Unraveling the functional role of the orphan solute carrier, SLC22A24 in the transport of steroid conjugates through metabolomic and genome-wide association studies.

Variation in steroid hormone levels has wide implications for health and disease. The genes encoding the proteins involved in steroid disposition represent key determinants of interindividual variation in steroid levels and ultimately, their effects. Beginning with metabolomic data from genome-wide...

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Main Authors: Sook Wah Yee, Adrian Stecula, Huan-Chieh Chien, Ling Zou, Elena V Feofanova, Marjolein van Borselen, Kit Wun Kathy Cheung, Noha A Yousri, Karsten Suhre, Jason M Kinchen, Eric Boerwinkle, Roshanak Irannejad, Bing Yu, Kathleen M Giacomini
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-09-01
Series:PLoS Genetics
Online Access:https://doi.org/10.1371/journal.pgen.1008208
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spelling doaj-5623312d5ce545b0ae5d208f5ebfc7e62021-04-21T14:21:50ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042019-09-01159e100820810.1371/journal.pgen.1008208Unraveling the functional role of the orphan solute carrier, SLC22A24 in the transport of steroid conjugates through metabolomic and genome-wide association studies.Sook Wah YeeAdrian SteculaHuan-Chieh ChienLing ZouElena V FeofanovaMarjolein van BorselenKit Wun Kathy CheungNoha A YousriKarsten SuhreJason M KinchenEric BoerwinkleRoshanak IrannejadBing YuKathleen M GiacominiVariation in steroid hormone levels has wide implications for health and disease. The genes encoding the proteins involved in steroid disposition represent key determinants of interindividual variation in steroid levels and ultimately, their effects. Beginning with metabolomic data from genome-wide association studies (GWAS), we observed that genetic variants in the orphan transporter, SLC22A24 were significantly associated with levels of androsterone glucuronide and etiocholanolone glucuronide (sentinel SNPs p-value <1x10-30). In cells over-expressing human or various mammalian orthologs of SLC22A24, we showed that steroid conjugates and bile acids were substrates of the transporter. Phylogenetic, genomic, and transcriptomic analyses suggested that SLC22A24 has a specialized role in the kidney and appears to function in the reabsorption of organic anions, and in particular, anionic steroids. Phenome-wide analysis showed that functional variants of SLC22A24 are associated with human disease such as cardiovascular diseases and acne, which have been linked to dysregulated steroid metabolism. Collectively, these functional genomic studies reveal a previously uncharacterized protein involved in steroid homeostasis, opening up new possibilities for SLC22A24 as a pharmacological target for regulating steroid levels.https://doi.org/10.1371/journal.pgen.1008208
collection DOAJ
language English
format Article
sources DOAJ
author Sook Wah Yee
Adrian Stecula
Huan-Chieh Chien
Ling Zou
Elena V Feofanova
Marjolein van Borselen
Kit Wun Kathy Cheung
Noha A Yousri
Karsten Suhre
Jason M Kinchen
Eric Boerwinkle
Roshanak Irannejad
Bing Yu
Kathleen M Giacomini
spellingShingle Sook Wah Yee
Adrian Stecula
Huan-Chieh Chien
Ling Zou
Elena V Feofanova
Marjolein van Borselen
Kit Wun Kathy Cheung
Noha A Yousri
Karsten Suhre
Jason M Kinchen
Eric Boerwinkle
Roshanak Irannejad
Bing Yu
Kathleen M Giacomini
Unraveling the functional role of the orphan solute carrier, SLC22A24 in the transport of steroid conjugates through metabolomic and genome-wide association studies.
PLoS Genetics
author_facet Sook Wah Yee
Adrian Stecula
Huan-Chieh Chien
Ling Zou
Elena V Feofanova
Marjolein van Borselen
Kit Wun Kathy Cheung
Noha A Yousri
Karsten Suhre
Jason M Kinchen
Eric Boerwinkle
Roshanak Irannejad
Bing Yu
Kathleen M Giacomini
author_sort Sook Wah Yee
title Unraveling the functional role of the orphan solute carrier, SLC22A24 in the transport of steroid conjugates through metabolomic and genome-wide association studies.
title_short Unraveling the functional role of the orphan solute carrier, SLC22A24 in the transport of steroid conjugates through metabolomic and genome-wide association studies.
title_full Unraveling the functional role of the orphan solute carrier, SLC22A24 in the transport of steroid conjugates through metabolomic and genome-wide association studies.
title_fullStr Unraveling the functional role of the orphan solute carrier, SLC22A24 in the transport of steroid conjugates through metabolomic and genome-wide association studies.
title_full_unstemmed Unraveling the functional role of the orphan solute carrier, SLC22A24 in the transport of steroid conjugates through metabolomic and genome-wide association studies.
title_sort unraveling the functional role of the orphan solute carrier, slc22a24 in the transport of steroid conjugates through metabolomic and genome-wide association studies.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2019-09-01
description Variation in steroid hormone levels has wide implications for health and disease. The genes encoding the proteins involved in steroid disposition represent key determinants of interindividual variation in steroid levels and ultimately, their effects. Beginning with metabolomic data from genome-wide association studies (GWAS), we observed that genetic variants in the orphan transporter, SLC22A24 were significantly associated with levels of androsterone glucuronide and etiocholanolone glucuronide (sentinel SNPs p-value <1x10-30). In cells over-expressing human or various mammalian orthologs of SLC22A24, we showed that steroid conjugates and bile acids were substrates of the transporter. Phylogenetic, genomic, and transcriptomic analyses suggested that SLC22A24 has a specialized role in the kidney and appears to function in the reabsorption of organic anions, and in particular, anionic steroids. Phenome-wide analysis showed that functional variants of SLC22A24 are associated with human disease such as cardiovascular diseases and acne, which have been linked to dysregulated steroid metabolism. Collectively, these functional genomic studies reveal a previously uncharacterized protein involved in steroid homeostasis, opening up new possibilities for SLC22A24 as a pharmacological target for regulating steroid levels.
url https://doi.org/10.1371/journal.pgen.1008208
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