Literature DB >> 23668665

Identification of a novel indoline derivative for in vivo fluorescent imaging of blood-brain barrier disruption in animal models.

Yuhei Nishimura1, Kenichiro Yata, Tsuyoshi Nomoto, Tomoaki Ogiwara, Kohei Watanabe, Taichi Shintou, Akira Tsuboyama, Mie Okano, Noriko Umemoto, Zi Zhang, Miko Kawabata, Beibei Zhang, Junya Kuroyanagi, Yasuhito Shimada, Takeshi Miyazaki, Takeshi Imamura, Hidekazu Tomimoto, Toshio Tanaka.   

Abstract

Disruption of the blood-brain barrier (BBB) can occur in various pathophysiological conditions. Administration of extraneous tracers that can pass the disrupted, but not the intact, BBB and detection of the extravasation have been widely used to assess BBB disruption in animal models. Although several fluorescent tracers have been successfully used, the administration of these tracers basically requires intravascular injection, which can be laborious when using small animals such as zebrafish. To identify fluorescent tracers that could be easily administered into various animal models and visualize the BBB disruption in vivo, we prepared nine structurally related indoline derivatives (IDs) as a minimum set of diverse fluorescent compounds. We found that one ID, ZMB741, had the highest affinity for serum albumin and emitted the strongest fluorescence in the presence of serum albumin of the nine IDs tested. The affinity to serum albumin and the fluorescence intensity was superior to those of Evans blue and indocyanine green that have been conventionally used to assess the BBB disruption. We showed that ZMB741 could be administered into zebrafish by static immersion or mice by intraperitoneal injection and visualizes the active disruption of their BBB. These results suggest that ZMB741 can be a convenient and versatile tool for in vivo fluorescent imaging of BBB disruption in various animal models. The strategy used in this study can also be applied to diversity-oriented libraries to identify novel fluorescent tracers that may be superior to ZMB741.

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Year:  2013        PMID: 23668665      PMCID: PMC3750685          DOI: 10.1021/cn400010t

Source DB:  PubMed          Journal:  ACS Chem Neurosci        ISSN: 1948-7193            Impact factor:   4.418


  45 in total

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  6 in total

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