ABSTRACT
The cyclopentenone unit is a very powerful synthon for the synthesis of a variety of bioactive target molecules. This is due to the broad diversity of chemical modifications available for the enone structural motif. In particular, chiral cyclopentenones are important precursors in the asymmetric synthesis of target chiral molecules. This Review provides an overview of reported methods for enantioselective and asymmetric syntheses of cyclopentenones, including chemical and enzymatic resolution, asymmetric synthesis via Pauson-Khand reaction, Nazarov cyclization and organocatalyzed reactions, asymmetric functionalization of the existing cyclopentenone unit, and functionalization of chiral building blocks.
Subject(s)
Cyclopentanes/chemistry , Carbohydrates/chemistry , Catalysis , Cyclization , Cycloaddition Reaction , Cyclopentanes/chemical synthesis , Prostaglandins/chemical synthesis , Prostaglandins/chemistry , Prostaglandins A/chemical synthesis , Prostaglandins A/chemistry , Stereoisomerism , Transition Elements/chemistryABSTRACT
The new ditopic catecholamide 3,7,11-tris-{N-[3,4-(dihydroxybenzoyl)-aminopropyl]} derivative of a 14-membered tetraazamacrocycle containing pyridine (H(6)L(1)) has been synthesized. The protonation constants of (L(1))(6-) and the stability constants of its mono-, homo- and hetero-dinuclear complexes with Fe(3+), Cu(2+) and Zn(2+) metal ions were determined at 298.2 K and ionic strength 0.10 mol dm(-3) in KNO(3). The large overall basicity of the ligand was ascribed to the very high protonation constants of the catecholate groups, and its acid-base behaviour was correlated with the presence of tertiary nitrogen atoms and secondary amide functions. The UV-vis spectrum of the red solution of [FeL(1)](3-) complex exhibits the LMCT band of catecholate to iron(III), and its EPR spectrum revealed a typical isotropic signal of a rhombic distorted ferric centre in a high-spin state and E/D approximately 0.31, both characteristic of a tris-catecholate octahedral environment. The ligand forms with copper(II) and zinc(II) ions mono- and dinuclear protonated complexes and their stability constants were determined, except for the [ML(1)](4-) complexes as the last proton is released at very high pH. Electronic spectroscopic studies of the copper complexes revealed the involvement of catecholate groups in the coordination to the metal centre in the mono- and dinuclear copper(II) complexes. This information together with the determined stability constants indicated that the copper(II) ion can be involved in both types of coordination site of the ligand with comparable binding affinity. The EPR spectrum of [Cu(2)L(1)](2-) showed a well resolved seven-line hyperfine pattern of copper(II) dinuclear species typical of a paramagnetic triplet spin state with weak coupling between the two metal centres. Thermodynamically stable heterodinuclear complexes, [CuFeH(h)L(1)](h-1) (h = 0-3) and [CuZnH(h)L(1)](h-2) (h = 0-4), were formed as expected from a ditopic ligand having two dissimilar coordination sites. At physiological pH, the [CuFeL(1)](-) complex is formed at approximately 100%. The formation of the [CuFeH(h)L(1)](h-1) complexes in solution was supported by electronic spectroscopic measurements. The data indicated the specific coordination of each metal centre at the dissimilar sites of the ligand, the iron(III) bound to the oxygen donors of the catecholate arms and the copper(II) coordinated to the amine donors of the macrocyclic ring. The two metal centres are weakly coupled, due to the fairly large distance between them.
ABSTRACT
New N-(3-aminopropyl) (L1, L2) and (2-cyanoethyl) (L3, L4) derivatives of a 14-membered tetraazamacrocycle containing pyridine have been synthesized. The protonation constants of L1 and L2 and the stability constants of their complexes with Ni2+, Cu2+, Zn2+ and Cd2+ metal ions were determined in aqueous solutions by potentiometry, at 298.2 K and ionic strength 0.10 mol dm(-3) in KNO3. Both compounds have high overall basicity due to the presence of the aminopropyl arms. Their copper(II) complexes exhibit very high stability constants, which sharply decrease for the complexes of the other studied metal ions, as usually happens with polyamine ligands. Mono- and dinuclear complexes are formed with L2 as well as with L1, but the latter exhibits mononuclear complexes with slightly higher K(ML) values while the dinuclear complexes of L2 are thermodynamically more stable. The presence of these species in solution was supported by UV-VIS-NIR and EPR spectroscopic data. The single crystal structures of [Cu(H2L2)(ClO4)]3+ and [CoL3Cl]+ revealed that the metal centres are surrounded by the four nitrogen atoms of the macrocycle and one monodentate ligand, adopting distorted square pyramidal geometries. In the [CoL3Cl]+ complex, the macrocycle adopts a folded arrangement with the nitrogen atom opposite to the pyridine at the axial position while in the [Cu(H2L2)(ClO4)]3+ complex, the macrocycle adopts a planar conformation with the three aminopropyl arms located at the same side of the macrocyclic plane.
