The conformations of all stereoisomers of PMRI cyclotetrapeptide mimetics 1 – 8 are essentially determined by the predisposition of the diamine to stabilize β‐turns. The peptide mimetics can be regarded as 3D scaffolds for designing molecules with a predictable display of the pharmacophores. We used the models for testing novel RGD analogues as αvβ3‐integrin receptor antagonists.
The main objective of this work was to investigate the different effects of transition metals (TiO2, VCl3, HfCl4) on the hydrogen desorption/absorption of NaAlH4. The HfCl4 doped NaAlH4 showed the lowest temperature of the first desorption at 85 °C, while the one doped with VCl3 or TiO2 desorbed at 135 °C and 155 °C, respectively. Interestingly, the temperature of desorption in subsequent cycles of the NaAlH4 doped with TiO2 reduced to 140 °C. On the contrary, in the case of NaAlH4 doped with HfCl4 or VCl3, the temperature of desorption increased to 150 °C and 175 °C, respectively. This may be because Ti can disperse in NaAlH4 better than Hf and V; therefore, this affected segregation of the sample after the desorption. The maximum hydrogen absorption capacity can be restored up to 3.5 wt% by doping with TiO2, while the amount of restored hydrogen was lower for HfCl4 and VCl3 doped samples. XRD analysis demonstrated that no Ti-compound was observed for the TiO2 doped samples. In contrast, there was evidence of Al–V alloy in the VCl3 doped sample and Al–Hf alloy in the HfCl4 doped sample after subsequent desorption/absorption. As a result, the V- or Hf-doped NaAlH4 showed the lower ability to reabsorb hydrogen and required higher temperature in the subsequent desorptions. 相似文献
The convergent validity of popularly used open-ended and closed-ended self-report measures of smoking was examined. Carbon monoxide (CO) samples were obtained from 11th-grade Canadian students as an independent method of assessing recent smoking. In addition to CO, 5 known psychosocial correlates of smoking (attitude, subjective norm, risk taking, best friend's smoking, and other friends' smoking) were used to estimate convergence with the self-report smoking indices. Results indicate that both simple closed-ended scales, with only a few response options, and more continuous, open-ended measures performed about equally as well as correlates of CO and the psychosocial measures, but only if the open-ended scales were subjected to a normalizing transformation to optimize their convergence. After this transformation was performed, convergence depended more on the time-span covered by the self-report indices than on the open-ended/closed-ended distinction. Implications of these results for different assessment goals were discussed. (PsycINFO Database Record (c) 2010 APA, all rights reserved) 相似文献
Palmar and axillary hyperhidrosis are best treated surgically by endoscopic transthoracic upper dorsal sympathectomy. At present, this methodology relies on (at least) double trocar insertion (per side), carbon dioxide insufflation, or both. We present a new minimally invasive endoscopic transthoracic technique, performed by a single-entry specifically modified thoracoscope and without the need for carbon dioxide insufflation, with the aim to reduce the drawbacks associated with the above-mentioned, currently adopted endoscopic technique. In our opinion, this "single-entry" technique, compared with the other reported approaches, should theoretically minimize any damage to the intercostal neurovascular bundle, while avoiding the complications related to carbon dioxide insufflation. 相似文献
A gene encoding a bifunctional homodimeric dihydrofolate reductase-
thymidylate synthase (DHFR-TS) was constructed by destroying the stop codon
of Escherichia coli dihydrofolate reductase (DHFR) and joining the coding
sequences of the monofunctional enzymes by a five amino acid linker. The
protein was designed to mimic features of active site proximity and
electrostatics in the protozoan DHFR-TSs which are believed to be important
in channeling of the DHFR substrate, H2folate, to TS. The genetically
engineered catalytically active homodimeric bifunctional DHFR-TS was
expressed, purified and characterized. The component activities of the
purified bifunctional enzyme had kinetic properties similar to those of the
monofunctional TS and DHFR, but unlike the authentic bifunctional enzymes
from protozoa this enzyme did not kinetically channel dihydrofolate from
DHFR to TS.
