ABSTRACT
Here we prepare pH-responsive complex molecular hydrogels from oppositely charged tetrapeptidic components that can be pH-tuned resulting in interconversion between different networks. Two different systems are described based on tetrapeptides with an alternating sequence of non-polar (F) and polar (D or K) residues. Co-aggregated hydrogels are easily formed in situ at neutral pH whereas one-component networks are maintained after changing into acidic or basic pH. These systems have been applied for the pH selective release of two hydrophobic dyes - Methylene Blue and Bromothymol Blue - as drug models. Different release profiles have been observed depending on the characteristics of the network as well as the pH of the media. These materials offer great potential as multidrug carriers.
ABSTRACT
We examine the self-assembly of a peptide A6H comprising a hexa-alanine sequence A6 with a histidine (H) "head group", which chelates Zn(2+) cations. We study the self-assembly of A6H and binding of Zn(2+) ions in ZnCl2 solutions, under acidic and neutral conditions. A6H self-assembles into nanotapes held together by a ß-sheet structure in acidic aqueous solutions. By dissolving A6H in acidic ZnCl2 solutions, the carbonyl oxygen atoms in A6H chelate the Zn(2+) ions and allow for ß-sheet formation at lower concentrations, consequently reducing the onset concentration for nanotape formation. A6H mixed with water or ZnCl2 solutions under neutral conditions produces short sheets or pseudocrystalline tapes, respectively. The imidazole ring of A6H chelates Zn(2+) ions in neutral solutions. The internal structure of nanosheets and pseudocrystalline sheets in neutral solutions is similar to the internal structure of A6H nanotapes in acidic solutions. Our results show that it is possible to induce dramatic changes in the self-assembly and chelation sites of A6H by changing the pH of the solution. However, it is likely that the amphiphilic nature of A6H determines the internal structure of the self-assembled aggregates independent from changes in chelation.
Subject(s)
Chelating Agents/chemistry , Peptides/chemistry , Surface-Active Agents/chemistry , Zinc/chemistry , Alanine/chemistry , Histidine/chemistry , Hydrogen-Ion Concentration , Particle Size , Peptides/chemical synthesis , Surface PropertiesABSTRACT
The conformation of a model peptide AAKLVFF based on a fragment of the amyloid beta peptide Abeta16-20, KLVFF, is investigated in methanol and water via solution NMR experiments and molecular dynamics computer simulations. In previous work, we have shown that AAKLVFF forms peptide nanotubes in methanol and twisted fibrils in water. Chemical shift measurements were used to investigate the solubility of the peptide as a function of concentration in methanol and water. This enabled the determination of critical aggregation concentrations. The solubility was lower in water. In dilute solution, diffusion coefficients revealed the presence of intermediate aggregates in concentrated solution, coexisting with NMR-silent larger aggregates, presumed to be beta-sheets. In water, diffusion coefficients did not change appreciably with concentration, indicating the presence mainly of monomers, coexisting with larger aggregates in more concentrated solution. Concentration-dependent chemical shift measurements indicated a folded conformation for the monomers/intermediate aggregates in dilute methanol, with unfolding at higher concentration. In water, an antiparallel arrangement of strands was indicated by certain ROESY peak correlations. The temperature-dependent solubility of AAKLVFF in methanol was well described by a van't Hoff analysis, providing a solubilization enthalpy and entropy. This pointed to the importance of solvophobic interactions in the self-assembly process. Molecular dynamics simulations constrained by NOE values from NMR suggested disordered reverse turn structures for the monomer, with an antiparallel twisted conformation for dimers. To model the beta-sheet structures formed at higher concentration, possible model arrangements of strands into beta-sheets with parallel and antiparallel configurations and different stacking sequences were used as the basis for MD simulations; two particular arrangements of antiparallel beta-sheets were found to be stable, one being linear and twisted and the other twisted in two directions. These structures were used to simulate circular dichroism spectra. The roles of aromatic stacking interactions and charge transfer effects were also examined. Simulated spectra were found to be similar to those observed experimentally (in water or methanol) which show a maximum at 215 or 218 nm due to pi-pi* interactions, when allowance is made for a 15-18 nm red-shift that may be due to light scattering effects.
Subject(s)
Amyloid beta-Peptides/chemistry , Methanol/chemistry , Peptide Fragments/chemistry , Amino Acid Sequence , Computer Simulation , Humans , Molecular Dynamics Simulation , Nuclear Magnetic Resonance, Biomolecular , Protein Folding , Protein Multimerization , Protein Structure, Secondary , Solubility , ThermodynamicsABSTRACT
Dioxapolyaza cyclophanes derived from resorcinol and different polyamine chains have been studied in aqueous solution as abiotic receptors for nucleotides. The presence of the additional ethyleneoxy subunits is reflected in a higher basicity and in a significant increase in the log K values for the interaction with nucleotides relative to that of related polyazacyclophanes.
