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Copy number variations in
monozygotic twins
discordant for schizophrenia
Christina A. Castellani, Sujit Maiti, Kiran Kumar HB,
Richard L. O’Reilly and Shiva M. Singh
The University of Western Ontario
Schizophrenia, OMIM 181500
• > 1% of the population
• Characterized by a distortion of reality
• Heritability estimates of ~80%
• Significant disease heterogeneity
• Most cases singleton in the family
• Complex inheritance patterns
• Greatest risk is family history
Complex and Subjective diagnosis
Schizophrenia Inheritance
Search for genes: progress to date
• Chromosomal abnormalities (22q11, 1q42.1)
• Candidate gene approach (COMT, PRODH)
• Early linkage based on few markers (DTNBP1,
NRG1, DAOA)
• Genome wide association studies
(ZNF804A)
Despite increasing numbers (>6,000) of patients
and controls (>12,000), few genes have been
identified and results are difficult to reproduce
 Conclusions?
Two Unique Families
Family - 1
I-2-1
Schizophrenia
I-2-2
Bipolar
Disorder
I-1-1
Compulsive
Personality
Disorder
I-1-2
Family - 2
II-2-1
Schizophrenia
II-2-2
II-1-1 II-1-2
Copy Number Variation
• A candidate for disease associated
variation in humans
• Variable copies of DNA segments
• DNA deletions, insertions, duplications
• > 1kb and up to several mb
• 77% of CNVs are currently predicted to
include genes
• Covering about 12% of the genome in
healthy individuals
Affymetrix Genome Wide
Human SNP Array 6.0
• Median intermarker distance of less than 700 bp
• Provides breakpoint identification
• 1.8 Million Genetic Markers
> 906, 000 SNP Probes
> 946, 000 CNV Probes
Detection of Copy Number Variations
Chromosome CNV Architecture
Lee, Charles. 2007. Nature Genetics S39.
Copy Number Variation (CNV)
Distribution of CNV among family
members according to size
CNVs Size
Family 1 Family 2
I-1-1 I-1-2 I-2-1 I-2-2 Total II-1-1 II-1-2 II-2-1 II-2-2 Total
<=100 kb 0 0 0 0 0 2 0 0 1 3
>100 to 200 kb 17 18 15 20 70 119 50 24 24 217
>200 to 300 kb 11 6 4 10 31 25 6 13 9 53
>300 to 400 kb 5 5 6 5 21 11 3 1 4 19
>400 to 500 kb 2 0 2 2 6 6 1 1 2 10
>500 to 1000 kb 6 2 4 7 19 7 2 5 2 16
>1 to 10 Mb 9 4 5 3 21 5 2 4 5 16
>10 to 20 Mb 5 0 0 0 5 0 0 0 0 0
>20 Mb 3 0 0 0 3 2 0 2 2 6
Total 58 35 36 47 176 177 64 50 49 340
Distribution of CNVs within
family members
Chromosome Wide CNV Distribution
Chr No.
Family 1 Family 2
I.1 I.2 II.1 II.2 Total I.1 I.2 II.1 II.2 Total
1 4 2 2 2 10 11 2 6 6 25
2 4 2 5 5 16 11 2 2 3 18
3 1 4 2 3 10 7 4 4 2 17
4 4 3 2 4 13 8 1 3 2 14
5 0 0 0 0 0 12 0 2 1 15
6 0 0 0 0 0 10 2 0 0 12
7 2 6 3 4 15 10 5 3 4 22
8 1 0 3 3 7 7 3 3 3 16
9 1 1 2 3 7 4 4 3 4 15
10 2 1 1 1 5 3 5 1 1 10
11 3 1 2 1 7 5 1 2 2 10
12 0 1 0 1 2 4 3 0 1 8
13 0 0 0 0 0 40 1 1 0 42
14 4 6 3 5 18 4 6 5 3 18
15 4 3 1 3 11 2 6 6 8 22
16 2 1 2 3 8 9 1 1 1 12
17 4 1 2 3 10 8 2 2 1 13
18 0 0 0 0 0 1 0 0 1 2
19 0 1 0 0 1 7 3 2 1 13
20 0 0 0 0 0 0 0 0 1 1
21 1 2 2 3 8 2 3 2 1 8
22 3 0 3 2 8 3 1 1 1 6
X 18 0 1 1 20 9 9 1 2 21
Total 58 35 36 47 176 177 64 50 49 340
Gain/Loss Profiles
Gain/Loss Profiles
Gene and Pathway Analysis
Family 1: affected patient (schizophrenia) had
unique CNVs that overlapped 8 genes
Family 2: affected patient (schizophrenia) had
unique CNVs that overlapped 3 genes
Genes in the affected individual of family 1
harboured genes involved in starch and
sucrose metabolism networks (2.2 E-06)
