Ethnically biased microsatellites contribute to differential gene expression and glutathione metabolism in Africans and Europeans.

Approximately three percent of the human genome is occupied by microsatellites: a type of short tandem repeat (STR). Microsatellites have well established effects on (a) the genetic structure of diverse human populations and (b) expression of nearby genes. These lines of inquiry have uncovered 3,984...

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Main Authors: Nick Kinney, Lin Kang, Harpal Bains, Elizabeth Lawson, Mesam Husain, Kumayl Husain, Inderjit Sandhu, Yongdeok Shin, Javan K Carter, Ramu Anandakrishnan, Pawel Michalak, Harold Garner
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2021-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0249148
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spelling doaj-4ba67c4616214ab08552862c3d7aa19d2021-04-08T04:30:29ZengPublic Library of Science (PLoS)PLoS ONE1932-62032021-01-01163e024914810.1371/journal.pone.0249148Ethnically biased microsatellites contribute to differential gene expression and glutathione metabolism in Africans and Europeans.Nick KinneyLin KangHarpal BainsElizabeth LawsonMesam HusainKumayl HusainInderjit SandhuYongdeok ShinJavan K CarterRamu AnandakrishnanPawel MichalakHarold GarnerApproximately three percent of the human genome is occupied by microsatellites: a type of short tandem repeat (STR). Microsatellites have well established effects on (a) the genetic structure of diverse human populations and (b) expression of nearby genes. These lines of inquiry have uncovered 3,984 ethnically biased microsatellite loci (EBML) and 28,375 expression STRs (eSTRs), respectively. We hypothesize that a combination of EBML, eSTRs, and gene expression data (RNA-seq) can be used to show that microsatellites contribute to differential gene expression and phenotype in human populations. In fact, our previous study demonstrated a degree of mutual overlap between EBML and eSTRs but fell short of quantifying effects on gene expression. The present work aims to narrow the gap. First, we identify 313 overlapping EBML/eSTRs and recapitulate their mutual overlap. The 313 EBML/eSTRs are then characterized across ethnicity and tissue type. We use RNA-seq data to pursue validation of 49 regions that affect whole blood gene expression; 32 out of 54 affected genes are differentially expressed in Africans and Europeans. We quantify the relative contribution of these 32 genes to differential expression; fold change tends to be less than other differentially expressed genes. Repeat length correlates with expression for 15 of the 32 genes; two are conspicuously involved in glutathione metabolism. Finally, we repurpose a mathematical model of glutathione metabolism to investigate how a single polymorphic microsatellite affects phenotype. We conclude with a testable prediction that microsatellite polymorphisms affect GPX7 expression and oxidative stress in Africans and Europeans.https://doi.org/10.1371/journal.pone.0249148
collection DOAJ
language English
format Article
sources DOAJ
author Nick Kinney
Lin Kang
Harpal Bains
Elizabeth Lawson
Mesam Husain
Kumayl Husain
Inderjit Sandhu
Yongdeok Shin
Javan K Carter
Ramu Anandakrishnan
Pawel Michalak
Harold Garner
spellingShingle Nick Kinney
Lin Kang
Harpal Bains
Elizabeth Lawson
Mesam Husain
Kumayl Husain
Inderjit Sandhu
Yongdeok Shin
Javan K Carter
Ramu Anandakrishnan
Pawel Michalak
Harold Garner
Ethnically biased microsatellites contribute to differential gene expression and glutathione metabolism in Africans and Europeans.
PLoS ONE
author_facet Nick Kinney
Lin Kang
Harpal Bains
Elizabeth Lawson
Mesam Husain
Kumayl Husain
Inderjit Sandhu
Yongdeok Shin
Javan K Carter
Ramu Anandakrishnan
Pawel Michalak
Harold Garner
author_sort Nick Kinney
title Ethnically biased microsatellites contribute to differential gene expression and glutathione metabolism in Africans and Europeans.
title_short Ethnically biased microsatellites contribute to differential gene expression and glutathione metabolism in Africans and Europeans.
title_full Ethnically biased microsatellites contribute to differential gene expression and glutathione metabolism in Africans and Europeans.
title_fullStr Ethnically biased microsatellites contribute to differential gene expression and glutathione metabolism in Africans and Europeans.
title_full_unstemmed Ethnically biased microsatellites contribute to differential gene expression and glutathione metabolism in Africans and Europeans.
title_sort ethnically biased microsatellites contribute to differential gene expression and glutathione metabolism in africans and europeans.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2021-01-01
description Approximately three percent of the human genome is occupied by microsatellites: a type of short tandem repeat (STR). Microsatellites have well established effects on (a) the genetic structure of diverse human populations and (b) expression of nearby genes. These lines of inquiry have uncovered 3,984 ethnically biased microsatellite loci (EBML) and 28,375 expression STRs (eSTRs), respectively. We hypothesize that a combination of EBML, eSTRs, and gene expression data (RNA-seq) can be used to show that microsatellites contribute to differential gene expression and phenotype in human populations. In fact, our previous study demonstrated a degree of mutual overlap between EBML and eSTRs but fell short of quantifying effects on gene expression. The present work aims to narrow the gap. First, we identify 313 overlapping EBML/eSTRs and recapitulate their mutual overlap. The 313 EBML/eSTRs are then characterized across ethnicity and tissue type. We use RNA-seq data to pursue validation of 49 regions that affect whole blood gene expression; 32 out of 54 affected genes are differentially expressed in Africans and Europeans. We quantify the relative contribution of these 32 genes to differential expression; fold change tends to be less than other differentially expressed genes. Repeat length correlates with expression for 15 of the 32 genes; two are conspicuously involved in glutathione metabolism. Finally, we repurpose a mathematical model of glutathione metabolism to investigate how a single polymorphic microsatellite affects phenotype. We conclude with a testable prediction that microsatellite polymorphisms affect GPX7 expression and oxidative stress in Africans and Europeans.
url https://doi.org/10.1371/journal.pone.0249148
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