Ancestry of the Timorese: Age-related macular degeneration associated genotype and allele sharing among human populations from throughout the world
We observed that the third leading cause of blindness in the world, age-related macular degeneration (AMD), occurs at a very low documented frequency in a population-based cohort from Timor-Leste. Thus, we determined a complete catalogue of the ancestry of the Timorese by analysis of whole exome ch...
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doaj-e217c6f67d6f4902bf609dc79de92a4a2020-11-25T00:33:47ZengFrontiers Media S.A.Frontiers in Genetics1664-80212015-07-01610.3389/fgene.2015.00238148655Ancestry of the Timorese: Age-related macular degeneration associated genotype and allele sharing among human populations from throughout the worldMargaux A Morrison0Tiago R Magalhaes1Tiago R Magalhaes2Jacqueline eRamke3Silvia E Smith4Sean eEnnis5Sean eEnnis6Claire L Simpson7Laura ePortas8Laura ePortas9Federico eMurgia10Federico eMurgia11Jeeyun eAhn12Jeeyun eAhn13Caitlin eDardenne14Katie eMayne15Rosann eRobinson16Denise J Morgan17Garry eBrian18Lucy eLee19Lucy eLee20Se Joon eWoo21Se Joon eWoo22Fani eZacharaki23Evangelia E Tsironi24Joan W Miller25Ivana K Kim26Kyu Hyung ePark27Kyu Hyung ePark28Joan E Bailey-Wilson29Lindsay A Farrer30Dwight eStambolian31Margaret M DeAngelis32University of UtahOur Lady’s Children’s HospitalSchool of Medicine and Medical Science, University College DublinThe Fred Hollows Foundation New ZealandUniversity of UtahSchool of Medicine and Medical Science, University College DublinOur Lady’s Children’s HospitalNational Institutes of HealthNational Institutes of HealthThe National Research CouncilNational Institutes of HealthThe National Research CouncilSeoul National University College of MedicineSeoul Metropolitan Government Seoul National University Boramae Medical CenterUniversity of UtahUniversity of UtahUniversity of UtahUniversity of UtahThe Fred Hollows Foundation New ZealandThe Fred Hollows Foundation New ZealandUniversity in LondonSeoul National University College of MedicineSeoul National University Bundang HospitalUniversity of Thessaly School of MedicineUniversity of Thessaly School of MedicineMassachusetts Eye and Ear Infirmary, Harvard Medical SchoolMassachusetts Eye and Ear Infirmary, Harvard Medical SchoolSeoul National University College of MedicineSeoul National University Bundang HospitalNational Institutes of HealthBoston University Schools of Medicine and Public HealthUniversity of PennsylvaniaUniversity of UtahWe observed that the third leading cause of blindness in the world, age-related macular degeneration (AMD), occurs at a very low documented frequency in a population-based cohort from Timor-Leste. Thus, we determined a complete catalogue of the ancestry of the Timorese by analysis of whole exome chip data and haplogroup analysis of SNP genotypes determined by sequencing the Hypervariable I and II regions of the mitochondrial genome and 17 genotyped YSTR markers obtained from 535 individuals. We genotyped 20 previously reported AMD-associated SNPs in the Timorese to examine their allele frequencies compared to and between previously documented AMD cohorts of varying ethnicities. For those without AMD (average age > 55 years), genotype and allele frequencies were similar for most SNPs with a few exceptions. The major risk allele of HTRA1 rs11200638 (10q26) was at a significantly higher frequency in the Timorese, as well as 3 of the 5 protective CFH (1q32) SNPs (rs800292, rs2284664, and rs12066959). Additionally, the most commonly associated AMD-risk SNP, CFH rs1061170 (Y402H), was also seen at a much lower frequency in the Korean and Timorese populations than in the assessed Caucasian populations (C ~7% vs. ~40%, respectively). The difference in allele frequencies between the Timorese population and the other genotyped populations, along with the haplogroup analysis, also highlight the genetic diversity of the Timorese. Specifically, the most common ancestry groupings were Oceanic (Melanesian and Papuan) and Eastern Asian (specifically Han Chinese). The low prevalence of AMD in the Timorese population (2 of 535 randomly selected participants) may be due to the enrichment of protective alleles in this population at the 1q32 locus.http://journal.frontiersin.org/Journal/10.3389/fgene.2015.00238/fullEpidemiologyPopulation Geneticsancestryage-related macular degenerationcomplex disease |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Margaux A Morrison Tiago R Magalhaes Tiago R Magalhaes Jacqueline eRamke Silvia E Smith Sean eEnnis Sean eEnnis Claire L Simpson Laura ePortas Laura ePortas Federico eMurgia Federico eMurgia Jeeyun eAhn Jeeyun eAhn Caitlin eDardenne Katie eMayne Rosann eRobinson Denise J Morgan Garry eBrian Lucy eLee Lucy eLee Se Joon eWoo Se Joon eWoo Fani eZacharaki Evangelia E Tsironi Joan W Miller Ivana K Kim Kyu Hyung ePark Kyu Hyung ePark Joan E Bailey-Wilson Lindsay A Farrer Dwight eStambolian Margaret M DeAngelis |
