Genetic architecture reconciles linkage and association studies of complex traits

Estonian Biobank Research Team; LifeLines Cohort Study

doi:10.1038/s41588-024-01940-2

Genetic architecture reconciles linkage and association studies of complex traits

Estonian Biobank Research Team, LifeLines Cohort Study

Research output: Contribution to journal › Article › peer-review

Abstract

Linkage studies have successfully mapped loci underlying monogenic disorders, but mostly failed when applied to common diseases. Conversely, genome-wide association studies (GWASs) have identified replicable associations between thousands of SNPs and complex traits, yet capture less than half of the total heritability. In the present study we reconcile these two approaches by showing that linkage signals of height and body mass index (BMI) from 119,000 sibling pairs colocalize with GWAS-identified loci. Concordant with polygenicity, we observed the following: a genome-wide inflation of linkage test statistics; that GWAS results predict linkage signals; and that adjusting phenotypes for polygenic scores reduces linkage signals. Finally, we developed a method using recombination rate-stratified, identity-by-descent sharing between siblings to unbiasedly estimate heritability of height (0.76 ± 0.05) and BMI (0.55 ± 0.07). Our results imply that substantial heritability remains unaccounted for by GWAS-identified loci and this residual genetic variation is polygenic and enriched near these loci.

Original language	English (US)
Pages (from-to)	2352-2360
Number of pages	9
Journal	Nature Genetics
Volume	56
Issue number	11
DOIs	https://doi.org/10.1038/s41588-024-01940-2
State	Published - Nov 2024

ASJC Scopus subject areas

Genetics

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10.1038/s41588-024-01940-2

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@article{8f4103bd456c425f82e97eb569611bec,

title = "Genetic architecture reconciles linkage and association studies of complex traits",

abstract = "Linkage studies have successfully mapped loci underlying monogenic disorders, but mostly failed when applied to common diseases. Conversely, genome-wide association studies (GWASs) have identified replicable associations between thousands of SNPs and complex traits, yet capture less than half of the total heritability. In the present study we reconcile these two approaches by showing that linkage signals of height and body mass index (BMI) from 119,000 sibling pairs colocalize with GWAS-identified loci. Concordant with polygenicity, we observed the following: a genome-wide inflation of linkage test statistics; that GWAS results predict linkage signals; and that adjusting phenotypes for polygenic scores reduces linkage signals. Finally, we developed a method using recombination rate-stratified, identity-by-descent sharing between siblings to unbiasedly estimate heritability of height (0.76 ± 0.05) and BMI (0.55 ± 0.07). Our results imply that substantial heritability remains unaccounted for by GWAS-identified loci and this residual genetic variation is polygenic and enriched near these loci.",

author = "{Estonian Biobank Research Team} and {LifeLines Cohort Study} and Julia Sidorenko and Baptiste Couvy-Duchesne and Kemper, {Kathryn E.} and Moen, {Gunn Helen} and Laxmi Bhatta and {\AA}svold, {Bj{\o}rn Olav} and Reedik M{\"a}gi and Alireza Ani and Rujia Wang and Nolte, {Ilja M.} and Nolte, {Ilja M.} and Scott Gordon and Caroline Hayward and Archie Campbell and Benjamin, {Daniel J.} and David Cesarini and Evans, {David M.} and Goddard, {Michael E.} and Haley, {Chris S.} and David Porteous and Medland, {Sarah E.} and Martin, {Nicholas G.} and Harold Snieder and Andres Metspalu and Kristian Hveem and Ben Brumpton and Visscher, {Peter M.} and Loic Yengo",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer Nature America, Inc. 2024.",

year = "2024",

month = nov,

doi = "10.1038/s41588-024-01940-2",

language = "English (US)",

volume = "56",

pages = "2352--2360",

journal = "Nature Genetics",

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T1 - Genetic architecture reconciles linkage and association studies of complex traits

AU - Estonian Biobank Research Team

AU - LifeLines Cohort Study

AU - Sidorenko, Julia

AU - Couvy-Duchesne, Baptiste

AU - Kemper, Kathryn E.

AU - Moen, Gunn Helen

AU - Bhatta, Laxmi

AU - Åsvold, Bjørn Olav

AU - Mägi, Reedik

AU - Ani, Alireza

AU - Wang, Rujia

AU - Nolte, Ilja M.

AU - Gordon, Scott

AU - Hayward, Caroline

AU - Campbell, Archie

AU - Benjamin, Daniel J.

AU - Cesarini, David

AU - Evans, David M.

AU - Goddard, Michael E.

AU - Haley, Chris S.

AU - Porteous, David

AU - Medland, Sarah E.

AU - Martin, Nicholas G.

AU - Snieder, Harold

AU - Metspalu, Andres

AU - Hveem, Kristian

AU - Brumpton, Ben

AU - Visscher, Peter M.

AU - Yengo, Loic

PY - 2024/11

Y1 - 2024/11

N2 - Linkage studies have successfully mapped loci underlying monogenic disorders, but mostly failed when applied to common diseases. Conversely, genome-wide association studies (GWASs) have identified replicable associations between thousands of SNPs and complex traits, yet capture less than half of the total heritability. In the present study we reconcile these two approaches by showing that linkage signals of height and body mass index (BMI) from 119,000 sibling pairs colocalize with GWAS-identified loci. Concordant with polygenicity, we observed the following: a genome-wide inflation of linkage test statistics; that GWAS results predict linkage signals; and that adjusting phenotypes for polygenic scores reduces linkage signals. Finally, we developed a method using recombination rate-stratified, identity-by-descent sharing between siblings to unbiasedly estimate heritability of height (0.76 ± 0.05) and BMI (0.55 ± 0.07). Our results imply that substantial heritability remains unaccounted for by GWAS-identified loci and this residual genetic variation is polygenic and enriched near these loci.

AB - Linkage studies have successfully mapped loci underlying monogenic disorders, but mostly failed when applied to common diseases. Conversely, genome-wide association studies (GWASs) have identified replicable associations between thousands of SNPs and complex traits, yet capture less than half of the total heritability. In the present study we reconcile these two approaches by showing that linkage signals of height and body mass index (BMI) from 119,000 sibling pairs colocalize with GWAS-identified loci. Concordant with polygenicity, we observed the following: a genome-wide inflation of linkage test statistics; that GWAS results predict linkage signals; and that adjusting phenotypes for polygenic scores reduces linkage signals. Finally, we developed a method using recombination rate-stratified, identity-by-descent sharing between siblings to unbiasedly estimate heritability of height (0.76 ± 0.05) and BMI (0.55 ± 0.07). Our results imply that substantial heritability remains unaccounted for by GWAS-identified loci and this residual genetic variation is polygenic and enriched near these loci.

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U2 - 10.1038/s41588-024-01940-2

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M3 - Article

C2 - 39375568

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SN - 1061-4036

VL - 56

SP - 2352

EP - 2360

JO - Nature Genetics

JF - Nature Genetics

IS - 11

ER -

Genetic architecture reconciles linkage and association studies of complex traits

Abstract

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