前列腺癌中维生素 D 代谢活性相关生物效应及相应治疗靶点的探索

IF 3.9 2区 医学 Q2 NUTRITION & DIETETICS Nutrition & Metabolism Pub Date : 2024-04-02 DOI:10.1186/s12986-024-00791-2
Lei Ding, Yong Wang, Zhentao Tang, Chenbo Ni, Qian Zhang, Qidi Zhai, Chao Liang, Jie Li
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引用次数: 0

摘要

以往的研究明确表明,维生素 D(VD)代谢途径对前列腺癌(PCa)的预后和激素治疗的敏感性有重大影响。然而,其确切的内在机制仍不清楚。我们利用与 VD 合成和 VD 受体相关的基因,对 1045 例 PCa 患者进行了分子图谱分析。然后,我们确定了与患者分层密切相关的高度可变基因模块。随后,我们将这些模块与 PCa 和邻近癌旁组织之间的差异表达基因进行了交叉分析。经过单因素回归和 LASSO 回归等缜密程序,我们剔除了无关变量,构建了预后模型。在计算出的风险评分所定义的高危亚组中,我们分析了它们在细胞浸润、免疫状态、突变情况和药物敏感性方面的差异。最后,我们选择了载脂蛋白 E(APOE)作为进一步的实验探索对象,以评估其作为治疗靶点的潜力。本研究建立的预后模型具有值得称道的预测功效。我们观察到各种 T 细胞亚型浸润减少,抗原递呈细胞共刺激信号表达降低。突变分析表明,高危人群的 TP53 和 FOXA 基因突变频率较高。值得注意的是,药物敏感性分析表明,高危患者对针对 Bcl-2 和 MAPK 通路的分子抑制剂的反应性更高。最后,我们的研究还证实,APOE 会上调 PCa 细胞的增殖和侵袭能力,同时增强对雄激素受体拮抗剂治疗的耐受性。这项综合研究阐明了这一代谢途径协调 PCa 生物行为的潜在机制,研究结果有望推动 PCa 综合疗法的开发。
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Exploration of vitamin D metabolic activity-related biological effects and corresponding therapeutic targets in prostate cancer
Previous studies have unequivocally demonstrated that the vitamin D (VD) metabolism pathway significantly influences prognosis and sensitivity to hormone therapy in prostate cancer (PCa). However, the precise underlying mechanism remains unclear. We performed molecular profiling of 1045 PCa patients, leveraging genes linked to VD synthesis and VD receptors. We then identified highly variable gene modules with substantial associations with patient stratification. Subsequently, we intersected these modules with differentially expressed genes between PCa and adjacent paracancerous tissues. Following a meticulous process involving single-factor regression and LASSO regression to eliminate extraneous variables and construct a prognostic model. Within the high-risk subgroup defined by the calculated risk score, we analyzed their differences in cell infiltration, immune status, mutation landscape, and drug sensitivity. Finally, we selected Apolipoprotein E (APOE), which featured prominently in this model for further experimental exploration to evaluate its potential as a therapeutic target. The prognostic model established in this study had commendable predictive efficacy. We observed diminished infiltration of various T-cell subtypes and reduced expression of co-stimulatory signals from antigen-presenting cells. Mutation analysis revealed that the high-risk cohort harbored a higher frequency of mutations in the TP53 and FOXA genes. Notably, drug sensitivity analysis suggested the heightened responsiveness of high-risk patients to molecular inhibitors targeting the Bcl-2 and MAPK pathways. Finally, our investigation also confirmed that APOE upregulates the proliferative and invasive capacity of PCa cells and concurrently enhances resistance to androgen receptor antagonist therapy. This comprehensive study elucidated the potential mechanisms through which this metabolic pathway orchestrates the biological behavior of PCa and findings hold promise in advancing the development of combination therapies in PCa.
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来源期刊
Nutrition & Metabolism
Nutrition & Metabolism 医学-营养学
CiteScore
8.40
自引率
0.00%
发文量
78
审稿时长
4-8 weeks
期刊介绍: Nutrition & Metabolism publishes studies with a clear focus on nutrition and metabolism with applications ranging from nutrition needs, exercise physiology, clinical and population studies, as well as the underlying mechanisms in these aspects. The areas of interest for Nutrition & Metabolism encompass studies in molecular nutrition in the context of obesity, diabetes, lipedemias, metabolic syndrome and exercise physiology. Manuscripts related to molecular, cellular and human metabolism, nutrient sensing and nutrient–gene interactions are also in interest, as are submissions that have employed new and innovative strategies like metabolomics/lipidomics or other omic-based biomarkers to predict nutritional status and metabolic diseases. Key areas we wish to encourage submissions from include: -how diet and specific nutrients interact with genes, proteins or metabolites to influence metabolic phenotypes and disease outcomes; -the role of epigenetic factors and the microbiome in the pathogenesis of metabolic diseases and their influence on metabolic responses to diet and food components; -how diet and other environmental factors affect epigenetics and microbiota; the extent to which genetic and nongenetic factors modify personal metabolic responses to diet and food compositions and the mechanisms involved; -how specific biologic networks and nutrient sensing mechanisms attribute to metabolic variability.
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