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NIPT for Microdeletions
& Single Gene Disorders
Yuval Yaron, MD
Tel Aviv Sourasky Medical Center
Disclosures
• Consultant, Teva Pharmaceuticals Inc.
Distributor of Verifi®
• Consultant, FugeneGenetics.
Distributor of Harmony®
• Member, Clinical Expert panel
Illumina Reproductive & Genomic Health
Manufacturer of Sequencing Products, Verifi®
Human Genome = Encyclopedia
Chromosome = Volume
Gene = Page
Genome = 3,000,000,000
Exome = 2% of the Genome
Genetic Aberrations
• Chromosomal
o Numerical
o Structural
• Submicroscopic
o Deletions
o Duplications
• Sequence variants
o Polymorphisms
o Mutations
Genetic Aberrations
• Chromosomal
• Numerical
• Structural
• Submicroscopic
• Deletions
• Duplications
• Sequence variants
• Polymorphisms
• Mutations
Basic NIPT Detects ~83% of
Chromosomal Anomalies
Modified from Wellesley et al. European Journal of Human Genetics 2012;20:521–526
Basic NIPT would Miss 17% of Anomalies
Modified from Wellesley et al. European Journal of Human Genetics 2012;20:521–526
NIPT for Rare Autosomal Trisomies
• Some laboratories include NIPT screening for:
trisomy 9, trisomy 16 and trisomy 22
• However most of such conceptuses
spontaneously abort in the 1st trimester
(unless mosaic).
• With each added condition there is the
potential for an additional 0.1% to the false
positive rates
• Questionable benefit
Genetic Aberrations
• Chromosomal
• Numerical
• Structural
• Submicroscopic
o Deletions
o Duplications
• Sequence variants
• Polymorphisms
• Mutations
Microdeletions
Common Microdeletions
Prader Willi
4 Mb del 15q11-13
Williams-Beuren
1.5 Mb del 7q11.23
DiGeorge / VCF
3.5 Mb del 22q11
Known Microdeletions
Chromosomal Microarray (CMA)
Comparative Genomic Hybridization
Detects Deletions & Duplications
Risk of Significant Deletion/Duplication
• Autism or MR + dysmorphism 10%-20%
• Fetus with ultrasound anomaly 5%-7%
• No Risk, normal karyotype 0.5%
CNVs Following Normal Karyotype
Total
CNV
with Clinical
Significance
(%)
Pathogenic
CNV
(%)
CNV of Uncertain Clinical
Significance
Benign CNV
(%)
Indication for
Prenatal
Diagnosis
Potential
Clinical
Significance
(%)
Likely Benign
CNV
(%)
6.02.83.22.532.7US Anomaly
1.70.51.31.931.9Maternal Age
1.60.41.21.833.9Screen Positive
1.30.50.80.830.1Other *
2.50.91.61.832.3All
Genetic Counseling for
Variants of Unclear Significance (VOUSs)
NIPT for Microdeletions
Srinavasan A, et al. Noninvasive detection of fetal subchromosome abnormalities via deep
sequencing of maternal plasma. Am J Human Genet 2013;92:1-10
Fetal Microdeletions Detected by NIPT
Commercial Microdeletion Panels
Syndrome Locus Estimated
prevalence
Deletion size
(Mb)
≥3 Mb
DiGeorge/
velocardiofacial syndrome
22q11.2 1:2000 - 1:4000 3 85%
Monosomy 1p36 1p36 1:5000 - 1:10,000 1.5 - 10.5 85%
Angelman syndrome or
Prader-Willi syndrome
15q11.2-q13 1:20,000 5 – 6 70%
5p- Cri-du-Chat syndrome 5p15 1:50,000 10 - 30 99%
4p- Wolf-Hirschhorn syndrome 4p16.3 1:50,000 1.9 – 30 99%
Yaron et al. 2015, Obstet Gynecol, in Press
22q11.2 Deletion
● Overlaps Velocardiofacial/DiGeorge Syndrome
● De novo (~90%) or inherited (~10%)
● Variable phenotype
● Congenital heart defect (74%)
● Palate abnormalities (69%)
● Learning difficulties (70–90%)
● Characteristic facial features
● Thymic and parathyroid abnormalities
1p36 Deletion Syndrome
• Significant developmental delay
• Behavioral problems
• Hypotonia (95%)
• Brain abnormalities (90%)
• Congenital heart defects (70%)
• Eye problems (50%%)
• Distinct facial features
• Growth abnormalities
Prader-Willi Syndrome
• Infantile hypotonia
• Hypothalamic hypogonadism
• Mild to moderate DD
• Initial FTT
• Later Obesity
• Short stature
Prader Willi Syndrome
• Paternal copy expressed
• Maternal copy silenced
Angelman Syndrome
• Severe DD
