Polymorphic MLH1 and risk of cancer after methylating chemotherapy for Hodgkin lymphoma

L J Worrillow; A G Smith; K Scott; M Andersson; A J Ashcroft; G M Dores; B Glimelius; E Holowaty; G H Jackson; G L Jones; C F Lynch; G Morgan; E Pukkala; D Scott; H H Storm; P R Taylor; M Vyberg; E Willett; L B Travis; J M Allan

doi:10.1136/jmg.2007.053850

Polymorphic MLH1 and risk of cancer after methylating chemotherapy for Hodgkin lymphoma

L J Worrillow, A G Smith, K Scott, M Andersson, A J Ashcroft, G M Dores, B Glimelius, E Holowaty, G H Jackson, G L Jones, C F Lynch, G Morgan, E Pukkala, D Scott, H H Storm, P R Taylor, M Vyberg, E Willett, L B Travis, J M Allan

Research output: Contribution to journal › Journal article › Research › peer-review

41 Citations (Scopus)

Abstract

BACKGROUND AND OBJECTIVE: Methylating agents are effective chemotherapy agents for Hodgkin lymphoma, but are associated with the development of second primary cancers. Cytotoxicity of methylating agents is mediated primarily by the DNA mismatch repair (MMR) system. Loss of MLH1, a major component of DNA MMR, results in tolerance to the cytotoxic effects of methylating agents and persistence of mutagenised cells at high risk of malignant transformation. We hypothesised that a common substitution in the basal promoter of MLH1 (position -93, rs1800734) modifies the risk of cancer after methylating chemotherapy. METHODS: 133 patients who developed cancer following chemotherapy and/or radiotherapy (n = 133), 420 patients diagnosed with de novo myeloid leukaemia, 242 patients diagnosed with primary Hodgkin lymphoma, and 1177 healthy controls were genotyped for the MLH1 -93 polymorphism by allelic discrimination polymerase chain reaction (PCR) and restriction fragment length polymorphism assay. Odds ratios and 95% confidence intervals for cancer risk by MLH1 -93 polymorphism status, and stratified by previous exposure to methylating chemotherapy, were calculated using unconditional logistic regression. RESULTS: Carrier frequency of the MLH1 -93 variant was higher in patients who developed therapy related acute myeloid leukaemia (t-AML) (75.0%, n = 12) or breast cancer (53.3%. n = 15) after methylating chemotherapy for Hodgkin lymphoma compared to patients without previous methylating exposure (t-AML, 30.4%, n = 69; breast cancer patients, 27.2%, n = 22). The MLH1 -93 variant allele was also over-represented in t-AML cases when compared to de novo AML cases (36.9%, n = 420) and healthy controls (36.3%, n = 952), and was associated with a significantly increased risk of developing t-AML (odds ratio 5.31, 95% confidence interval 1.40 to 20.15), but only in patients previously treated with a methylating agent. CONCLUSIONS: These data support the hypothesis that the common polymorphism at position -93 in the core promoter of MLH1 defines a risk allele for the development of cancer after methylating chemotherapy for Hodgkin lymphoma. However, replication of this finding in larger studies is suggested.

Original language	English
Journal	Journal of Medical Genetics
Volume	45
Pages (from-to)	142-6
Number of pages	4
ISSN	1468-6244
DOIs	https://doi.org/10.1136/jmg.2007.053850
Publication status	Published - 2008
Externally published	Yes

Keywords

Adaptor Proteins, Signal Transducing
Adolescent
Adult
Aged
Alleles
Antineoplastic Agents, Alkylating
Base Sequence
Case-Control Studies
DNA Methylation
DNA Primers
DNA Repair
Female
Hodgkin Disease
Humans
Leukemia, Myeloid, Acute
Male
Middle Aged
Neoplasms, Second Primary
Nuclear Proteins
Polymorphism, Genetic
Promoter Regions, Genetic
Risk Factors

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Worrillow, L. J., Smith, A. G., Scott, K., Andersson, M., Ashcroft, A. J., Dores, G. M., Glimelius, B., Holowaty, E., Jackson, G. H., Jones, G. L., Lynch, C. F., Morgan, G., Pukkala, E., Scott, D., Storm, H. H., Taylor, P. R., Vyberg, M., Willett, E., Travis, L. B., & Allan, J. M. (2008). Polymorphic MLH1 and risk of cancer after methylating chemotherapy for Hodgkin lymphoma. Journal of Medical Genetics, 45, 142-6. https://doi.org/10.1136/jmg.2007.053850