Subject(s)
Crown Ethers/chemistry , Electrons , Hydrocarbons, Aromatic/chemistry , Nucleotides/chemistry , Oxygen/chemistry , Computer Simulation , Magnetic Resonance Spectroscopy , Models, Molecular , PotentiometryABSTRACT
The interaction with Cu2+ and dopamine of three polyazacyclophanes containing pyrazole fragments as spacers is described. Formation of mixed complexes Cu2+-macrocycle-dopamine has been studied by potentiometric methods in aqueous solution. The crystal structures of the complexes [Cu2(L1)(H2O)2](ClO4)4*2H2O (4) (L1 = 13,26-dibenzyl-3,6,9,12,13,16,19,22,25,26-decaazatricyclo[22.2.1.1(11,14)]octacosa-1(27),11,14(28),24-tetraene) and [Cu2(H-1L3)](HClO4)(ClO4)2*2H2O (6) (L3 = 1,4,7,8,11,14,17,20,21,24,29,32,33,36-tetradecaazapentacyclo[12.12.12.1(6,9).1(19,22).1(31,34)]hentetraconta-6,9(41),19(40),21,31,34(39)-hexaene) are presented. In the first one (4), each Cu2+ coordination site is made up by the three nitrogens of the polyamine bridge, a sp2 pyrazole nitrogen and one water molecule that occupies the axial position of a square pyramid. The distance between the copper ions is 6.788(2) A. In the crystal structure of 6, the coordination geometry around each Cu2+ is square pyramidal with its base being formed by two secondary nitrogens of the bridge and two nitrogen atoms of two different pyrazolate units which act as exobidentate ligands. The axial positions are occupied by the bridgehead nitrogen atoms; the elongation is more pronounced in one of the two sites [Cu(1)-N(1), 2.29(2) A; Cu(2)-N(6), 2.40(1) A]. The Cu-N distances involving the deprotonated pyrazole moieties are significantly shorter than those of the secondary nitrogens. The Cu(1)...Cu(2) distance is 3.960(3) A. The pyrazole in the noncoordinating bridge does not deprotonate and lies to one side of the macrocyclic cavity. One of the aliphatic nitrogens of this bridge is protonated and hydrogen bonded to a water molecule, which is further connected to the sp2 nitrogen of the pyrazole moiety through a hydrogen bond. The solution studies reveal a ready deprotonation of the pyrazole units induced by coordination to Cu2+. In the case of L2 (L2 = 3,6,9,12,13,16,19,22,25,26-decaazatricyclo[22.2.1.1(11,14)]octacosa-1(27),11,14(28),24-tetraene), deprotonation of both pyrazole subunits is already observed at pH ca. 4 for 2:1 Cu2+:L2 molar ratios. All three free receptors interact with dopamine in aqueous solution. L3 is a receptor particularly interesting with respect to the values of the interaction constants over five logarithmic units at neutral pH, which might suggest an encapsulation of dopamine in the macrocyclic cage. All three receptors form mixed complexes Cu2+-L-dopamine. The affinity for the formation of ternary dopamine complexes is particularly high in the case of the binuclear Cu2+ complexes of the 1-benzyl derivative L1.
Subject(s)
Copper/chemistry , Dopamine/chemistry , Organometallic Compounds/chemistry , Polyamines/chemistry , Pyrazoles/chemistry , Cations, Divalent , Crystallography, X-Ray , Electrochemistry , Kinetics , Models, Molecular , Molecular Structure , ThermodynamicsABSTRACT
Forty-two patients have been surgically treated for medically uncontrollable epilepsy, using the Talairach and Bancaud methodology. The mean age of the patients was 19 years (range 6-54 years). The location of the epileptogenic zone was:frontal in 18 patients, temporal in 14, temporo-parieto-occipital junction in 4, parietal in 4 and occipital in 2. The overall surgical results are: 20 patients are seizure free and 6 patients had occasional seizures (62% success rate). There has been a significant decrease in the number of seizures in 12 patients. The seizures persist in 4 patients. Only two patients, both with a parietal focus, presented additional postoperative neurological deficit (mild paresis in the contralateral lover limb). This was preoperatively foreseen, and accepted by the patient, on guarantees of the removal of the epileptogenic zone and amelioration of seizures.
Subject(s)
Epilepsy/surgery , Postoperative Complications/etiology , Stereotaxic Techniques , Adolescent , Adult , Brain Mapping , Cerebral Cortex/surgery , Child , Follow-Up Studies , Humans , Middle AgedSubject(s)
Critical Care , Liver Diseases/surgery , Liver Transplantation , Postoperative Care , Adult , Humans , Liver Diseases/nursing , Middle AgedABSTRACT
The authors present 4 patients with medically uncontrollable epilepsy of tumoural aetiology (grade I-II gliomas). In two of them, CT scan showed probable neoplastic lesions, located deeply in the left frontal and right temporal lobes respectively, reflected in the SEG studies only in the second case. The other two were patients with left frontal gliomas in whom seizures did not disappear after removal of the tumour. After SEEG studies defined the epileptogenic zone and the lesion and these were removed, complete suppression of the seizures was achieved in two patients and the other two only unfrequently suffered seizures. We emphasize the importance of SEEG studies for success in treating patients with gliomata previously diagnosed by CT scan, and who have seizures uncontrolled by anticonvulsants as the only symptom.
