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Molecular markers to predict outcome to antiangiogenic therapies in colorectal cancer: Current evidence and future perspectives

机译:分子标记物预测大肠癌抗血管生成疗法的结果:当前证据和未来展望

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Angiogenesis is a universal requirement for the growth of solid tumours beyond the limits of oxygen diffusion from the existing vasculature. The expression and function of proangiogenic and antiangiogenic factors are altered in solid malignancies to drive net neoangiogenesis. Vascular endothelial growth factor (VEGF) has been confirmed in several clinical trials as an important therapeutic target in colorectal cancer (CRC) treatment. However, given that the efficacy of antiangiogenic agents appears to be limited to a subset of patients, the identification of who will obtain the greater benefit from this therapy or suffer from specific toxicities and when or for how long they should be administered in the treatment algorithm are major open questions for clinicians and challenges for present and future research. Current evidence indicates some predictive value for particular circulating measures, such as an increase in VEGF, a decrease in vascular endothelial growth factor receptor 2 (VEGFR-2) or circulating endothelial cells, tissue biomarkers, microvessel density, KRAS and BRAF gene mutations or polymorphisms affecting components of the VEGF pathway. Many questions relating to these and other surrogate biomarkers, however, remain unanswered and their clinical usefulness has yet to be proven. This review will focus on the present status of knowledge and future perspectives for developing molecular tools to foresee and monitor antiangiogenic therapy activity in CRC patients.
机译:血管生成是实体瘤生长超出现有脉管的氧扩散限制的普遍要求。实体恶性肿瘤中促血管生成和抗血管生成因子的表达和功能发生改变,以驱动净新血管生成。血管内皮生长因子(VEGF)已在多项临床试验中得到确认,是结直肠癌(CRC)治疗中的重要治疗靶标。但是,鉴于抗血管生成剂的疗效似乎仅限于一部分患者,因此确定谁将从该疗法中获得更大的益处或遭受特定的毒性以及在治疗算法中何时或将其给予多久进行鉴定是临床医生面临的主要开放性问题,也是当前和未来研究的挑战。目前的证据表明,对于某些特定的循环测量有一定的预测价值,例如VEGF的增加,血管内皮生长因子受体2(VEGFR-2)或循环内皮细胞的减少,组织生物标志物,微血管密度,KRAS和BRAF基因突变或多态性影响VEGF途径的成分。然而,与这些和其他替代生物标志物有关的许多问题仍未得到解答,其临床实用性尚未得到证实。这项审查将侧重于知识的现状和开发分子工具以预测和监测CRC患者抗血管生成治疗活动的未来前景。

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