Genes involved with folate uptake and distribution and their association with colorectal cancer risk

Jane C. Figueiredo; A. Joan Levine; Won H. Lee; David V. Conti; Jenny N. Poynter; Peter T. Campbell; David Duggan; Juan Pablo Lewinger; Maria Elena Martinez; Cornelia M. Ulrich; Polly Newcomb; John Potter; Paul J. Limburg; John Hopper; Mark A. Jenkins; Loic Le Marchand; John A. Baron; Robert W. Haile

doi:10.1007/s10552-009-9489-6

Genes involved with folate uptake and distribution and their association with colorectal cancer risk

Jane C. Figueiredo, A. Joan Levine, Won H. Lee, David V. Conti, Jenny N. Poynter, Peter T. Campbell, David Duggan, Juan Pablo Lewinger, Maria Elena Martinez, Cornelia M. Ulrich, Polly Newcomb, John Potter, Paul J. Limburg, John Hopper, Mark A. Jenkins, Loic Le Marchand, John A. Baron, Robert W. Haile

Research output: Contribution to journal › Article › peer-review

27 Scopus citations

Abstract

Folate status is an important predictor of colorectal cancer risk. Common genetic variants in genes involved in regulating cellular folate levels might also predict risk, but there are limited data on this issue. We conducted a family-based case-control association study of variants in four genes involved in folate uptake and distribution: FOLR1, FPGS, GGH and SLC19A1, using 1, 750 population-based and 245 clinic-based cases of pathologically confirmed colorectal cancer and their unaffected relatives participating in the Colon Cancer Family Registries. Standardized questionnaires, administered to all participants, collected information on risk factors and diet. Standard molecular techniques were used to determine microsatellite instability (MSI) status on cases. tagSNPs (n = 29) were selected based on coverage as assessed by pairwise r². We found no evidence that tagSNPs in these genes were associated with risk of colorectal cancer. For the SLC19A1-rs1051266 (G80A, Arg27His) missense polymorphism, the A/A genotype was not associated with risk of colorectal cancer using population-based (OR = 1.00; 95% CI = 0.81-1.23) or clinic-based (OR = 0.75; 95% CI = 0.44-1.29) families compared to the G/A and G/G genotypes. We found no evidence that the association between any tagSNP and CRC risk was modified by multivitamin use, folic acid use and dietary folate intake and total folate intake. The odds ratios were similar, irrespective of MSI status, tumor subsite and family history of colorectal cancer. In conclusion, we found no significant evidence that genetic variants in FOLR1, GGH, FPGS and SLC19A1 are associated with the risk of colorectal cancer.

Original language	English (US)
Pages (from-to)	597-608
Number of pages	12
Journal	Cancer Causes and Control
Volume	21
Issue number	4
DOIs	https://doi.org/10.1007/s10552-009-9489-6
State	Published - Apr 2010
Externally published	Yes

Keywords

Case-control
Clinic-based
Colorectal cancer
Folate
Folate receptor 1 (FOLR1)
Folylpolyglutamate synthase (FPGS)
Gamma-glutamyl hydrolase (GGH) family-based
Polymorphisms
Population-based
Reduced folate carrier (RFC)
Solute carrier family 19 (SLC19A1)

ASJC Scopus subject areas

Oncology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1007/s10552-009-9489-6

Cite this

Figueiredo, J. C., Levine, A. J., Lee, W. H., Conti, D. V., Poynter, J. N., Campbell, P. T., Duggan, D., Lewinger, J. P., Martinez, M. E., Ulrich, C. M., Newcomb, P., Potter, J., Limburg, P. J., Hopper, J., Jenkins, M. A., Le Marchand, L., Baron, J. A., & Haile, R. W. (2010). Genes involved with folate uptake and distribution and their association with colorectal cancer risk. Cancer Causes and Control, 21(4), 597-608. https://doi.org/10.1007/s10552-009-9489-6

Figueiredo, JC, Levine, AJ, Lee, WH, Conti, DV, Poynter, JN, Campbell, PT, Duggan, D, Lewinger, JP, Martinez, ME, Ulrich, CM, Newcomb, P, Potter, J, Limburg, PJ, Hopper, J, Jenkins, MA, Le Marchand, L, Baron, JA & Haile, RW 2010, 'Genes involved with folate uptake and distribution and their association with colorectal cancer risk', Cancer Causes and Control, vol. 21, no. 4, pp. 597-608. https://doi.org/10.1007/s10552-009-9489-6