ABSTRACT
Derivatives of synthetic macrocyclic compounds, MCC, 12- and 14-membered tetraazamacrocycles with N-pendant arms, such as N-methyl (Mepy14), N-acetate (DOTA, TETA and ac3py14) and N-methylphosphonate (DOTP) groups, were investigated in terms of their in vitro activity against Mycobacterium avium and for intracellular clearance, using the murine macrophage cell line J-774. Perspective results on a laboratory strain, of opaque morphology, showed in vitro activity with varying inhibitory patterns from one compound to another. The most active compounds, such as TETA, presented N-acetate pendant arms. Inhibition levels of 90% and above were obtained at 50 mg/l. Inhibition was confirmed with both the free compound and its iron(III) complex for DOTP, Mepy14, ac3py14, and TETA. However, with DOTA, no inhibitory effect was observed for the iron(III) complex, suggesting that chelation was at the origin of the inhibitory effect or that the donor atoms of the ligand were strongly involved. Nevertheless, simple experiments indicated that ferric ion might not be responsible for this reversed activity. Intracellular activity using 50 mg/l of TETA confirmed in vitro results with the laboratory strain. Results expressed as relative growth (%), of the drug-containing samples compared to control samples ranged from 2 to 123% (growth promotion) with no apparent relationship between inhibitory activity and the colony morphology of the strains. These studies showed that the evaluation of synthetic macrocycles may be relevant in development of a new family of compounds for use against M. avium infections.
Subject(s)
Anti-Bacterial Agents/pharmacology , Macrocyclic Compounds/pharmacology , Mycobacterium avium Complex/drug effects , Animals , Cell Line , Heterocyclic Compounds, 2-Ring/pharmacology , Macrocyclic Compounds/chemistry , Macrophages/microbiology , Mice , Microbial Sensitivity Tests , Molecular Structure , Mycobacterium avium Complex/growth & development , Oxazoles/pharmacology , Pyrimidinones/pharmacologyABSTRACT
Two N-methylphosphonic acid derivatives of a 14-membered tetraazamacrocycle containing pyridine have been synthesized, H(4)L(1) and H(6)L(2). The protonation constants of these compounds and the stability constants of complexes of both ligands with Ni(2+), Cu(2+) and Zn(2+) were determined by potentiometric methods at 298 K and ionic strength 0.10 mol dm(-3) in NMe(4)NO(3). The high overall basicity of both compounds is ascribed to the presence of the phosphonate arms. (1)H and (31)P NMR spectroscopic titrations were performed to elucidate the sequence of protonation, which were complemented by conformational analysis studies. The complexes of these ligands have stability constants of the order of or higher than those formed with ligands having the same macrocyclic backbone but acetate arms. At pH = 7 the highest pM values were found for solutions containing the compound with three acetate groups, followed immediately by those of H(6)L(2), however, as expected, the increasing pH favours the complexes of ligands containing phosphonate groups. The single-crystal structure of Na(2)[Cu(HL(1))]NO(3)x8H(2)O has shown that the coordination geometry around the copper atom is a distorted square pyramid. Three nitrogen atoms of the macrocyclic backbone and one oxygen atom from one methylphosphonate arm define the basal plane, and the apical coordination is accomplished via the nitrogen atom trans to the pyridine ring of the macrocycle. To achieve this geometric arrangement, the macrocycle adopts a folded conformation. This structure seems consistent with Uv-vis-NIR spectroscopy for the Ni(2+) and the Cu(2+) complexes and with the EPR for the latter.
ABSTRACT
A set of tetraaza macrocycles containing pyridine and methylcarboxylate (ac(3)py14) or methylphosphonate (MeP(2)py14 and P(3)py14) pendant arms were prepared and their stability constants with La(3+), Sm(3+), Gd(3+) and Ho(3+) determined by potentiometry at 25 degrees C and 0.10 M ionic strength in NMe(4)NO(3). The metal:ligand ratio for (153)Sm and (166)Ho and for ac(3)py14, MeP(2)py14 and P(3)py14, as well as the pH of the reaction mixtures, were optimized to achieve a chelation efficiency higher than 98%. These radiocomplexes are hydrophilic and have a significant plasmatic protein binding. In vitro stability was studied in physiological solutions and in human serum. All complexes are stable in saline and PBS, but 20% of radiochemical impurities were detected after 24 h of incubation in serum. Biodistribution studies in mice indicated a slow rate of clearance from blood and muscle, a high and rapid liver uptake and a very slow rate of total radioactivity excretion. Some bone uptake was observed for complexes with MeP(2)py14 and P(3)py14, which was enhanced with time and the number of methylphosphonate groups. This biological profile supports the in vitro instability found in serum and is consistent with the thermodynamic stability constants found for these complexes.
