Repozytorium

Tetraacetatodirhodium(II) complexes with tris(methoxyphenyl)phosphines, their reactivity, structure, and antitumor activity.

Autorzy

Florian P. Pruchnik

Radosław Starosta

Zbigniew Ciunik

Adam Opolski

Joanna Wietrzyk

E. Wojdat

Danuta Duś

Rok wydania

2001

Czasopismo

Canadian Journal of Chemistry

Numer woluminu

79

Strony

868-877

DOI

10.1139/v01-080

Kolekcja

Naukowa

Język

Angielski

Typ publikacji

Artykuł

Streszczenie

Reactions of [Rh2(µ-OAc)4(H2O)2] ([1·(H2O)2]) with tris(3-methoxyphenyl)phosphine at 1:1 and 1:2 molar ratios yield, first, the appropriate adducts: [1·(H2O){P(C6H4-3-OMe)3}] and [1·{P(C6H4-3-OMe)3}2], and then [Rh2(µ-OAc)3{µ-(C6H3-3-OMe)P(C6H4-3-OMe)2}(HOAc)2] ([2·(HOAc)2]), and [Rh2(µ-OAc)2{µ-(C6H3-3-OMe)P(C6H4-3-OMe)2}2(HOAc)2] ([3·(HOAc)2]) complexes, respectively. They have been characterized by spectroscopic methods. The molecular structure of [3·(HOAc)(H2O)] has been determined crystallographically. The complexes [3·(HOAc)2], [Rh2(µ-OAc)3{µ-(C6H3-4-OMe)P(C6H4-4-OMe)2}(HOAc)2] ([4·(HOAc)2]), and [Rh2(µ-OAc)2{µ-(C6H3-4-OMe)P(C6H4-4-OMe)2}2(HOAc)2] ([5·(HOAc)2]) reversibly react with CO giving mono- and biadducts. Antitumor activity of binuclear rhodium(II) compounds [3·(HOAc)2], [Rh2(µ-OAc)3{µ-(C6H3-2-O)P(C6H3-2-OMe)2}(HOAc)] ([6·(HOAc)]), and [Rh2(µ-OAc)3{µ-(C6H3-6-OMe-2-O)P[(C6H3-2,6-(OMe)2]2}(HOAc)] ([7·(HOAc)]) have been investigated in vitro. The most active agent for investigated tumor lines is complex [6·(HOAc)]. It shows higher activity than cisplatin (cis-[PtCl2(NH3)2]). Antitumor activity decreases in the series: [6·(HOAc)] > [7·(HOAc)] > [3·(HOAc)2]. Activity of all investigated rhodium(II) complexes is higher than that of [1·(H2O)2].Key words: dirhodium(II) complexes, functionalized phosphines, aryl phosphines, ferrocenylmethylphosphines, adducts with CO, antitumor activity, orthometallation reactions.

Adres publiczny

https://doi.org/10.1139/v01-080

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