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用于(19)F磁共振成像的具有增强肿瘤摄取特性的蛋白质同型半胱氨酸酰胺的设计

Design of protein homocystamides with enhanced tumor uptake properties for (19)F magnetic resonance imaging.

作者信息

Chubarov Alexey S, Zakharova Olga D, Koval Olga A, Romaschenko Alexander V, Akulov Andrey E, Zavjalov Evgenii L, Razumov Ivan A, Koptyug Igor V, Knorre Dmitry G, Godovikova Tatyana S

机构信息

Institute of Chemical Biology and Fundamental Medicine, SB RAS, 630090 Novosibirsk, Russia; Novosibirsk State University, 630090 Novosibirsk, Russia.

Institute of Chemical Biology and Fundamental Medicine, SB RAS, 630090 Novosibirsk, Russia.

出版信息

Bioorg Med Chem. 2015 Nov 1;23(21):6943-54. doi: 10.1016/j.bmc.2015.09.043. Epub 2015 Sep 30.

Abstract

Straightforward and reliable tools for in vivo imaging of tumors can benefit the studies of cancer development, as well as contribute to successful diagnosis and treatment of cancer. (19)F NMR offers an exceptional quantitative way of in vivo imaging of the infused agents because of the lack of (19)F signals from the endogenous molecules in the body. The purpose of this study is to develop molecular probes with appropriate NMR characteristics and the biocompatibility for in vivo applications using (19)F MRI. We have studied the reaction between perfluorotoluene and homocysteine thiolactone resulting in the formation of N-substituted homocysteine thiolactone derivative. It has been shown that the reaction occurs selectively at the para position. This fluorine-labeled homocysteine thiolactone has been employed for the introduction of a perfluorotoluene group as a (19)F-containing tag into human serum albumin. The modified protein has been studied in terms of its ability to aggregate and promote the formation of free radicals. By comparing the properties of N-perfluorotoluene-homocystamide of albumin with N-homocysteinylated albumin, it has been revealed that blocking of the alpha-amino group of the homocysteine residue in the fluorinated albumin conjugate inhibits the dangerous aggregation process, as well as free radical formation. A dual-labeled albumin-based molecular probe for (19)F MRI and fluorescence microscopy has been obtained by functionalizing the protein with both maleimide of a fluorescent dye and a fluorinated thiolactone derivative. The incubation of cells with this conjugate did not reveal any significant reduction in cell viability with respect to the parent albumin. The perfluorotoluene-labeled albumin has been demonstrated to act as a promising agent for in vivo (19)F MRI.

摘要

用于肿瘤体内成像的简单可靠工具有助于癌症发展的研究,并有助于癌症的成功诊断和治疗。由于体内内源性分子缺乏(19)F信号,(19)F核磁共振提供了一种用于注入剂体内成像的特殊定量方法。本研究的目的是利用(19)F磁共振成像开发具有适当核磁共振特性和生物相容性的用于体内应用的分子探针。我们研究了全氟甲苯与同型半胱氨酸硫内酯之间的反应,结果形成了N-取代的同型半胱氨酸硫内酯衍生物。已表明该反应选择性地发生在对位。这种氟标记的同型半胱氨酸硫内酯已被用于将全氟甲苯基团作为含(19)F的标签引入人血清白蛋白。已对修饰后的蛋白质的聚集能力和促进自由基形成的能力进行了研究。通过比较白蛋白的N-全氟甲苯-同型半胱氨酸酰胺与N-同型半胱氨酸化白蛋白的性质,发现氟化白蛋白缀合物中同型半胱氨酸残基的α-氨基被封闭可抑制危险的聚集过程以及自由基的形成。通过用荧光染料的马来酰亚胺和氟化硫内酯衍生物对蛋白质进行功能化,获得了一种用于(19)F磁共振成像和荧光显微镜的双标记白蛋白基分子探针。用这种缀合物孵育细胞并未显示相对于亲本白蛋白细胞活力有任何显著降低。全氟甲苯标记的白蛋白已被证明是一种有前途的用于体内(19)F磁共振成像的试剂。

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