• Movement disorder-ataxia
• Acquired microcephaly
• Seizures
• Unique behavior
(Happy Puppet)
Angelman Syndrome
● Maternal copy expressed
● Paternal copy silenced
5p Deletion /Cri du Chat Syndrome
• Cat Like Cry
• Severe DD / Behavioral problems
• Microcephaly
• Dysmorphic Features
• Deletions 3 - 30 Mb
• 90% de novo
• 10% parental balanced translocation
4p- Deletion/ Wolf-Hirschhorn Syndrome
• Syndrome
• Microcephaly
• Micrognathia,
• Short philtrum,
• Prominent glabella
• Ocular hypertelorism,
• Dysplastic ears and periauricular tags
• Growth and mental retardation
Microdeletion Panel - NATERA
Microdeletion Panel - ILLUMINA
Microdeletion Panel - SEQUENOM
MaterniT® GENOME - SEQUENOM
NIPT Microdeletion Panels - Pros
• Microdeletions are relatively common
• Some more severe than Down syndrome
• Are not part of routine serum screening
• Incidence is independent of age or ethnicity
• Many have no ultrasound findings
• Can occur spontaneously without family history
NIPT Microdeletion Panels - Cons
• Not validated in clinical studies
• Most studies used spiked serum samples
• Not all del22q cases detected
(only 85% 3Mb deletions)
• Not all Prader Willi/Angelman cases detected
(only ~70% due to deletions)
• Microdeletion burden not significantly altered
NIPT Microdeletion Panels - Cons
• In high-risk patients (i.e. with U/S anomalies)
o Increased risk of missed diagnoses
• In low-risk patients
o Low PPV and increased false positive rates
Predictive Values (PPV & NPV)
• Positive Predictive Value
o Given an abnormal result -
what is the chance of truly having the Condition ?
o “How worried should I be ?”
• Negative Predictive Value
o Given an normal result -
what is the chance of truly NOT having the Condition ?
o “How reassured Can I be ?”
PPV Influenced by Prevalence
Positive Predictive Values T21
52.5%
91.8%
99.2%
0% 20% 40% 60% 80% 100%
1:1000
1:100
1:10
Prevalence
Based on Gil MM et al. Ultrasound Obstet Gynecol 2015; 45: 249–266
Positive Predictive Values
In a 35 year old patient assuming 99.9% sensitivity at 0.1% FPR
0%
10%
20%
30%
40%
50%
60%
70%
80%
90%
T21 T18 T13 22q11 1p36 15q 5p-
Yaron et al. Obstet Gynecol, in Press
Genetic Aberrations
• Chromosomal
o Numeric
o Structural
• Submicroscopic Copy Number Variants (CNVs)
o Deletions
o Duplications
• Sequence variants
o Single nucleotide polymorphisms (SNPs)
o Pathogenic mutations
Paternally-Inherited &
de novo Dominant Mutations
Paternally-Inherited Mutations
Lo and Chiu Nature Reviews Genetics 2007;8:71–77
Paternally inherited or de novo
autosomal dominant disorders
Monogenic disorder Approach to NIPD
Achondroplasia • Detection or exclusion of paternal or
de novo allele reported as
diagnostic.
• Technologies used include a variety
of PCR approaches, dPCR and NGS
Apert syndrome
Early onset primary dystonia I
Thanatophoric dysplasia
Huntington's disease
• Not fully accurate. Invasive testing
recommended for diagnosis
Paternally Inherited Mutations
Autosomal dominant disease
Autosomal recessive conditions where
parents carry different altered alleles
Monogenic disorder Approach to NIPD
a & β-thalassaemia • Exclusion of paternal allele reduces
risk to zero.
• Detection of the paternal allele
indicates an increased risk (to 50%)
and invasive testing is required for
definitive diagnosis.
• Technologies used include PCR,
dPCR and NGS have been reported
CAH
Cystic fibrosis
Leber congenital amaurosis
Propionic acidemia
Frasers syndrome
AR polycystic kidney disease
Paternally Inherited Mutations
Autosomal recessive disease
Autosomal recessive conditions where
parents carry the same altered allele
Monogenic disorder Approach to NIPD
Sickle cell anaemia
• Estimation of allelic ratios
required, so accurate estimation
of fetal fraction needed.
• Currently can only be done using
dPCR or NGS.
