3D facial phenotyping by biometric sibling matching used in contemporary genomic methodologies

The analysis of contemporary genomic data typically operates on one-dimensional phenotypic measurements (e.g. standing height). Here we report on a data-driven, family-informed strategy to facial phenotyping that searches for biologically relevant traits and reduces multivariate 3D facial shape variability into amendable univariate measurements, while preserving its structurally complex nature. We performed a biometric identification of siblings in a sample of 424 children, defining 1,048 sib-shared facial traits. Subsequent quantification and analyses in an independent European cohort (n = 8,246) demonstrated significant heritability for a subset of traits (0.17–0.53) and highlighted 218 genome-wide significant loci (38 also study-wide) associated with facial variation shared by siblings. These loci showed preferential enrichment for active chromatin marks in cranial neural crest cells and embryonic craniofacial tissues and several regions harbor putative craniofacial genes, thereby enhancing our knowledge on the genetic architecture of normal-range facial variation.

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Insights into the genetic architecture of the human face

10.1101/2020.05.12.090555 ◽

2020 ◽

Cited By ~ 2

Author(s):

Julie D. White ◽

Karlijne Indencleef ◽

Sahin Naqvi ◽

Ryan J. Eller ◽

Jasmien Roosenboom ◽

...

Keyword(s):

Genetic Variants ◽

Genetic Architecture ◽

Cell Types ◽

Human Face ◽

Normal Range ◽

Enhancer Activity ◽

Limb Morphogenesis ◽

Cranial Neural Crest Cells ◽

Genomic Regions

AbstractThe human face is complex and multipartite, and characterization of its genetic architecture remains intriguingly challenging. Applying GWAS to multivariate shape phenotypes, we identified 203 genomic regions associated with normal-range facial variation, 117 of which are novel. The associated regions are enriched for both genes relevant to craniofacial and limb morphogenesis and enhancer activity in cranial neural crest cells and craniofacial tissues. Genetic variants grouped by their contribution to similar aspects of facial variation show high within-group correlation of enhancer activity, and four SNP pairs display evidence of epistasis, indicating potentially coordinated actions of variants within the same cell types or tissues. In sum, our analyses provide new insights for understanding how complex morphological traits are shaped by both individual and coordinated genetic actions.

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Genetics of OCD

10.1093/med/9780190228163.003.0019 ◽

2017 ◽

Author(s):

Paul Arnold

Keyword(s):

Genetic Architecture ◽

Individual Treatment ◽

Clear Understanding ◽

Obsessive Compulsive ◽

Compulsive Disorder ◽

Glutamate Signaling ◽

Gene Environment ◽

Genome Wide ◽

Significant Heritability ◽

Candidate Gene Studies

Obsessive-compulsive disorder (OCD) often runs in families and has been shown to have significant heritability. It is genetically complex, and two decades of genetic work have not converged on a clear understanding of genetic risk factors. However, accelerating progress in recent years has begun to generate some insights into the genetic architecture of the disorder, and greater clarity is likely to emerge in the coming decade. This chapter summarizes several lines of genetic work, including genome-wide genetic and linkage studies; candidate gene studies; and investigations of gene-environment interactions and of pharmacogenetics. One developing theme is that genetic variance in components of the brain’s glutamate signaling system may contribute to the development of OCD. Advancing understanding of the genetics of OCD may lead to new insights into pathobiology and to new tools to optimize individual treatment.

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A meta-analysis of genome-wide association studies for average daily gain and lean meat percentage in two Duroc pig populations

BMC Genomics ◽

10.1186/s12864-020-07288-1 ◽

2021 ◽

Vol 22 (1) ◽

Author(s):

Shenping Zhou ◽

Rongrong Ding ◽

Fanming Meng ◽

Xingwang Wang ◽

Zhanwei Zhuang ◽

...

