab Network
New York Genome Center
Lung Cancer ConsortiumGenome Canada Grant
GeneInsight Lab – View of Networked Data
GeneInsight LabGeneInsight Lab
Reporting EngineReporting Engine
LaboratoryKnowledgebase
LaboratoryKnowledgebase
Case RepositoryCase Repository
GeneInsight ClinicGeneInsight Clinic
Patient Genomic Profile RepositoryPatient Genomic
Profile Repository
Alerting EngineAlerting Engine
EHR ConnectivityEHR Connectivity
Supports Molecular Diagnostic Labs
Supports Molecular Diagnostic Labs
Supports Clinicians WhoOrder Genetic Tests
Supports Clinicians WhoOrder Genetic Tests
The GeneInsight Suite
Keeping up with Genomics
~4% of case per year received medium or high alerts (.33% per month)
GeneInsight Alert Delivery
This screenshot was taken from a demonstration system – the content of this screen should not be used for any clinical purpose
Acknowledgements
The General Genome Report