• Limited application in female
fetuses.
Y-chromosome sequences can be
used in male-bearing pregnancies
β-thalassaemia
Autosomal Recessive Conditions
Autosomal Recessive Conditions
Depth of Sequencing
Is This the Future of Amniocentesis ?

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20150918 - Y Yuval - NIPT for Microdeletions & Single Gene Disorders

  • 1. NIPT for Microdeletions & Single Gene Disorders Yuval Yaron, MD Tel Aviv Sourasky Medical Center
  • 2. Disclosures • Consultant, Teva Pharmaceuticals Inc. Distributor of Verifi® • Consultant, FugeneGenetics. Distributor of Harmony® • Member, Clinical Expert panel Illumina Reproductive & Genomic Health Manufacturer of Sequencing Products, Verifi®
  • 3. Human Genome = Encyclopedia
  • 6. Genome = 3,000,000,000 Exome = 2% of the Genome
  • 7. Genetic Aberrations • Chromosomal o Numerical o Structural • Submicroscopic o Deletions o Duplications • Sequence variants o Polymorphisms o Mutations
  • 8. Genetic Aberrations • Chromosomal • Numerical • Structural • Submicroscopic • Deletions • Duplications • Sequence variants • Polymorphisms • Mutations
  • 9. Basic NIPT Detects ~83% of Chromosomal Anomalies Modified from Wellesley et al. European Journal of Human Genetics 2012;20:521–526
  • 10. Basic NIPT would Miss 17% of Anomalies Modified from Wellesley et al. European Journal of Human Genetics 2012;20:521–526
  • 11. NIPT for Rare Autosomal Trisomies • Some laboratories include NIPT screening for: trisomy 9, trisomy 16 and trisomy 22 • However most of such conceptuses spontaneously abort in the 1st trimester (unless mosaic). • With each added condition there is the potential for an additional 0.1% to the false positive rates • Questionable benefit
  • 12. Genetic Aberrations • Chromosomal • Numerical • Structural • Submicroscopic o Deletions o Duplications • Sequence variants • Polymorphisms • Mutations
  • 14. Common Microdeletions Prader Willi 4 Mb del 15q11-13 Williams-Beuren 1.5 Mb del 7q11.23 DiGeorge / VCF 3.5 Mb del 22q11
  • 18. Detects Deletions & Duplications
  • 19. Risk of Significant Deletion/Duplication • Autism or MR + dysmorphism 10%-20% • Fetus with ultrasound anomaly 5%-7% • No Risk, normal karyotype 0.5%
  • 20.
  • 21. CNVs Following Normal Karyotype Total CNV with Clinical Significance (%) Pathogenic CNV (%) CNV of Uncertain Clinical Significance Benign CNV (%) Indication for Prenatal Diagnosis Potential Clinical Significance (%) Likely Benign CNV (%) 6.02.83.22.532.7US Anomaly 1.70.51.31.931.9Maternal Age 1.60.41.21.833.9Screen Positive 1.30.50.80.830.1Other * 2.50.91.61.832.3All
  • 22. Genetic Counseling for Variants of Unclear Significance (VOUSs)
  • 24. Srinavasan A, et al. Noninvasive detection of fetal subchromosome abnormalities via deep sequencing of maternal plasma. Am J Human Genet 2013;92:1-10 Fetal Microdeletions Detected by NIPT
  • 25. Commercial Microdeletion Panels Syndrome Locus Estimated prevalence Deletion size (Mb) ≥3 Mb DiGeorge/ velocardiofacial syndrome 22q11.2 1:2000 - 1:4000 3 85% Monosomy 1p36 1p36 1:5000 - 1:10,000 1.5 - 10.5 85% Angelman syndrome or Prader-Willi syndrome 15q11.2-q13 1:20,000 5 – 6 70% 5p- Cri-du-Chat syndrome 5p15 1:50,000 10 - 30 99% 4p- Wolf-Hirschhorn syndrome 4p16.3 1:50,000 1.9 – 30 99% Yaron et al. 2015, Obstet Gynecol, in Press
  • 26. 22q11.2 Deletion ● Overlaps Velocardiofacial/DiGeorge Syndrome ● De novo (~90%) or inherited (~10%) ● Variable phenotype ● Congenital heart defect (74%) ● Palate abnormalities (69%) ● Learning difficulties (70–90%) ● Characteristic facial features ● Thymic and parathyroid abnormalities
  • 27. 1p36 Deletion Syndrome • Significant developmental delay • Behavioral problems • Hypotonia (95%) • Brain abnormalities (90%) • Congenital heart defects (70%) • Eye problems (50%%) • Distinct facial features • Growth abnormalities
  • 28. Prader-Willi Syndrome • Infantile hypotonia • Hypothalamic hypogonadism • Mild to moderate DD • Initial FTT • Later Obesity • Short stature
