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Tumor detection using (18)F-labeled matrix metalloproteinase-2 inhibitor.

机译:使用(18)F标记的基质金属蛋白酶2抑制剂进行肿瘤检测。

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摘要

Matrix metalloproteinase-2 (MMP-2) is a key enzyme involved in tumor invasiveness. (2R)-2- [4-(6-[(18)F]Fluorohex-1-ynyl)-benzenesulfonylamino]-3-methylbutyric acid ([(18)F]SAV03), a new fluorine-18 labeled MMP-2 inhibitor developed for tumor imaging with PET, was biologically evaluated using in vivo tumor model. Enzymatic MMP-2 assay of SAV03 yielded an IC(50) value of 1.9 &mgr;M. Biodistribution study of [(18)F]SAV03 using Ehrlich tumor bearing mice showed that the uptake in tumor was higher than in other organs, except for the liver, small intestine, and bone. When [(18)F]SAV03M, a methyl ester of [(18)F]SAV03, was used as a prodrug, the uptake in liver at 30 min after injection decreased by half and that in tumor increased by 2.4 times, compared with [(18)F]SAV03. Radio-thin-layer chromatographic analysis of [(18)F]SAV03M metabolites revealed that administered [(18)F]SAV03M was easily converted to the parent drug in vivo and accumulated in tumor tissue. Thus, [(18)F]SAV03M is suitable as the prodrug of [(18)F]SAV03 with potent efficacy. Whole body autoradiography using [(18)F]SAV03M also indicated tumor-specific accumulation of radioactivity, while higher accumulations in bone and intestinal contents were observed. Our results suggest that [(18)F]SAV03M could be potentially suitable for tumor imaging with PET.
机译:基质金属蛋白酶2(MMP-2)是涉及肿瘤侵袭性的关键酶。 (2R)-2- [4-(6-[(18)F]氟己基-1-炔基)-苯磺酰基氨基] -3-甲基丁酸([(18)F] SAV03),一种新的被氟18标记的MMP-使用体内肿瘤模型生物学评估了开发用于PET肿瘤成像的2种抑制剂。 SAV03的酶促MMP-2分析得出的IC(50)值为1.9M。 [(18)F] SAV03的使用Ehrlich荷瘤小鼠的生物分布研究表明,除肝脏,小肠和骨骼外,对肿瘤的摄取高于其他器官。当使用[(18)F] SAV03的甲酯[(18)F] SAV03M作为前药时,注射后30分钟肝脏中的摄取减少一半,而肿瘤中的摄取增加2.4倍。 [(18)F] SAV03。 [(18)F] SAV03M代谢产物的放射性薄层色谱分析表明,所给药的[(18)F] SAV03M在体内易于转化为母体药物并在肿瘤组织中积累。因此,[(18)F] SAV03M适合作为具有有效功效的[(18)F] SAV03的前药。使用[(18)F] SAV03M的全身放射自显影也显示了肿瘤特异性放射性的积累,而观察到骨和肠内容物的积累更高。我们的研究结果表明[(18)F] SAV03M可能潜在地适合用PET进行肿瘤成像。

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