Nucleotide Variation at Msn and Alas2, Two Genes Flanking the Centromere of the X Chromosome in Humans

doi:10.1534/genetics.167.1.423

Nucleotide Variation at Msn and Alas2, Two Genes Flanking the Centromere of the X Chromosome in Humans

Michael W. Nachman^a, Susan L. D'Agostino^a, Christopher R. Tillquist^b, Zahra Mobasher^b, and Michael F. Hammer^a,b
^a Department of Ecology and Evolutionary Biology, Division of Biotechnology, University of Arizona, Tucson, Arizona 85721
^b Genomic Analysis and Technology Core, Division of Biotechnology, University of Arizona, Tucson, Arizona 85721

Corresponding author: Michael W. Nachman, Biosciences West Bldg., University of Arizona, Tucson, AZ 85721., nachman{at}u.arizona.edu (E-mail)

Communicating editor: M. A. F. NOOR

The centromeric region of the X chromosome in humans experienceslow rates of recombination over a considerable physical distance.In such a region, the effects of selection may extend to linkedsites that are far away. To investigate the effects of thisrecombinational environment on patterns of nucleotide variability,we sequenced 4581 bp at Msn and 4697 bp at Alas2, two genessituated on either side of the X chromosome centromere, in aworldwide sample of 41 men, as well as in one common chimpanzeeand one orangutan. To investigate patterns of linkage disequilibrium(LD) across the centromere, we also genotyped several informativesites from each gene in 120 men from sub-Saharan Africa. Bystudying X-linked loci in males, we were able to recover haplotypesand study long-range patterns of LD directly. Overall patternsof variability were remarkably similar at these two loci. Bothloci exhibited (i) very low levels of nucleotide diversity (amongthe lowest seen in the human genome); (ii) a strong skew inthe distribution of allele frequencies, with an excess of bothvery-low and very-high-frequency derived alleles in non-Africanpopulations; (iii) much less variation in the non-African thanin the African samples; (iv) very high levels of populationdifferentiation; and (v) complete LD among all sites withinloci. We also observed significant LD between Msn and Alas2in Africa, despite the fact that they are separated by $~$ 10 Mb.These observations are difficult to reconcile with a simpledemographic model but may be consistent with positive and/orpurifying selection acting on loci within this large regionof low recombination.

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