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Abstract
For most of the world, human genome structure at a population level is shaped by interplay between ancient geographic isolation and more recent demographic shifts, factors that are captured by the concepts of biogeographic ancestry and admixture, respectively. The ancestry of non-admixed individuals can often be traced to a specific population in a precise region, but current approaches for studying admixed individuals generally yield coarse information in which genome ancestry proportions are identified according to continent of origin. Here we introduce a new analytic strategy for this problem that allows fine-grained characterization of admixed individuals with respect to both geographic and genomic coordinates. Ancestry segments from different continents, identified with a probabilistic model, are used to construct and study “virtual genomes” of admixed individuals. We apply this approach to a cohort of 492 parent–offspring trios from Mexico City. The relative contributions from the three continental-level ancestral populations—Africa, Europe, and America—vary substantially between individuals, and the distribution of haplotype block length suggests an admixing time of 10–15 generations. The European and Indigenous American virtual genomes of each Mexican individual can be traced to precise regions within each continent, and they reveal a gradient of Amerindian ancestry between indigenous people of southwestern Mexico and Mayans of the Yucatan Peninsula. This contrasts sharply with the African roots of African Americans, which have been characterized by a uniform mixing of multiple West African populations. We also use the virtual European and Indigenous American genomes to search for the signatures of selection in the ancestral populations, and we identify previously known targets of selection in other populations, as well as new candidate loci. The ability to infer precise ancestral components of admixed genomes will facilitate studies of disease-related phenotypes and will allow new insight into the adaptive and demographic history of indigenous people.
Highlights
During the past decade, data generated by high-throughput genotyping technologies have enabled studies probing into two central questions in human evolutionary biology: the characterization of human population genetic structure, and the search for the molecular signature of natural selection
Detailed knowledge about the ancestral origin of an admixed population provides insight regarding the history of the population itself, and affords opportunities to study the evolutionary biology of the ancestral populations
We analyzed the high-density genotype data of nearly 1,500 Mexican individuals from Mexico City, who are admixed among Indigenous Americans, Europeans, and Africans
Summary
Data generated by high-throughput genotyping technologies have enabled studies probing into two central questions in human evolutionary biology: the characterization of human population genetic structure, and the search for the molecular signature of natural selection. Insights gleaned from these studies have provided important clues for understanding the phenotypic diversity of our species, and variables representing population structure are routinely incorporated as covariates in genome-wide association studies of complex traits and diseases. Using data from the Human Genome DiversityCEPH Panel (HGDP), a recent and comprehensive survey suggests that, while adaptation to local environment is a common theme throughout human evolution, the genetic loci involved in adaptation show little overlap among non-contiguous geographic regions [9].
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