Genes implicated in thiopurine-induced toxicity: Comparing TPMT enzyme activity with clinical phenotype and exome data in a paediatric IBD cohort

The aim of our study was to assess the utility of next generation sequencing (NGS) for predicting toxicity and clinical response to thiopurine drugs in paediatric patients with inflammatory bowel disease. Exome data for 100 patients were assessed against biochemically measured TPMT enzyme activity,...

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Bibliographic Details
Published inScientific reports Vol. 6; no. 1; p. 34658
Main Authors Coelho, Tracy, Andreoletti, Gaia, Ashton, James J, Batra, Akshay, Afzal, Nadeem Ahmad, Gao, Yifang, Williams, Anthony P, Beattie, Robert M, Ennis, Sarah
Format Journal Article
LanguageEnglish
Published England Nature Publishing Group 05.10.2016
Subjects
Adolescent
Azathioprine - administration & dosage
Azathioprine - adverse effects
Child
Child, Preschool
Colitis, Ulcerative - drug therapy
Colitis, Ulcerative - enzymology
Colon
Crohn Disease - drug therapy
Crohn Disease - enzymology
Crohn Disease - genetics
Crohn's disease
Enzymatic activity
Enzymes
Exome
Female
Genes
Genome-Wide Association Study
Genotyping
High-Throughput Nucleotide Sequencing
Humans
Infant
Inflammatory bowel diseases
Intestine
Male
Mercaptopurine - administration & dosage
Mercaptopurine - adverse effects
Methyltransferases - genetics
Methyltransferases - metabolism
Mutation
Side effects
Sulfurtransferases - genetics
Sulfurtransferases - metabolism
Toxicity
Ulcerative colitis
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Summary:The aim of our study was to assess the utility of next generation sequencing (NGS) for predicting toxicity and clinical response to thiopurine drugs in paediatric patients with inflammatory bowel disease. Exome data for 100 patients were assessed against biochemically measured TPMT enzyme activity, clinical response and adverse effects. The TPMT gene and a panel of 15 other genes implicated in thiopurine toxicity were analysed using a gene based statistical test (SKAT-O test). Nine patients out of 100 (Crohn's disease- 67, ulcerative colitis- 23 and IBDU-10) had known TPMT mutations associated with deficient enzyme activity. A novel and a highly pathogenic TPMT variant not detectable through standard genotyping, was identified through NGS in an individual intolerant to thiopurines. Of the 14 patients intolerant to thiopurines, NGS identified deleterious TPMT variants in 5 individuals whereas the biochemical test identified 8 individuals as intolerant (sensitivity 35.7% and 57.14%; specificity 93.75% and 50% respectively). SKAT-O test identified a significant association between MOCOS gene and TPMT activity (p = 0.0015), not previously reported. Although NGS has the ability to detect rare or novel variants not otherwise identified through standard genotyping, it demonstrates no clear advantage over the biochemical test in predicting toxicity in our modest cohort.
Bibliography:These authors contributed equally to this work.
ISSN:2045-2322
2045-2322
DOI:10.1038/srep34658