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血管内皮生长因子(VEGF)作为癌症相关静脉血栓形成的生物标志物:一项荟萃分析。

Vascular Endothelial Growth Factor (VEGF) as a Biomarker for Cancer-Associated Venous Thrombosis: A Meta-analysis.

作者信息

Brown Alison M, Nock Sophie, Musgrave Kathryn, Unsworth Amanda J

机构信息

Department of Blood Sciences, The Newcastle upon Tyne Hospitals NHS Foundation Trust, United Kingdom.

Department of Life Sciences, Faculty of Science and Engineering, Manchester Metropolitan University, Manchester, United Kingdom.

出版信息

TH Open. 2025 Feb 10;9:a25134381. doi: 10.1055/a-2513-4381. eCollection 2025.

Abstract

Cancer-associated thrombosis affects between 1 and 20% of all patients diagnosed with cancer and is associated with significant morbidity and a poorer prognosis. Risk assessment scores exist which include the measurement of biomarkers, and which aim to identify patients at a higher risk of developing thrombotic events, but these are poor predictors and rarely used in routine clinical practice. VEGF is a potent angiogenic factor, produced by tumour cells, and released by platelets and is essential for tumour growth and progression. It also plays a role in the promotion of thrombosis through platelet activation and adhesion, and by inducing the expression of tissue factor. Therefore, the potential of VEGF to be used as a biomarker to predict cancer-associated thrombosis requires further investigation. This study reviewed the published literature to determine whether circulating VEGF levels are associated with increased risk of venous thromboembolism in patients with cancer. PubMed and OVID databases were systematically searched according to PRISMA guidelines for relevant papers using the keywords "cancer" AND "thrombosis" AND "VEGF" up to July 2023. Inclusion and exclusion criteria were applied. Seven papers (1,528 participants) were identified and included in the meta-analysis, three of which (922 participants) measured VEGF before a thrombotic event, and the remaining four (606 participants) measured VEGF at the time of the thrombosis. Our results showed that although plasma and serum VEGF tended to be higher in those who subsequently developed thrombosis than those who did not (mean difference 70.2 pg/mL for serum, and 11.44 pg/mL for plasma VEGF, 95% CI -2.39-25.73,  = 0.10), this was not found to be statistically significant. However, analysis of VEGF following blood sampling at the time of thrombosis showed a stronger statistically significant association between increased VEGF levels and presence of thrombosis (mean difference 117.02 pg/mL for serum, and 116.6 pg/mL for plasma VEGF, 95% CI 55.42-190.82,  = 0.0004). Based on current studies, whilst it is increased at the time of thrombosis, VEGF is not effective as a predictive biomarker of CAT.

摘要

癌症相关血栓形成影响1%至20%的癌症确诊患者,与显著的发病率和较差的预后相关。现有的风险评估评分包括生物标志物的测量,旨在识别发生血栓事件风险较高的患者,但这些评分预测效果不佳,很少用于常规临床实践。血管内皮生长因子(VEGF)是一种由肿瘤细胞产生、血小板释放的强效血管生成因子,对肿瘤生长和进展至关重要。它还通过血小板激活和黏附以及诱导组织因子表达在促进血栓形成中发挥作用。因此,VEGF作为预测癌症相关血栓形成生物标志物的潜力需要进一步研究。本研究回顾已发表的文献,以确定循环VEGF水平是否与癌症患者静脉血栓栓塞风险增加相关。根据PRISMA指南,截至2023年7月,在PubMed和OVID数据库中系统检索使用关键词“癌症”“血栓形成”和“VEGF”的相关论文。应用纳入和排除标准。确定七篇论文(1528名参与者)并纳入荟萃分析,其中三篇(922名参与者)在血栓事件发生前测量VEGF,其余四篇(606名参与者)在血栓形成时测量VEGF。我们的结果表明,尽管随后发生血栓形成的患者血浆和血清VEGF往往高于未发生血栓形成的患者(血清平均差异70.2 pg/mL,血浆VEGF平均差异11.44 pg/mL,95%CI -2.39 - 25.73,P = 0.10),但未发现具有统计学意义。然而,对血栓形成时采血后的VEGF分析显示,VEGF水平升高与血栓形成之间存在更强的统计学显著关联(血清平均差异117.02 pg/mL,血浆VEGF平均差异116.6 pg/mL,95%CI 55.42 - 190.82,P = 0.0004)。基于目前的研究,虽然VEGF在血栓形成时升高,但它作为癌症相关血栓形成的预测生物标志物效果不佳。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/13c2/12020352/be606bdae286/10-1055-a-2513-4381-i24100027-1.jpg

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