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Factors affecting the dynamics and heterogeneity of the EPR effect: pathophysiological and pathoanatomic features, drug formulations and physicochemical factors

机译:影响EPR效应的动力学和异质性的因素:病理生理学和病理解剖学特征,药物制剂和理化因素

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Introduction The enhanced permeability and retention (EPR) effect serves as the foundation of anticancer nanomedicine design. EPR effect-based drug delivery is an effective strategy for most solid tumors. However, the degree of efficacy depends on the pathophysiological conditions of tumors, drug formulations, and other factors. Areas covered Vascular mediators including nitric oxide, bradykinin , and prostaglandins are vital for facilitating and maintaining EPR effect dynamics. Progression to large, advanced cancers may induce activated blood coagulation cascades, which lead to thrombus formation in tumor vasculature. Rapidly growing tumors cause obstructed or suppressed blood flow in tumor vasculature related to embolism or occluded blood vessels. The resulting limited tumor blood flow leads to less drug delivered to tumors, i.e. no or poor EPR effect. High stromal content also suppresses vascular permeability and drug diffusion. Restoring obstructed tumor blood flow and improving tumor vascular permeability via vascular mediators will improve drug delivery and the EPR effect. Physicochemical features of nanomedicines also influence therapeutic outcomes and are vital for the EPR effect. Expert opinion The tumor microenvironment, especially tumor blood flow, is critical for a potent EPR effect. A rational strategy for circumventing EPR effect barriers must include restoring tumor blood flow.
机译:引言 增强的渗透性和保留 (EPR) 效应是抗癌纳米药物设计的基础。基于EPR效应的药物递送是大多数实体瘤的有效策略。然而,疗效程度取决于肿瘤的病理生理条件、药物制剂和其他因素。覆盖的区域 血管介质包括一氧化氮、缓激肽和前列腺素,对于促进和维持 EPR 效应动态至关重要。进展为大型晚期癌症可能会诱导活化的血液凝固级联反应,从而导致肿瘤脉管系统中血栓形成。快速生长的肿瘤会导致与栓塞或血管闭塞相关的肿瘤脉管系统中的血流受阻或抑制。由此产生的肿瘤血流受限导致输送到肿瘤的药物减少,即没有或较差的 EPR 效果。高基质含量还会抑制血管通透性和药物扩散。通过血管介质恢复受阻的肿瘤血流并改善肿瘤血管通透性将改善药物递送和 EPR 效应。纳米药物的理化特性也会影响治疗结果,并且对EPR效应至关重要。专家意见 肿瘤微环境,尤其是肿瘤血流,对于有效的 EPR 效应至关重要。规避EPR效应障碍的合理策略必须包括恢复肿瘤血流。

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