韩国男性膀胱癌发生前的代谢变化:一项来自 KCPS-II 队列的巢式病例对照研究。

IF 6 3区 医学 Q1 CELL BIOLOGY
Youngmin Han, Unchong Kim, Keum Ji Jung, Ji-Young Lee, Kwangbae Lee, Sang Yop Shin, Heejin Kimm, Sun Ha Jee
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引用次数: 0

摘要

背景:对韩国人膀胱癌(BLCA)的研究仍然缺乏,尤其是在预测BLCA方面。本研究旨在发现与膀胱癌发病相关的代谢特征,并确认其作为生物标志物的潜力:我们利用韩国癌症预防研究(KCPS)-II 设计了两项巢式病例对照研究。我们随机选取了年龄在35-69岁之间的男性,按招募机构分为两组[第一组,BLCA(n = 35)与对照组(n = 35);第二组,BLCA(n = 31)与对照组(n = 31)]。对基线血清样本进行非靶向代谢组学分析,并进行 OPLS-DA 和网络分析。所有 KCPS 参与者的 BLCA 遗传风险评分(GRS)计算结果用于解读代谢组学数据:结果:BLCA 组的关键代谢特征是赖氨酸代谢和色氨酸-吲哚代谢失调。此外,由反映这些代谢特征的代谢物(赖氨酸、色氨酸、吲哚、吲哚丙烯酸和吲哚乙醛)组成的预测模型显示出强大的 BLCA 预测能力(AUC:0.959 [0.929-0.989])。BLCA中GRS高组和GRS低组之间的代谢差异结果表明,BLCA的发病机制与遗传易感性有关。此外,利用 GRS 和五个重要代谢物建立的模型对 BLCA 的预测能力很强(AUC:0.990 [0.980-1.000]):结论:本研究显示的代谢特征可能与 BLCA 的发病机制密切相关。结论:本研究显示的代谢特征可能与 BLCA 的发病机制密切相关,其中涉及的代谢物可能是 BLCA 的预测性生物标志物。它可用于 BLCA 的早期诊断、预后诊断和治疗目标。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Metabolic changes preceding bladder cancer occurrence among Korean men: a nested case-control study from the KCPS-II cohort.

Background: Bladder cancer (BLCA) research in Koreans is still lacking, especially in focusing on the prediction of BLCA. The current study aimed to discover metabolic signatures related to BLCA onset and confirm its potential as a biomarker.

Methods: We designed two nested case-control studies using Korean Cancer Prevention Study (KCPS)-II. Only males aged 35-69 were randomly selected and divided into two sets by recruitment organizations [set 1, BLCA (n = 35) vs. control (n = 35); set 2, BLCA (n = 31) vs. control (n = 31)]. Baseline serum samples were analyzed by non-targeted metabolomics profiling, and OPLS-DA and network analysis were performed. Calculated genetic risk score (GRS) for BLCA from all KCPS participants was utilized for interpreting metabolomics data.

Results: Critical metabolic signatures shown in the BLCA group were dysregulation of lysine metabolism and tryptophan-indole metabolism. Furthermore, the prediction model consisting of metabolites (lysine, tryptophan, indole, indoleacrylic acid, and indoleacetaldehyde) reflecting these metabolic signatures showed mighty BLCA predictive power (AUC: 0.959 [0.929-0.989]). The results of metabolic differences between GRS-high and GRS-low groups in BLCA indicated that the pathogenesis of BLCA is associated with a genetic predisposition. Besides, the predictive ability for BLCA on the model using GRS and five significant metabolites was powerful (AUC: 0.990 [0.980-1.000]).

Conclusion: Metabolic signatures shown in the present research may be closely associated with BLCA pathogenesis. Metabolites involved in these could be predictive biomarkers for BLCA. It could be utilized for early diagnosis, prognostic diagnosis, and therapeutic targets for BLCA.

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来源期刊
自引率
1.70%
发文量
17
审稿时长
14 weeks
期刊介绍: Cancer & Metabolism welcomes studies on all aspects of the relationship between cancer and metabolism, including: -Molecular biology and genetics of cancer metabolism -Whole-body metabolism, including diabetes and obesity, in relation to cancer -Metabolomics in relation to cancer; -Metabolism-based imaging -Preclinical and clinical studies of metabolism-related cancer therapies.
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