PtI2(DACH), the iodido analogue of oxaliplatin as a candidate for colorectal cancer treatment: chemical and biological features

被引:37
作者
Cirri, D. [1 ]
Pillozzi, S. [2 ]
Gabbiani, C. [3 ]
Tricomi, J. [1 ]
Bartoli, G. [1 ,2 ]
Stefanini, M. [4 ]
Michelucci, E. [5 ]
Arcangeli, A. [1 ]
Messori, L. [1 ]
Marzo, T. [1 ,3 ]
机构
[1] Univ Florence, Dept Chem, Lab Met Med MetMed, Via Lastruccia 3, I-50019 Sesto Fiorentino, Italy
[2] Univ Florence, Dept Expt & Clin Med, Viale GB Morgagni 50, I-50134 Florence, Italy
[3] Univ Pisa, Dept Chem & Ind Chem, Via Moruzzi 13, I-56124 Pisa, Italy
[4] DIVAL Toscana Srl, Via Madonna Piano 6, I-50119 Sesto Fiorentino, Italy
[5] Univ Florence, Mass Spectrometry Ctr CISM, Via U Schiff 6, I-50019 Sesto Fiorentino, Italy
关键词
MASS-SPECTROMETRY; CISPLATIN; LYSOZYME; ADDUCTS; CARBOPLATIN;
D O I
10.1039/c6dt03867k
中图分类号
O61 [无机化学];
学科分类号
070301 ; 081704 ;
摘要
Colorectal cancer (CRC) is a global health problem being the fourth most common cause of death due to cancer worldwide. Oxaliplatin plays a key role in current CRC treatment but shows serious drawbacks, such as a high systemic toxicity and the frequent insurgence of Pt resistance. In search of novel and more efficacious Pt-based drugs for CRC treatment, we synthesized and characterised PtI2(DACH), an oxaliplatin analogue. PtI2(DACH) was obtained through the replacement of bidentate oxalate with two iodides. PtI2(DACH) turned out to be more lipophilic than oxaliplatin, a fact that led to an enhancement of its cellular uptake. In contrast to oxaliplatin, PtI2(DACH) showed a scarce reactivity towards model proteins, while maintaining affinity for a standard DNA oligo. Notably, PtI2(DACH) induced cytotoxicities roughly comparable to those of oxaliplatin in three representative CRC cell lines. Moreover, it was able to trigger cell apoptosis, to an extent even better than cisplatin and oxaliplatin. Overall, a rather promising picture emerges for this novel Pt drug that merits, in our opinion, a deeper and more extensive preclinical evaluation.
引用
收藏
页码:3311 / 3317
页数:7
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