Repeat Elements at de novo CNV
Breakpoints
de novo CNVs
• Meiotic de novo (in both twins, N=12)
• Mitotic de novo (in one twin only, N=28)
• Three de novo regions that were novel,
harbouring three genes
– PSMC1: 26S protease regulatory subunit 4
– C14orf102: highly conserved gene, no known
function
– KIAA0146: function unknown, expressed in brain
among other tissues
Twin Based Approach
• 6 pairs of MZ twins discordant for
schizophrenia
– Average number of CNVs per individual = 37.25
– Gains more frequent than losses
– 31 novel CNVs across 12 samples
– The majority (211 CNVs) were within 100 and 200
kb in size
Ingenuity Pathway Analysis (IPA)
Physiological System or Disease P-Value # Genes
Genetic Disorder 2.16 E-03 - 4.64 E-02 10
Neurological Disease 2.16 E-03 - 4.64 E-02 14
Nervous System Development and Function 9.16 E-03 3
In Summary
Copy Number Variants were found to:
– be frequent,
– harbour repeats at their breakpoints,
– overlap genes associated with
neurological networks,
– be both meiotic and mitotic in origin
– vary in location across patients
CNV differences can be detected
in MZ twins and are patient specific
Acknowledgements
We would like to acknowledge the following groups for their
funding and support:
- Canadian Institutes for Health Research (CIHR)
- Ontario Mental Health Foundation (OMHF)
- Schizophrenia Society of Ontario (SSO)
- The University of Western Ontario
A special thanks to David Carter (London Regional Genomics
Center) and the individuals who contributed samples for
use in this study.

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Copy number variations in monozygotic twins discordant for schizophrenia

  • 1. Copy number variations in monozygotic twins discordant for schizophrenia Christina A. Castellani, Sujit Maiti, Kiran Kumar HB, Richard L. O’Reilly and Shiva M. Singh The University of Western Ontario
  • 2. Schizophrenia, OMIM 181500 • > 1% of the population • Characterized by a distortion of reality • Heritability estimates of ~80% • Significant disease heterogeneity • Most cases singleton in the family • Complex inheritance patterns • Greatest risk is family history
  • 5. Search for genes: progress to date • Chromosomal abnormalities (22q11, 1q42.1) • Candidate gene approach (COMT, PRODH) • Early linkage based on few markers (DTNBP1, NRG1, DAOA) • Genome wide association studies (ZNF804A) Despite increasing numbers (>6,000) of patients and controls (>12,000), few genes have been identified and results are difficult to reproduce  Conclusions?
  • 6. Two Unique Families Family - 1 I-2-1 Schizophrenia I-2-2 Bipolar Disorder I-1-1 Compulsive Personality Disorder I-1-2 Family - 2 II-2-1 Schizophrenia II-2-2 II-1-1 II-1-2
  • 7. Copy Number Variation • A candidate for disease associated variation in humans • Variable copies of DNA segments • DNA deletions, insertions, duplications • > 1kb and up to several mb • 77% of CNVs are currently predicted to include genes • Covering about 12% of the genome in healthy individuals
  • 8. Affymetrix Genome Wide Human SNP Array 6.0 • Median intermarker distance of less than 700 bp • Provides breakpoint identification • 1.8 Million Genetic Markers > 906, 000 SNP Probes > 946, 000 CNV Probes Detection of Copy Number Variations
  • 9. Chromosome CNV Architecture Lee, Charles. 2007. Nature Genetics S39.
