Aleksanyan Diana V, Churusova Svetlana G, Konovalov Aleksandr V, Rybalkina Ekaterina Yu, Laletina Lidia A, Ryzhmanova Yana V, Nelyubina Yulia V, Soloveva Svetlana A, Lyubimov Sergey E, Peregudov Alexander S, Klemenkova Zinaida S, Kozlov Vladimir A
A. N. Nesmeyanov Institute of Organoelement Compounds, Russian Academy of Sciences, ul. Vavilova 28, Str. 1, Moscow 119334, Russia.
N. N. Blokhin National Medical Research Center of Oncology of the Ministry of Health of the Russian Federation, Kashirskoe Shosse 23, Moscow 115478, Russia.
Int J Mol Sci. 2025 May 9;26(10):4536. doi: 10.3390/ijms26104536.
The development of new, more effective, and selective anticancer agents is one of the most important tasks of modern medicinal chemistry. Recently, we have found that non-classical Pd(II) pincer complexes derived from thiophosphoryl-appended picolinamides exhibit promising cytotoxic properties. In this work, the potential of this class of metal-based derivatives was studied on an extended family of Pd(II) complexes with a deprotonated amide core featuring thiophosphoryl pendant arms, readily obtained by the direct cyclopalladation of new functionalized amide ligands upon interaction with PdCl(NCPh) under mild conditions. The ligands, in turn, were obtained by conventional amide coupling methods using (aminobenzyl)- and (aminomethyl)diphenylphosphine sulfides as the key precursors and different - and -donor-substituted carboxylic acids. The effect of an acid component and carbon chirality in the ligand framework on the bioactivity of the resulting Pd(II) pincer complexes was elucidated by evaluating their cytotoxicity against different solid and blood cancer cell lines, apoptosis induction ability, and P-glycoprotein (P-gp) affinity, which revealed the high anticancer potential of some of them, and in particular, the potential to overcome drug resistance associated with P-gp overexpression. The representative palladocycle was also shown to possess moderate antibacterial activity.
开发新型、更有效且更具选择性的抗癌药物是现代药物化学最重要的任务之一。最近,我们发现源自硫代磷酰基连接的吡啶甲酰胺的非经典Pd(II)钳形配合物具有良好的细胞毒性。在这项工作中,我们对这类金属基衍生物的潜力进行了研究,研究对象是一个扩展的Pd(II)配合物家族,其具有去质子化的酰胺核心,带有硫代磷酰基侧链,通过新的功能化酰胺配体在温和条件下与PdCl(NCPh)相互作用直接环钯化即可轻松获得。反过来,这些配体是通过常规酰胺偶联方法获得的,使用(氨基苄基)-和(氨基甲基)二苯基膦硫化物作为关键前体以及不同的σ-和π-供体取代的羧酸。通过评估所得Pd(II)钳形配合物对不同实体和血液癌细胞系的细胞毒性、凋亡诱导能力和P-糖蛋白(P-gp)亲和力,阐明了配体框架中酸成分和碳手性对其生物活性的影响,这揭示了其中一些配合物具有很高的抗癌潜力,特别是克服与P-gp过表达相关的耐药性的潜力。代表性的钯环还显示出适度的抗菌活性。