@article{005b91c3d0904a7597497eac93a6faec,

title = "Polymorphic MLH1 and risk of cancer after methylating chemotherapy for Hodgkin lymphoma",

abstract = "BACKGROUND AND OBJECTIVE: Methylating agents are effective chemotherapy agents for Hodgkin lymphoma, but are associated with the development of second primary cancers. Cytotoxicity of methylating agents is mediated primarily by the DNA mismatch repair (MMR) system. Loss of MLH1, a major component of DNA MMR, results in tolerance to the cytotoxic effects of methylating agents and persistence of mutagenised cells at high risk of malignant transformation. We hypothesised that a common substitution in the basal promoter of MLH1 (position -93, rs1800734) modifies the risk of cancer after methylating chemotherapy. METHODS: 133 patients who developed cancer following chemotherapy and/or radiotherapy (n = 133), 420 patients diagnosed with de novo myeloid leukaemia, 242 patients diagnosed with primary Hodgkin lymphoma, and 1177 healthy controls were genotyped for the MLH1 -93 polymorphism by allelic discrimination polymerase chain reaction (PCR) and restriction fragment length polymorphism assay. Odds ratios and 95% confidence intervals for cancer risk by MLH1 -93 polymorphism status, and stratified by previous exposure to methylating chemotherapy, were calculated using unconditional logistic regression. RESULTS: Carrier frequency of the MLH1 -93 variant was higher in patients who developed therapy related acute myeloid leukaemia (t-AML) (75.0%, n = 12) or breast cancer (53.3%. n = 15) after methylating chemotherapy for Hodgkin lymphoma compared to patients without previous methylating exposure (t-AML, 30.4%, n = 69; breast cancer patients, 27.2%, n = 22). The MLH1 -93 variant allele was also over-represented in t-AML cases when compared to de novo AML cases (36.9%, n = 420) and healthy controls (36.3%, n = 952), and was associated with a significantly increased risk of developing t-AML (odds ratio 5.31, 95% confidence interval 1.40 to 20.15), but only in patients previously treated with a methylating agent. CONCLUSIONS: These data support the hypothesis that the common polymorphism at position -93 in the core promoter of MLH1 defines a risk allele for the development of cancer after methylating chemotherapy for Hodgkin lymphoma. However, replication of this finding in larger studies is suggested.",

keywords = "Adaptor Proteins, Signal Transducing, Adolescent, Adult, Aged, Alleles, Antineoplastic Agents, Alkylating, Base Sequence, Case-Control Studies, DNA Methylation, DNA Primers, DNA Repair, Female, Hodgkin Disease, Humans, Leukemia, Myeloid, Acute, Male, Middle Aged, Neoplasms, Second Primary, Nuclear Proteins, Polymorphism, Genetic, Promoter Regions, Genetic, Risk Factors",

author = "Worrillow, {L J} and Smith, {A G} and K Scott and M Andersson and Ashcroft, {A J} and Dores, {G M} and B Glimelius and E Holowaty and Jackson, {G H} and Jones, {G L} and Lynch, {C F} and G Morgan and E Pukkala and D Scott and Storm, {H H} and Taylor, {P R} and M Vyberg and E Willett and Travis, {L B} and Allan, {J M}",

year = "2008",

doi = "10.1136/jmg.2007.053850",

language = "English",

volume = "45",

pages = "142--6",

journal = "Journal of Medical Genetics",

issn = "1468-6244",

publisher = "B M J Group",

}

Worrillow, LJ, Smith, AG, Scott, K, Andersson, M, Ashcroft, AJ, Dores, GM, Glimelius, B, Holowaty, E, Jackson, GH, Jones, GL, Lynch, CF, Morgan, G, Pukkala, E, Scott, D, Storm, HH, Taylor, PR, Vyberg, M, Willett, E, Travis, LB & Allan, JM 2008, 'Polymorphic MLH1 and risk of cancer after methylating chemotherapy for Hodgkin lymphoma', Journal of Medical Genetics, vol. 45, pp. 142-6. https://doi.org/10.1136/jmg.2007.053850

TY - JOUR

T1 - Polymorphic MLH1 and risk of cancer after methylating chemotherapy for Hodgkin lymphoma

