Thiopurine methyltransferase (TPMT) genotype and early treatment response to mercaptopurine in childhood acute lymphoblastic leukemia

Martin Stanulla; Elke Schaeffeler; Thomas Flohr; Gunnar Cario; André Schrauder; Martin Zimmermann; Karl Welte; Wolf-Dieter Ludwig; Claus R Bartram; Ulrich M Zanger; Michel Eichelbaum; Martin Schrappe; Matthias Schwab

doi:10.1001/jama.293.12.1485

Thiopurine methyltransferase (TPMT) genotype and early treatment response to mercaptopurine in childhood acute lymphoblastic leukemia

JAMA. 2005 Mar 23;293(12):1485-9. doi: 10.1001/jama.293.12.1485.

Authors

Martin Stanulla¹, Elke Schaeffeler, Thomas Flohr, Gunnar Cario, André Schrauder, Martin Zimmermann, Karl Welte, Wolf-Dieter Ludwig, Claus R Bartram, Ulrich M Zanger, Michel Eichelbaum, Martin Schrappe, Matthias Schwab

Affiliation

¹ Department of Pediatric Hematology and Oncology, Hannover Medical School, Hannover, Germany. Stanulla.Martin@MH-Hannover.de

PMID: 15784872
DOI: 10.1001/jama.293.12.1485

Abstract

Context: Early response to multiagent chemotherapy, including mercaptopurine, as measured by minimal residual disease is an important prognostic factor for children with acute lymphoblastic leukemia (ALL). Thiopurine methyltransferase (TPMT) is involved in the metabolism of mercaptopurine and subject to genetic polymorphism, with heterozygous individuals having intermediate and homozygous mutant individuals having very low TPMT activity.

Objective: To assess the association of TPMT genotype with minimal residual disease load before and after treatment with mercaptopurine in the early treatment course of childhood ALL.

Design, setting, and patients: TPMT genotyping of childhood ALL patients (n = 814) in Germany consecutively enrolled in the ALL-BFM (Berlin-Frankfurt-Münster) 2000 study from October 1999 to September 2002. Minimal residual disease was analyzed on treatment days 33 and 78 for risk-adapted treatment stratification. A 4-week cycle of mercaptopurine was administered between these 2 minimal residual disease measurements. Patients (n = 4) homozygous for a mutant TPMT allele, and consequently deficient in TPMT activity, were treated with reduced doses of mercaptopurine and, therefore, not included in the analyses.

Main outcome measures: Minimal residual disease load before (day 33) and after (day 78) mercaptopurine treatment. Loads smaller than 10(-4) were defined as negative.

Results: Patients (n = 55) heterozygous for allelic variants of TPMT conferring lower enzyme activity had a significantly lower rate of minimal residual disease positivity (9.1%) compared with patients (n = 755) with homozygous wild-type alleles (22.8%) on day 78 (P = .02). This translated into a 2.9-fold reduction in risk for patients with wild-type heterozygous alleles (relative risk, 0.34; 95% confidence interval, 0.13-0.86).

Conclusions: TPMT genotype has a substantial impact on minimal residual disease after administration of mercaptopurine in the early course of childhood ALL, most likely through modulation of mercaptopurine dose intensity. Our findings support a role for minimal residual disease analyses in the assessment of genotype-phenotype associations in multiagent chemotherapeutic trials.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Antimetabolites, Antineoplastic / therapeutic use*
Child
Child, Preschool
Female
Genotype
Humans
Infant
Male
Mercaptopurine / therapeutic use*
Methyltransferases / genetics*
Neoplasm, Residual
Precursor Cell Lymphoblastic Leukemia-Lymphoma / drug therapy*
Precursor Cell Lymphoblastic Leukemia-Lymphoma / enzymology
Precursor Cell Lymphoblastic Leukemia-Lymphoma / genetics*
Prognosis

Substances

Antimetabolites, Antineoplastic
Mercaptopurine
Methyltransferases
thiopurine methyltransferase