ITA
ENG

PH-DEPENDENT COMPETITION BETWEEN KAPPA(2)N7,O(P) MACROCHELATION AND MU-N-1,N-7 OLIGOMER FORMATION FOR (ETA(6)-ARENE)RU-II COMPLEXES OF ADENOSINE AND GUANOSINE 5'-MONO-PHOSPHATES, 5'-DI-PHOSPHATES AND 5'-TRI-PHOSPHATES

Authors

KORN S SHELDRICK WS

Citation

S. Korn et Ws. Sheldrick, PH-DEPENDENT COMPETITION BETWEEN KAPPA(2)N7,O(P) MACROCHELATION AND MU-N-1,N-7 OLIGOMER FORMATION FOR (ETA(6)-ARENE)RU-II COMPLEXES OF ADENOSINE AND GUANOSINE 5'-MONO-PHOSPHATES, 5'-DI-PHOSPHATES AND 5'-TRI-PHOSPHATES, Journal of the Chemical Society. Dalton transactions, (12), 1997, pp. 2191-2199

Citations number

Categorie Soggetti

Chemistry Inorganic & Nuclear

Journal title

Journal of the Chemical Society. Dalton transactions → ACNP

ISSN journal

03009246

Issue

Year of publication

1997

Pages

2191 - 2199

Database

ISI

SICI code

0300-9246(1997):12<2191:PCBKMA>2.0.ZU;2-J

Abstract

The pH-dependent reaction of [Ru(eta(6)-C6H6)(D2O)(3)](2+) with adenos ine and guanosine 5'-mono-, -di- and -tri-phosphates has been studied by H-1 and P-31-{H-1} NMR spectroscopy. Diastereomeric mu-1 kappa N-1: 2 kappa(2)N(6), N-7 co-ordinated cyclic trimers of the type [{Ru(5'-AM P)(eta(6)-C6H6)}(3)] predominate for adenosine 5'-monophosphate (5'-AM P(2-)) in the range pH 3.30-9.18. An X-ray structural analysis of the RuSRuSRuS diastereomer [{Ru(5'-AMP)(eta(6)-p-MeC6H4Pr1)}(3)] .7.5H(2) O 1b established a pronounced degree of conformational flexibility in the sugar and phosphate residues. In contrast to 5'-AMP(2)-, cyclic tr imers cannot be observed in more strongly acid solution (pH less than or equal to 3.16) for the equilibrium system 5'-ATP-(eta(6)-C6H6)Ru-I I (5'-ATP(4-) = adenosine 5'-triphosphate) and remain relatively minor species even at neutral or higher pH values. As confirmed by pronoun ced low-held P-31-{H-1} NMR shifts of up to 7.8 and 8.6 ppm for the be ta- and gamma-phosphorus atoms, kappa(3)N(7), O(P-beta), O(P-gamma) ma crochelates provide the dominant metal species in acid solution. Time- dependent NMR studies for 5'-ADP-(eta(6)-C6H6)Ru-II (5'-ADP(3-) = aden osine 5'-diphosphate) indicated that initial macrochelation of this nu cleotide is followed by cleavage of the beta-phosphate group and forma tion of cyclic trimers of 5'-AMP(2-). Reaction of guanosine 5'-monopho sphate (5'-GMP(2-)) with [Ru(eta(6)-C6H6)(D2O)(3)](2+) afforded kappa N-7-co-ordinated 1:1 and 2:1 complexes in the range pH 3.69-8.38. In addition to analogous 1:1 and 2:1 species, kappa(3)N(7), O(P-beta), O( P-gamma) macrochelates are observed for the 5'-GTP-(eta(6)-C6H6)Ru-II equilibrium system (5'-GTP(4-) = guanosine 5'-triphosphate) in,acid so lution. Initial macrochelation in the 5'-GDP-(eta(6)-C6H6)Ru-II system (5'-GDP(3-) = guanosine 5'-diphosphate) again leads to rapid cleavage of the terminal beta-phosphate function.