@article{60e096e209914df3a2fcd70c180a443b,

title = "Genes involved with folate uptake and distribution and their association with colorectal cancer risk",

abstract = "Folate status is an important predictor of colorectal cancer risk. Common genetic variants in genes involved in regulating cellular folate levels might also predict risk, but there are limited data on this issue. We conducted a family-based case-control association study of variants in four genes involved in folate uptake and distribution: FOLR1, FPGS, GGH and SLC19A1, using 1, 750 population-based and 245 clinic-based cases of pathologically confirmed colorectal cancer and their unaffected relatives participating in the Colon Cancer Family Registries. Standardized questionnaires, administered to all participants, collected information on risk factors and diet. Standard molecular techniques were used to determine microsatellite instability (MSI) status on cases. tagSNPs (n = 29) were selected based on coverage as assessed by pairwise r2. We found no evidence that tagSNPs in these genes were associated with risk of colorectal cancer. For the SLC19A1-rs1051266 (G80A, Arg27His) missense polymorphism, the A/A genotype was not associated with risk of colorectal cancer using population-based (OR = 1.00; 95% CI = 0.81-1.23) or clinic-based (OR = 0.75; 95% CI = 0.44-1.29) families compared to the G/A and G/G genotypes. We found no evidence that the association between any tagSNP and CRC risk was modified by multivitamin use, folic acid use and dietary folate intake and total folate intake. The odds ratios were similar, irrespective of MSI status, tumor subsite and family history of colorectal cancer. In conclusion, we found no significant evidence that genetic variants in FOLR1, GGH, FPGS and SLC19A1 are associated with the risk of colorectal cancer.",

keywords = "Case-control, Clinic-based, Colorectal cancer, Folate, Folate receptor 1 (FOLR1), Folylpolyglutamate synthase (FPGS), Gamma-glutamyl hydrolase (GGH) family-based, Polymorphisms, Population-based, Reduced folate carrier (RFC), Solute carrier family 19 (SLC19A1)",

author = "Figueiredo, {Jane C.} and Levine, {A. Joan} and Lee, {Won H.} and Conti, {David V.} and Poynter, {Jenny N.} and Campbell, {Peter T.} and David Duggan and Lewinger, {Juan Pablo} and Martinez, {Maria Elena} and Ulrich, {Cornelia M.} and Polly Newcomb and John Potter and Limburg, {Paul J.} and John Hopper and Jenkins, {Mark A.} and {Le Marchand}, Loic and Baron, {John A.} and Haile, {Robert W.}",

note = "Funding Information: Funding This work was supported by the National Cancer Institute, National Institutes of Health under RFA # CA-95-011 and through cooperative agreements with the Australasian Colorectal Cancer Family Registry (U01 CA097735), the USC Familial Colorectal Neoplasia Collaborative Group (U01 CA074799), the Mayo Clinic Cooperative Family Registry for Colon Cancer Studies (U01 CA074800), the Ontario Registry for Studies of Familial Colorectal Cancer (U01 CA074783), the Seattle Colorectal Cancer Family Registry (U01 CA074794), and the University of Hawaii Colorectal Cancer Family Registry (U01 CA074806) as well as NCI T32 CA009142 (JNP), NCI R01 CA112237 (RWH), NCI PO1 CA41108 (MEM), CA23074 (MEM) and CA95060 (MEM). P. T. C. and J. C. F. were supported in part by National Cancer Institute of Canada post-PhD Fellowships (#18735 and #17602).",

year = "2010",

month = apr,

doi = "10.1007/s10552-009-9489-6",

language = "English (US)",

volume = "21",

pages = "597--608",

journal = "Cancer Causes and Control",

issn = "0957-5243",

publisher = "Springer Netherlands",

number = "4",

}

TY - JOUR

T1 - Genes involved with folate uptake and distribution and their association with colorectal cancer risk

AU - Figueiredo, Jane C.

AU - Levine, A. Joan

AU - Lee, Won H.

AU - Conti, David V.

AU - Poynter, Jenny N.

AU - Campbell, Peter T.

AU - Duggan, David

AU - Lewinger, Juan Pablo

AU - Martinez, Maria Elena

AU - Ulrich, Cornelia M.

AU - Newcomb, Polly

AU - Potter, John

AU - Limburg, Paul J.

AU - Hopper, John

AU - Jenkins, Mark A.

AU - Le Marchand, Loic

AU - Baron, John A.

AU - Haile, Robert W.