AU - Worrillow, L J

AU - Smith, A G

AU - Scott, K

AU - Andersson, M

AU - Ashcroft, A J

AU - Dores, G M

AU - Glimelius, B

AU - Holowaty, E

AU - Jackson, G H

AU - Jones, G L

AU - Lynch, C F

AU - Morgan, G

AU - Pukkala, E

AU - Scott, D

AU - Storm, H H

AU - Taylor, P R

AU - Vyberg, M

AU - Willett, E

AU - Travis, L B

AU - Allan, J M

PY - 2008

Y1 - 2008

N2 - BACKGROUND AND OBJECTIVE: Methylating agents are effective chemotherapy agents for Hodgkin lymphoma, but are associated with the development of second primary cancers. Cytotoxicity of methylating agents is mediated primarily by the DNA mismatch repair (MMR) system. Loss of MLH1, a major component of DNA MMR, results in tolerance to the cytotoxic effects of methylating agents and persistence of mutagenised cells at high risk of malignant transformation. We hypothesised that a common substitution in the basal promoter of MLH1 (position -93, rs1800734) modifies the risk of cancer after methylating chemotherapy. METHODS: 133 patients who developed cancer following chemotherapy and/or radiotherapy (n = 133), 420 patients diagnosed with de novo myeloid leukaemia, 242 patients diagnosed with primary Hodgkin lymphoma, and 1177 healthy controls were genotyped for the MLH1 -93 polymorphism by allelic discrimination polymerase chain reaction (PCR) and restriction fragment length polymorphism assay. Odds ratios and 95% confidence intervals for cancer risk by MLH1 -93 polymorphism status, and stratified by previous exposure to methylating chemotherapy, were calculated using unconditional logistic regression. RESULTS: Carrier frequency of the MLH1 -93 variant was higher in patients who developed therapy related acute myeloid leukaemia (t-AML) (75.0%, n = 12) or breast cancer (53.3%. n = 15) after methylating chemotherapy for Hodgkin lymphoma compared to patients without previous methylating exposure (t-AML, 30.4%, n = 69; breast cancer patients, 27.2%, n = 22). The MLH1 -93 variant allele was also over-represented in t-AML cases when compared to de novo AML cases (36.9%, n = 420) and healthy controls (36.3%, n = 952), and was associated with a significantly increased risk of developing t-AML (odds ratio 5.31, 95% confidence interval 1.40 to 20.15), but only in patients previously treated with a methylating agent. CONCLUSIONS: These data support the hypothesis that the common polymorphism at position -93 in the core promoter of MLH1 defines a risk allele for the development of cancer after methylating chemotherapy for Hodgkin lymphoma. However, replication of this finding in larger studies is suggested.

AB - BACKGROUND AND OBJECTIVE: Methylating agents are effective chemotherapy agents for Hodgkin lymphoma, but are associated with the development of second primary cancers. Cytotoxicity of methylating agents is mediated primarily by the DNA mismatch repair (MMR) system. Loss of MLH1, a major component of DNA MMR, results in tolerance to the cytotoxic effects of methylating agents and persistence of mutagenised cells at high risk of malignant transformation. We hypothesised that a common substitution in the basal promoter of MLH1 (position -93, rs1800734) modifies the risk of cancer after methylating chemotherapy. METHODS: 133 patients who developed cancer following chemotherapy and/or radiotherapy (n = 133), 420 patients diagnosed with de novo myeloid leukaemia, 242 patients diagnosed with primary Hodgkin lymphoma, and 1177 healthy controls were genotyped for the MLH1 -93 polymorphism by allelic discrimination polymerase chain reaction (PCR) and restriction fragment length polymorphism assay. Odds ratios and 95% confidence intervals for cancer risk by MLH1 -93 polymorphism status, and stratified by previous exposure to methylating chemotherapy, were calculated using unconditional logistic regression. RESULTS: Carrier frequency of the MLH1 -93 variant was higher in patients who developed therapy related acute myeloid leukaemia (t-AML) (75.0%, n = 12) or breast cancer (53.3%. n = 15) after methylating chemotherapy for Hodgkin lymphoma compared to patients without previous methylating exposure (t-AML, 30.4%, n = 69; breast cancer patients, 27.2%, n = 22). The MLH1 -93 variant allele was also over-represented in t-AML cases when compared to de novo AML cases (36.9%, n = 420) and healthy controls (36.3%, n = 952), and was associated with a significantly increased risk of developing t-AML (odds ratio 5.31, 95% confidence interval 1.40 to 20.15), but only in patients previously treated with a methylating agent. CONCLUSIONS: These data support the hypothesis that the common polymorphism at position -93 in the core promoter of MLH1 defines a risk allele for the development of cancer after methylating chemotherapy for Hodgkin lymphoma. However, replication of this finding in larger studies is suggested.

KW - Adaptor Proteins, Signal Transducing

KW - Adolescent

KW - Adult

KW - Aged

KW - Alleles

KW - Antineoplastic Agents, Alkylating

KW - Base Sequence

KW - Case-Control Studies

KW - DNA Methylation

KW - DNA Primers

KW - DNA Repair

KW - Female

KW - Hodgkin Disease

KW - Humans

KW - Leukemia, Myeloid, Acute

KW - Male

KW - Middle Aged

KW - Neoplasms, Second Primary

KW - Nuclear Proteins

KW - Polymorphism, Genetic

KW - Promoter Regions, Genetic

KW - Risk Factors

U2 - 10.1136/jmg.2007.053850

DO - 10.1136/jmg.2007.053850

M3 - Journal article

SN - 1468-6244

VL - 45

SP - 142

EP - 146

JO - Journal of Medical Genetics

JF - Journal of Medical Genetics

ER -

Polymorphic MLH1 and risk of cancer after methylating chemotherapy for Hodgkin lymphoma

Abstract

Keywords

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