Advancements in steroidal Pt(II) & Pt(IV) derivatives for targeted chemotherapy (2000-2023)

被引:0
|
作者
Sheikh, Hamdullah Khadim [1 ,3 ]
Ortiz, Cindy Juliet Cristancho [2 ]
Arshad, Tanzila [3 ]
Padron, Jose M. [1 ]
Khan, Haroon [4 ]
机构
[1] Univ La Laguna, Inst Univ Bioorgan Antonio Gonzalez, San Cristobal la Laguna, Spain
[2] Univ Fed Alfenas, Inst Quim, Alfenas, Brazil
[3] Univ Karachi, Fac Pharm, Karachi, Pakistan
[4] Abdul Wali Khan Univ Mardan, Dept Pharm, Mardan 23200, Pakistan
关键词
Alkylating agents; Steroids; DNA nucleobases; Crosslinking reagents; Cisplatin; Antineoplastic agents; Estrogen; Androgen; Bile acid; Cholesterol; ANTITUMOR ESTRADIOL-PLATINUM(II) HYBRID; BIOLOGICALLY IMPORTANT LIGANDS; ESTROGEN-RECEPTOR-ALPHA; PLATINUM(II) COMPLEXES; BILE-ACID; CYTOSTATIC ACTIVITY; METAL-COMPLEXES; DRUG-DELIVERY; STRUCTURAL-CHARACTERIZATION; CISPLATIN SENSITIVITY;
D O I
10.1016/j.ejmech.2024.116438
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
One of the key strategies in chemotherapy involves crosslinking the DNA strands of cancer cells to impede their replication, with platinum (Pt) coordination compounds being a prominent class and cisplatin being its major representative. Steroidal ligands tethered to DNA interactive Pt core act as drug carriers for targeted therapy. While crosslinking of nuclear or mitochondrial DNA strands using coordination complexes has been studied for years, there remains a lack of comprehensive reviews addressing the advancements made in steroidal-Pt derivatives. This review specifically focuses on advancements made in steroid-tethered structural derivatives of Pt (II) or prodrug Pt(IV) for targeted chemotherapy, synthesized between 2000 and 2023. This period was deliberately chosen due to the widespread use of computational techniques for more accurate structure-based drugdesign in last two decades. This review discusses the strategy behind tethering steroidal ligands such as testosterone, estrogen, bile acids, and cholesterol to the central DNA interactive Pt core through specific linker groups. The steroidal ligands function as drug delivery vehicles of DNA interactive Pt core and bind with their respective target receptors or proteins that are often overexpressed in cancer cells, thus enabling targeted delivery of Pt moiety to interact with DNA. We discussed structural features such as the location of the linker group on the steroid, the mono, bi, and tridentate configuration of the chelating arm in coordination with Pt, and the rigidity and flexibility of the linker group. The comparative in vitro, in vivo activities, and relative binding affinities of the designed compounds against standard Pt drugs are also discussed. We also provided a critique of observed trends and shortcomings. Our review will provide insights into future molecular designing of targeted DNA crosslinkers and their structural optimization to achieve desired drug properties. From this analysis, we proposed further research directions leading to the future of targeted chemotherapy.
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页数:20
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