spellingShingle |
Margaux A Morrison Tiago R Magalhaes Tiago R Magalhaes Jacqueline eRamke Silvia E Smith Sean eEnnis Sean eEnnis Claire L Simpson Laura ePortas Laura ePortas Federico eMurgia Federico eMurgia Jeeyun eAhn Jeeyun eAhn Caitlin eDardenne Katie eMayne Rosann eRobinson Denise J Morgan Garry eBrian Lucy eLee Lucy eLee Se Joon eWoo Se Joon eWoo Fani eZacharaki Evangelia E Tsironi Joan W Miller Ivana K Kim Kyu Hyung ePark Kyu Hyung ePark Joan E Bailey-Wilson Lindsay A Farrer Dwight eStambolian Margaret M DeAngelis Ancestry of the Timorese: Age-related macular degeneration associated genotype and allele sharing among human populations from throughout the world Frontiers in Genetics Epidemiology Population Genetics ancestry age-related macular degeneration complex disease |
author_facet |
Margaux A Morrison Tiago R Magalhaes Tiago R Magalhaes Jacqueline eRamke Silvia E Smith Sean eEnnis Sean eEnnis Claire L Simpson Laura ePortas Laura ePortas Federico eMurgia Federico eMurgia Jeeyun eAhn Jeeyun eAhn Caitlin eDardenne Katie eMayne Rosann eRobinson Denise J Morgan Garry eBrian Lucy eLee Lucy eLee Se Joon eWoo Se Joon eWoo Fani eZacharaki Evangelia E Tsironi Joan W Miller Ivana K Kim Kyu Hyung ePark Kyu Hyung ePark Joan E Bailey-Wilson Lindsay A Farrer Dwight eStambolian Margaret M DeAngelis |
author_sort |
Margaux A Morrison |
title |
Ancestry of the Timorese: Age-related macular degeneration associated genotype and allele sharing among human populations from throughout the world |
title_short |
Ancestry of the Timorese: Age-related macular degeneration associated genotype and allele sharing among human populations from throughout the world |
title_full |
Ancestry of the Timorese: Age-related macular degeneration associated genotype and allele sharing among human populations from throughout the world |
title_fullStr |
Ancestry of the Timorese: Age-related macular degeneration associated genotype and allele sharing among human populations from throughout the world |
title_full_unstemmed |
Ancestry of the Timorese: Age-related macular degeneration associated genotype and allele sharing among human populations from throughout the world |
title_sort |
ancestry of the timorese: age-related macular degeneration associated genotype and allele sharing among human populations from throughout the world |
publisher |
Frontiers Media S.A. |
series |
Frontiers in Genetics |
issn |
1664-8021 |
publishDate |
2015-07-01 |
description |
We observed that the third leading cause of blindness in the world, age-related macular degeneration (AMD), occurs at a very low documented frequency in a population-based cohort from Timor-Leste. Thus, we determined a complete catalogue of the ancestry of the Timorese by analysis of whole exome chip data and haplogroup analysis of SNP genotypes determined by sequencing the Hypervariable I and II regions of the mitochondrial genome and 17 genotyped YSTR markers obtained from 535 individuals. We genotyped 20 previously reported AMD-associated SNPs in the Timorese to examine their allele frequencies compared to and between previously documented AMD cohorts of varying ethnicities. For those without AMD (average age > 55 years), genotype and allele frequencies were similar for most SNPs with a few exceptions. The major risk allele of HTRA1 rs11200638 (10q26) was at a significantly higher frequency in the Timorese, as well as 3 of the 5 protective CFH (1q32) SNPs (rs800292, rs2284664, and rs12066959). Additionally, the most commonly associated AMD-risk SNP, CFH rs1061170 (Y402H), was also seen at a much lower frequency in the Korean and Timorese populations than in the assessed Caucasian populations (C ~7% vs. ~40%, respectively). The difference in allele frequencies between the Timorese population and the other genotyped populations, along with the haplogroup analysis, also highlight the genetic diversity of the Timorese. Specifically, the most common ancestry groupings were Oceanic (Melanesian and Papuan) and Eastern Asian (specifically Han Chinese). The low prevalence of AMD in the Timorese population (2 of 535 randomly selected participants) may be due to the enrichment of protective alleles in this population at the 1q32 locus. |
topic |
Epidemiology Population Genetics ancestry age-related macular degeneration complex disease |
url |
http://journal.frontiersin.org/Journal/10.3389/fgene.2015.00238/full |
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