Genetic variants in SLC22A17 and SLC22A7 are associated with anthracycline-induced cardiotoxicity in children

AUTHOR GROUP

doi:https://doi.org/10.2217/PGS.15.61

Genetic variants in SLC22A17 and SLC22A7 are associated with anthracycline-induced cardiotoxicity in children

AUTHOR GROUP

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

To identify novel variants associated with anthracycline-induced cardiotoxicity and to assess these in a genotype-guided risk prediction model. Two cohorts treated for childhood cancer (n = 344 and 218, respectively) were genotyped for 4578 SNPs in drug ADME and toxicity genes. Significant associations were identified in SLC22A17 (rs4982753; p = 0.0078) and SLC22A7 (rs4149178; p = 0.0034), with replication in the second cohort (p = 0.0071 and 0.047, respectively). Additional evidence was found for SULT2B1 and several genes related to oxidative stress. Adding the SLC22 variants to the prediction model improved its discriminative ability (AUC 0.78 vs 0.75 [p = 0.029]). Two novel variants in SLC22A17 and SLC22A7 were significantly associated with anthracycline-induced cardiotoxicity and improved a genotype-guided risk prediction model, which could improve patient risk stratification

Original language	English
Pages (from-to)	1065-1076
Journal	Pharmacogenomics
Volume	16
Issue number	10
DOIs	https://doi.org/10.2217/PGS.15.61
Publication status	Published - 2015

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https://doi.org/10.2217/PGS.15.61

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@article{f835625e1fdf46df8036599bcc96b757,

title = "Genetic variants in SLC22A17 and SLC22A7 are associated with anthracycline-induced cardiotoxicity in children",

abstract = "To identify novel variants associated with anthracycline-induced cardiotoxicity and to assess these in a genotype-guided risk prediction model. Two cohorts treated for childhood cancer (n = 344 and 218, respectively) were genotyped for 4578 SNPs in drug ADME and toxicity genes. Significant associations were identified in SLC22A17 (rs4982753; p = 0.0078) and SLC22A7 (rs4149178; p = 0.0034), with replication in the second cohort (p = 0.0071 and 0.047, respectively). Additional evidence was found for SULT2B1 and several genes related to oxidative stress. Adding the SLC22 variants to the prediction model improved its discriminative ability (AUC 0.78 vs 0.75 [p = 0.029]). Two novel variants in SLC22A17 and SLC22A7 were significantly associated with anthracycline-induced cardiotoxicity and improved a genotype-guided risk prediction model, which could improve patient risk stratification",

author = "Henk Visscher and Rassekh, {S. Rod} and Sandor, {George S.} and Caron, {Huib N.} and {van Dalen}, {Elvira C.} and Kremer, {Leontien C.} and {van der Pal}, {Helena J.} and Rogers, {Paul C.} and Rieder, {Michael J.} and Carleton, {Bruce C.} and Hayden, {Michael R.} and Ross, {Colin J.} and {AUTHOR GROUP} and Michael Hayden and Bruce Carleton and Colin Ross and Stuart MacLeod and Wyeth Wasserman and Craig Mitton and Anne Smith and Claudette Hildebrand and Pastrana, {Lucila Castro} and Reza Ghannadan and Rod Rassekh and Fudan Miao and Michelle Higginson and Adrienne Borrie and Ursula Amstutz and Amit Bhavsar and Cheri Nijssen-Jordan and David Johnson and Linda Verbeek and Rick Kaczowka and Paul Grundy and Kent Stobart and Bev Wilson and Sunil Desai and Maria Spavor and Linda Churcher and Terence Chow and Kevin Hall and Nick Honcharik and Sara Israels and Shanna Chan and Byron Garnham and Michelle Staub and Michael Rieder and Becky Malkin and Carol Portwine and Amy Cranston and Gideon Koren",

year = "2015",

doi = "https://doi.org/10.2217/PGS.15.61",

language = "English",

volume = "16",

pages = "1065--1076",

journal = "Pharmacogenomics",

issn = "1462-2416",

publisher = "Future Medicine Ltd.",

number = "10",

}

TY - JOUR

T1 - Genetic variants in SLC22A17 and SLC22A7 are associated with anthracycline-induced cardiotoxicity in children

AU - Visscher, Henk

AU - Rassekh, S. Rod

AU - Sandor, George S.

