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冷冻切片成像揭示肺内药物剂量的定量检测及空间分布

Quantitative detection of drug dose and spatial distribution in the lung revealed by Cryoslicing Imaging.

作者信息

Barapatre Nirav, Symvoulidis Panagiotis, Möller Winfried, Prade Friedrich, Deliolanis Nikolaos C, Hertel Sebastian, Winter Gerhard, Yildirim Ali Ö, Stoeger Tobias, Eickelberg Oliver, Ntziachristos Vasilis, Schmid Otmar

机构信息

Comprehensive Pneumology Center, Member of the German Center for Lung Research, Max-Lebsche-Platz 31, 81377 Munich, Germany; Institute of Lung Biology and Disease, Helmholtz Zentrum München, 85764 Neuherberg, Germany.

Institute of Biological and Medical Imaging, Helmholtz Zentrum München and Technische Universität München, 85764 Neuherberg, Germany.

出版信息

J Pharm Biomed Anal. 2015 Jan;102:129-36. doi: 10.1016/j.jpba.2014.09.001. Epub 2014 Sep 8.

Abstract

Administration of drugs via inhalation is an attractive route for pulmonary and systemic drug delivery. The therapeutic outcome of inhalation therapy depends not only on the dose of the lung-delivered drug, but also on its bioactivity and regional distribution. Fluorescence imaging has the potential to monitor these aspects already during preclinical development of inhaled drugs, but quantitative methods of analysis are lacking. In this proof-of-concept study, we demonstrate that Cryoslicing Imaging allows for 3D quantitative fluorescence imaging on ex vivo murine lungs. Known amounts of fluorescent substance (nanoparticles or fluorophore-drug conjugate) were instilled in the lungs of mice. The excised lungs were measured by Cryoslicing Imaging. Herein, white light and fluorescence images are obtained from the face of a gradually sliced frozen organ block. A quantitative representation of the fluorescence intensity throughout the lung was inferred from the images by accounting for instrument noise, tissue autofluorescence and out-of-plane fluorescence. Importantly, the out-of-plane fluorescence correction is based on the experimentally determined effective light attenuation coefficient of frozen murine lung tissue (10.0 ± 0.6 cm(-1) at 716 nm). The linear correlation between pulmonary total fluorescence intensity and pulmonary fluorophore dose indicates the validity of this method and allows direct fluorophore dose assessment. The pulmonary dose of a fluorescence-labeled drug (FcγR-Alexa750) could be assessed with an estimated accuracy of 9% and the limit of detection in ng regime. Hence, Cryoslicing Imaging can be used for quantitative assessment of dose and 3D distribution of fluorescence-labeled drugs or drug carriers in the lungs of mice.

摘要

通过吸入方式给药是肺部和全身药物递送的一种有吸引力的途径。吸入疗法的治疗效果不仅取决于肺部递送药物的剂量,还取决于其生物活性和区域分布。荧光成像有潜力在吸入药物的临床前开发阶段就对这些方面进行监测,但缺乏定量分析方法。在这项概念验证研究中,我们证明冷冻切片成像能够对离体小鼠肺部进行三维定量荧光成像。将已知量的荧光物质(纳米颗粒或荧光团 - 药物缀合物)注入小鼠肺部。通过冷冻切片成像对切除的肺部进行测量。在此过程中,从逐渐切片的冷冻器官块表面获取白光和荧光图像。通过考虑仪器噪声、组织自发荧光和面外荧光,从图像中推断出整个肺部荧光强度的定量表示。重要的是,面外荧光校正基于实验确定的冷冻小鼠肺组织在716nm处的有效光衰减系数(10.0±0.6 cm(-1))。肺部总荧光强度与肺部荧光团剂量之间的线性相关性表明了该方法的有效性,并允许直接进行荧光团剂量评估。一种荧光标记药物(FcγR - Alexa750)的肺部剂量可以以估计9%的准确度和纳克级别的检测限进行评估。因此,冷冻切片成像可用于定量评估荧光标记药物或药物载体在小鼠肺部的剂量和三维分布。

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