简法合成甲地孕酮

本文报道了合成甲地孕酮的简便方法,即以17α-乙酰氧基-黄体酮(3)为原料,将其烯醇醚(4)经Mannich反应,或将△~(3,5)-3,17α-二乙酰氧基-黄体酮(2)与二乙氧基甲烷反应,生成6-次甲基-17α-乙酰氧基-黄体酮(5),然后将5用钯/碳酸钙作催化剂转位得目的物甲地孕酮(6b),总收率分别为56%和50%(均以17α-羟基-黄体酮(1)为起始物)。     

On the Integration by Parts and Characterization of a Fractional Diffusion Process北大核心CSCD

本文研究分数扩散过程和其分部积分公式的关系.首先利用Bismut方法给出拉回公式,进而得到分数扩散过程的分部积分公式。反过来,证明了分数扩散过程可由其分部积分公式唯一刻画.     

A Multi-Scale Method for Distributed Convex Optimization with Constraints

Journal of Optimization Theory and Applications - This paper proposes a multi-scale method to design a continuous-time distributed algorithm for constrained convex optimization problems by using...     

Multiple attribute decision-making method based on projection model for dual hesitant fuzzy set

Fuzzy Optimization and Decision Making - In the decision-making process, retaining the original data information has become a most crucial step. Dual hesitant fuzzy sets (DHFS), which can reflect...     

Symmetries and generalizedW∞ algebra of the modified KP equation

The infinitely many symmetries with arbitrary functions of timet for the potential modified Kadomtsev-Petviashvilli equation are obtained by using a simple direct method. These symmetries constitute a generalization of the well-knownW algebra.     

Probing the kinetic landscape of transient peptide-protein interactions by use of peptide (15)n NMR relaxation dispersion spectroscopy: binding of an antithrombin peptide to human prothrombin

Protein-ligand interactions may lead to the formation of multiple molecular complexes in dynamic exchange, affecting the kinetic and thermodynamic characteristics of the binding equilibrium. We followed the dissociation kinetics of the transient and specific complex of an antithrombotic peptide N-acetyl-Asp(55)-Phe-Glu-Glu-Ile-Pro(60)-Glu-Glu-Tyr-Leu-Gln(65) with human prothrombin by use of (15)N NMR relaxation dispersion spectroscopy of the peptide. Every one of the five (15)N-labeled adjacent residues of the peptide exhibited apparently different kinetic exchange and relaxation behaviors, which were especially evident at different concentrations of prothrombin. Binding-induced (15)N relaxation dispersion of residues Phe(56), Glu(57), Glu(58), and Ile(59) can be fitted phenomenologically to a two-site on-and-off exchange mechanism with physically feasible relaxation and kinetic parameters obtained for residues Phe(56), Glu(58), and Ile(59), independent of the prothrombin concentration. The apparent kinetic parameters of Glu(57) show some dependence on the concentration of prothrombin and the extracted transverse relaxation rate for Glu(57) in the bound state was severalfold higher than that expected for a protein-peptide complex with a size of approximately 72 kDa. In addition, the equilibrium population of the bound peptide obtained for Glu(57) was inconsistent with those for Phe(56), Glu(58), and Ile(59) and with the prothrombin/peptide ratios used in the experiments. These discrepancies can be explained by the presence of two conformations for the peptide-protein complex exchanging at a rate of approximately 100 s(-)(1). In all, our study shows that fast dissociation of protein-peptide complexes can be studied quantitatively using peptide (15)N NMR relaxation dispersion measurements without a precise knowledge of the peptide and protein concentrations. In addition, protein titration was found to improve the accuracy of quantitative analysis and may make it possible to determine the rate of conformational changes within the protein-peptide complex.