Keyword(s):

Candidate Genes ◽

Growth And Development ◽

Genetic Architecture ◽

Association Studies ◽

Meta Analysis ◽

Average Daily Gain ◽

Genome Wide Association ◽

Genome Wide Association Studies ◽

Genome Wide ◽

Daily Gain

Abstract Background Average daily gain (ADG) and lean meat percentage (LMP) are the main production performance indicators of pigs. Nevertheless, the genetic architecture of ADG and LMP is still elusive. Here, we conducted genome-wide association studies (GWAS) and meta-analysis for ADG and LMP in 3770 American and 2090 Canadian Duroc pigs. Results In the American Duroc pigs, one novel pleiotropic quantitative trait locus (QTL) on Sus scrofa chromosome 1 (SSC1) was identified to be associated with ADG and LMP, which spans 2.53 Mb (from 159.66 to 162.19 Mb). In the Canadian Duroc pigs, two novel QTLs on SSC1 were detected for LMP, which were situated in 3.86 Mb (from 157.99 to 161.85 Mb) and 555 kb (from 37.63 to 38.19 Mb) regions. The meta-analysis identified ten and 20 additional SNPs for ADG and LMP, respectively. Finally, four genes (PHLPP1, STC1, DYRK1B, and PIK3C2A) were detected to be associated with ADG and/or LMP. Further bioinformatics analysis showed that the candidate genes for ADG are mainly involved in bone growth and development, whereas the candidate genes for LMP mainly participated in adipose tissue and muscle tissue growth and development. Conclusions We performed GWAS and meta-analysis for ADG and LMP based on a large sample size consisting of two Duroc pig populations. One pleiotropic QTL that shared a 2.19 Mb haplotype block from 159.66 to 161.85 Mb on SSC1 was found to affect ADG and LMP in the two Duroc pig populations. Furthermore, the combination of single-population and meta-analysis of GWAS improved the efficiency of detecting additional SNPs for the analyzed traits. Our results provide new insights into the genetic architecture of ADG and LMP traits in pigs. Moreover, some significant SNPs associated with ADG and/or LMP in this study may be useful for marker-assisted selection in pig breeding.

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Genetic architecture underlying the expression of eight α-amylase trypsin inhibitors

Theoretical and Applied Genetics ◽

10.1007/s00122-021-03906-y ◽

2021 ◽

Author(s):

Khaoula EL Hassouni ◽

Malte Sielaff ◽

Valentina Curella ◽

Manjusha Neerukonda ◽

Willmar Leiser ◽

...

Keyword(s):

Genetic Architecture ◽

Intestinal Inflammation ◽

Wheat Breeding ◽

Trypsin Inhibitors ◽

Potential Candidate ◽

Lipid Transfer ◽

Wheat Cultivars ◽

Genome Wide ◽

Close Physical Proximity ◽

Major Qtl

Abstract Key message Wheat cultivars largely differ in the content and composition of ATI proteins, but heritability was quite low for six out of eight ATIs. The genetic architecture of ATI proteins is built up of few major and numerous small effect QTL. Abstract Amylase trypsin inhibitors (ATIs) are important allergens in baker’s asthma and suspected triggers of non-celiac wheat sensitivity (NCWS) inducing intestinal and extra-intestinal inflammation. As studies on the expression and genetic architecture of ATI proteins in wheat are lacking, we evaluated 149 European old and modern bread wheat cultivars grown at three different field locations for their content of eight ATI proteins. Large differences in the content and composition of ATIs in the different cultivars were identified ranging from 3.76 pmol for ATI CM2 to 80.4 pmol for ATI 0.19, with up to 2.5-fold variation in CM-type and up to sixfold variation in mono/dimeric ATIs. Generally, heritability estimates were low except for ATI 0.28 and ATI CM2. ATI protein content showed a low correlation with quality traits commonly analyzed in wheat breeding. Similarly, no trends were found regarding ATI content in wheat cultivars originating from numerous countries and decades of breeding history. Genome-wide association mapping revealed a complex genetic architecture built of many small, few medium and two major quantitative trait loci (QTL). The major QTL were located on chromosomes 3B for ATI 0.19-like and 6B for ATI 0.28, explaining 70.6 and 68.7% of the genotypic variance, respectively. Within close physical proximity to the medium and major QTL, we identified eight potential candidate genes on the wheat reference genome encoding structurally related lipid transfer proteins. Consequently, selection and breeding of wheat cultivars with low ATI protein amounts appear difficult requiring other strategies to reduce ATI content in wheat products.

