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141.
利用统一建模语言,并结合当前较为成熟的三层架构,设计并实现了远程教育系统。说明了如何利用UML来完成系统的分析与设计,并以此为指导,在三层架构的基础上完成系统各功能模块的代码实现。本系统三层架构的搭建是通过freemarker标签来构建视图层,采用Hibernate完成数据库的访问操作,使用SpringMVC来完成架构的整合。这种UML建模与架构结合的开发方式在Web系统开发中有较强的通用性。  相似文献   
142.
针对钢铁企业的轨梁万能生产线在生产中存在的新产品调试生产周期过长、生产瓶颈不易诊断、设备利用率低等问题,分析了钢铁企业轨梁万能生产线不同于传统离散制造以及流程制造过程的特点,在此基础上建立了半连续半离散的轨梁万能生产线的Petri网模型和各设备的仿真组件模型,开发了轨梁万能生产线的仿真系统,并用一个实际的工程应用案例,验证了该仿真模型及其系统的可操作性以及有效性,达到了提高生产现场轨梁万能生产线的生产效率和产能的目的.  相似文献   
143.
A model of a gamma sterilizer was built using the ITS/ACCEPT Monte Carlo code and verified through dosimetry. Individual dosimetry measurements in homogeneous material were pooled to represent larger bodies that could be simulated in a reasonable time. With the assumptions and simplifications described, dose predictions were within 2–5% of dosimetry. The model was used to simulate product movement through the sterilizer and to predict information useful for process optimization and facility design.  相似文献   
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Mitochondrial Outer Membrane (MOM) Permeabilization (MOMP) is a critical event in the mitochondrial types of apoptosis. MOMP is controled by the proteins of the Bcl-2 family and its two proapoptotic members Bak and Bax are the key effectors of MOMP. Voltage-dependent anion channel 2 (VDAC2) is an integral membrane protein that plays an important role in the regulation of Bak and Bax apoptotic function, but underlying mechanisms are not fully understood. In the present article, the mechanisms of MOMP regulation mediated by VDAC2 were explored using structure-based modeling. We show that Bak, prior to an apoptotic stimulus, possesses two low-energy conformations of high shape – and polar complementarity in respect to VDAC2, resulting in two high-affinity modes of Bak binding to VDAC2, one with Bak fully residing in the cytosol and the other with Bak α9 helix inserted into the membrane. Even higher binding affinity of VDAC2 for tBid (truncated Bid/p15) was established, suggesting the tBid-mediated displacement of Bak from the VDAC2/Bak complex resulting in the formation of the VDAC2/tBid complex. The structural analysis of the interaction of this complex with Bax revealed a very high binding affinity of this complex for Bax, suggesting the recruitment of Bax to the MOM by this complex under apoptotic conditions. Besides, we revealed one more low-energy structure of Bax of high binding affinity towards the VDAC2/tBid complex and with helix α9 inserted into the membrane.  相似文献   
147.
Modeling of catalytic coke formation in thermal cracking reactors   总被引:1,自引:0,他引:1  
At the start-up period, the most important mechanism in the coke production with a clean reactor surface is the catalytic mechanism. The study of this mechanism can be very useful for the better comprehension of the coke production process. In this paper, a model was designed for such a production through the utilization of a catalytic mechanism and a kinetic model, capable of interpreting the catalytic coke production on the reactor surface. For the determination of the model reliability, the experimental data related to the naphtha feed, existing in literature, were used. In addition, the constant parameters of the model, the velocity and the activation energy constants, associated to the kinetic model, were calculated. The results of the developed model were in satisfactory agreement with the experimental data. Eventually, the catalytic coke amount in comparison with the total coke production on the reactor surface and its significance were under investigation.  相似文献   
148.
Both in electrodialysis and in reverse electrodialysis ionic shortcut currents through feed and drain channels cause a considerable loss in efficiency. Model calculations based on an equivalent electric system of a reverse electrodialysis stack reveal that the effect of these salt bridges could be reduced via a proper stack design. The critical parameters which are to be optimized are ρ/r and R/r, where ρ is the lateral resistance along the spacers, R is the resistance of the feed and drain channels between two adjacent cells, and r is the internal resistance of a cell. Because these two parameters are dimensionless, different stacks can be easily compared. The model is validated with two experimental stacks differing in membrane type and spacer thickness, one with large ionic shortcut currents and one where this effect is less. The loss in efficiency decreased from 25 to 5% for a well-designed stack. The loss of efficiency in reverse electrodialysis and in electrodialysis can be reduced with the aid of the design parameters presented in this paper.  相似文献   
149.
In recent decades, high-temperature oxygen reduction reaction on mixed conducting cathodes were investigated intensively by many researchers. Computational approaches as well as electrochemical and spectroscopic studies have been made to elucidate the kinetics. Contribution of oxygen vacancy to the reaction rate was suggested in multiple reports, and plausible reaction pathways were proposed based on density functional theory (DFT) calculations. The picture of oxygen reduction reaction has become clearer in these years. However, there still is a discussion about a credible formula that represents the current–voltage relationships. Discrepancies are found among the reported data on the magnitude of the rate constant and on its dependencies on partial pressure and temperature. The difference is significant between a model electrode and a practical porous electrode. Comparison of the results suggests the existence of series reaction barriers, that is, the surface reaction and subsurface transport, which should be considered for consistent representation of the total electrode process.  相似文献   
150.
Summary G-protein-coupled receptors all share the seven transmembrane helix motif similar to bacteriorhodopsin. This similarity was exploited to build models for these receptors. From an analysis of a multi-sequence alignment of 225 G-protein-coupled receptors belonging to the rhodopsin-like superfamily, conclusions could be drawn about functional residues. Seven residues in the transmembrane regions are conserved throughout all aligned receptors. These residues cluster at the cytosolic side of the transmembrane helices and are for all rhodopsin-like G-protein-coupled receptors implied in signal transduction. An analysis of correlated mutations reveals a number of residues, both in the helices and in the cytosolic loops, that might be important in the signal transduction pathway in subfamilies of this receptor family.  相似文献   
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