  • 29. Prader Willi Syndrome • Paternal copy expressed • Maternal copy silenced
  • 30. Angelman Syndrome • Severe DD • Movement disorder-ataxia • Acquired microcephaly • Seizures • Unique behavior (Happy Puppet)
  • 31. Angelman Syndrome ● Maternal copy expressed ● Paternal copy silenced
  • 32. 5p Deletion /Cri du Chat Syndrome • Cat Like Cry • Severe DD / Behavioral problems • Microcephaly • Dysmorphic Features • Deletions 3 - 30 Mb • 90% de novo • 10% parental balanced translocation
  • 33. 4p- Deletion/ Wolf-Hirschhorn Syndrome • Syndrome • Microcephaly • Micrognathia, • Short philtrum, • Prominent glabella • Ocular hypertelorism, • Dysplastic ears and periauricular tags • Growth and mental retardation
  • 38. NIPT Microdeletion Panels - Pros • Microdeletions are relatively common • Some more severe than Down syndrome • Are not part of routine serum screening • Incidence is independent of age or ethnicity • Many have no ultrasound findings • Can occur spontaneously without family history
  • 39. NIPT Microdeletion Panels - Cons • Not validated in clinical studies • Most studies used spiked serum samples • Not all del22q cases detected (only 85% 3Mb deletions) • Not all Prader Willi/Angelman cases detected (only ~70% due to deletions) • Microdeletion burden not significantly altered
  • 40. NIPT Microdeletion Panels - Cons • In high-risk patients (i.e. with U/S anomalies) o Increased risk of missed diagnoses • In low-risk patients o Low PPV and increased false positive rates
  • 41. Predictive Values (PPV & NPV) • Positive Predictive Value o Given an abnormal result - what is the chance of truly having the Condition ? o “How worried should I be ?” • Negative Predictive Value o Given an normal result - what is the chance of truly NOT having the Condition ? o “How reassured Can I be ?”
  • 42. PPV Influenced by Prevalence
  • 43. Positive Predictive Values T21 52.5% 91.8% 99.2% 0% 20% 40% 60% 80% 100% 1:1000 1:100 1:10 Prevalence Based on Gil MM et al. Ultrasound Obstet Gynecol 2015; 45: 249–266
  • 44. Positive Predictive Values In a 35 year old patient assuming 99.9% sensitivity at 0.1% FPR 0% 10% 20% 30% 40% 50% 60% 70% 80% 90% T21 T18 T13 22q11 1p36 15q 5p- Yaron et al. Obstet Gynecol, in Press
  • 45. Genetic Aberrations • Chromosomal o Numeric o Structural • Submicroscopic Copy Number Variants (CNVs) o Deletions o Duplications • Sequence variants o Single nucleotide polymorphisms (SNPs) o Pathogenic mutations
  • 46. Paternally-Inherited & de novo Dominant Mutations
  • 47. Paternally-Inherited Mutations Lo and Chiu Nature Reviews Genetics 2007;8:71–77
  • 48. Paternally inherited or de novo autosomal dominant disorders Monogenic disorder Approach to NIPD Achondroplasia • Detection or exclusion of paternal or de novo allele reported as diagnostic. • Technologies used include a variety of PCR approaches, dPCR and NGS Apert syndrome Early onset primary dystonia I Thanatophoric dysplasia Huntington's disease • Not fully accurate. Invasive testing recommended for diagnosis
  • 50. Autosomal recessive conditions where parents carry different altered alleles Monogenic disorder Approach to NIPD a & β-thalassaemia • Exclusion of paternal allele reduces risk to zero. • Detection of the paternal allele indicates an increased risk (to 50%) and invasive testing is required for definitive diagnosis. • Technologies used include PCR, dPCR and NGS have been reported CAH Cystic fibrosis Leber congenital amaurosis Propionic acidemia Frasers syndrome AR polycystic kidney disease
  • 52. Autosomal recessive conditions where parents carry the same altered allele Monogenic disorder Approach to NIPD Sickle cell anaemia • Estimation of allelic ratios required, so accurate estimation of fetal fraction needed. • Currently can only be done using dPCR or NGS. • Limited application in female fetuses. Y-chromosome sequences can be used in male-bearing pregnancies β-thalassaemia
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  • 59. Is This the Future of Amniocentesis ?