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Anal Chem. 2018 Aug 7;90(15):8831-8837. doi: 10.1021/acs.analchem.8b00816. Epub 2018 Jul 16.
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Nanocapsule-mediated cytosolic siRNA delivery for anti-inflammatory treatment.纳米胶囊介导的细胞质 siRNA 递送来进行抗炎治疗。
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Multimodal laser ablation/desorption imaging analysis of Zn and MMP-11 in breast tissues.多模态激光烧蚀/解吸成像分析乳腺组织中的 Zn 和 MMP-11。
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双质谱组织成像技术在纳米载体分布及其生化效应中的应用。

Dual Mass Spectrometric Tissue Imaging of Nanocarrier Distributions and Their Biochemical Effects.

机构信息

Department of Chemistry , University of Massachusetts , Amherst , Massachusetts 01003 , United States.

出版信息

Anal Chem. 2020 Jan 21;92(2):2011-2018. doi: 10.1021/acs.analchem.9b04398. Epub 2019 Dec 30.

DOI:10.1021/acs.analchem.9b04398
PMID:31825199
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7086473/
Abstract

Nanomaterial-based drug delivery vehicles are able to deliver therapeutics in a controlled, targeted manner. Currently, however, there are limited analytical methods that can detect both nanomaterial distributions and their biochemical effects concurrently. In this study, we demonstrate that matrix assisted laser desorption/ionization mass spectrometry imaging (MALDI-MSI) and laser ablation inductively coupled plasma mass spectrometry imaging (LA-ICP-MSI) can be used together to obtain nanomaterial distributions and biochemical consequences. These studies employ nanoparticle-stabilized capsules (NPSCs) loaded with siRNA as a testbed. MALDI-MSI experiments on spleen tissues from intravenously injected mice indicate that NPSCs loaded with anti-TNF-α siRNA cause changes to the lipid composition in white pulp regions of the spleen, as anticipated, based on pathways known to be affected by TNF-α, whereas NPSCs loaded with scrambled siRNA do not cause the predicted changes. Interestingly, LA-ICP-MSI experiments reveal that the NPSCs primarily localize in the red pulp, suggesting that the observed changes in lipid composition are due to diffusive rather than localized effects on TNF-α production. Such information is only accessible by combining data from the two modalities, which we accomplish by using the heme signals from MALDI-MSI and iron signals from LA-ICP-MSI to overlay the images. Several unexpected changes in lipid composition also occur in regions where the NPSCs are found, suggesting that the NPSCs themselves can influence tissue biochemistry as well.

摘要

基于纳米材料的药物输送载体能够以可控、靶向的方式输送治疗药物。然而,目前用于同时检测纳米材料分布和其生化效应的分析方法有限。在这项研究中,我们证明了基质辅助激光解吸/电离质谱成像(MALDI-MSI)和激光烧蚀电感耦合等离子体质谱成像(LA-ICP-MSI)可以结合使用,以获得纳米材料的分布和生化后果。这些研究采用载有 siRNA 的纳米颗粒稳定胶囊(NPSCs)作为试验台。对静脉注射小鼠脾脏组织进行 MALDI-MSI 实验表明,载有抗 TNF-α siRNA 的 NPSCs 导致脾脏白髓区域的脂质组成发生变化,这与已知受 TNF-α影响的途径相符,而载有乱序 siRNA 的 NPSCs 则不会导致预期的变化。有趣的是,LA-ICP-MSI 实验表明 NPSCs 主要定位于红髓,这表明观察到的脂质组成变化是由于 TNF-α 产生的扩散而非局部影响所致。只有通过结合两种模式的数据才能获得此类信息,我们通过使用 MALDI-MSI 的血红素信号和 LA-ICP-MSI 的铁信号来叠加图像来实现这一目标。在 NPSCs 所在的区域也发生了几种意想不到的脂质组成变化,这表明 NPSCs 本身也会影响组织生物化学。