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第二个硝咪唑类氧化还原中心对缺氧标志物蓄积的影响:99mTc 标记的双硝咪唑丙烯胺肟配合物的合成与体外评价。

Effect of a second nitroimidazole redox centre on the accumulation of a hypoxia marker: synthesis and in vitro evaluation of 99mTc-labeled bisnitroimidazole propylene amine oxime complexes.

机构信息

Beijing National Laboratory for Molecular Sciences, Radiochemistry and Radiation Chemistry Key Laboratory of Fundamental Science, College of Chemistry and Molecular Engineering, Peking University, Beijing 100871, China.

出版信息

Bioorg Med Chem Lett. 2012 Jan 1;22(1):172-7. doi: 10.1016/j.bmcl.2011.11.042. Epub 2011 Nov 18.

DOI:10.1016/j.bmcl.2011.11.042
PMID:22153341
Abstract

Up to now, most of the hypoxia markers contain only one nitroimidazole redox centre, such as Oxo[[3,3,9,9-tetramethyl-1-(2-nitro-1H-imidazol-1-yl)-4,8-diazaundecane-2,10-dione dioximato] (3-)-N,N',N″,N″']-technetium ((99m)Tc-1, BMS181321). Introducing a second nitroimidazole redox centre may enhance the hypoxic accumulation of the markers. In the present work, four (99m)Tc-1 (BMS181321, containing one 2-nitroimidazole) analogues, that is, (99m)Tc-2 (containing two 2-nitroimidazoles), (99m)Tc-3 (containing one 4-nitroimidazole), (99m)Tc-4 (containing two 4-nitroimidazoles) and (99m)Tc-5 (containing both a 2-nitroimidazole and a 4-nitroimidazole) were synthesized, and the hypoxic accumulation was evaluated in vitro using murine sarcoma S180 cells. (99m)Tc-3 and (99m)Tc-4 displayed no significant anoxic/normoxic differentials, whereas (99m)Tc-1 (BMS181321), (99m)Tc-2 and (99m)Tc-5 showed high anoxic cellular uptakes. The anoxic uptake of (99m)Tc-2 reached up to 59.0±0.9% at 4h, which was 2.4 times as that of (99m)Tc-1. (99m)Tc-2 displayed high hypoxic accumulation, indicating that introducing a second nitroimidazole redox centre, that is, 2-nitroimidazole, affected the hypoxic accumulation. Consequently, (99m)Tc-2 may serve as a viable candidate for hypoxia marker. This finding may eventually lead to the development of compounds containing multi-redox centres as hypoxia markers.

摘要

到目前为止,大多数缺氧标志物仅包含一个硝基咪唑氧化还原中心,如 Oxo[[3,3,9,9-四甲基-1-(2-硝基-1H-咪唑-1-基)-4,8-二氮杂十一烷-2,10-二酮二肟](3-)-N,N',N″,N″']-锝((99m)Tc-1,BMS181321)。引入第二个硝基咪唑氧化还原中心可能会增强标志物的缺氧积累。在本工作中,合成了四种(99m)Tc-1(BMS181321,包含一个 2-硝基咪唑)类似物,即(99m)Tc-2(包含两个 2-硝基咪唑)、(99m)Tc-3(包含一个 4-硝基咪唑)、(99m)Tc-4(包含两个 4-硝基咪唑)和(99m)Tc-5(包含一个 2-硝基咪唑和一个 4-硝基咪唑),并在体外使用鼠肉瘤 S180 细胞评估了其缺氧积累。(99m)Tc-3 和(99m)Tc-4 没有表现出明显的缺氧/常氧差异,而(99m)Tc-1(BMS181321)、(99m)Tc-2 和(99m)Tc-5 显示出较高的缺氧细胞摄取率。(99m)Tc-2 的缺氧摄取在 4 小时时达到 59.0±0.9%,是(99m)Tc-1 的 2.4 倍。(99m)Tc-2 显示出较高的缺氧积累,表明引入第二个硝基咪唑氧化还原中心,即 2-硝基咪唑,影响了缺氧积累。因此,(99m)Tc-2 可能成为缺氧标志物的可行候选物。这一发现最终可能导致开发含有多氧化还原中心的化合物作为缺氧标志物。

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