School of Chemistry and Physics, University of KwaZulu-Natal, Private Bag X01, Scottsville, Pietermaritzburg 3209, South Africa; Department of Chemistry, Maseno University, P.O. Box 333-40105, Maseno, Kenya.
School of Chemistry and Physics, University of KwaZulu-Natal, Private Bag X01, Scottsville, Pietermaritzburg 3209, South Africa.
J Inorg Biochem. 2020 Dec;213:111261. doi: 10.1016/j.jinorgbio.2020.111261. Epub 2020 Sep 29.
Four [(N^N^N)PdCl] complexes [chloride-(2,2':6',2''-terpyridine)Pd(II)]Cl (PdL1), [chlorido(2,6-bis(N-pyrazol-2-yl)pyridine)Pd(II)]Cl (PdL2), [chlorido(2,6-bis(3,5-dimethyl-N-pyrazol-2-yl)pyridine)Pd(II)]Cl (PdL3) and [chlorido(2,6-bis(3,5-dimethyl-N-pyrazol-2-ylmethyl)pyridine)Pd(II)]BF (PdL4) were synthesized and characterized. The rates of substitution of these Pd(II) complexes with thiourea nucleophiles viz; thiourea (Tu), N,N'-dimethylthiourea (Dmtu) and N,N,N',N'-tetramethylthiourea (Tmtu) was investigated under pseudo first-order conditions as a function of nucleophile concentration [Nu] and temperature using the stopped-flow technique. The observed rate constants vary linearly with [Nu]; k = k[Nu] and decreased in the order: PdL1 > PdL2 > PdL3 ≫ PdL4. The lower π-acceptability of the cis-coordinated N-pyrazol-2-yl groups (which coordinates via pyrazollic-N π-donor atoms) of the PdL2-4 significantly decelerates the reactivity relative to PdL1. Furthermore, the six-membered chelates having methylene bridge in PdL4 do not allow π-extension in the ligand and introduces steric hindrance further lowering the reactivity. Trends in DFT calculated data supported the observed reactivity trend. Spectrophotometric titration data of complexes with calf thymus DNA (CT-DNA) and viscosity measurements of the resultant mixtures suggested that associative interactions occur between the complexes and CT-DNA, likely through groove binding with high binding constants (K = 10 M). In vitro MTT [3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide] cytotoxic activity data showed that PdL1 was the most potent complex against MCF7 breast cancer cells; its IC value is lower than that of cisplatin. The results demonstrate how modification of a spectator ligand can be used to slow down the reactivity of Pd(II) complexes. This is of special importance in controlling drug toxicity in both pharmaceutical and biomedical applications.
合成并表征了四个[(N^N^N)PdCl]配合物[氯化(2,2':6',2''-三联吡啶)Pd(II)]Cl(PdL1)、[氯化(2,6-双(N-吡唑-2-基)吡啶)Pd(II)]Cl(PdL2)、[氯化(2,6-双(3,5-二甲基-N-吡唑-2-基)吡啶)Pd(II)]Cl(PdL3)和[氯化(2,6-双(3,5-二甲基-N-吡唑-2-基甲基)吡啶)Pd(II)]BF(PdL4)。在假一级条件下,用硫脲亲核试剂(硫脲(Tu)、N,N'-二甲基硫脲(Dmtu)和 N,N,N',N'-四甲基硫脲(Tmtu))研究了这些 Pd(II)配合物的取代速率,作为亲核试剂浓度[Nu]和温度的函数,使用停流技术。观察到的速率常数与[Nu]线性相关;k=k[Nu],并按以下顺序降低:PdL1>PdL2>PdL3≫PdL4。PdL2-4 中顺式配位的 N-吡唑-2-基基团(通过吡唑氮π-供体原子配位)的较低π-接受性显著减缓了反应性,相对于 PdL1。此外,在 PdL4 中具有亚甲基桥的六元螯合物不允许配体中的π-延伸,并进一步引入空间位阻,从而降低反应性。DFT 计算数据的趋势支持观察到的反应性趋势。与小牛胸腺 DNA(CT-DNA)的配合物的分光光度滴定数据和所得混合物的粘度测量表明,复合物与 CT-DNA 之间发生缔合相互作用,可能通过沟槽结合具有高结合常数(K=10M)。体外 MTT[3-(4,5-二甲基噻唑-2-基)-2,5-二苯基四唑溴盐]细胞毒性活性数据表明,PdL1 是对 MCF7 乳腺癌细胞最有效的复合物;其 IC 值低于顺铂。结果表明,如何修饰 spectator 配体可用于减缓 Pd(II)配合物的反应性。这在控制药物毒性方面在制药和生物医学应用中都非常重要。
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