Menu
Ancestry
Core Reports
Exclusive Admixture Reports Comprehensive ancestry breakdowns
Maternal Haplogroup (MTDNA) Trace your maternal lineage
Paternal Haplogroup (YDNA) Discover your paternal ancestry
Historical Population Origins Ancient population connections
Contemporary Population Origins Modern ethnic composition
Deep Analysis
Shared Roots: Ancient Matches Global ancient matches
Ancient Global Composition 12,000 years of ancient matches
Deep Ancestry Analysis Pre-historic ancestry composition
HLA Heritage Analysis Immune system genetic origins
DNA Low Coverage Report Ancient signals in low coverage regions
X-Chromosome Admixture X-Chromosome ancestry analysis
1000 Genomes HGDP K72 72 global populations analysis
Specialized Reports
Celtic Report Celtic heritage analysis
Denisovan Report Denisovan DNA percentage
Farmers and Hunter-Gatherers Neolithic migration patterns
Jewish Report Jewish genetic heritage
Neanderthal Report Neanderthal DNA percentage
Viking Report Norse ancestry connection
See All Ancestry Reports
Studio
G25 Analysis
G25 Studio Free Advanced genetic distance analysis
G25 Coordinates Your personal G25 coordinates
G25 Calculator Explorer Free Explore G25 calculators database
G25 Advanced Tools Fit Modeler, PCA, Heatmaps and more
Admixture Analysis
Admixture Calculators Free Analyze your ancestry composition
Admixture Studio Desktop Professional desktop application
AI Assistant AI-powered ancestry insights
Data and Research
Samples Database Explorer Browse 9,000+ ancient samples from 3,000+ sites
Haplogroup Explorer Explore Y-DNA and mtDNA haplogroups
Ancestry Publications Explorer Research papers and studies
Ancestral Cultures Explore ancient cultures and civilizations
DNA Matches Analyzer Analyze DNA relative matches
See All Studio Tools
Traits
Analysis
Traits Overview Comprehensive traits analysis
Traits Reports Individual trait reports
Traits Ancestry Origins Chromosome-level trait analysis
Health & Traits Publications Scientific publications database
Predictions
Predicted Appearance Physical traits prediction
Predicted Blood Type Free Blood type prediction
Are Your Parents Related? Free Parental relatedness analysis
Personality Report Personality traits prediction
Economic & Political Preferences Genetic influence on preferences
See All Traits Reports
Data & Research
Databases
Samples Database Explorer Browse 9,000+ ancient samples from 3,000+ sites
Haplogroup Explorer Explore Y-DNA and mtDNA haplogroups
Ancestral Cultures Explore ancient cultures and civilizations
Publications & Methods
Ancestry Publications Explorer Research papers and studies
Health & Traits Publications Scientific publications database
Analysis Methods Learn about DNA analysis techniques
Services
DNA Enhancement
DNA Imputation Extend your DNA coverage
DNA Merging Create DNA Superkit
RAW File Maximizer Maximize RAW file compatibility
DNA Kit Studio Desktop Free Professional DNA analysis suite
File Converters
VCF to RAW Converter Convert VCF files to RAW format
RAW to VCF Converter Convert RAW files to VCF format
PLINK to RAW Converter Convert PLINK files to RAW format
BCF to RAW Converter Convert BCF files to RAW format
23andMe Imputed Converter Convert 23andMe imputed to RAW
Sequencing Tools
WGS (BAM/CRAM) to RAW Convert WGS files to RAW format
FASTQ Alignment to T2T Align FASTQ to T2T reference
FASTQ to RAW Converter Convert FASTQ files to RAW format
Analysis Tools
Kit Comparer Free Compare two DNA kits directly
RAW File Comparer Free Compare raw DNA files
RAW File Analyzer Free Analyze DNA file quality
Compatibility
Supported DNA Providers View all compatible RAW formats
See All DNA Services
Packages Store Upload RAW Sign In
GWAS Study

The impact of low-frequency and rare variants on lipid levels.

Surakka I, Horikoshi M, Mägi R et al.

