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首页> 外文期刊>Organometallics >Organometallic Palladium Complexes with a Water-Soluble Iminophosphorane Ligand As Potential Anticancer Agents
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Organometallic Palladium Complexes with a Water-Soluble Iminophosphorane Ligand As Potential Anticancer Agents

机译:水溶性亚氨基正膦配体作为潜在抗癌剂的有机金属钯配合物

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摘要

The synthesis and characterization of a new water-soluble iminophosphorane ligand TPA=N-C(O)-2BrC _6H _4 (1, C,N-IM; TPA = 1,3,5-triaza-7-phosphaadamantane) is reported. Oxidative addition of 1 to Pd _2(dba) _3 affords the orthopalladated dimer [Pd(μ-Br){C _6H _4(C(O)N=TPA-kC,N)-2}] _2 (2) as a mixture of cis and trans isomers (1:1 molar ratio) where the iminophosphorane moeity behaves as a C,N-pincer ligand. By addition of different neutral or monoanionic ligands to 2, the bridging chlorides can be cleaved and a variety of hydrophilic or water-soluble mononuclear organometallic palladium(II) complexes of the type [Pd{C _6H _4(C(O)N=TPA-kC,N)-2}(L-L)] (L-L = acac (3); S _2CNMe 2 (4); 4,7-diphenyl-1,10- phenanthrolinedisulfonic acid disodium salt C _(12)H _6N _2(C _6H _4SO _3Na) _2 (5)), [Pd{C _6H _4(C(O)N=TPA-kC,N)-2}(L)Br] (L = P(mC _6H _4SO _3Na) 3 (6); P(3-pyridyl) 3 (7)), and [Pd(C _6H _4(C(O)N=TPA)-2}(TPA) 2Br] (8) are obtained as single isomers. All new complexes were tested as potential anticancer agents, and their cytotoxicity properties were evaluated in vitro against human Jurkat-T acute lymphoblastic leukemia cells, normal T-lymphocytes (PBMC), and DU-145 human prostate cancer cells. Compounds [Pd(μ-Br){C _6H _4(C(O)N=TPA-kC,N)-2}] _2 (2) and [Pd{C _6H _4(C(O)N=TPA-kC,N)-2}(acac)] (3) (which has been crystallographically characterized) display higher cytotoxicity against the above-mentioned cancer cell lines while being less toxic to normal T-lymphocytes (peripheral blood mononuclear cells: PBMC). In addition, 3 is very toxic to cisplatin-resistant Jurkat shBak, indicating a cell death pathway that may be different from that of cisplatin. The interaction of 2 and 3 with plasmid (pBR322) DNA is much weaker than that of cisplatin, pointing to an alternative biomolecular target for these cytotoxic compounds. All the compounds show an interaction with human serum albumin faster than that of cisplatin.
机译:报道了一种新型的水溶性亚氨基正膦配体TPA = N-C(O)-2BrC_6H_4(1,C,N-IM; TPA = 1,3,5-triaza-7-phosphaadamantane)的合成和表征。将1氧化添加到Pd _2(dba)_3中,得到正钯的二聚体[Pd(μ-Br){C _6H _4(C(O)N = TPA-kC,N)-2}] _2(2)作为混合物的顺式和反式异构体(摩尔比为1:1),其中亚氨基膦烷部分表现为C,N-钳位配体。通过向2中添加不同的中性或单阴离子配体,可以裂解桥联的氯化物,并形成[Pd {C _6H _4(C(O)N = TPA]]类型的各种亲水性或水溶性单核有机金属钯(II)络合物-kC,N)-2}(LL)](LL = acac(3); S _2CNMe 2(4); 4,7-二苯基-1,10-菲咯啉二磺酸二钠盐C _(12)H _6N _2( C _6H _4SO _3Na)_2(5)),[Pd {C _6H _4(C(O)N = TPA-kC,N)-2}(L)Br](L = P(mC _6H _4SO _3Na)3( 6); P(3-吡啶基)3(7))和[Pd(C _6H _4(C(O)N = TPA)-2}(TPA)2Br](8)为单一异构体。测试了该复合物作为潜在的抗癌药,并在体外评估了其对人Jurkat-T急性淋巴细胞白血病细胞,正常T淋巴细胞(PBMC)和DU-145人前列腺癌细胞的细胞毒性。[Pd(μ-Br ){C _6H _4(C(O)N = TPA-kC,N)-2}] _2(2)和[Pd {C _6H _4(C(O)N = TPA-kC,N)-2}( acac)](3)(已通过晶体学表征)显示出更高的抗abov细胞毒性e。提到的癌细胞系,但对正常的T淋巴细胞(外周血单核细胞:PBMC)的毒性较小。此外,3对耐顺铂的Jurkat shBak毒性很大,表明细胞死亡途径可能与顺铂不同。 2和3与质粒(pBR322)DNA的相互作用比顺铂弱得多,这为这些细胞毒性化合物提供了另一种生物分子靶标。所有这些化合物与人血清白蛋白的相互作用都比顺铂更快。

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