COMT genotype, micronutrients in the folate metabolic pathway and breast cancer risk

doi:10.1093/carcin/22.10.1661

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Carcinogenesis, Vol. 22, No. 10, 1661-1665, October 2001
© 2001 Oxford University Press

MOLECULAR EPIDEMIOLOGY AND CANCER PREVENTION

COMT genotype, micronutrients in the folate metabolic pathway and breast cancer risk

Julie E. Goodman¹, Jackie A. Lavigne³, Kana Wu², Kathy J. Helzlsouer², Paul T. Strickland¹, Jacob Selhub⁴ and James D. Yager¹^,5

¹ Department of Environmental Health Sciences and
² Department of Epidemiology, Johns Hopkins University, Bloomberg School of Public Health, Baltimore, MD 21205,
³ Division of Cancer Prevention, National Cancer Institute, Bethesda, MD 20892 and
⁴ Jean Mayer US Department of Agriculture Human Nutrition Research Center on Aging, Department of Vitamin Bioavailability, Tufts University, Boston, MA 02111, USA

Catechol-O-methyltransferase (COMT) catalyzes the O-methylationof catechol estrogens (CEs), using S-adenosylmethionine (SAM)as a methyl donor. Several studies have indicated that the val108metCOMT polymorphism, which results in a 3–4-fold decreasein activity, is associated with increased breast cancer risk.Folate, whose intake levels have also been associated with breastcancer risk, and other micronutrients in the folate metabolicpathway influence levels of SAM and S-adenosylhomocysteine (SAH),a COMT inhibitor generated by the demethylation of SAM. Becausethese micronutrients have been shown to alter SAM and SAH levels,we hypothesized that they could also affect COMT-catalyzed CEmethylation. Although measurements of SAM and SAH were not initiallycollected, a secondary analysis of data from two nested case-controlstudies was performed to examine whether serum levels of folate,vitamin B12 (B12), pyridoxal 5'-phosphate (PLP), cysteine andhomocysteine, in conjunction with COMT genotype, were associatedwith breast cancer risk. COMT^HH (high activity COMT homozygote)breast cancer cases had statistically significantly lower levelsof homocysteine (P = 0.05) and cysteine (P = 0.04) and higherlevels of PLP (P = 0.02) than COMT^HH controls. In contrast,COMT^LL (low activity COMT homozygote) cases had higher levelsof homocysteine than COMT^LL controls (P = 0.05). No associationswere seen between B12, COMT genotype, and breast cancer risk.An increasing number of COMT^L alleles was significantly associatedwith increased breast cancer risk in women with below medianlevels of folate (P_trend = 0.05) or above median levels of homocysteine(P_trend = 0.02). These findings are consistent with a role forcertain folate pathway micronutrients in mediating the associationbetween COMT genotype and breast cancer risk.

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