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The Y-chromosome tree bursts into leaf: 13,000 high-confidence SNPs covering the majority of known clades.

journal contribution
posted on 2015-11-30, 10:46 authored by Pille Hallast, Chiara Batini, Daniel Zadik, Pierpaolo Maisano Maisano Delser, Jon H. Wetton, E. Arroyo-Pardo, GL. Cavalleri, P. de Knijff, G. Destro Bisol, B. M. Dupuy, H. A. Eriksen, L. B. Jorde, Turi E. King, M. H. Larmuseau, A. López de Munain, A. M. López-Parra, A. Loutradis, J. Milasin, A. Novelletto, H. Pamjav, A. Sajantila, W. Schempp, Matt Sears, A. Tolun, C. Tyler-Smith, A. Van Geystelen, S. Watkins, B. Winney, Mark A. Jobling
Many studies of human populations have used the male-specific region of the Y chromosome (MSY) as a marker, but MSY sequence variants have traditionally been subject to ascertainment bias. Also, dating of haplogroups has relied on Y-specific short tandem repeats (STRs), involving problems of mutation rate choice, and possible long-term mutation saturation. Next-generation sequencing can ascertain single nucleotide polymorphisms (SNPs) in an unbiased way, leading to phylogenies in which branch-lengths are proportional to time, and allowing the times-to-most-recent-common-ancestor (TMRCAs) of nodes to be estimated directly. Here we describe the sequencing of 3.7 Mb of MSY in each of 448 human males at a mean coverage of 51×, yielding 13,261 high-confidence SNPs, 65.9% of which are previously unreported. The resulting phylogeny covers the majority of the known clades, provides date estimates of nodes, and constitutes a robust evolutionary framework for analyzing the history of other classes of mutation. Different clades within the tree show subtle but significant differences in branch lengths to the root. We also apply a set of 23 Y-STRs to the same samples, allowing SNP- and STR-based diversity and TMRCA estimates to be systematically compared. Ongoing purifying selection is suggested by our analysis of the phylogenetic distribution of nonsynonymous variants in 15 MSY single-copy genes.

History

Citation

Molecular Biology and Evolution, 2015, 32 (3), pp. 661-673

Author affiliation

/Organisation/COLLEGE OF MEDICINE, BIOLOGICAL SCIENCES AND PSYCHOLOGY/MBSP Non-Medical Departments/Department of Genetics

Version

  • VoR (Version of Record)

Published in

Molecular Biology and Evolution

Publisher

Oxford University Press (OUP)

issn

0737-4038

eissn

1537-1719

Copyright date

2014

Available date

2015-11-30

Publisher version

http://mbe.oxfordjournals.org/content/32/3/661

Language

en

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