PGX TPMT and NUDT15 Genotyping for Detection of TPMT and NUDT15 Variants Affecting Drug Metabolism

PGX TPMT and NUDT15 Genotyping For detection of TPMT and NUDT15 variants affecting drug metabolism

Clinical Background

• NUDT15 is a negative regulator of thiopurine activation and toxicity. • TPMT and NUDT15 affect thiopurine drugs such as azathioprine, 6-mercaptopurine or 6- thioguanine. • Defects in the TPMT gene lead to decreased methylation and decreased inactivation of 6MP, which enhances bone marrow toxicity and may cause myelosuppression, anemia, bleeding tendency, leukopenia and infection. • NUDT15 catalyzes the conversion of cytotoxic thioguanine triphosphate (TGTP) metabolites to the less toxic thioguanine monophosphate. • Metabolizer phenotypes can be predicted by the TPMT and NUDT15 genotypes. • The clinical impact of the TPMT and NUDT15 genotype is influenced by involvement of other metabolic pathways and other non-genetic factors. Epidemiology

• TPMT variant frequency is ethnicity dependent. TPMT*3A is present in approximately 3% of Caucasians, Mediterranean descent, South Americans; 5% Mexican descent and 1% Middle Eastern descent. TMPT*3C is present in approximately 5% of individuals of African descent. • NUDT15 variant frequency is ethnicity dependent. NUDT15*3 is present in approximately 7% of individuals of south/central Asian descent. NUDT15*5 is present in approximately 1% of individuals of East Asian descent. • The poor metabolizer phenotype is caused by two non-functional alleles. Genetics

• The TPMT gene has nine exons and is located on chromosome 6p22.3. • The NUDT15 gene has three exons and is located on chromosome 13q14.2. • Inheritance is autosomal recessive. • Penetrance is drug-dependent. Indications for Ordering Indiana University School of Medicine Genetics Testing Laboratories 975 W. Walnut St., IB350 Indianapolis, IN. 46202 Tel. 317-274-7597

• Pre-therapeutic testing to identify individuals who should avoid, or may require unconventional doses of medications metabolized by TPMT and NUDT15. Interpretation

• If no variants are detected either for TPMT or NUDT15, this suggests a *1 allele and normal enzymatic activity. • If one decreased functional or non-functional variant is detected, intermediate-to-normal enzymatic activity is predicted. • If two non-functional variants are present on opposite alleles, this predicts low enzymatic activity and a poor metabolizer phenotype. • Genotype results should be interpreted in the context of the individual clinical situation. Consultation with a clinical pharmacy professional is recommended.

Methodology

• Real-time polymerase chain reaction (PCR) and hydrolysis probe analysis.

Variants in TPMT and NUDT15 Assay

Predicted enzyme Allele variant dbSNP activity

TPMT*1 Assumed when no variant detected Normal

TPMT*2 c.238G>C rs1800462 No function

Indiana University School of Medicine Genetics Testing Laboratories 975 W. Walnut St., IB350 Indianapolis, IN. 46202 Tel. 317-274-7597

TPMT*3A c.460G>A and c.719A>G rs1800460 and rs1142345 No function

TPMT*3B c.460G>A rs1800460 No function

TPMT*3C c.719A>G rs1142345 No function

NUDT15*1 Assumed when no variant detected Normal

NUDT15*3 c.415C>T (also in *2 haplotype) rs116855232 No function

NUDT15*5 c.52G>A rs186364861 Uncertain function

Indiana University School of Medicine Genetics Testing Laboratories 975 W. Walnut St., IB350 Indianapolis, IN. 46202 Tel. 317-274-7597