N1 - Funding Information: Funding This work was supported by the National Cancer Institute, National Institutes of Health under RFA # CA-95-011 and through cooperative agreements with the Australasian Colorectal Cancer Family Registry (U01 CA097735), the USC Familial Colorectal Neoplasia Collaborative Group (U01 CA074799), the Mayo Clinic Cooperative Family Registry for Colon Cancer Studies (U01 CA074800), the Ontario Registry for Studies of Familial Colorectal Cancer (U01 CA074783), the Seattle Colorectal Cancer Family Registry (U01 CA074794), and the University of Hawaii Colorectal Cancer Family Registry (U01 CA074806) as well as NCI T32 CA009142 (JNP), NCI R01 CA112237 (RWH), NCI PO1 CA41108 (MEM), CA23074 (MEM) and CA95060 (MEM). P. T. C. and J. C. F. were supported in part by National Cancer Institute of Canada post-PhD Fellowships (#18735 and #17602).

PY - 2010/4

Y1 - 2010/4

N2 - Folate status is an important predictor of colorectal cancer risk. Common genetic variants in genes involved in regulating cellular folate levels might also predict risk, but there are limited data on this issue. We conducted a family-based case-control association study of variants in four genes involved in folate uptake and distribution: FOLR1, FPGS, GGH and SLC19A1, using 1, 750 population-based and 245 clinic-based cases of pathologically confirmed colorectal cancer and their unaffected relatives participating in the Colon Cancer Family Registries. Standardized questionnaires, administered to all participants, collected information on risk factors and diet. Standard molecular techniques were used to determine microsatellite instability (MSI) status on cases. tagSNPs (n = 29) were selected based on coverage as assessed by pairwise r2. We found no evidence that tagSNPs in these genes were associated with risk of colorectal cancer. For the SLC19A1-rs1051266 (G80A, Arg27His) missense polymorphism, the A/A genotype was not associated with risk of colorectal cancer using population-based (OR = 1.00; 95% CI = 0.81-1.23) or clinic-based (OR = 0.75; 95% CI = 0.44-1.29) families compared to the G/A and G/G genotypes. We found no evidence that the association between any tagSNP and CRC risk was modified by multivitamin use, folic acid use and dietary folate intake and total folate intake. The odds ratios were similar, irrespective of MSI status, tumor subsite and family history of colorectal cancer. In conclusion, we found no significant evidence that genetic variants in FOLR1, GGH, FPGS and SLC19A1 are associated with the risk of colorectal cancer.

AB - Folate status is an important predictor of colorectal cancer risk. Common genetic variants in genes involved in regulating cellular folate levels might also predict risk, but there are limited data on this issue. We conducted a family-based case-control association study of variants in four genes involved in folate uptake and distribution: FOLR1, FPGS, GGH and SLC19A1, using 1, 750 population-based and 245 clinic-based cases of pathologically confirmed colorectal cancer and their unaffected relatives participating in the Colon Cancer Family Registries. Standardized questionnaires, administered to all participants, collected information on risk factors and diet. Standard molecular techniques were used to determine microsatellite instability (MSI) status on cases. tagSNPs (n = 29) were selected based on coverage as assessed by pairwise r2. We found no evidence that tagSNPs in these genes were associated with risk of colorectal cancer. For the SLC19A1-rs1051266 (G80A, Arg27His) missense polymorphism, the A/A genotype was not associated with risk of colorectal cancer using population-based (OR = 1.00; 95% CI = 0.81-1.23) or clinic-based (OR = 0.75; 95% CI = 0.44-1.29) families compared to the G/A and G/G genotypes. We found no evidence that the association between any tagSNP and CRC risk was modified by multivitamin use, folic acid use and dietary folate intake and total folate intake. The odds ratios were similar, irrespective of MSI status, tumor subsite and family history of colorectal cancer. In conclusion, we found no significant evidence that genetic variants in FOLR1, GGH, FPGS and SLC19A1 are associated with the risk of colorectal cancer.

KW - Case-control

KW - Clinic-based

KW - Colorectal cancer

KW - Folate

KW - Folate receptor 1 (FOLR1)

KW - Folylpolyglutamate synthase (FPGS)

KW - Gamma-glutamyl hydrolase (GGH) family-based

KW - Polymorphisms

KW - Population-based

KW - Reduced folate carrier (RFC)

KW - Solute carrier family 19 (SLC19A1)

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DO - 10.1007/s10552-009-9489-6

M3 - Article

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AN - SCOPUS:77953293418

SN - 0957-5243

VL - 21

SP - 597

EP - 608

JO - Cancer Causes and Control

JF - Cancer Causes and Control

IS - 4

ER -

Genes involved with folate uptake and distribution and their association with colorectal cancer risk

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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