[摘要] English: New alkylferrocene-containing β-diketones of the type (Cp-R)-Fe-(Cp-COCH2COCH3), where R =C9H19, C10H21, C12H25, C14H29 and C18H37 as well as (Cp)-Fe-(R-Cp-COCH2COCH3), (Cp-R)-Fe-(R-Cp-COCH2COCH3) and (Cp-R)-Fe-(Cp-COCH2CO-Cp)-Fe-(Cp-R) with R = C10H21 or C12H25were prepared by Claisen condensation of acetyl-alkylferrocene derivatives and the appropriateester under the influence of lithium diisopropylamide. Complexation of all the β-diketones with[RhCl2(cod)2] in DMF gave the [Rh(β-diketonato)(cod)] complexes. The pKa/ values of the new β-diketone derivatives were determined spectroscopically in water containing 10 % acetonitrile (v/v).The keto-enol isomerization kinetics of all new β-diketones was studied in CDCl3 by 1H NMRspectroscopy.Electrochemical studies revealed that all the β-diketones exhibited an electrochemically andchemically reversible one-electron transfer process for the Fc/Fc+ couple. The redox active centreof all the β-diketones exhibited Eo/ values that are independent of the alkyl chain length of theferrocene-containing β-diketones due to the lack of conjugation between the ferrocenyl group andthe alkyl R groups. Cyclic voltammetry results of all the rhodium complexes showed that the RhInucleus exhibited an electrochemically quasi reversible process.Substitution reactions of the β-diketonato ligand from [Rh(β-diketonato)(cod)] with 1,10-phenanthroline exhibited saturation kinetics. Second-order rate constants, k2, were determined fromthe linear plots of 1/kobs against 1/[1,10-phenanthroline]. The large negative activation entropyvalues suggested an association mechanism. All substitution reactions had no observablemechanistic solvent pathway.Phase studies showed that the ferrocenyl derivatives and free β-diketones exhibited solid state phasechanges while the rhodium(I) complexes showed no pronounced melting or crystallization peaksdue to very slow crystallization kinetics.Cytotoxic properties in terms of potential anticancer applications of selected β-diketones and theirrhodium complexes are described. Cytotoxicity of these complexes was probed with respect tohuman colorectal (CoLo) and human cervix epitheloid (HeLa) cancer cell lines. All the drugs thatwere investigated in this study had lower IC50 values than the rhodium complexes without longchain alkyl substituents.