Benzaldehyde thiosemicarbazone complexes of platinum: Syntheses, structures and cytotoxic properties

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• 作者：Sarmistha Halder ; Piyali Paul ; Shie-Ming Peng ; Gene-Hsiang Lee ; Asama Mukherjee ; Sushanta Dutta ; Utpal Sanyal ; Samaresh Bhattacharya
• 关键词：Benzaldehyde thiosemicarbazones ; Platinum complexes ; Syntheses ; Structures ; Cytotoxic properties
• 刊名：Polyhedron
• 出版年：2012
• 出版时间：19 September, 2012
• 年：2012
• 卷：45
• 期：1
• 页码：177-184
• 全文大小：623 K

文摘

The reaction of 4-R-benzaldehyde thiosemicarbazones (denoted in general as H₂L-R, where H₂ stands for the two dissociable protons and R (R = OCH₃, CH₃, H, Cl and NO₂) for the substituent on the phenyl ring) with [Pt(PPh₃)₂Cl₂] in the presence of NEt₃ afforded a family of organometallic complexes of platinum(II) of the type [Pt(PPh₃)(L-R)]. Reaction of the same group of ligands with K₂[PtCl₄] in the presence of NEt₃ afforded complexes of the type [Pt(HL-R)₂]. The crystal structure of [Pt(PPh₃)(L-CH₃)] and [Pt(HL-CH₃)₂] have been determined. In the [Pt(PPh₃)(L-R)] complexes, the benzaldehyde thiosemicarbazones are coordinated to platinum as dianionic tridentate C,N,S-donors. In the [Pt(HL-R)₂] complexes, the benzaldehyde thiosemicarbazones are coordinated to the metal center as bidentate N,S-donors, forming five-membered chelate rings, and with reference to the structure of the uncoordinated thiosemicarbazone ligand, this coordination mode is associated with a change in stereochemistry around the CN bond. All the [Pt(PPh₃)(L-R)] and [Pt(HL-R)₂] complexes display intense absorptions in the visible and ultraviolet regions. The cytotoxic effects of these complexes, examined on the human leukemia cell line HL-60 and human lymphoma cell line U-937, have shown that all the [Pt(PPh₃)(L-R)] and [Pt(HL-R)₂] complexes are cytotoxic in nature and their IC₅₀ values indicate their potential use as antitumor agents.