1 / 33

Array CGH diagnosing developmental disorders

Array CGH diagnosing developmental disorders. Nigel P. Carter. Solid Tumours. Nature 408, 248-254 (9 November 2000) The age of cancer. Ronald A. DePinho. Ratio. Position on Chromosome. Conventional CGH. Test Genomic DNA (Tumor DNA). Reference Genomic DNA. Cot-1 DNA. gain.

hang
Télécharger la présentation

Array CGH diagnosing developmental disorders

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript

  1. Array CGH diagnosing developmentaldisorders Nigel P. Carter

  2. Solid Tumours Nature 408, 248-254 (9 November 2000) The age of cancer. Ronald A. DePinho

  3. Ratio Position on Chromosome Conventional CGH Test Genomic DNA (Tumor DNA) Reference Genomic DNA Cot-1 DNA gain deletion

  4. Conventional CGH

  5. Improve resolution by replacing metaphase chromosomes as targets for CGH with spatially separated DNA clones spotted at high density onto glass slides CGH On Microarrays • Resolution of metaphase CGH ~ 3-5 Mb • Resolution will be dependent on clone size and density

  6. Ratio Position on Sequence Array-CGH Reference Genomic DNA Test Genomic DNA (Patient DNA) Cot-1 DNA

  7. 1Mb Resolution Array • 167 BACs/PACs • containing known oncogenes/tumour suppressor genes • telomeric clone set • (S. Knight, Oxford) • 3523 clones • all spotted in duplicate • clone set publicly available Heike Fiegler Fiegler et al. (2003) Genes Chromosomes and Cancer 36:361-374

  8. Hybridisation With 769P DNA

  9. Copy number changes in patients with learning difficulty and dysmorphology 50 patients 12 with one imbalance Shaw-Smith C, Redon R, Rickman L, Rio M, Willatt L, Fiegler H et al., J. Med Genet 2004; 41:241-248 None of the copy number changes are in common

  10. Copy number changes in patients with learning difficulty and dysmorphology 50 patients 12 with one imbalance

  11. Deletion at 9q22.3 Feeding difficulties in the first months of life Pre- and post-natal overgrowth (weight, length, OFC > +3 SD) Psychomotor delay and hyperactivity (still unable to walk unaided at six years of age, no speech) Hypotonia, trigonocephaly, epicanthic folds, small mouth with a thin upper lip, thickened ears with ear lobule indentation, downslanting palpebral fissures, short neck, pectus excavatum, strabismus, umbilical hernia,thyroglossal cyst, advanced carpal maturation at birth and ventriculomegaly Is the de novo 9q22.3 deletion responsible for the phenotype?

  12. Similar deletion at 9q22.3 Chromosome 9 Richard Redon, Laurence Colleaux

  13. 9q22.3 deletion Syndrome Feeding difficulties in the first months of life Pre- and post-natal overgrowth (weight, length, OFC > +3 SD) Psychomotor delay and hyperactivity (still unable to walk unaided at six years of age, no speech) Hypotonia, trigonocephaly, epicanthic folds, small mouth with a thin upper lip, thickened ears with ear lobule indentation, downslanting palpebral fissures, short neck, pectus excavatum, strabismus, umbilical hernia,thyroglossal cyst, advanced carpal maturation at birth and ventriculomegaly

  14. Informed Consent Without consent your patients are not visible to others and others’ patients are not visible to you DECIPHER DECIPHER

  15. International CollaborationDel 14q11.2 Syndrome Vancouver Cambridge • Symptoms/Phenotype • Developmental delay • Autism spectrum disorder • Hypotonia • Squint • Normal growth parameters • Mild dysmorphisms • eg. hypoplastic nasal bridge, short nose with long philtrum, prominent antihelices etc. • Candidate genes • SUPT16H Subunit of FACT • Chromatin binding and remodelling • CHD8 Epigenetic regulation of transcription • NDRG2 Neurite outgrowth Zahir F et al. Novel deletions of 14q11.2 associated with mental retardation and similar minor anomalies in three children. J Med Genet 2007 May 2007 epub

  16. Cambridge San Paulo

  17. The Sanger Institute Whole Genome Tiling Path Array 27,000 clones covering the whole human genome Heike Fiegler

  18. Deletion on Chromosome 1 Log2 ratio Richard Redon

  19. Oligonucleotide Arrays

  20. 30,000 BACs 500,000 SNPs 42,000,000 oligos

  21. Deciphering Developmental Disorders ‘To advance clinical genetic practice for children with developmental disorders by the systematic application of the latest microarray and sequencing methods while addressing the new ethical challenges raised’ Health Innovation Challenge Fund

  22. 8 DDD Genetic Counsellors with Clinicians in 23 Regional Services Full consent – ethics research and support WT Sanger Institute Array-CGH and Genotyping Extended regions of homozygosity Variant association 8 DDD Genetic Counsellors with Clinicians in 23 Regional Services Ethical research and support 12,000 undiagnosed cases 24,000 parents 1,000 normal controls plus external control data >2,000 diagnosed cases open release in DECIPHER Newly identified genes cf. copy number data 10,000 undiagnosed cases WT Clinical Research Facilities/Regional Services Case selection and testing Detailed Phenotying Sanger Institute Specific exon resequencing in patients Mouse models Sanger Institute DDD DNA Collection Sanger Institute Exon Resequencing Mutation detection (funded by Sanger Institute) Genetic counselling with patients and families Family/public engagement Controlled data access for research Design of optimised arrays and sequence-based diagnostic assays 12,000 cases and 24,000 parents

  23. Array Design • 2 million probe array-CGH (Proband) • Copy number changes • 5 probes per exon, conserved regions, linc RNAs • CNVs • Genome backbone probes – every ~3 kb • > 700+100k SNP genotyping array (Trios) • SNP association, extended regions LOH • CNV tagging SNPs • 100k probes filling gaps

  24. Acknowledgements DECIPHER Team Manuel Corpas, Eugene Bragin Paul Bevan, Stephen Clayton, Diana Rajan Helen Firth, Nigel Carter, Steven Van Vooren (Data Mining) Shola Richards, Roger Pettett, Heike Fiegler, Dimitrios Kalaitzopolous and all DECIPHER Consortium members, patients and families

  25. Acknowledgements DDD • 23 UK Regional Genetics Services • Nigel Carter, Matthew Hurles, Jeff Barrett • Helen Firth, David Fitzpatrick • Mike Parker • Programmers – Adrian Tivey, Tom Fitzgerald, Stephen Clayton, Daniele Pietrobelli • Wet lab - Susan Gribble, Elena Prigmore, Di Rajan, Kirsty Ambridge, Daniel Barrett, Netravathi Krishnappa, Tanya Bayzetinova • + 1 Statistical Geneticist • Project Manager – Caroline Wright • Social Scientist/Ethicist – Anna Middleton • Sanger Pipelines • DECIPHER Team

More Related