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Vol. 12, Issue 12, 1815-1826, December 2002

LETTER
Evidence for a Fast, Intrachromosomal Conversion Mechanism From Mapping of Nucleotide Variants Within a Homogeneous alpha -Satellite DNA Array

Dirk Schindelhauer,1,2,4 and Tobias Schwarz3

1 Institute of Human Genetics, Technical University of Munich, Munich, Germany; 2 GSF-Institute of Human Genetics, Neuherberg, Germany; 3 Department of Medical Genetics, Children's Hospital, Ludwig Maximilians University, Munich, Germany

Assuming that patterns of sequence variants within highly homogeneous centromeric tandem repeat arrays can tell us which molecular turnover mechanisms are presently at work, we analyzed the alpha -satellite tandem repeat array DXZ1 of one human X chromosome. Here we present accurate snapshots from this dark matter of the genome. We demonstrate stable and representative cloning of the array in a P1 artificial chromosome (PAC) library, use samples of higher-order repeats subcloned from five unmapped PACs (120-160 kb) to identify common variants, and show that such variants are presently in a fixed transition state. To characterize patterns of variant spread throughout homogeneous array segments, we use a novel partial restriction and pulsed-field gel electrophoresis mapping approach. We find an older large-scale (35-50 kb) duplication event supporting the evolutionarily important unequal crossing-over hypothesis, but generally find independent variant occurrence and a paucity of potential de novo mutations within segments of highest homogeneity (99.1%-99.3%). Within such segments, a highly nonrandom variant clustering within adjacent higher-order repeats was found in the absence of haplotypic repeats. Such variant clusters are hardly explained by interchromosomal, fixation-driving mechanisms and likely reflect a fast, localized, intrachromosomal sequence conversion mechanism.

[Supplemental material is available online at www.genome.org and www.pedgen.med.uni-muenchen.de. The sequence data from this study have been submitted to DDBJ, EMBL, and GenBank under accession nos. AJ509815-AJ509823, AJ509829-AJ509852, AJ509874-AJ510031. The following individuals kindly provided reagents, samples, or unpublished information as indicated in the paper: P. Warburton, and C. Roos.]

4 Corresponding author.

12:1815-1826 ©2002 by Cold Spring Harbor Laboratory Press  ISSN 1088-9051/02 $5.00
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