25961943 PubMed ID
GWAS Study Type
62166 Participants
Explore Publication View on PubMed
Scroll to explore
Chapter I

Publication Details

Comprehensive information about this research publication

Journal Nat Genet
Publication Date 2015-05-11
Disease/Trait HDL cholesterol
DOI 10.1038/ng.3300
ISSN 1546-1718

Authors

SI
Surakka I
HM
Horikoshi M
MR
Mägi R
SA
Sarin AP
MA
Mahajan A
LV
Lagou V
ML
Marullo L
FT
Ferreira T
MB
Miraglio B
TS
Timonen S
KJ
Kettunen J
PM
Pirinen M
KJ
Karjalainen J
TG
Thorleifsson G
HS
Hägg S
HJ
Hottenga JJ
IA
Isaacs A
LC
Ladenvall C
BM
Beekman M
ET
Esko T
RJ
Ried JS
NC
Nelson CP
WC
Willenborg C
GS
Gustafsson S
WH
Westra HJ
BM
Blades M
DC
de Craen AJ
DG
de Geus EJ
DJ
Deelen J
GH
Grallert H
HA
Hamsten A
HA
Havulinna AS
HC
Hengstenberg C
HJ
Houwing-Duistermaat JJ
HE
Hyppönen E
KL
Karssen LC
LT
Lehtimäki T
LV
Lyssenko V
MP
Magnusson PK
ME
Mihailov E
MM
Müller-Nurasyid M
MJ
Mpindi JP
PN
Pedersen NL
PB
Penninx BW
PM
Perola M
PT
Pers TH
PA
Peters A
RJ
Rung J
SJ
Smit JH
SV
Steinthorsdottir V
TM
Tobin MD
TN
Tsernikova N
VL
van Leeuwen EM
VJ
Viikari JS
WS
Willems SM
WG
Willemsen G
SH
Schunkert H
EJ
Erdmann J
SN
Samani NJ
KJ
Kaprio J
LL
Lind L
GC
Gieger C
MA
Metspalu A
SP
Slagboom PE
GL
Groop L
VD
van Duijn CM
EJ
Eriksson JG
JA
Jula A
SV
Salomaa V
BD
Boomsma DI
PC
Power C
RO
Raitakari OT
IE
Ingelsson E
JM
Järvelin MR
TU
Thorsteinsdottir U
FL
Franke L
IE
Ikonen E
KO
Kallioniemi O
PV
Pietiäinen V
LC
Lindgren CM
SK
Stefansson K
PA
Palotie A
MM
McCarthy MI
MA
Morris AP
PI
Prokopenko I
RS
Ripatti S
View on PubMed View DOI More from Journal Similar Studies
Chapter II

Abstract

Summary of the research findings

Using a genome-wide screen of 9.6 million genetic variants achieved through 1000 Genomes Project imputation in 62,166 samples, we identify association to lipid traits in 93 loci, including 79 previously identified loci with new lead SNPs and 10 new loci, 15 loci with a low-frequency lead SNP and 10 loci with a missense lead SNP, and 2 loci with an accumulation of rare variants. In six loci, SNPs with established function in lipid genetics (CELSR2, GCKR, LIPC and APOE) or candidate missense mutations with predicted damaging function (CD300LG and TM6SF2) explained the locus associations. The low-frequency variants increased the proportion of variance explained, particularly for low-density lipoprotein cholesterol and total cholesterol. Altogether, our results highlight the impact of low-frequency variants in complex traits and show that imputation offers a cost-effective alternative to resequencing.

up to 62,166 European ancestry individuals

Chapter III

Study Statistics

Key metrics and study information

62166
Total Participants
GWAS
Study Type
No
Replicated
European
Ancestry
Finland, Sweden, Iceland, Netherlands, Germany, U.K., Estonia
Recruitment Country
Chapter IV

Analysis

Comprehensive review of health and genetic findings

Important Disclaimer: This review has been performed semi-automatically and is provided for informational purposes only. While we strive for accuracy, this analysis may contain errors, omissions, or misinterpretations of the original research. DNA Genics disclaims all liability for any inaccuracies, errors, or consequences arising from the use of this information. Users should independently verify all information and consult original research publications before making any decisions based on this content. This analysis is not intended as a substitute for professional scientific review or medical advice.

Analysis In Progress

Our analysis of this publication is currently being prepared. Please check back soon for comprehensive insights into the health and genetic findings discussed in this research.

Explore More Research

Discover the latest findings in health and genetic research

Browse All Publications