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Human Molecular Genetics Advance Access published online on April 21, 2009
Human Molecular Genetics, doi:10.1093/hmg/ddp187
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© 2009 The Author(s)
This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/2.0/uk/) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

Characterization of six human disease-associated inversion polymorphisms

Francesca Antonacci1, Jeffrey M. Kidd1, Tomas Marques-Bonet1, Mario Ventura2, Priscillia Siswara1, Zhaoshi Jiang1 and Evan E. Eichler1,*

1 Department of Genome Sciences and Howard Hughes Medical Institute, University of Washington, Seattle, WA, 98195 USA 2 Department of Genetics and Microbiology, University of Bari, Bari, 70126 Italy

* Corresponding author: Evan E. Eichler, Ph.D. University of Washington School of Medicine, Howard Hughes Medical Institute, Box 355065, Foege S413C, 1705 NE Pacific St. Seattle, WA 98195 E-mail: eee{at}gs.washington.edu

Received February 26, 2009; Revised April 8, 2009; Accepted April 16, 2009

The human genome is a highly dynamic structure that shows a wide range of genetic polymorphic variation. Unlike other types of structural variation, little is known about inversion variants within normal individuals because such events are typically balanced and are difficult to detect and analyze by standard molecular approaches. Using sequence-based, cytogenetic and genotyping approaches, we characterized six large inversion polymorphisms that map to regions associated with genomic disorders with complex segmental duplications mapping at the breakpoints. We developed a metaphase FISH-based assay to genotype inversions and analyzed the chromosomes of 27 individuals from three HapMap populations. In this subset, we find that these inversions are less frequent or absent in Asians when compared to European and Yoruban populations. Analyzing multiple individuals from outgroup species of great apes, we show that most of these large inversion polymorphisms are specific to the human lineage with two exceptions, 17q21.31 and 8p23 inversions, which are found to be similarly polymorphic in other great ape species and where the inverted allele represents the ancestral state. Investigating linkage disequilibrium relationships with genotyped SNPs, we provide evidence that most of these inversions appear to have arisen on at least two different haplotype backgrounds. In these cases, discovery and genotyping methods based on SNPs may be confounded and molecular cytogenetics remains the only method to genotype these inversions.


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