Human Adaptation to Arsenic-Rich Environments.

Schlebusch, Carina M; Gattepaille, Lucie M; Engström, Karin; Vahter, Marie; Jakobsson, Mattias; Broberg Palmgren, Karin

Human Adaptation to Arsenic-Rich Environments.

Mark

Schlebusch, Carina M ; Gattepaille, Lucie M ; Engström, Karin ^LU ; Vahter, Marie ; Jakobsson, Mattias and Broberg Palmgren, Karin ^LU

(2015) In Molecular biology and evolution 32(6). p.1544-1555

Abstract: Adaptation drives genomic changes; however, evidence of specific adaptations in humans remains limited. We found that inhabitants of the northern Argentinean Andes, an arid region where elevated arsenic concentrations in available drinking water is common, have unique arsenic metabolism, with efficient methylation and excretion of the major metabolite dimethylated arsenic and a less excretion of the highly toxic monomethylated metabolite. We genotyped women from this population for 4,301,332 single nucleotide polymorphisms (SNPs) and found a strong association between the AS3MT (arsenic [+3 oxidation state] methyltransferase) gene and mono- and dimethylated arsenic in urine, suggesting that AS3MT functions as the major gene for arsenic... (More); Adaptation drives genomic changes; however, evidence of specific adaptations in humans remains limited. We found that inhabitants of the northern Argentinean Andes, an arid region where elevated arsenic concentrations in available drinking water is common, have unique arsenic metabolism, with efficient methylation and excretion of the major metabolite dimethylated arsenic and a less excretion of the highly toxic monomethylated metabolite. We genotyped women from this population for 4,301,332 single nucleotide polymorphisms (SNPs) and found a strong association between the AS3MT (arsenic [+3 oxidation state] methyltransferase) gene and mono- and dimethylated arsenic in urine, suggesting that AS3MT functions as the major gene for arsenic metabolism in humans. We found strong genetic differentiation around AS3MT in the Argentinean Andes population, compared with a highly related Peruvian population (FST = 0.014) from a region with much less environmental arsenic. Also, 13 of the 100 SNPs with the highest genome-wide Locus-Specific Branch Length occurred near AS3MT. In addition, our examination of extended haplotype homozygosity indicated a selective sweep of the Argentinean Andes population, in contrast to Peruvian and Colombian populations. Our data show that adaptation to tolerate the environmental stressor arsenic has likely driven an increase in the frequencies of protective variants of AS3MT, providing the first evidence of human adaptation to a toxic chemical. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/5265296

author

Schlebusch, Carina M ; Gattepaille, Lucie M ; Engström, Karin ^LU ; Vahter, Marie ; Jakobsson, Mattias and Broberg Palmgren, Karin ^LU

organization

Division of Occupational and Environmental Medicine, Lund University

publishing date

2015

type

Contribution to journal

publication status

published

subject

Environmental Health and Occupational Health

in

Molecular biology and evolution

volume

32

issue

6

pages

1544 - 1555

publisher

Oxford University Press

external identifiers

pmid:25739736
wos:000356259600015
scopus:84930715906

ISSN

0737-4038

DOI

10.1093/molbev/msv046

language

English

LU publication?

yes

id

e3e57b57-8c6b-4f3b-a57a-21e0af53bda3 (old id 5265296)

alternative location

http://www.ncbi.nlm.nih.gov/pubmed/25739736?dopt=Abstract

date added to LUP

2016-04-01 11:11:40

date last changed

2024-01-07 09:59:59

@article{e3e57b57-8c6b-4f3b-a57a-21e0af53bda3,
  abstract     = {{Adaptation drives genomic changes; however, evidence of specific adaptations in humans remains limited. We found that inhabitants of the northern Argentinean Andes, an arid region where elevated arsenic concentrations in available drinking water is common, have unique arsenic metabolism, with efficient methylation and excretion of the major metabolite dimethylated arsenic and a less excretion of the highly toxic monomethylated metabolite. We genotyped women from this population for 4,301,332 single nucleotide polymorphisms (SNPs) and found a strong association between the AS3MT (arsenic [+3 oxidation state] methyltransferase) gene and mono- and dimethylated arsenic in urine, suggesting that AS3MT functions as the major gene for arsenic metabolism in humans. We found strong genetic differentiation around AS3MT in the Argentinean Andes population, compared with a highly related Peruvian population (FST = 0.014) from a region with much less environmental arsenic. Also, 13 of the 100 SNPs with the highest genome-wide Locus-Specific Branch Length occurred near AS3MT. In addition, our examination of extended haplotype homozygosity indicated a selective sweep of the Argentinean Andes population, in contrast to Peruvian and Colombian populations. Our data show that adaptation to tolerate the environmental stressor arsenic has likely driven an increase in the frequencies of protective variants of AS3MT, providing the first evidence of human adaptation to a toxic chemical.}},
  author       = {{Schlebusch, Carina M and Gattepaille, Lucie M and Engström, Karin and Vahter, Marie and Jakobsson, Mattias and Broberg Palmgren, Karin}},
  issn         = {{0737-4038}},
  language     = {{eng}},
  number       = {{6}},
  pages        = {{1544--1555}},
  publisher    = {{Oxford University Press}},
  series       = {{Molecular biology and evolution}},
  title        = {{Human Adaptation to Arsenic-Rich Environments.}},
  url          = {{http://dx.doi.org/10.1093/molbev/msv046}},
  doi          = {{10.1093/molbev/msv046}},
  volume       = {{32}},
  year         = {{2015}},
}

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Human Adaptation to Arsenic-Rich Environments.