The Evolution and Functional Impact of Human Deletion Variants Shared with Archaic Hominin Genomes

Lin, Yen-Lung; Pavlidis, Pavlos; Karakoç, Emre; Ajay, Jerry; Gökçümen, Ömer

doi:10.1093/molbev/msu405

Cited by 49 publications

(55 citation statements)

References 45 publications

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“…One study has highlighted DMBT1 to be a strong candidate for ancient balancing selection in the genome (49). Another recent study has identified the region upstream of DMBT1 to show unusually negative Tajima's D (in the fifth percentile genome wide) in Europeans, supporting our model of selection (50). However, the effect on SNP diversity of a rapidly mutating CNV undergoing fluctuating geographically structured selection remains unclear.…”

Section: Discussionmentioning

confidence: 52%

Evolution of the rapidly mutating human salivary agglutinin gene ( DMBT1 ) and population subsistence strategy

Polley

Louzada

Forni

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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The dietary change resulting from the domestication of plant and animal species and development of agriculture at different locations across the world was one of the most significant changes in human evolution. An increase in dietary carbohydrates caused an increase in dental caries following the development of agriculture, mediated by the cariogenic oral bacterium Streptococcus mutans. Salivary agglutinin [SAG, encoded by the deleted in malignant brain tumors 1 (DMBT1) gene] is an innate immune receptor glycoprotein that binds a variety of bacteria and viruses, and mediates attachment of S. mutans to hydroxyapatite on the surface of the tooth. In this study we show that multiallelic copy number variation (CNV) within DMBT1 is extensive across all populations and is predicted to result in between 7-20 scavenger-receptor cysteinerich (SRCR) domains within each SAG molecule. Direct observation of de novo mutation in multigeneration families suggests these CNVs have a very high mutation rate for a protein-coding locus, with a mutation rate of up to 5% per gamete. Given that the SRCR domains bind S. mutans and hydroxyapatite in the tooth, we investigated the association of sequence diversity at the SAG-binding gene of S. mutans, and DMBT1 CNV. Furthermore, we show that DMBT1 CNV is also associated with a history of agriculture across global populations, suggesting that dietary change as a result of agriculture has shaped the pattern of CNV at DMBT1, and that the DMBT1-S. mutans interaction is a promising model of host-pathogenculture coevolution in humans.copy number variation | agriculture | DMBT1 | mutation | structural variation

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Section: Discussionmentioning

confidence: 52%

Evolution of the rapidly mutating human salivary agglutinin gene ( DMBT1 ) and population subsistence strategy

Polley

Louzada

Forni

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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“…This ~32kb deletion variant overlaps 2 genes, LCE3B and LCE3C , which are both involved in skin tissue repair. We recently showed that this deletion variant is derived in the Homo lineage and that the deletion is present in the Denisovan genome, but absent in the Neanderthal genome [13]. In the same study, we were able to rule out archaic introgression and concluded that incomplete lineage sorting best explains the observed allele sharing at this locus.…”

Section: Introductionmentioning

confidence: 72%

“…The green boxes represent π and Tajima’s D scores calculated for the size-matched downstream regions of non-exonic ancient deletions. These deletions are comparable to the LCE3BC deletion in the sense that they were also found to have evolved before Human Neanderthal/Denisovan divergence and that they are similarly high in allele frequency [58]. P -values (Wilcoxon Test) are shown on top of the comparisons …”

Section: Resultsmentioning

confidence: 99%

“…In a recent study, we searched for unusually old deletion variants that affect coding sequences. Specifically, we identified exonic deletions that evolved before Human-Neanderthal divergence (>500-1,000KYA) [13]. We surmised that it is unlikely for a loss-of-function gene deletion to be maintained for this long, especially under negative selection.…”

Section: Introductionmentioning

confidence: 99%

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The psoriasis-associated deletion of late cornified envelope genes LCE3B and LCE3C has been maintained under balancing selection since Human Denisovan divergence

Pajic

Lin

et al. 2016

BMC Evol Biol

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BackgroundA common, 32kb deletion of LCE3B and LCE3C genes is strongly associated with psoriasis. We recently found that this deletion is ancient, predating Human-Denisovan divergence. However, it was not clear why negative selection has not removed this deletion from the population.ResultsHere, we show that the haplotype block that harbors the deletion (i) retains high allele frequency among extant and ancient human populations; (ii) harbors unusually high nucleotide variation (π, P < 4.1 × 10−3); (iii) contains an excess of intermediate frequency variants (Tajima’s D, P < 3.9 × 10−3); and (iv) has an unusually long time to coalescence to the most recent common ancestor (TSel, 0.1 quantile).ConclusionsOur results are most parsimonious with the scenario where the LCE3BC deletion has evolved under balancing selection in humans. More broadly, this is consistent with the hypothesis that a balance between autoimmunity and natural vaccination through increased exposure to pathogens maintains this deletion in humans.Electronic supplementary materialThe online version of this article (doi:10.1186/s12862-016-0842-6) contains supplementary material, which is available to authorized users.

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“…a higher rate of genetic drift [5]. This suggests that weakly deleterious exonic alleles may have been effectively neutral and drifted up in frequency in Neanderthals [28–30], only to be slowly selected against after introgressing into modern human populations of larger effective size. To test this hypothesis, we simulated a simple model of a population split between AMH and Neanderthals, using a range of plausible Neanderthal population sizes after the split.…”

Section: Resultsmentioning

confidence: 99%

The Strength of Selection against Neanderthal Introgression

2016

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Hybridization between humans and Neanderthals has resulted in a low level of Neanderthal ancestry scattered across the genomes of many modern-day humans. After hybridization, on average, selection appears to have removed Neanderthal alleles from the human population. Quantifying the strength and causes of this selection against Neanderthal ancestry is key to understanding our relationship to Neanderthals and, more broadly, how populations remain distinct after secondary contact. Here, we develop a novel method for estimating the genome-wide average strength of selection and the density of selected sites using estimates of Neanderthal allele frequency along the genomes of modern-day humans. We confirm that East Asians had somewhat higher initial levels of Neanderthal ancestry than Europeans even after accounting for selection. We find that the bulk of purifying selection against Neanderthal ancestry is best understood as acting on many weakly deleterious alleles. We propose that the majority of these alleles were effectively neutral—and segregating at high frequency—in Neanderthals, but became selected against after entering human populations of much larger effective size. While individually of small effect, these alleles potentially imposed a heavy genetic load on the early-generation human–Neanderthal hybrids. This work suggests that differences in effective population size may play a far more important role in shaping levels of introgression than previously thought.

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The Evolution and Functional Impact of Human Deletion Variants Shared with Archaic Hominin Genomes

Cited by 49 publications

References 45 publications

Evolution of the rapidly mutating human salivary agglutinin gene ( DMBT1 ) and population subsistence strategy

Evolution of the rapidly mutating human salivary agglutinin gene ( DMBT1 ) and population subsistence strategy

The psoriasis-associated deletion of late cornified envelope genes LCE3B and LCE3C has been maintained under balancing selection since Human Denisovan divergence

The Strength of Selection against Neanderthal Introgression

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