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Metabonomic Variations Associated with AOM-Induced Precancerous Colorectal Lesions and Resveratrol Treatment 期刊论文

编号：

44186afb-01eb-431f-b511-042c5f4d348a
作者：

Liao, Wen#^[2]Wei, Hai(魏海)^[2]Wang, Xiaoyan^[3];Qiu, Yunping^[1];Gou, Xiaojun^[2];Zhang, Xiaolei(张晓雷)^[2]Zhou, Mingmei(周明眉)^[2]Wu, Jianbing^[2];Wu, Tao^[2];Kou, Fang(寇芳)^[2]Zhang, Yongyu(张永煜)^[2]Bian, Zhaoxiang^[4];Xie, Guoxiang*^[1]Jia, Wei(贾伟)*^[1,2]
语种：

英文
期刊：

JOURNAL OF PROTEOME RESEARCH ISSN：1535-3893 2012 年 11 卷 6 期 (3436 - 3448) ; JUN
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关键词：

colorectal cancer azoxymethane AOM resveratrol gas chromatography time-of-flight mass spectrometry GC-TOFMS metabonomics
摘要：

Resveratrol (Res), 3,5,4'-trihydroxy-trans-stilbene, is an antioxidant found in the skin of red grapes and in several other plants. This phenolic compound has been recently reported to possess cancer chemopreventive activity that inhibits the process of carcinogenesis. However, the mechanisms underlying its anticancer effects remain largely unresolved. In this study, we investigated the chemoprotective effects of dietary Res in an azoxymethane (AOM) induced precancerous colorectal lesion model in male Wistar rats. The metabolic alterations in urine, sera, and colonic tissues of experimental rats perturbed by AOM intervention as well as the Res treatment were measured by a gas chromatography time-of-flight mass spectrometry (GC-TOFMS) analysis. Significant alterations of metabolites were observed in AOM group in urine, sera, and colonic tissues, which were attenuated by Res treatment and concurrent with the histopathological improvement with significantly decreased aberrant crypt foci (ACF) incidence. Representative metabolites include depleted glucose, beta-hydroxybutyrate (ketone body), hypoxanthine, and elevated branched chain amino acids (isoleucine and valine) and tryptophan in colonic tissue, as well as elevated serum aminooxyacetate and urinary 4-hydroxyphenylacetate and xanthurenate. These metabolic changes suggest that the preventive effect of Res is associated with attenuation of impaired glucose and lipid metabolism and elevated protein breakdown in colonic tissues from AOM-exposed rats. It also appears that Res induced significant metabolic alterations independent of the AOM-induced metabolic changes. The significantly altered metabolites identified in Res-AOM group relative to AOM group include arachidonate, linoleate, glutamate, docosahexaenoate, palmitelaidate, 2-aminobutyrate, pyroglutamate, and threonate, all of which are involved in inflammation and oxidation processes. This suggests that Res exerts the chemopreventive effects on ACE formation by anti-inflammatory and antioxidant mechanisms in addition to amelioration of AOM-induced mitochondrial disruption.
推荐引用方式
GB/T 7714：

Liao Wen,Wei Hai,Wang Xiaoyan, et al. Metabonomic Variations Associated with AOM-Induced Precancerous Colorectal Lesions and Resveratrol Treatment [J].JOURNAL OF PROTEOME RESEARCH,2012,11(6):3436-3448.
APA：

Liao Wen,Wei Hai,Wang Xiaoyan,Qiu Yunping,&Jia Wei.(2012).Metabonomic Variations Associated with AOM-Induced Precancerous Colorectal Lesions and Resveratrol Treatment .JOURNAL OF PROTEOME RESEARCH,11(6):3436-3448.
MLA：

Liao Wen, et al. "Metabonomic Variations Associated with AOM-Induced Precancerous Colorectal Lesions and Resveratrol Treatment" .JOURNAL OF PROTEOME RESEARCH 11,6(2012):3436-3448.
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