排序方式: 共有46条查询结果,搜索用时 46 毫秒
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McIntosh R Ellis D Gil-Lostes J Dalby KJ Rosair GM Welch AJ 《Dalton transactions (Cambridge, England : 2003)》2005,(10):1842-1846
Reduction of the tethered carborane 1,2-(CH2)3-1,2-closo-C2B10H10 followed by treatment with CoCl2/NaCp, [(p-cymene)RuCl2]2(p-cymene=C6H4MeiPr-1,4), (PMe2Ph)2PtCl2 or (dppe)NiCl2(dppe=Ph2PCH2CH2PPh2) affords reasonable yields of the new 13-vertex metallacarboranes 1,2-(CH2)3-4-Cp-4,1,2-closo-CoC2B10H10 (1), 1,2-(CH2)3-4-(p-cymene)-4,1,2-closo-RuC2B10H10 (2), 1,2-(CH2)3-4,4-(PMe2Ph)2-4,1,2-closo-PtC2B10H10 (3) and 1,2-(CH2)3-4,4-(dppe)-4,1,2-closo-NiC2B10H10 (4), respectively. All compounds were characterised spectroscopically and crystallographically. The cobalt and ruthenium species 1 and 2 have Cs symmetry in both solution and the solid state, having henicosahedral cage structures featuring a trapezoidal C1C2B9B5 face. The platinum and nickel compounds 3 and 4 have asymmetric docosahedral cage structures in the crystal (the more so for 4 than for 3) although both appear, by 11B and 31P NMR spectroscopy, to have Cs symmetry in solution. Low-temperature experiments on the more soluble platinacarborane could not freeze out the diamond-trapezium-diamond fluctional process that we assume is operating in solution, and we therefore conclude that this process has a relatively low activation barrier, probably <35 kJ mol-1. 相似文献
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N. Andersen T. Andersen P. Dalby T. Royer 《Zeitschrift für Physik D Atoms, Molecules and Clusters》1988,9(4):315-318
The orientation of Na(3p) states created in 3–13 keV Na(3s)-He collisions has been studied by the polarised photon-scattered particle coincidence technique at scattering angles corresponding to the impact-parameter range 1–2 a.u. In the standard geometry, at large impact parameters the excitation process exhibits a very high degree of orientation with about 90% of the Na(3p) states havingm 1=?1. Strong reduction in this propensity is observed at impact parameters smaller than about 1.3 a.u., where a molecular curve crossing causes simultaneous He(n=2) excitation. In this region, also ionisation becomes important. 相似文献
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Prof. Dr. Ian Paterson Mengyang Xuan Dr. Stephen M. Dalby 《Angewandte Chemie (International ed. in English)》2014,53(28):7286-7289
As a potent neurotrophic agent, the sesquiterpenoid jiadifenolide represents a valuable small‐molecule lead for the potential therapeutic treatment of neurodegenerative diseases. A stereocontrolled total synthesis of this densely functionalized natural product is reported, central to which is an adventurous samarium‐mediated cyclization reaction to establish the tricyclic core and the adjacent C5 and C6 quaternary stereocenters. 相似文献
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[reaction: see text] A stereo-controlled synthesis of the fully elaborated C26-C40 tricyclic [5,6,6]-bis-spiroacetal of spirastrellolide A containing the C28 chlorine substituent is reported, exploiting asymmetric Sharpless dihydroxylation and boron-mediated allylation methodology. 相似文献
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Bing-Xin Yang Yi-Han Kao Janos Kirz Chang-Xin Gu R.N. Bhargava D.A. Cammack R.J. Dalby 《Physics letters. A》1985,113(5):283-288
Transmission measurements of the extended X-ray absorption fine structure above the oxygen K-edge have been made by using a new scintillation detection technique. The absorption spectrum is in close resemblance with the total electron yield spectrum recorded at the same time. This new technique is of interest for studies of soft X-ray absorption spectroscopy for thin films of solid materials. 相似文献
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Accurately predicting phosphorylation sites in proteins is an important issue in postgenomics, for which how to efficiently extract the most predictive features from amino acid sequences for modeling is still challenging. Although both the distributed encoding method and the bio-basis function method work well, they still have some limits in use. The distributed encoding method is unable to code the biological content in sequences efficiently, whereas the bio-basis function method is a nonparametric method, which is often computationally expensive. As hidden Markov models (HMMs) can be used to generate one model for one cluster of aligned protein sequences, the aim in this study is to use HMMs to extract features from amino acid sequences, where sequence clusters are determined using available biological knowledge. In this novel method, HMMs are first constructed using functional sequences only. Both functional and nonfunctional training sequences are then inputted into the trained HMMs to generate functional and nonfunctional feature vectors. From this, a machine learning algorithm is used to construct a classifier based on these feature vectors. It is found in this work that (1) this method provides much better prediction accuracy than the use of HMMs only for prediction, and (2) the support vector machines (SVMs) algorithm outperforms decision trees and neural network algorithms when they are constructed on the features extracted using the trained HMMs. 相似文献
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Rainey MA Callaway K Barnes R Wilson B Dalby KN 《Journal of the American Chemical Society》2005,127(30):10494-10495
Five hundred protein kinases phosphorylate 10 000 proteins in human cells. Frequently, more than one site in a protein is phosphorylated, and often by more than one protein kinase. The mechanistic basis underlying the overlapping specificity of the phospho-proteome is not well understood. We are interested in understanding why ERK2, a proline-directed protein kinase, phosphorylates only a fraction of the (S/T-P) sites found in the surface loops of proteins, at an appreciable rate. To address this fundamental question, we utilized a well-established protein substrate EtsDelta138, which comprises a globular ERK2-recognition domain (pnt domain) and an unstructured peptide-like N-terminal tail. This tail contains T38, the sole ERK2 phosphorylation site. We mutated the TP motif, which is recognized by the active site and found that mutagenesis of the T-38/P-39 motif to TD, TR, TA, TG, and TV has no effect on the stability of the ternary complex but does decrease kcat. We also investigated the effect of perturbing the binding between ERK2 and the pnt domain, which occurs outside the active site, to find that mutation of the pnt domain (F120A) leads to a 10-fold decrease in binding but the kcat remains the same. The data support a mechanism of proximity-mediated catalysis, where the docking of the pnt domain, outside the active site, increases the effective concentration of the TP motif near the active site. The data are consistent with the notion that the interaction between ERK2 and the pnt domain provides uniform binding energy and stabilizes each enzyme intermediate and transition state to an equal extent. While other steps on the reaction pathway contribute towards the specificity of the ERK2 reaction, a docking interaction provides the initial basis for substrate recognition. Those residues within the docked complex, which have the ability to access the active site with an appropriate geometry, can be phosphorylated at an efficient rate if followed by a proline or small hydrophobic amino acid. 相似文献
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