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Targeting Somatostatin Receptors By Functionalized Mesoporous Silica Nanoparticles - Are We Striking Home?

机译:通过功能化的介孔二氧化硅纳米粒子靶向生长抑素受体-我们在回家吗?

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摘要

The concept of delivering nanoformulations to desired tissues by means of targeting membrane receptors of high local abundance by ligands anchored to the nanocarrier has gained a lot of attention over the last decade. Currently, there is no unanimous opinion on whether surface functionalization of nanocarriers by targeting ligands translates into any real benefit in terms of pharmacokinetics or treatment outcomes. Having examined the published nanocarriers designed to engage with somatostatin receptors, we realized that in the majority of cases targetability claims were not supported by solid evidence of targeting ligand-targeted receptor coupling, which is the very crux of a targetability concept. Here, we present an approach to characterize targetability of mesoporous silica-based nanocarriers functionalized with ligands of somatostatin receptors. The targetability proof in our case comes from a functional assay based on a genetically-encoded cAMP probe, which allows for real-time capture of receptor activation in living cells, triggered by targeting ligands on nanoparticles. We elaborate on the development and validation of the assay, highlighting the power of proper functional tests in the characterization pipeline of targeted nanoformulations.
机译:在过去的十年中,通过锚定在纳米载体上的配体靶向高局部丰度的膜受体,将纳米制剂输送到所需组织的概念引起了广泛关注。当前,关于通过靶向配体的纳米载体的表面功能化是否转化为药代动力学或治疗结果方面的任何真正益处,尚无一致意见。在检查了已设计的与生长抑素受体结合的纳米载体后,我们意识到在大多数情况下,靶向性主张并没有得到靶向配体-靶向受体偶联的可靠证据,这是靶向性概念的关键所在。在这里,我们提出了一种表征生长抑素受体配体功能化的介孔二氧化硅基纳米载体靶向性的方法。在我们的案例中,可靶向性证明来自基于基因编码的cAMP探针的功能测定,该测定可实时捕获活细胞中激活受体的活化,该活化是由靶向纳米粒子上的配体触发的。我们详细介绍了该检测方法的开发和验证,重点介绍了在靶向纳米制剂表征流程中进行适当功能测试的功能。

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