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A computer modeling procedure for assessing the stereochemicalsuitability of pairs of residues in proteins as potential sitesfor introduction of cystine disulfide crosslinks has been developed.Residue pairs with C – C distances of 6.5 Å andCbeta;–Cß distances of 4.5 Å are chosenfor geometrical fixation of S atoms using the program MODIP.The stereochemistry of the modeled disulfides is evaluated usinglimits for the structural parameters of the various torsionangles and S–S bond length in the disulfide bridge. Theability of the procedure to correctly model disulfides has beenchecked with examples of cystine peptides of known crystal structuresand 103 disulfide bridges from 25 available protein crystalstructures determined at 2 Å resolution. An analysis ofresults on three proteins with engineered disulfides, T4 lysozyme,dihydrofolate reductase and subtilisin, is presented. Two positionsfor the introduction of ‘stereochemically optimal’disulfides are identified in subtilisin. 相似文献
Ultra-fine fiber mats of cellulose acetate (CA; Mw ≈ 30?000 Da; degree of acetyl substitution ≈ 2.4) containing four different types of model drugs, i.e., naproxen (NAP), indomethacin (IND), ibuprofen (IBU), and sulindac (SUL), were successfully prepared by electrospinning from 16% w/v CA solutions in 2:1 v/v acetone/N,N-dimethylacetamide (DMAc). The amount of the drugs in the solutions was fixed at 20 wt.% based on the weight of CA powder. The morphology of the drug-loaded electrospun (e-spun) CA fiber mats was smooth, with the average diameters of these fibers ranging between 263 and 297 nm. No presence of the drug aggregates of any kind was observed on the surfaces of these fibers, suggesting that the drugs were encapsulated well within the fibers. After submersion in the acetate buffer solution at 37 °C for 24 h, the drug-loaded e-spun CA fiber mats swelled particularly well (i.e., 570-630%), while the corresponding solvent-cast film counterparts did not. The release characteristics of the model drugs from both the drug-loaded CA fiber mats and the drug-loaded as-cast CA films were carried out by the total immersion method in the acetate buffer solution at 37 °C. At any given immersion time point, the release of the drugs from the drug-loaded e-spun CA fiber mats was greater than that from the corresponding as-cast films. The maximum release of the drugs from both the drug-loaded fiber mats and films could be ranked as follows: NAP > IBU > IND > SUL. 相似文献
The complex pathway which links the agonist-cell membrane receptor binding to the response at the genome level involves, among other elements, protein kinase C (PKC). Agonists acting at the cell membrane can affect an autonomous nuclear polyphosphoinositide signaling system inducing an activation of nuclear phosphoinositidase activity and a subsequent translocation of PKC to the nuclear region. The fine localization of PKC has been investigated by means of electron microscopy quantitative immunogold labeling in 3T3 mouse fibroblasts, mitogenically stimulated by IGF-I. The enzyme, which in untreated cells is present in the cytoplasm, except for the organelles, and in the nucleoplasm, after IGF-I treatment is reduced in the cytoplasm and almost doubled in the nucleus. The PKC isoform translocated to the nucleus is the alpha isozyme, which is found not only associated with the nuclear envelope but mainly with the interchromatin domains. By using in situ matrix preparations, PKC appears to be retained at the nuclear matrix level, both at the nuclear lamina and at the inner nuclear matrix, suggesting a direct involvement in the phosphorylation of nuclear proteins which are responsible for the regulation of DNA replication. 相似文献
The ultrastructure of proteoglycans (PGs) in the tectorial membrane (TM) of the mature chinchilla cochlea was investigated using the cationic dye Cuprolinic blue. When used at a high critical electrolyte concentration, Cuprolinic blue has been shown specifically to bind to the glycosaminoglycan residues of sulfated PGs. After Cuprolinic blue treatment, PGs were observed in the TM which were represented as rod-shaped, electron-dense structures. A perifibrillar, primarily orthogonal, array of PGs was associated with the type A protofibrils. These PGs were distributed in 50 nm intervals along the length of the type A protofibrils. A less common orientation was parallel to the axis of the type A protofibrils. PGs did not appear to be associated with the type B protofibrils. Based upon previous results by other investigators, the TM contains types II and IX collagen, and it appears likely that the type A protofibrils are composed of collagen type II. PGs visualized in the TM in this study thus may represent the glycosaminoglycan residue of type IX collagen which is associated with the type II collagen fibrils. Alternatively, the TM PGs may be small dermatan or chondroitin sulfate PGs. 相似文献
