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小鼠体内单个天然胰岛的可视化。

In vivo visualization of single native pancreatic islets in the mouse.

作者信息

Balla Dávid Z, Gottschalk Sven, Shajan G, Ueberberg Sandra, Schneider Stephan, Hardtke-Wolenski Matthias, Jaeckel Elmar, Hoerr Verena, Faber Cornelius, Scheffler Klaus, Pohmann Rolf, Engelmann Jörn

机构信息

High-Field Magnetic Resonance Centre, Max-Planck-Institute for Biological Cybernetics, Tübingen, Germany.

出版信息

Contrast Media Mol Imaging. 2013 Nov-Dec;8(6):495-504. doi: 10.1002/cmmi.1580.

Abstract

The purpose of this study was to investigate the potential of a novel targeted contrast agent (CA) for the in vivo visualization of single native pancreatic islets, the sites of insulin production, in the pancreas of mice using magnetic resonance imaging (MRI). The CA for intravenous administration was composed of the β-cell-specific single-chain antibody fragment, SCA B1, and ferromagnetic carbon-coated cobalt nanoparticles. MRI experiments were performed at 7, 9.4 and 16.4 T in excised organs (pancreas, liver, kidney, spleen), at 7 T in mice fixed in formalin and at 9.4 and 16.4 T in living mice. Image contrast in untreated control animals was compared with images from mice treated with unspecific and specific CA. For the validation of MRI results, selected pancreases were subjected to immunohistochemical staining and numerical contrast simulations were performed. Ex vivo results and the outcome of immunohistochemistry suggest that islets are marked only by the CA containing SCA B1. Strong accumulation of particles was found also in other investigated organs owing to the uptake by the reticuloendothelial system, but the contrast in the MR images is clearly distinguishable from the islet specific contrast in pancreases and numerical predictions. In vivo experiments based on averaged dynamic sampling with 66 × 66 × 100 µm³ and triggered acquisition with 90 × 90 × 200 µm³ nominal resolution resulted in similar particle contrast to in in vitro measurements. The newly developed CA and MRI strategies have the potential to be used for studying mouse diabetes models by visualizing single native pancreatic islets.

摘要

本研究的目的是利用磁共振成像(MRI)研究一种新型靶向造影剂(CA)在小鼠胰腺中对单个天然胰岛(胰岛素产生部位)进行体内可视化的潜力。用于静脉注射的CA由β细胞特异性单链抗体片段SCA B1和铁磁碳包覆钴纳米颗粒组成。MRI实验在7、9.4和16.4 T下对切除的器官(胰腺、肝脏、肾脏、脾脏)进行,在7 T下对用福尔马林固定的小鼠进行,在9.4和16.4 T下对活体小鼠进行。将未处理对照动物的图像对比度与用非特异性和特异性CA处理的小鼠的图像进行比较。为了验证MRI结果,对选定的胰腺进行免疫组织化学染色并进行数值对比度模拟。离体结果和免疫组织化学结果表明,只有含有SCA B1的CA才能标记胰岛。由于网状内皮系统的摄取,在其他研究器官中也发现了颗粒的强烈积累,但MR图像中的对比度与胰腺中的胰岛特异性对比度和数值预测明显不同。基于平均动态采样(66×66×100 µm³)和触发采集(90×90×200 µm³标称分辨率)的体内实验产生的颗粒对比度与体外测量结果相似。新开发的CA和MRI策略有潜力通过可视化单个天然胰腺胰岛来用于研究小鼠糖尿病模型。

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