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Genetics of complex traits: prediction of phenotype, identification of causal polymorphisms and genetic architecture

Proceedings of The Royal Society B Biological Sciences ◽

10.1098/rspb.2016.0569 ◽

2016 ◽

Vol 283 (1835) ◽

pp. 20160569 ◽

Cited By ~ 52

Author(s):

M. E. Goddard ◽

K. E. Kemper ◽

I. M. MacLeod ◽

A. J. Chamberlain ◽

B. J. Hayes

Keyword(s):

Complex Traits ◽

Genetic Architecture ◽

Quantitative Traits ◽

Association Studies ◽

Genome Wide Association Studies ◽

Nucleotide Polymorphisms ◽

Crop Breeding ◽

Single Nucleotide ◽

Genome Wide ◽

Phenotype Identification

Complex or quantitative traits are important in medicine, agriculture and evolution, yet, until recently, few of the polymorphisms that cause variation in these traits were known. Genome-wide association studies (GWAS), based on the ability to assay thousands of single nucleotide polymorphisms (SNPs), have revolutionized our understanding of the genetics of complex traits. We advocate the analysis of GWAS data by a statistical method that fits all SNP effects simultaneously, assuming that these effects are drawn from a prior distribution. We illustrate how this method can be used to predict future phenotypes, to map and identify the causal mutations, and to study the genetic architecture of complex traits. The genetic architecture of complex traits is even more complex than previously thought: in almost every trait studied there are thousands of polymorphisms that explain genetic variation. Methods of predicting future phenotypes, collectively known as genomic selection or genomic prediction, have been widely adopted in livestock and crop breeding, leading to increased rates of genetic improvement.

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A combination of genome-wide association study and selection signature analysis dissects the genetic architecture underlying bone traits in chickens

animal ◽

10.1016/j.animal.2021.100322 ◽

2021 ◽

Vol 15 (8) ◽

pp. 100322

Author(s):

Y.D. Li ◽

X. Liu ◽

Z.W. Li ◽

W.J. Wang ◽

Y.M. Li ◽

...

Keyword(s):

Association Study ◽

Genetic Architecture ◽

Genome Wide Association Study ◽

Genome Wide Association ◽

Signature Analysis ◽

Selection Signature ◽

Genome Wide

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Genetic architecture of common bunt resistance in winter wheat using genome-wide association study

BMC Plant Biology ◽

10.1186/s12870-018-1435-x ◽

2018 ◽

Vol 18 (1) ◽

Cited By ~ 10

Author(s):

Amira M. I. Mourad ◽

Ahmed Sallam ◽

Vikas Belamkar ◽

Ezzat Mahdy ◽

Bahy Bakheit ◽

...

Keyword(s):

Winter Wheat ◽

Association Study ◽

Genetic Architecture ◽

Genome Wide Association Study ◽

Genome Wide Association ◽

Common Bunt ◽

Genome Wide ◽

Bunt Resistance

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Faculty Opinions recommendation of Genome-wide association analyses identify 44 risk variants and refine the genetic architecture of major depression.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.733105041.793567849 ◽

2019 ◽

Author(s):

Benjamin Neale

Keyword(s):

Major Depression ◽

Genetic Architecture ◽

Genome Wide Association ◽

Association Analyses ◽

Risk Variants ◽

Genome Wide

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Better estimation of SNP heritability from summary statistics provides a new understanding of the genetic architecture of complex traits

10.1101/284976 ◽

2018 ◽

Cited By ~ 6

Author(s):

Doug Speed ◽

David J Balding

Keyword(s):

Complex Traits ◽

Genetic Architecture ◽

Large Scale ◽

Association Studies ◽

Genome Wide Association Studies ◽

Summary Statistics ◽

Confounding Bias ◽

Conserved Regions ◽

Genome Wide ◽

Variation Explained

LD Score Regression (LDSC) has been widely applied to the results of genome-wide association studies. However, its estimates of SNP heritability are derived from an unrealistic model in which each SNP is expected to contribute equal heritability. As a consequence, LDSC tends to over-estimate confounding bias, under-estimate the total phenotypic variation explained by SNPs, and provide misleading estimates of the heritability enrichment of SNP categories. Therefore, we present SumHer, software for estimating SNP heritability from summary statistics using more realistic heritability models. After demonstrating its superiority over LDSC, we apply SumHer to the results of 24 large-scale association studies (average sample size 121 000). First we show that these studies have tended to substantially over-correct for confounding, and as a result the number of genome-wide significant loci has under-reported by about 20%. Next we estimate enrichment for 24 categories of SNPs defined by functional annotations. A previous study using LDSC reported that conserved regions were 13-fold enriched, and found a further twelve categories with above 2-fold enrichment. By contrast, our analysis using SumHer finds that conserved regions are only 1.6-fold (SD 0.06) enriched, and that no category has enrichment above 1.7-fold. SumHer provides an improved understanding of the genetic architecture of complex traits, which enables more efficient analysis of future genetic data.

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