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Metabolomics and transcriptomics identify pathway differences between visceral and subcutaneous adipose tissue in colorectal cancer patients: the ColoCare study

机译:代谢组学和转录组学确定大肠癌患者内脏和皮下脂肪组织之间的途径差异:ColoCare研究

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>Background: Metabolic and transcriptomic differences between visceral adipose tissue (VAT) and subcutaneous adipose tissue (SAT) compartments, particularly in the context of obesity, may play a role in colorectal carcinogenesis. We investigated the differential functions of their metabolic compositions.>Objectives: Biochemical differences between adipose tissues (VAT compared with SAT) in patients with colorectal carcinoma (CRC) were investigated by using mass spectrometry metabolomics and gene expression profiling. Metabolite compositions were compared between VAT, SAT, and serum metabolites. The relation between patients’ tumor stage and metabolic profiles was assessed.>Design: Presurgery blood and paired VAT and SAT samples during tumor surgery were obtained from 59 CRC patients (tumor stages I–IV) of the ColoCare cohort. Gas chromatography time-of-flight mass spectrometry and liquid chromatography quadrupole time-of-flight mass spectrometry were used to measure 1065 metabolites in adipose tissue (333 identified compounds) and 1810 metabolites in serum (467 identified compounds). Adipose tissue gene expression was measured by using Illumina’s HumanHT-12 Expression BeadChips.>Results: Compared with SAT, VAT displayed elevated markers of inflammatory lipid metabolism, free arachidonic acid, phospholipases (PLA2G10), and prostaglandin synthesis–related enzymes (PTGD/PTGS2S). Plasmalogen concentrations were lower in VAT than in SAT, which was supported by lower gene expression of FAR1, the rate-limiting enzyme for ether-lipid synthesis in VAT. Serum sphingomyelin concentrations were inversely correlated (P = 0.0001) with SAT adipose triglycerides. Logistic regression identified lipids in patients’ adipose tissues, which were associated with CRC tumor stage.>Conclusions: As one of the first studies, we comprehensively assessed differences in metabolic, lipidomic, and transcriptomic profiles between paired human VAT and SAT and their association with CRC tumor stage. We identified markers of inflammation in VAT, which supports prior evidence regarding the role of visceral adiposity and cancer. This trial was registered at as .
机译:>背景:内脏脂肪组织(VAT)与皮下脂肪组织(SAT)隔室之间的代谢和转录组差异,特别是在肥胖的情况下,可能在结直肠癌的发生中起作用。我们研究了其代谢成分的差异功能。>目的:通过质谱代谢组学和基因表达谱分析,研究了结直肠癌(CRC)患者脂肪组织之间的生化差异(VAT与SAT相比)。比较了VAT,SAT和血清代谢产物之间的代谢产物组成。评估了患者肿瘤分期与代谢状况之间的关系。>设计:从ColoCare队列的59名CRC患者(术前I–IV期)中获得了术前血液以及配对的VAT和SAT样本。 。气相色谱飞行时间质谱法和液相色谱四极杆飞行时间质谱法用于测量脂肪组织中的1065种代谢物(333种已鉴定化合物)和血清中1810种代谢物(467种已鉴定化合物)。使用Illumina的HumanHT-12表达BeadChips测量脂肪组织的基因表达。>结果:与SAT相比,VAT显示出炎症脂质代谢,游离花生四烯酸,磷脂酶(PLA2G10)和前列腺素合成的标记物升高–相关酶(PTGD / PTGS2S)。 VAT中血浆中的血浆生成素浓度低于SAT中,这是由于FAR1基因的较低表达所支持的,FAR1是VAT中醚脂合成的限速酶。血清鞘磷脂浓度与SAT甘油三酸酯成反比(P = 0.0001)。 Logistic回归确定了患者脂肪组织中与CRC肿瘤分期相关的脂质。>结论:作为首批研究之一,我们全面评估了成对的人类VAT之间代谢,脂质组和转录组谱的差异和SAT及其与CRC肿瘤分期的关系。我们确定了增值税中的炎症标志物,这支持了关于内脏脂肪和癌症作用的先前证据。该审判的注册地址为。

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