Circulating Metabolites and Survival Among Patients With Pancreatic Cancer.
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Abstract | BACKGROUND: Pancreatic tumors cause changes in whole-body metabolism, but whether prediagnostic circulating metabolites predict survival is unknown. METHODS: We measured 82 metabolites by liquid chromatography-mass spectrometry in prediagnostic plasma from 484 pancreatic cancer case patients enrolled in four prospective cohort studies. Association of metabolites with survival was evaluated using Cox proportional hazards models adjusted for age, cohort, race/ethnicity, cancer stage, fasting time, and diagnosis year. After multiple-hypothesis testing correction, a P value of .0006 or less (.05/82) was considered statistically significant. Based on the results, we evaluated 33 tagging single-nucleotide polymorphisms (SNPs) in the ACO1 gene, requiring a P value of less than .002 (.05/33) for statistical significance. All statistical tests were two-sided. RESULTS: Two metabolites in the tricarboxylic acid (TCA) cycle--isocitrate and aconitate--were statistically significantly associated with survival. Participants in the highest vs lowest quintile had hazard ratios (HRs) for death of 1.89 (95% confidence interval [CI] = 1.06 to 3.35, Ptrend .001) for isocitrate and 2.54 (95% CI = 1.42 to 4.54, Ptrend .001) for aconitate. Isocitrate is interconverted with citrate via the intermediate aconitate in a reaction catalyzed by the enzyme aconitase 1 (ACO1). Therefore, we investigated the citrate to aconitate plus isocitrate ratio and SNPs in the ACO1 gene. The ratio was strongly associated with survival (P trend .001) as was the SNP rs7874815 in the ACO1 gene (hazard ratio for death per minor allele = 1.37, 95% CI = 1.16 to 1.61, P .001). Patients had an approximately three-fold hazard for death when possessing one or more minor alleles at rs7874851 and high aconitate or isocitrate. CONCLUSIONS: Prediagnostic circulating levels of TCA cycle intermediates and inherited ACO1 genotypes were associated with survival among patients with pancreatic cancer. |
Year of Publication | 2016
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Journal | J Natl Cancer Inst
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Volume | 108
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Issue | 6
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Pages | djv409
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Date Published | 2016 Jun
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ISSN | 1460-2105
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DOI | 10.1093/jnci/djv409
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PubMed ID | 26755275
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PubMed Central ID | PMC4849356
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Grant list | 32105-6 / PHS HHS / United States
R35 CA197449 / CA / NCI NIH HHS / United States
T32 GM007287 / GM / NIGMS NIH HHS / United States
N01WH22110 / WH / WHI NIH HHS / United States
CA130288 / CA / NCI NIH HHS / United States
F30 CA183474 / CA / NCI NIH HHS / United States
CA 97193 / CA / NCI NIH HHS / United States
HL 26490 / HL / NHLBI NIH HHS / United States
42107-26 / PHS HHS / United States
32115 / PHS HHS / United States
R01 CA49449 / CA / NCI NIH HHS / United States
32100-2 / PHS HHS / United States
24152 / PHS HHS / United States
HL 34595 / HL / NHLBI NIH HHS / United States
R01 CA124908 / CA / NCI NIH HHS / United States
CA 40360 / CA / NCI NIH HHS / United States
42129-32 / PHS HHS / United States
NIH R01 CA124908 / CA / NCI NIH HHS / United States
CA 34944 / CA / NCI NIH HHS / United States
P01 CA87969 / CA / NCI NIH HHS / United States
32118-32119 / PHS HHS / United States
UM1 CA167552 / CA / NCI NIH HHS / United States
32108-9 / PHS HHS / United States
Howard Hughes Medical Institute / United States
NIH P50 CA127003 / CA / NCI NIH HHS / United States
UM1 CA186107 / CA / NCI NIH HHS / United States
32122 / PHS HHS / United States
44221 / PHS HHS / United States
P50 CA127003 / CA / NCI NIH HHS / United States
32111-13 / PHS HHS / United States
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