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在缺血小鼠模型中血管生成过程中 VEGF 受体分子分布的体内成像。

In vivo imaging of the molecular distribution of the VEGF receptor during angiogenesis in a mouse model of ischemia.

机构信息

Department of Nano-Medical Science, Graduate School of Medicine, Tohoku University, Sendai, Japan.

出版信息

Blood. 2011 Sep 29;118(13):e93-e100. doi: 10.1182/blood-2010-12-322842. Epub 2011 Aug 5.

Abstract

Vascular endothelial growth factor (VEGF) plays a critical role in angiogenesis and has been applied to medical therapy. However, because vascular imaging at the molecular level is impossible, the detailed in vivo dynamics of VEGF and its receptor (VEGFR) remain unknown. In this study, to understand the molecular distribution of VEGF and the VEGFR, we prepared ischemic mice with a new surgical method and induced angiogenesis in the gastrocnemius muscle. Then, we made a VEGF-conjugated fluorescence nanoparticle and performed staining of VEGFR-expressing cells with the fluorescent probe, demonstrating the high affinity of the probe for VEGFR. To observe the physiologic molecular distribution of VEGFR, we performed in vivo single-particle imaging of gastrocnemius in the ischemic leg with the fluorescent probe. The results suggested that only a 3-fold difference of VEGFR distribution is involved in the formation of branched vasculature in angiogenesis, although previous ex vivo data showed a 13-fold difference in its distribution, indicating that a method inducing a several-fold local increase of VEGFR concentration may be effective in generating site-specific angiogenesis in ischemic disease. This new in vivo imaging of ischemic mice could make useful contributions to understanding the mechanisms of angiogenesis and to developing a VEGFR-related drug.

摘要

血管内皮生长因子(VEGF)在血管生成中起着关键作用,并已应用于医学治疗。然而,由于血管的分子水平成像不可能实现,因此 VEGF 和其受体(VEGFR)的详细体内动力学仍不清楚。在这项研究中,为了了解 VEGF 和 VEGFR 的分子分布,我们用一种新的手术方法制备了缺血性小鼠,并在比目鱼肌中诱导血管生成。然后,我们制备了一种 VEGF 缀合的荧光纳米颗粒,并使用荧光探针对表达 VEGFR 的细胞进行染色,证明了探针对 VEGFR 的高亲和力。为了观察 VEGFR 的生理分子分布,我们使用荧光探针对缺血腿中的比目鱼肌进行了体内单颗粒成像。结果表明,尽管先前的离体数据显示其分布存在 13 倍的差异,但在血管生成中分支血管形成中仅涉及 VEGFR 分布的 3 倍差异,这表明诱导 VEGFR 浓度局部增加几倍的方法可能在缺血性疾病中产生特定部位的血管生成方面是有效的。这种新的缺血性小鼠体内成像方法可能有助于理解血管生成的机制,并开发与 VEGFR 相关的药物。

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