  • 11. Distribution of CNV among family members according to size CNVs Size Family 1 Family 2 I-1-1 I-1-2 I-2-1 I-2-2 Total II-1-1 II-1-2 II-2-1 II-2-2 Total <=100 kb 0 0 0 0 0 2 0 0 1 3 >100 to 200 kb 17 18 15 20 70 119 50 24 24 217 >200 to 300 kb 11 6 4 10 31 25 6 13 9 53 >300 to 400 kb 5 5 6 5 21 11 3 1 4 19 >400 to 500 kb 2 0 2 2 6 6 1 1 2 10 >500 to 1000 kb 6 2 4 7 19 7 2 5 2 16 >1 to 10 Mb 9 4 5 3 21 5 2 4 5 16 >10 to 20 Mb 5 0 0 0 5 0 0 0 0 0 >20 Mb 3 0 0 0 3 2 0 2 2 6 Total 58 35 36 47 176 177 64 50 49 340
  • 12. Distribution of CNVs within family members
  • 13. Chromosome Wide CNV Distribution Chr No. Family 1 Family 2 I.1 I.2 II.1 II.2 Total I.1 I.2 II.1 II.2 Total 1 4 2 2 2 10 11 2 6 6 25 2 4 2 5 5 16 11 2 2 3 18 3 1 4 2 3 10 7 4 4 2 17 4 4 3 2 4 13 8 1 3 2 14 5 0 0 0 0 0 12 0 2 1 15 6 0 0 0 0 0 10 2 0 0 12 7 2 6 3 4 15 10 5 3 4 22 8 1 0 3 3 7 7 3 3 3 16 9 1 1 2 3 7 4 4 3 4 15 10 2 1 1 1 5 3 5 1 1 10 11 3 1 2 1 7 5 1 2 2 10 12 0 1 0 1 2 4 3 0 1 8 13 0 0 0 0 0 40 1 1 0 42 14 4 6 3 5 18 4 6 5 3 18 15 4 3 1 3 11 2 6 6 8 22 16 2 1 2 3 8 9 1 1 1 12 17 4 1 2 3 10 8 2 2 1 13 18 0 0 0 0 0 1 0 0 1 2 19 0 1 0 0 1 7 3 2 1 13 20 0 0 0 0 0 0 0 0 1 1 21 1 2 2 3 8 2 3 2 1 8 22 3 0 3 2 8 3 1 1 1 6 X 18 0 1 1 20 9 9 1 2 21 Total 58 35 36 47 176 177 64 50 49 340
  • 16. Gene and Pathway Analysis Family 1: affected patient (schizophrenia) had unique CNVs that overlapped 8 genes Family 2: affected patient (schizophrenia) had unique CNVs that overlapped 3 genes Genes in the affected individual of family 1 harboured genes involved in starch and sucrose metabolism networks (2.2 E-06)
  • 17. Repeat Elements at de novo CNV Breakpoints
  • 18. de novo CNVs • Meiotic de novo (in both twins, N=12) • Mitotic de novo (in one twin only, N=28) • Three de novo regions that were novel, harbouring three genes – PSMC1: 26S protease regulatory subunit 4 – C14orf102: highly conserved gene, no known function – KIAA0146: function unknown, expressed in brain among other tissues
  • 19. Twin Based Approach • 6 pairs of MZ twins discordant for schizophrenia – Average number of CNVs per individual = 37.25 – Gains more frequent than losses – 31 novel CNVs across 12 samples – The majority (211 CNVs) were within 100 and 200 kb in size
  • 20. Ingenuity Pathway Analysis (IPA) Physiological System or Disease P-Value # Genes Genetic Disorder 2.16 E-03 - 4.64 E-02 10 Neurological Disease 2.16 E-03 - 4.64 E-02 14 Nervous System Development and Function 9.16 E-03 3
  • 21. In Summary Copy Number Variants were found to: – be frequent, – harbour repeats at their breakpoints, – overlap genes associated with neurological networks, – be both meiotic and mitotic in origin – vary in location across patients CNV differences can be detected in MZ twins and are patient specific
  • 22. Acknowledgements We would like to acknowledge the following groups for their funding and support: - Canadian Institutes for Health Research (CIHR) - Ontario Mental Health Foundation (OMHF) - Schizophrenia Society of Ontario (SSO) - The University of Western Ontario A special thanks to David Carter (London Regional Genomics Center) and the individuals who contributed samples for use in this study.

Notas del editor

  1. 20 min, including 3-5 min for questions
  2. Overlapping symtoms
  3. Concordance rates for MZ twins average 48%Concordance rates for DZ twins average 14%
  4. We are now more sure than ever that schizophrenia is not controlled by one defining marker or variant. We require unique approaches. Highly heterogenous. Different families may have different causal mutations.
  5. Unique due to MZ twins – discordance – inheritance patterns can be analyzed
  6. A new layer of genomic complexityCNVs are defined as compared to a reference genome
  7. Each SNP or CNV on the chip is assessed using a perfect match (PM) method and 4 probes per SNP are present on the array.202,000 known CNV probes&gt;906,000 SNP probes, &gt;946,000 CNV probes, TCAG probesAccurate breakpoint identification helpful for downstream identification of genes and precision in comparing samples.
  8. CNV present in Dad and both twins, inherited CNV
  9. Over 10 per cent of the CNVs identified were novel, not found in the database of genomic variantsAvg. Number of CNV per person = 64.5
  10. Known reported deletion syndrome on chromosome 13
  11. Affected and Unaffected, 13 differences between the two, 50 CNVs in top, 49 CNVs on bottom
  12. Affected and Unaffected, 4 differences between the two, 37 in top, 48 in bottom
  13. Say something about each of these genesPSMC1 has previously been implicated in a neurodegenerative model
  14. Of 66 genesPSMC1?C14orf102?