6533b82cfe1ef96bd128f3e6

RESEARCH PRODUCT

Synthesis and protonation behaviour of the macrocycle 2,6,10,13,17,21-hexaaza[22]metacyclophane. Thermodynamic and NMR studies on the interaction of 2,6,10,13,17,21-hexaaza[22]metacyclophane and on the open-chain polyamine 4,8,11,15-tetraazaoctadecane-1,18-diamine with ATP, ADP and AMP

Conxa SorianoEnrique García-españaJosé-m. LlinaresJuan A. AguilarJ. A. RamirezJoséa. GuerreroSantiago V. Luis

subject

chemistry.chemical_classificationChemistryStereochemistryProtein subunitProtonationRing (chemistry)Inorganic Chemistrychemistry.chemical_compoundDiamineMaterials ChemistryNucleotideATP–ADP translocasePhysical and Theoretical ChemistryPolyamineCyclophane

description

Abstract The novel cyclophane receptor 2,6,10,13,17,21-hexaaza[22]metacyclophane (L) has been synthesised and characterised. The acid-base behaviour and interaction with ATP, ADP and AMP have been studied by potentiometry in 0.15 mol dm−3 at 298.1 K and multinuclear NMR. L presents in its protonated forms a molecular organization which enables its multipoint binding with nucleotides. Salt-bridge formation occur between the polyammonium sites of L and the phosphate chain of the nucleotides while π-stacking between the meta-phenylene subunit incorporated in the receptor and the adenine ring of the nucleotides.

yearjournalcountryeditionlanguage
1996-05-01Inorganica Chimica Acta
https://doi.org/10.1016/0020-1693(96)05075-x