Novel Y Chromosome Retrocopies in Canids Revealed through a Genome-Wide Association Study for Sex

Tsai, Kate L.; Evans, Judith; Noorai, Rooksana E.; Starr-Moss, Alison N.; Clark, Leigh Anne

doi:10.3390/genes10040320

Cited by 22 publications

(30 citation statements)

References 43 publications

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“…The availability of a complete genome assembly including both sex chromosomes, and the rigorous elimination of sequences aligning to any of them, may potentially allow detecting genome-wide signatures of SAS based on intersex differentiation data alone (Lucotte et al, 2016), although the reliability of such approaches awaits validation. We also note that if the transfer of autosomal sequences to the Y chromosome includes genes that retain expression in the new location (Mahajan & Bachtrog, 2017;Tsai et al, 2019), autosomal genes may appear to show concurrent intersex differences in both allele frequency and gene expression levels when ignoring copies on a missing sex chromosome.…”

Section: Hidr Snpsmentioning

confidence: 87%

“…DNA segments closely related between autosomes and the Y chromosome may thus cause the alignment of Y-specific alleles to autosomes, thus potentially producing SNPs showing high intersex differentiation. This scenario leads to two testable predictions (see also Dou et al, 2012;McKinney, Waples, Seeb, & Seeb, 2017;Tsai, Evans, Noorai, Starr-Moss, & Clark, 2019).…”

Section: Testing If High Intersex Differentiation Is Driven By the mentioning

confidence: 98%

“…This scenario leads to two testable predictions (see also Dou et al, 2012;McKinney, Waples, Seeb, & Seeb, 2017;Tsai, Evans, Noorai, Starr-Moss, & Clark, 2019). We here considered that both the reference genome and the new de novo genome are derived from a female (XX) individual.…”

Section: Testing If High Intersex Differentiation Is Driven By the mentioning

confidence: 99%

“…Having ruled out reference genome misassembly as an explanation for strong autosomal differentiation between the sexes, we addressed a second hypothesis focused on reference genome incompleteness: that DNA segments similar to autosomal chromosome regions occur on the Y chromosome that is not part of any current genome assembly, and that these segments harbour private genetic variants that cause intersex differentiation when aligning to their autosomal counterparts (see also Tsai et al, 2019). Consistent with this idea, we observed that SNPs located within HIDRs showed a systematically reduced MAF in the female relative to the male pool ( Figure 2b).…”

Section: High Intersex Autosomal Differentiation Arises From Dna Sementioning

confidence: 99%

“…This leads us to propose a model in which an autosomal DNA segment is first copied to the Y chromosome (see also Koerich, Wang, Clark, & Carvalho, 2008;Tsai et al, 2019), experiences mutation at the new location, and then, to variable extent, experiences further copy number expansion on the Y chromosome ( Figure 5). Consistent with this model, the male-female read depth ratios of the HIDR SNPs tended to form distinct clusters overlapping with 1.5, 2, and 2.5 (Figure 4) …”

Section: High Intersex Autosomal Differentiation Arises From Dna Sementioning

confidence: 99%

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Widespread intersex differentiation across the stickleback genome – The signature of sexually antagonistic selection?

et al. 2019

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Females and males within a species commonly have distinct reproductive roles, and the associated traits may be under perpetual divergent natural selection between the sexes if their sex‐specific control has not yet evolved. Here, we explore whether such sexually antagonistic selection can be detected based on the magnitude of differentiation between the sexes across genome‐wide genetic polymorphisms by whole‐genome sequencing of large pools of female and male threespine stickleback fish. We find numerous autosomal genome regions exhibiting intersex allele frequency differences beyond the range plausible under pure sampling stochasticity. Alternative sequence alignment strategies rule out that these high‐differentiation regions represent sex chromosome segments misassembled into the autosomes. Instead, comparing allele frequencies and sequence read depth between the sexes reveals that regions of high intersex differentiation arise because autosomal chromosome segments got copied into the male‐specific sex chromosome (Y), where they acquired new mutations. Because the Y chromosome is missing in the stickleback reference genome, sequence reads derived from DNA copies on the Y chromosome still align to the original homologous regions on the autosomes. We argue that this phenomenon hampers the identification of sexually antagonistic selection within a genome, and can lead to spurious conclusions from population genomic analyses when the underlying samples differ in sex ratios. Because the hemizygous sex chromosome sequence (Y or W) is not represented in most reference genomes, these problems may apply broadly.

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Section: Hidr Snpsmentioning

confidence: 87%

Section: Testing If High Intersex Differentiation Is Driven By the mentioning

confidence: 98%

Section: Testing If High Intersex Differentiation Is Driven By the mentioning

confidence: 99%

Section: High Intersex Autosomal Differentiation Arises From Dna Sementioning

confidence: 99%

Section: High Intersex Autosomal Differentiation Arises From Dna Sementioning

confidence: 99%

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Widespread intersex differentiation across the stickleback genome – The signature of sexually antagonistic selection?

et al. 2019

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The search for sexually antagonistic genes: Practical insights from studies of local adaptation and statistical genomics

et al. 2020

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Sexually antagonistic (SA) genetic variation-in which alleles favored in one sex are disfavored in the other-is predicted to be common and has been documented in several animal and plant populations, yet we currently know little about its pervasiveness among species or its population genetic basis. Recent applications of genomics in studies of SA genetic variation have highlighted considerable methodological challenges to the identification and characterization of SA genes, raising questions about the feasibility of genomic approaches for inferring SA selection. The related fields of local adaptation and statistical genomics have previously dealt with similar challenges, and lessons from these disciplines can therefore help overcome current difficulties in applying genomics to study SA genetic variation. Here, we integrate theoretical and analytical concepts from local adaptation and statistical genomics research-including F ST and F IS statistics, genome-wide association studies, pedigree analyses, reciprocal transplant studies, and evolve-and-resequence experiments-to evaluate methods for identifying SA genes and genome-wide signals of SA genetic variation. We begin by developing theoretical models for between-sex F ST and F IS , including explicit null distributions for each statistic, and using them to critically evaluate putative multilocus signals of sex-specific selection in previously published datasets. We then highlight new statistics that address some of the limitations of F ST and F IS , along with applications of more direct approaches for characterizing SA genetic variation, which incorporate explicit fitness measurements. We finish by presenting practical guidelines for the validation and evolutionary analysis of candidate SA genes and discussing promising empirical systems for future work.

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A new method to identify fetal sex and trisomy 21 from the amniocentesis of pregnant women

Xiang

Wan²,

Liu

et al. 2019

Human Cell

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Novel Y Chromosome Retrocopies in Canids Revealed through a Genome-Wide Association Study for Sex

Cited by 22 publications

References 43 publications

Widespread intersex differentiation across the stickleback genome – The signature of sexually antagonistic selection?

Widespread intersex differentiation across the stickleback genome – The signature of sexually antagonistic selection?

The search for sexually antagonistic genes: Practical insights from studies of local adaptation and statistical genomics

A new method to identify fetal sex and trisomy 21 from the amniocentesis of pregnant women

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