Targeted Delivery of Proteasome Inhibitors to Somatostatin-Receptor-Expressing Cancer Cells by Octreotide Conjugation

被引:3
|
作者
Beck, Philipp [1 ]
Cui, Haissi [1 ]
Hegemann, Julian D. [2 ]
Marahiel, Mohammed A. [2 ]
Krueger, Achim [3 ]
Groll, Michael [1 ]
机构
[1] Tech Univ Munich, Ctr Integrated Prot Sci Munich, Dept Chem, D-85748 Garching, Germany
[2] Univ Marburg, Dept Chem Biochem, D-35032 Marburg, Germany
[3] Tech Univ Munich, Klinikum Rechts Isar, Inst Mol Immunol & Expt Oncol, D-81675 Munich, Germany
关键词
antitumor agents; drug delivery; drug design; proteasome inhibition; receptor-mediated uptake; PROTEIN-SYNTHESIS; TUMOR-CELLS; IN-VITRO; DOXORUBICIN; ANTICANCER; DNA; PACLITAXEL; THERAPY; ANALOGS; SYSTEMS;
D O I
10.1002/cmdc.201500449
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Clinical application of proteasome inhibitors (PIs) is so far limited to peripheral blood cancers due to the pronounced cytotoxicity towards all cell types. Targeted delivery of PIs could permit the treatment of other cancers along with decreasing side effects. Herein we describe the first small-molecule proteasome inhibitor conjugate for targeted delivery, created by fusing PIs to a synthetic ligand of somatostatin receptors, which are highly expressed in a variety of tumors. X-ray crystallographic studies and in vitro IC50 measurements demonstrated that addition of the cyclopeptide octreotide as a targeting vehicle does not affect the PI's binding mode. The cytotoxicity of the conjugate against somatostatin-receptor-expressing cells was up to 11-fold higher than that of a non-targeting surrogate. We have therefore established PIs as a new payload for drug conjugates and have shown that targeted delivery thereof could be a promising approach for the broader application of this FDA-approved class of compounds.
引用
收藏
页码:1969 / 1973
页数:5
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