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使用超声造影脂质体将贝伐单抗递送至动脉粥样硬化猪颈动脉组织。

Delivery of bevacizumab to atheromatous porcine carotid tissue using echogenic liposomes.

作者信息

Sutton J T, Haworth K J, Shanmukhappa S K, Moody M R, Klegerman M E, Griffin J K, Patton D M, McPherson D D, Holland C K

机构信息

a Biomedical Engineering Program, University of Cincinnati , Cincinnati , OH , USA.

f Philips Research North America , Cambridge , MA , USA.

出版信息

Drug Deliv. 2016 Nov;23(9):3594-3605. doi: 10.1080/10717544.2016.1212441. Epub 2016 Sep 30.

Abstract

Ultrasound is both a valuable diagnostic tool and a promoter of beneficial tissue bioeffects for the treatment of cardiovascular disease. Vascular effects can be mediated by mechanical oscillations of circulating microbubbles that may also encapsulate and shield therapeutic agents in the bloodstream. Here, the effect of color-Doppler ultrasound exposure on bevacizumab-loaded liposome delivery into the vascular bed was assessed in atheromatous porcine carotids. Bevacizumab, an anti-angiogenic antibody to vascular endothelial growth factor (VEGF-A), was loaded into echogenic liposomes (BEV-ELIP) and confirmed to be immunoreactive. BEV-ELIP flowing within the lumen were exposed to color-Doppler ultrasound at three acoustic pressures for 3.5 min during treatment at physiologic temperature and fluid pressure. To confirm the presence of bubble activity, cavitation was detected within the lumen by a single-element passive cavitation detector. After treatment, the artery was fixed at physiologic pressure and subjected to immunohistochemical analysis to assess the penetration of bevacizumab within the carotid wall. The results suggest that other factors may more strongly influence the deposition of bevacizumab into carotid tissue than color-Doppler ultrasound and cavitation. In both sets of arteries, preferential accumulation of bevacizumab occurred in locations associated with atheroma progression and neointimal thickening: fibrous tissue, necrotic plaque and areas near macrophage infiltration. The delivery of bevacizumab to carotid vascular tissue correlated with the properties of the tissue bed, such as permeability, or affinity for growth-factor binding. Future investigations using this novel therapeutic strategy may focus on characterizing the spatial extent of delivery and bevacizumab colocalization with biochemical markers of atheroma.

摘要

超声既是一种有价值的诊断工具,也是治疗心血管疾病的有益组织生物效应的促进因素。血管效应可由循环微泡的机械振荡介导,这些微泡还可在血流中包裹和保护治疗剂。在此,在动脉粥样硬化猪颈动脉中评估了彩色多普勒超声暴露对载有贝伐单抗的脂质体向血管床递送的影响。贝伐单抗是一种针对血管内皮生长因子(VEGF-A)的抗血管生成抗体,被载入回声脂质体(BEV-ELIP)并证实具有免疫反应性。在生理温度和流体压力下治疗期间,将在管腔内流动的BEV-ELIP在三种声压下暴露于彩色多普勒超声3.5分钟。为了确认气泡活动的存在,用单元素被动空化探测器在管腔内检测到空化。治疗后,在生理压力下固定动脉并进行免疫组织化学分析,以评估贝伐单抗在颈动脉壁内的渗透情况。结果表明,与彩色多普勒超声和空化相比,其他因素可能对贝伐单抗在颈动脉组织中的沉积影响更大。在两组动脉中,贝伐单抗均优先积聚在与动脉粥样硬化进展和新生内膜增厚相关的部位:纤维组织、坏死斑块和巨噬细胞浸润附近的区域。贝伐单抗向颈动脉血管组织的递送与组织床的特性相关,如通透性或对生长因子结合的亲和力。使用这种新型治疗策略的未来研究可能集中于表征递送的空间范围以及贝伐单抗与动脉粥样硬化生化标志物的共定位情况。

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Ultrasound Med Biol. 2016 Feb;42(2):518-27. doi: 10.1016/j.ultrasmedbio.2015.08.014. Epub 2015 Nov 4.
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