Review article: recent advances in pharmacogenetics and pharmacokinetics for safe and effective thiopurine therapy in inflammatory bowel disease

Moon, Won; Loftus, Edward V.

doi:10.1111/apt.13559

Cited by 77 publications

(74 citation statements)

References 216 publications

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“…ALL in childhood, IBD, autoimmune diseases) 19,20 pretreatment determination of the TPMT phenotype and subsequent pharmacogenetically-guided dosing of thiopurines, at least in TPMT deficient individuals, is recommended in routine clinical practice before commencing therapy. 5 Very recently a landmark randomized clinical trial strongly corroborates the clinical utility of upfront genetic testing for TPMT in patients treated with thiopurines to avoid hematotoxicity.…”

Section: Discussionmentioning

confidence: 99%

Polymorphic Variation in TPMT Is the Principal Determinant of TPMT Phenotype: A Meta‐Analysis of Three Genome‐Wide Association Studies

Tamm

Mägi

Tremmel

et al. 2017

Clin Pharma and Therapeutics

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Thiopurine-related hematotoxicity in paediatric acute lymphoblastic leukemia (ALL) and inflammatory bowel diseases has been linked to genetically defined variability in thiopurine S-methyltransferase (TPMT) activity. While gene testing of TPMT is being clinically implemented, it is unclear if additional genetic variation influences TPMT activity with consequences for thiopurine-related toxicity. To examine this possibility, we performed a genome-wide association study (GWAS) of red blood cell TPMT activity in 844 Estonian individuals and 245 paediatric ALL-cases. Additionally, we correlated genome-wide genotypes to human hepatic TPMT activity in 123 samples. Only genetic variants mapping to chromosome 6, including TPMT gene region, were significantly associated with TPMT activity (P<5.0×10−8) in each of the three GWAS and a joint meta-analysis of 1212 cases (top hit P=1.2×10−72). This finding is consistent with TPMT genotype being the primary determinant of TPMT activity, reinforcing the rationale for genetic testing of TPMT alleles in routine clinical practice to individualize MP dosage.

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Section: Discussionmentioning

confidence: 99%

Polymorphic Variation in TPMT Is the Principal Determinant of TPMT Phenotype: A Meta‐Analysis of Three Genome‐Wide Association Studies

Tamm

Mägi

Tremmel

et al. 2017

Clin Pharma and Therapeutics

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“…14 Measurement of pretreatment TPMT activity and metabolites while on treatment reduces the risk of adverse events and improves efficacy by up to 7% and 30%, respectively. 15 About 1 in 300 are missing the genes to produce any TPMT, about 11% are heterozygous for the wild type, and nearly 89% are homozygous for the wild type who produce high levels of TPMT. Although there are reports of AZA treatment success in TPMT-deficient leukemic children whose serum levels were intesnsely monitored, thiopurines are best avoided in the homozygous mutant population to avoid potentially lethal myelosuppression.…”

Section: Immunomodulatorsmentioning

confidence: 99%

Understanding the Cautions and Contraindications of Immunomodulator and Biologic Therapies for Use in Inflammatory Bowel Disease

Cohn

Dave

Loftus

2017

Inflammatory Bowel Diseases

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Ulcerative colitis and Crohn’s disease are chronic inflammatory bowel diseases for which there are no cures. These diseases are immunopathogenic, and medical treatment is centered on the temperance of a dysregulated immune response to allow mucosal healing and prevent the sequelae of fistulation and stenosis. Accordingly, the armamentarium of medications, which has expanded immensely in recent history, is not without significant infectious and neoplastic risks. Many of these untoward effects can be mitigated by screening and avoidance of contraindicated medications. This review seeks to highlight the cautions for use of immunomodulators, anticytokine and α4-integrin antagonists. The potential adverse events are further complicated by substantial heterogeneity in disease phenotype in the IBD population. Large patient registries and databases provide considerable experience and knowledge to calculate the incidence of safety outcomes. To identify rarer outcomes after prolonged therapy, more prospective studies and continued adverse event reporting will aid safe application and minimize potential harms.

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“…Furthermore, methylated metabolites generated by thiopurine S-methyltransferase (TPMT) activity have been identified as mediators of side effects in patients treated with azathioprine. Finally, systemic thiopurine administration may result in an increased susceptibility towards severe bacterial or viral infections due to general immunosuppressive effects 9. Remarkably, Oancea et al now provided data that strongly encourage the idea of topical thioguanine administration and thereby open new avenues to overcome the apparent inseparability of thiopurine efficacy and toxicity.…”

mentioning

confidence: 99%

“…Indeed, the activities of all master enzymes included in thiopurine metabolism (xanthine oxidase, TPMT, hypoxanthine phosphoribosyltransferase (HPRT) and inosine monophosphate dehydrogenase) show marked variations among individuals, which relevantly impact on the efficacy of active thiopurine formation 9. So, it is well known that, for instance, low TPMT activity results in an overwhelming generation of active TGN metabolites and is therefore associated with an increased risk for myelosuppressive side effects, while, vice versa, high TPMT activity favours the formation of inactive methylated metabolites and potentially goes along with non-responsiveness9 (figure 1). In a similar way, increased activity of the activating enzyme HPRT turned out to be associated with marked effects on leucocytes in thiopurine-treated patients with IBD 9.…”

mentioning

confidence: 99%

“…So, it is well known that, for instance, low TPMT activity results in an overwhelming generation of active TGN metabolites and is therefore associated with an increased risk for myelosuppressive side effects, while, vice versa, high TPMT activity favours the formation of inactive methylated metabolites and potentially goes along with non-responsiveness9 (figure 1). In a similar way, increased activity of the activating enzyme HPRT turned out to be associated with marked effects on leucocytes in thiopurine-treated patients with IBD 9. The main advantage of the now-described capacity of intestinal microbial or mucosal enzymes to catalyse a host-independent thioguanine metabolisation is again related to the resulting applicability of topical administration strategies and the subsequent prevention of systemic metabolite accumulation.…”

mentioning

confidence: 99%

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Microbiota: relevant player in thiopurine metabolisation?

Atreya

2016

Gut

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Review article: recent advances in pharmacogenetics and pharmacokinetics for safe and effective thiopurine therapy in inflammatory bowel disease

Abstract: SUMMARY BackgroundAzathioprine and mercaptopurine have a pivotal role in the treatment of inflammatory bowel disease (IBD). However, because of their complex metabolism and potential toxicities, optimal use of biomarkers to predict adverse effects and therapeutic response is paramount.

Cited by 77 publications

References 216 publications

Polymorphic Variation in TPMT Is the Principal Determinant of TPMT Phenotype: A Meta‐Analysis of Three Genome‐Wide Association Studies

Polymorphic Variation in TPMT Is the Principal Determinant of TPMT Phenotype: A Meta‐Analysis of Three Genome‐Wide Association Studies

Understanding the Cautions and Contraindications of Immunomodulator and Biologic Therapies for Use in Inflammatory Bowel Disease

Microbiota: relevant player in thiopurine metabolisation?

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