@article{10.1371/journal.pgen.1003984, doi = {10.1371/journal.pgen.1003984}, author = {Auton, Adam AND Rui Li, Ying AND Kidd, Jeffrey AND Oliveira, Kyle AND Nadel, Julie AND Holloway, J. Kim AND Hayward, Jessica J. AND Cohen, Paula E. AND Greally, John M. AND Wang, Jun AND Bustamante, Carlos D. AND Boyko, Adam R.}, journal = {PLOS Genetics}, publisher = {Public Library of Science}, title = {Genetic Recombination Is Targeted towards Gene Promoter Regions in Dogs}, year = {2013}, month = {12}, volume = {9}, url = {https://doi.org/10.1371/journal.pgen.1003984}, pages = {1-9}, abstract = {The identification of the H3K4 trimethylase, PRDM9, as the gene responsible for recombination hotspot localization has provided considerable insight into the mechanisms by which recombination is initiated in mammals. However, uniquely amongst mammals, canids appear to lack a functional version of PRDM9 and may therefore provide a model for understanding recombination that occurs in the absence of PRDM9, and thus how PRDM9 functions to shape the recombination landscape. We have constructed a fine-scale genetic map from patterns of linkage disequilibrium assessed using high-throughput sequence data from 51 free-ranging dogs, Canis lupus familiaris. While broad-scale properties of recombination appear similar to other mammalian species, our fine-scale estimates indicate that canine highly elevated recombination rates are observed in the vicinity of CpG rich regions including gene promoter regions, but show little association with H3K4 trimethylation marks identified in spermatocytes. By comparison to genomic data from the Andean fox, Lycalopex culpaeus, we show that biased gene conversion is a plausible mechanism by which the high CpG content of the dog genome could have occurred.}, number = {12}, }