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Published online before print January 18, 2001, 10.1101/gr.GR-1649R
January 18, 2001, 10.1101/gr.GR-1649R
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Vol. 11, Issue 2, 300-307, February 2001

RESOURCES
A cSNP Map and Database for Human Chromosome 21

Samuel Deutsch,1,2 Christian Iseli,3,4 Philipp Bucher,4,5 Stylianos E. Antonarakis,1,7 and Hamish S. Scott1,6

1 Division of Medical Genetics, University of Geneva Medical School, Geneva, Switzerland; 2 Graduate Program in Molecular and Cellular Biology, University of Geneva Medical School, Geneva, Switzerland; 3 Ludwig Institute for Cancer Research, Epalinges, Switzerland; 4 Swiss Bioinformatics Institute, Epalinges, Switzerland; 5 Swiss Institute for Experimental Cancer Research, Epalinges, Switzerland

Single nucleotide polymorphisms (SNPs) are likely to contribute to the study of complex genetic diseases. The genomic sequence of human chromosome 21q was recently completed with 225 annotated genes, thus permitting efficient identification and precise mapping of potential cSNPs by bioinformatics approaches. Here we present a human chromosome 21 (HC21) cSNP database and the first chromosome-specific cSNP map. Potential cSNPs were generated using three approaches: (1) Alignment of the complete HC21 genomic sequence to cognate ESTs and mRNAs. Candidate cSNPs were automatically extracted using a novel program for context-dependent SNP identification that efficiently discriminates between true variation, poor quality sequencing, and paralogous gene alignments. (2) Multiple alignment of all known HC21 genes to all other human database entries. (3) Gene-targeted cSNP discovery. To date we have identified 377 cSNPs averaging ~1 SNP per 1.5 kb of transcribed sequence, covering 65% of known genes in the chromosome. Validation of our bioinformatics approach was demonstrated by a confirmation rate of 78% for the predicted cSNPs, and in total 32% of the cSNPs in our database have been confirmed. The database is publicly available at http://csnp.unige.ch or http://csnp.isb-sib.ch. These SNPs provide a tool to study the contribution of HC21 loci to complex diseases such as bipolar affective disorder and allele-specific contributions to Down syndrome phenotypes.


6 Present address: Genetics and Bioinformatics Group, The Walter and Eliza Hall Institute of Medical Research, Post Office, Royal Melbourne Hospital, 3050 Victoria, Australia.

7 Corresponding author.


11:300-307 ©2001 by Cold Spring Harbor Laboratory Press  ISSN 1088-9051/01 $5.00

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