Thiopurine Methyltransferase Pharmacogenetics: Human Gene Cloning and Characterization of a Common Polymorphism

Abstract: Thiopurine methyltransferase (TPMT) catalyzes the S-methylation of thiopurine drugs. Individual variation in the toxicity and therapeutic efficacy of these drugs is associated with a common genetic polymorphism that controls levels of TPMT activity and immunoreactive protein in human tissues. Because of the clinical significance of the "pharmacogenetic" regulation of this enzyme, it would be important to clone the gene for TPMT in humans and to study the molecular basis for the genetic polymorphism. As a first… Show more

“…Furthermore, as pointed out previously, there is a strong correlation between relative levels of TPMT activity in the RBC and in other human tissues (Woodson et al, 1982;Szumlanski et al, 1992). Following the cloning of the TPMT gene and characterization of its most important polymorphisms (Szumlanski et al, 1996;Tai et al, 1996), determination of TPMT genotype was also shown to be useful for individualizing thiopurine drug therapy. However, both genotyping and phenotyping have their limitations.…”

“…Of the allozymes studied by Salavaggione et al (2005), TPMT*3A, *3B, *3C and *2 displayed the most striking effects. This phenomenon was first observed a decade ago when TPMT*3A, *3B and *3C were initially described (Szumlanski et al, 1996). In the course of those early experiments, these three allozymes, as well as WT TPMT, were expressed in COS-1 cells, and Western blot analysis was performed.…”

“…Levels of TPMT activity in the RBC reflect relative levels of that enzyme in the kidney, liver and lymphocyte (Van Loon and Weinshilboum, 1982;Woodson et al, 1982;Szumlanski et al, 1992;Coulthard et al, 1998). After the human TPMT cDNA and gene had been cloned and characterized (Honchel et al, 1993;Szumlanski et al, 1996;Tai et al, 1996), these phenotypic variations were shown to result primarily from variation in the sequence of the TPMT gene itself. A total of 21 TPMT genetic polymorphisms have been identified which are, or may be associated with decreased levels of TPMT enzyme activity and/or thiopurine drug-induced toxicity .…”

“…A total of 21 TPMT genetic polymorphisms have been identified which are, or may be associated with decreased levels of TPMT enzyme activity and/or thiopurine drug-induced toxicity . Eighteen of those polymorphisms (*2, *3A, *3B, *3C, *5-*14 and *16-*19) involve nonsynonymous coding single-nucleotide polymorphisms (cSNPs) (Krynetski et al, 1995;Szumlanski et al, 1996;Otterness et al, 1997;Lindqvist et al, 2004;Schaeffeler et al, 2004;Hamdan-Khalil et al, 2005), that is, alterations in single DNA nucleotides that alter the encoded amino acid. The *14 SNP disrupts the translation initiation codon (Lindqvist et al, 2004) and prevents translation of the enzyme protein , while *4 and *15 involve alterations in canonical mRNA splice site sequences (Otterness et al, 1998;Lindqvist et al, 2004) and *3D contains a premature stop codon (Otterness et al, 1997).…”

“…TPMT *3C, the most common functionally significant variant allele in East Asia (frequency approximately 2%), includes only the codon 240 SNP, and the rare TPMT *3B allele has only the codon 154 SNP (Figure 2) (Szumlanski et al, 1996). The presence of TPMT*3A and *3B result in a virtual lack of TPMT enzyme activity and protein in the tissues of subjects who carry these alleles and, as a result, patients homozygous for these alleles can suffer severe, life-threatening myelosuppression when treated with standard doses of thiopurines, that is, they are 'overdosed' on standard doses (Lennard et al, 1989(Lennard et al, , 1990Evans et al, 1991).…”

Thiopurine S-methyltransferase pharmacogenetics: insights, challenges and future directions

“…Furthermore, as pointed out previously, there is a strong correlation between relative levels of TPMT activity in the RBC and in other human tissues (Woodson et al, 1982;Szumlanski et al, 1992). Following the cloning of the TPMT gene and characterization of its most important polymorphisms (Szumlanski et al, 1996;Tai et al, 1996), determination of TPMT genotype was also shown to be useful for individualizing thiopurine drug therapy. However, both genotyping and phenotyping have their limitations.…”

“…Of the allozymes studied by Salavaggione et al (2005), TPMT*3A, *3B, *3C and *2 displayed the most striking effects. This phenomenon was first observed a decade ago when TPMT*3A, *3B and *3C were initially described (Szumlanski et al, 1996). In the course of those early experiments, these three allozymes, as well as WT TPMT, were expressed in COS-1 cells, and Western blot analysis was performed.…”

“…Levels of TPMT activity in the RBC reflect relative levels of that enzyme in the kidney, liver and lymphocyte (Van Loon and Weinshilboum, 1982;Woodson et al, 1982;Szumlanski et al, 1992;Coulthard et al, 1998). After the human TPMT cDNA and gene had been cloned and characterized (Honchel et al, 1993;Szumlanski et al, 1996;Tai et al, 1996), these phenotypic variations were shown to result primarily from variation in the sequence of the TPMT gene itself. A total of 21 TPMT genetic polymorphisms have been identified which are, or may be associated with decreased levels of TPMT enzyme activity and/or thiopurine drug-induced toxicity .…”

“…A total of 21 TPMT genetic polymorphisms have been identified which are, or may be associated with decreased levels of TPMT enzyme activity and/or thiopurine drug-induced toxicity . Eighteen of those polymorphisms (*2, *3A, *3B, *3C, *5-*14 and *16-*19) involve nonsynonymous coding single-nucleotide polymorphisms (cSNPs) (Krynetski et al, 1995;Szumlanski et al, 1996;Otterness et al, 1997;Lindqvist et al, 2004;Schaeffeler et al, 2004;Hamdan-Khalil et al, 2005), that is, alterations in single DNA nucleotides that alter the encoded amino acid. The *14 SNP disrupts the translation initiation codon (Lindqvist et al, 2004) and prevents translation of the enzyme protein , while *4 and *15 involve alterations in canonical mRNA splice site sequences (Otterness et al, 1998;Lindqvist et al, 2004) and *3D contains a premature stop codon (Otterness et al, 1997).…”

“…TPMT *3C, the most common functionally significant variant allele in East Asia (frequency approximately 2%), includes only the codon 240 SNP, and the rare TPMT *3B allele has only the codon 154 SNP (Figure 2) (Szumlanski et al, 1996). The presence of TPMT*3A and *3B result in a virtual lack of TPMT enzyme activity and protein in the tissues of subjects who carry these alleles and, as a result, patients homozygous for these alleles can suffer severe, life-threatening myelosuppression when treated with standard doses of thiopurines, that is, they are 'overdosed' on standard doses (Lennard et al, 1989(Lennard et al, , 1990Evans et al, 1991).…”

Thiopurine S-methyltransferase pharmacogenetics: insights, challenges and future directions

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