Enhanced metabolism of fucose through fucosidase overexpression is a signature of some cancer types, thus suggesting that fucosidase‐targetted ligands could play the role of drug‐delivery vectors. Herein, we describe the synthesis of a new series of pyrrolidine–ferrocene conjugates, consisting of a L ‐fuco‐configured dihydroxypyrrolidine as the fucosidase ligand armed with a cytotoxic ferrocenylamine moeity. Three‐dimensional structures of several of these fucosidase inhibitors reveal transition‐state‐mimicking 3E conformations. Elaboration with the ferrocenyl moiety results in sub‐micromolar inhibitors of both bovine and bacterial fucosidases, with the 3D structure of the latter revealing electron density indicative of highly mobile alkylferrocene compounds. The best compounds show a strong antiproliferative effect, with up to 100 % inhibition of the proliferation of MDA‐MB‐231 cancer cells at 50 μM . 相似文献
Reactions of the formamidinate ligand, RN(H)C(H)NR, LH, (R = 2,6-diisopropylphenyl), with AlMe3, AlMe2Cl, GaMe3 and ZnEt2 were investigated to examine potential coordination modes of the ligand and the effect of hydrolysis on the products. Nine new complexes have been fully characterized by X-ray crystallography and other spectroscopic techniques and highlight the diverse coordination modes of the formamidinate ligand. 相似文献
Lasso peptides are natural products that assume a unique lariat knot topology. Lasso peptide isopeptidases (IsoPs) eliminate this topology through isopeptide bond cleavage. To probe how these enzymes distinguish between substrates and hydrolyze only isopeptide bonds, we examined the structure and mechanism of a previously uncharacterized IsoP from the proteobacterium Sphingopyxis alaskensis RB2256 (SpI‐IsoP). We demonstrate that SpI‐IsoP efficiently and specifically linearizes the lasso peptide sphingopyxin I (SpI) and variants thereof. We also present crystal structures of SpI and SpI‐IsoP, revealing a threaded topology for the former and a prolyl oligopeptidase (POP)‐like fold for the latter. Subsequent structure‐guided mutational analysis allowed us to propose roles for active‐site residues. Our study sheds light on lasso peptide catabolism and expands the engineering potential of these fascinating molecules. 相似文献
The enoyl-acyl carrier protein reductase enzyme FabI is essential for fatty acid biosynthesis in Staphylococcus aureus and represents a promising target for the development of novel, urgently needed anti-staphylococcal agents. Here, we elucidate the mode of action of the kalimantacin antibiotics, a novel class of FabI inhibitors with clinically-relevant activity against multidrug-resistant S. aureus. By combining X-ray crystallography with molecular dynamics simulations, in vitro kinetic studies and chemical derivatization experiments, we characterize the interaction between the antibiotics and their target, and we demonstrate that the kalimantacins bind in a unique conformation that differs significantly from the binding mode of other known FabI inhibitors. We also investigate mechanisms of acquired resistance in S. aureus and identify key residues in FabI that stabilize the binding of the antibiotics. Our findings provide intriguing insights into the mode of action of a novel class of FabI inhibitors that will inspire future anti-staphylococcal drug development. 相似文献
The enoyl‐acyl carrier protein reductase enzyme FabI is essential for fatty acid biosynthesis in Staphylococcus aureus and represents a promising target for the development of novel, urgently needed anti‐staphylococcal agents. Here, we elucidate the mode of action of the kalimantacin antibiotics, a novel class of FabI inhibitors with clinically‐relevant activity against multidrug‐resistant S. aureus. By combining X‐ray crystallography with molecular dynamics simulations, in vitro kinetic studies and chemical derivatization experiments, we characterize the interaction between the antibiotics and their target, and we demonstrate that the kalimantacins bind in a unique conformation that differs significantly from the binding mode of other known FabI inhibitors. We also investigate mechanisms of acquired resistance in S. aureus and identify key residues in FabI that stabilize the binding of the antibiotics. Our findings provide intriguing insights into the mode of action of a novel class of FabI inhibitors that will inspire future anti‐staphylococcal drug development. 相似文献
Intradiffusion coefficients for36ClO
4–
have been measured in solutions of zinc perchlorate of concentration 0.1 to 3 mol dm–3 at 25°C by the diaphragm cell technique. In addition, intradiffusion coefficients for perchlorate ions in zinc chloride solutions have been measured over a concentration range at 25°C. The results confirm previous work on the effect of complexation on diffusion in zinc chloride solutions above a salt concentration of 0.1M. The present data, together with literature data for diffusion coefficients of the other species present in the zinc perchlorate electrolyte system, have enabled a simple analysis of the hydration around the zinc ions to be carried out. This indicates that the water diffusion data are consistent with the zinc ions having an effective hydration sphere of 11 (±2) water molecules. This is in keeping with values obtained for other simple divalent electrolytes using the same model. The model is extended here to allow analysis of water diffusion in zinc chloride solutions taking into account the presence of complexed chloro-zinc species. The experimental data are consistent with the effective hydration of the chloro-zinc complexes being independent of the number of chloride ligands and equal to 18±3 over a concentration range of 0 tol mol-dm–3. This postulate is discussed in terms of its consequences on the water ligand dynamics for the complex equilibria. 相似文献
Summary The resolution of the enantiomers of new acetylcholinesterase inhibitors by high-performance liquid chromatography (HPLC)
was investigated on stationary phases containing cellulose tris-(3,5 methylphenylcarbamide) (Chiralcel OD). The effects of
the mobile phase on retention, enantioselectivity and resolution were also studied. Ethanol and isopropanol were tested as
organic modifiers and the influence of diethylamine was investigated. The effect of temperature on chiral separations was
also studieded. 相似文献
Analytical HPLC methods using derivatized cellulose chiral stationary phases were developed for the direct enantioseparation of substituted [1-(imidazo-1-yl)-1-phenylmethyl)]-benzothiazolinone and benzoxazolinone derivatives with one chiral center. Those analogues of fadrozole constitute new potent nonsteroidal inhibitors of aromatase (P450 arom). The separations were made using normal phase methodology with a mobile phase consisting of n-hexane-alcohol (ethanol, 1-propanol, or 2-propanol) in various proportions, and a silica-based cellulose tris-3,5-dimethylphenylcarbamate (Chiralcel OD-H), or tris-methylbenzoate (Chiralcel OJ). The effects of concentration of various aliphatic alcohols in the mobile phase were studied. A better separation was achieved on cellulose carbamate phase compared with the cellulose ester phase. The effects of structural features of the solutes along with the temperature of the column on the discrimination between the enantiomers were examined. Baseline separation (Rs > 1.5) was easily obtained in many cases. 相似文献
Paddle wheels and pillars : Layered 3D metal–organic frameworks comprised of paddle‐wheel coordination units are constructed under a variety of conditions to incorporate bridging ligands (as illustrated) that impart desired properties, such as guest‐exchange behavior, luminescence, microporosity, and stability, to the material.
Whereas zinc dodecanoate in xylene exhibits a critical solution temperature, it does not do so in tetrachloromethane.Evidence is presented which suggests that the abrupt increase in solubility in xylene is not due to a phase change of the solid zinc dodecanoate. 相似文献
