Investigating causal relationships of blood and urine biomarkers with urological cancer risks: a mendelian randomization study and colocalization analyses.

IF 3.2 3区 医学 Q2 ONCOLOGY Journal of Cancer Pub Date : 2025-01-01 DOI:10.7150/jca.103669
Jian Li, Bing Yang, Lei Guo, Wenqi Huang, Qiong Hu, Hongting Yan, Rong Tan, Dongxin Tang
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Abstract

Background: Establishing the causal links between biomarkers and cancer enhances understanding of risk factors and facilitates the discovery of therapeutic targets. To this end, we used Mendelian randomization (MR) and colocalization analysis to explore the causal relationship of blood and urinary biomarkers (BUBs) with urological cancers (UCs). Methods: First, we used a two-sample MR study to explore the causal relationship between 33 BUBs and 4 UCs, while we performed reverse Mendelian randomization. After Bonferroni correction, for BUB and UC with significant causality we confirmed the direct causality by multivariate MR adjusting for relevant risk factors. We also applied two-step MR analysis to further explore the possible mediators between BUB and UC with significant causality, while colocalization analysis was performed for BUB, UC and possible mediators. Sensitivity analysis were performed to assess the robustness of the results. Results: A two-sample MR study found that there were 8 BUBs of CA, IGF-1, LPA, TP, CRE, BILD, TBIL and NAP with potential causality with some UCs (p<0.05), but after Bonferroni correction only IGF-1 had a significant causality with PCa (OR = 1.14, 95% CI: 1.06-1.23; p=0.0006<0.05/33). Moreover, the causal relationship between IGF-1 and PCa remained significant (P<0.05) after adjusting for relevant risk factors in the multivariate MR study. The two-step MR study found SHBG to be a mediator between IGF-1 and PCa, and the colocalization analysis found that there was a common causal variant (nearby gene TNS3) between IGF-1 and SHBG (PPH4=93.21%), which further confirmed the mediating effect of SHBG. Conclusion: Strong evidence from our study suggests that IGF-1 increases the risk of PCa by decreasing SHBG levels, and in addition some BUBs were found to have a potential causal relationship with UCs.

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研究血液和尿液生物标志物与泌尿系统癌症风险的因果关系:一项孟德尔随机研究和共定位分析。
背景:建立生物标志物与癌症之间的因果关系可以增强对危险因素的理解,并有助于发现治疗靶点。为此,我们使用孟德尔随机化(MR)和共定位分析来探索血液和尿液生物标志物(BUBs)与泌尿系统癌症(UCs)的因果关系。方法:首先,我们使用两样本MR研究来探索33个bub和4个UCs之间的因果关系,同时我们进行了反向孟德尔随机化。经Bonferroni校正后,对于具有显著因果关系的BUB和UC,我们通过对相关危险因素进行多变量MR校正,证实了直接因果关系。我们还应用两步磁共振分析进一步探讨了BUB和UC之间可能的中介因素,并对BUB、UC和可能的中介因素进行了共定位分析。进行敏感性分析以评估结果的稳健性。结果:一项双样本MR研究发现,CA、IGF-1、LPA、TP、CRE、BILD、TBIL和NAP有8个BUBs与某些UCs存在潜在的因果关系。结论:我们的研究强有力的证据表明,IGF-1通过降低SHBG水平增加了PCa的风险,并且发现一些BUBs与UCs存在潜在的因果关系。
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来源期刊
Journal of Cancer
Journal of Cancer ONCOLOGY-
CiteScore
8.10
自引率
2.60%
发文量
333
审稿时长
12 weeks
期刊介绍: Journal of Cancer is an open access, peer-reviewed journal with broad scope covering all areas of cancer research, especially novel concepts, new methods, new regimens, new therapeutic agents, and alternative approaches for early detection and intervention of cancer. The Journal is supported by an international editorial board consisting of a distinguished team of cancer researchers. Journal of Cancer aims at rapid publication of high quality results in cancer research while maintaining rigorous peer-review process.
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