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TNP修饰的链霉亲和素和抗生物素蛋白在肝脏中的蓄积:靶向放疗和化疗的潜在用途。

Liver accumulation of TNP-modified streptavidin and avidin: potential use for targeted radio- and chemotherapy.

作者信息

Schechter B, Arnon R, Freedman Y E, Chen L, Wilchek M

机构信息

Department of Immunology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

J Drug Target. 1996;4(3):171-9. doi: 10.3109/10611869609015974.

Abstract

Hepatic metastases of malignant tumors is a major problem in the treatment of cancers for which the liver is the most common site for recurrences. In the present study we describe a selective delivery system to the liver which may facilitate specific hepatic targeting of anti-cancer agents. Avidin and streptavidin are two biotin-binding proteins with extreme resistance to proteolytic activity. Trinitrophenyl (TNP) modification of these two proteins resulted in specific accumulation in mouse liver with levels of 40-50 percent per gram tissue (%/g) during a period of several days. The two modified proteins could target to the liver high doses of covalently bound radionuclide iodine-125, a biotinylated ligand such as biotinyl-tyrosine (BT) or large biotinylated carriers such as carboxymethyl dextran (CMdex, 40kDa). Appropriately derivatized dextrans serve as carriers for various chemotherapeutic drugs, as demonstrated here for cis-dichlorodiammineplatinum (CDDP). Specific liver targeting of CDDP complexed to CMdex-TNP-streptavidin could be monitored by flame atomic absorption spectrometry of the Pt metal: High levels of the Pt drug were concentrated in the liver for at least 15hr following its targeted delivery as compared to essentially undetectable levels after administration of the free drug.

摘要

恶性肿瘤的肝转移是癌症治疗中的一个主要问题,肝脏是癌症复发最常见的部位。在本研究中,我们描述了一种肝脏选择性递送系统,该系统可能有助于抗癌药物对肝脏的特异性靶向作用。抗生物素蛋白和链霉抗生物素蛋白是两种对蛋白水解活性具有极强抗性的生物素结合蛋白。对这两种蛋白质进行三硝基苯基(TNP)修饰后,在几天的时间里,它们在小鼠肝脏中特异性蓄积,蓄积水平达到每克组织40 - 50%(%/g)。这两种修饰后的蛋白质能够将高剂量的共价结合放射性核素碘 - 125、生物素化配体如生物素基酪氨酸(BT)或大型生物素化载体如羧甲基葡聚糖(CMdex,40kDa)靶向输送至肝脏。如本文所示,适当衍生化的葡聚糖可作为各种化疗药物的载体,顺二氯二氨铂(CDDP)就是一个例子。通过对Pt金属进行火焰原子吸收光谱法检测,可以监测与CMdex - TNP - 链霉抗生物素蛋白复合的CDDP对肝脏的特异性靶向作用:与游离药物给药后基本检测不到的水平相比,靶向递送Pt药物后,肝脏中Pt药物的高水平至少持续了15小时。

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