M2L4 coordination capsules with tunable anticancer activity upon guest encapsulation

被引:44
作者
Ahmedova, Anife [1 ]
Mihaylova, Rositsa [2 ]
Momekova, Denitsa [2 ]
Shestakova, Pavletta [3 ]
Stoykova, Silviya [1 ]
Zaharieva, Joana [1 ]
Yamashina, Masahiro [4 ]
Momekov, Georgi [2 ]
Akita, Munetaka [4 ]
Yoshizawa, Michito [4 ]
机构
[1] Univ Sofia, Fac Chem & Pharm, 1,J Bourchier Blvd, Sofia 1164, Bulgaria
[2] Med Univ Sofia, Fac Pharm, 2 Dunav St, Sofia 1000, Bulgaria
[3] Bulgarian Acad Sci, NMR Lab, Inst Organ Chem, Ctr Phytochem, Acad G Bonchev Str,Bl 9, Sofia 1113, Bulgaria
[4] Tokyo Inst Technol, Lab Chem & Life Sci, Inst Innovat Res, Midori Ku, 4259 Nagatsuta, Yokohama, Kanagawa 2268503, Japan
关键词
SOLUBLE ORGANOMETALLIC CAGES; RUTHENIUM METALLA-ASSEMBLIES; DRUG-DELIVERY; BIOLOGICAL LIGANDS; HEXACATIONIC PRISM; MOLECULAR CAPSULES; ANTHRACENE SHELLS; APOPTOTIC CELLS; HOST CAPABILITY; CANCER-CELLS;
D O I
10.1039/c6dt01801g
中图分类号
O61 [无机化学];
学科分类号
070301 ; 081704 ;
摘要
Metallosupramolecular cages and capsules have gained increasing popularity as both molecular containers and anticancer agents. For successful combination of these properties a thorough analysis of the effect of guest encapsulation on the host's cytotoxic properties is highly required. Here we report on the cytotoxicity modulation of Pt(II) and Pd(II)-linked M2L4 coordination capsules upon encapsulation of guest molecules such as pyrene and caffeine. The anticancer activity of the capsules against various human cancer cells (HT-29, T-24, HL-60 and its resistant counterparts HL-60/Dox and HL-60/CDDP) significantly altered upon the guest encapsulation. The encapsulation of pyrene molecules causes a decrease in the cytotoxicity of the Pt(II) capsule, which is stronger than that of the Pd(II) capsule. The cytotoxicities of the caffeine containing capsules are lower than that of the empty capsules (except for HL-60), but still superior to cisplatin under the same conditions. The observed trends in the anticancer activity of the capsules and their host-guest complexes correlate with their different stabilities toward glutathione, estimated by NMR-based kinetic experiments. Mechanistic insights into the observed cytotoxicities are obtained by fluorescence microscopy imaging of tumor cells treated with the capsules and their pyrene complexes. The data suggest the glutathione-triggered disassembly of the capsular structures as a potential activation pathway for their cytotoxicities.
引用
收藏
页码:13214 / 13221
页数:8
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