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凝集素固定荧光纳米球对人结肠癌细胞的体外/体内生物识别

In vitro/in vivo biorecognition of lectin-immobilized fluorescent nanospheres for human colorectal cancer cells.

作者信息

Sakuma Shinji, Yano Takanori, Masaoka Yoshie, Kataoka Makoto, Hiwatari Ken-ichiro, Tachikawa Hiroyuki, Shoji Yoshikazu, Kimura Ryoji, Ma Huaiyu, Yang Zhijian, Tang Li, Hoffman Robert M, Yamashita Shinji

机构信息

Faculty of Pharmaceutical Sciences, Setsunan University, 45-1 Nagaotoge-cho, Hirakata, Osaka 573-0101, Japan.

出版信息

J Control Release. 2009 Feb 20;134(1):2-10. doi: 10.1016/j.jconrel.2008.10.017. Epub 2008 Oct 31.

Abstract

Peanut agglutinin (PNA)-immobilized polystyrene nanospheres with surface poly(N-vinylacetamide) (PNVA) chains encapsulating coumarin 6 were designed as a novel colonoscopic imaging agent. PNA was a targeting moiety that binds to beta-D-galactosyl-(1-3)-N-acetyl-D-galactosamine, which is the terminal sugar of the Thomsen-Friedenreich antigen that is specifically expressed on the mucosal side of colorectal cancer cells. PNVA was immobilized with the aim of reducing nonspecific interactions between imaging agents and normal tissues. Coumarin 6 was encapsulated into nanosphere cores to provide endoscopically detectable fluorescence intensity. After incubation of imaging agents with human cells, the fluorescence intensity of imaging agent-bound cells was estimated quantitatively. The average fluorescence intensity of any type of colorectal cancer cell used in this study was higher than that of small intestinal epithelial cells that had not exposed the carbohydrate. The in vivo performance of imaging agents was subsequently evaluated using a human colorectal cancer orthotopic animal model. Imaging agent-derived strong fluorescence was observed at several sites of the large intestinal mucosa in the tumor-implanted nude mice after the luminal side of the colonic loop was contacted with imaging agents. In contrast, when mice that did not undergo tumor implantation were used, the fluorescence intensity on the mucosal surface was extremely low. Data indicated that imaging agents bound to colorectal cancer cells and the cancer cell-derived tumors with high affinity and specificity.

摘要

设计了一种新型的结肠镜成像剂,它是一种固定有花生凝集素(PNA)的聚苯乙烯纳米球,表面带有包裹香豆素6的聚(N - 乙烯基乙酰胺)(PNVA)链。PNA是一种靶向部分,可与β - D - 半乳糖基 -(1 - 3)- N - 乙酰 - D - 半乳糖胺结合,该糖是Thomsen - Friedenreich抗原的末端糖,在结肠癌细胞的黏膜侧特异性表达。固定PNVA的目的是减少成像剂与正常组织之间的非特异性相互作用。香豆素6被包裹在纳米球核心中,以提供可通过内镜检测到的荧光强度。将成像剂与人细胞孵育后,定量估计与成像剂结合的细胞的荧光强度。本研究中使用的任何类型的结肠癌细胞的平均荧光强度均高于未暴露该碳水化合物的小肠上皮细胞。随后使用人结肠癌原位动物模型评估成像剂的体内性能。在结肠环的腔侧与成像剂接触后,在植入肿瘤的裸鼠的大肠黏膜的几个部位观察到成像剂产生的强荧光。相比之下,当使用未植入肿瘤的小鼠时,黏膜表面的荧光强度极低。数据表明成像剂与结肠癌细胞和癌细胞衍生的肿瘤具有高亲和力和特异性结合。

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