AU - Caron, Huib N.

AU - van Dalen, Elvira C.

AU - Kremer, Leontien C.

AU - van der Pal, Helena J.

AU - Rogers, Paul C.

AU - Rieder, Michael J.

AU - Carleton, Bruce C.

AU - Hayden, Michael R.

AU - Ross, Colin J.

AU - AUTHOR GROUP

AU - Hayden, Michael

AU - Carleton, Bruce

AU - Ross, Colin

AU - MacLeod, Stuart

AU - Wasserman, Wyeth

AU - Mitton, Craig

AU - Smith, Anne

AU - Hildebrand, Claudette

AU - Pastrana, Lucila Castro

AU - Ghannadan, Reza

AU - Rassekh, Rod

AU - Miao, Fudan

AU - Higginson, Michelle

AU - Borrie, Adrienne

AU - Amstutz, Ursula

AU - Bhavsar, Amit

AU - Nijssen-Jordan, Cheri

AU - Johnson, David

AU - Verbeek, Linda

AU - Kaczowka, Rick

AU - Grundy, Paul

AU - Stobart, Kent

AU - Wilson, Bev

AU - Desai, Sunil

AU - Spavor, Maria

AU - Churcher, Linda

AU - Chow, Terence

AU - Hall, Kevin

AU - Honcharik, Nick

AU - Israels, Sara

AU - Chan, Shanna

AU - Garnham, Byron

AU - Staub, Michelle

AU - Rieder, Michael

AU - Malkin, Becky

AU - Portwine, Carol

AU - Cranston, Amy

AU - Koren, Gideon

PY - 2015

Y1 - 2015

N2 - To identify novel variants associated with anthracycline-induced cardiotoxicity and to assess these in a genotype-guided risk prediction model. Two cohorts treated for childhood cancer (n = 344 and 218, respectively) were genotyped for 4578 SNPs in drug ADME and toxicity genes. Significant associations were identified in SLC22A17 (rs4982753; p = 0.0078) and SLC22A7 (rs4149178; p = 0.0034), with replication in the second cohort (p = 0.0071 and 0.047, respectively). Additional evidence was found for SULT2B1 and several genes related to oxidative stress. Adding the SLC22 variants to the prediction model improved its discriminative ability (AUC 0.78 vs 0.75 [p = 0.029]). Two novel variants in SLC22A17 and SLC22A7 were significantly associated with anthracycline-induced cardiotoxicity and improved a genotype-guided risk prediction model, which could improve patient risk stratification

AB - To identify novel variants associated with anthracycline-induced cardiotoxicity and to assess these in a genotype-guided risk prediction model. Two cohorts treated for childhood cancer (n = 344 and 218, respectively) were genotyped for 4578 SNPs in drug ADME and toxicity genes. Significant associations were identified in SLC22A17 (rs4982753; p = 0.0078) and SLC22A7 (rs4149178; p = 0.0034), with replication in the second cohort (p = 0.0071 and 0.047, respectively). Additional evidence was found for SULT2B1 and several genes related to oxidative stress. Adding the SLC22 variants to the prediction model improved its discriminative ability (AUC 0.78 vs 0.75 [p = 0.029]). Two novel variants in SLC22A17 and SLC22A7 were significantly associated with anthracycline-induced cardiotoxicity and improved a genotype-guided risk prediction model, which could improve patient risk stratification

U2 - https://doi.org/10.2217/PGS.15.61

DO - https://doi.org/10.2217/PGS.15.61

M3 - Article

C2 - 26230641

SN - 1462-2416

VL - 16

SP - 1065

EP - 1076

JO - Pharmacogenomics

JF - Pharmacogenomics

IS - 10

ER -