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51.
Nowadays, tandem structures have become a valuable competitor to conventional silicon solar cells, especially for perovskite over silicon, as metal halides surpassed Si with tunable bandgaps, high absorption coefficient, low deposition, and preparation costs. This led to a remarkable enhancement in the overall efficiency of the whole cell and its characteristics. Consequently, this expands the usage of photovoltaic technology in various fields of applications not only under conventional light source spectrum in outdoor areas, i.e., AM1.5G, but also under artificial light sources found indoors with broadband intensity values, such as Internet of things (IoTs) applications to name a few. We introduce a numerical model to analyze perovskite/Si tandem cells (PSSTCs) using both crystalline silicon (c-Si) and hydrogenated amorphous silicon (a-Si:H) experimentally validated as base cells. All proposed layers have been studied with J-V characteristics and energy band diagrams under AM1.5G by using SCAPS-1D software version 3.7.7. Thereupon, the proposed architectures were tested under various artificial lighting spectra. The proposed structures of Li4Ti5O12/CsPbCl3/MAPbBr3/CH3NH3PbI3/Si recorded a maximum power conversion efficiency (PCE) of 25.25% for c-Si and 17.02% for a-Si:H, with nearly 7% enhancement concerning the Si bare cell in both cases. 相似文献
52.
Acousto-optic (AO) devices are important spatial light modulators. They can be used as light-beam deflectors, rf true-time-delay lines, etc. To increase their spur-free dynamic range, we present what to our knowledge is a novel multichannel AO device structure, in which different channels have different carrier frequencies, so a wideband signal can automatically be decomposed into a set of narrow-band signals. Design, fabrication, and testing of this 24-channel, 10-mus AO spatial light modulator are addressed. 相似文献
53.
Sebastiani G Godtliebsen F Jones RA Haraldseth O Muller TB Rinck PA 《IEEE transactions on medical imaging》1996,15(3):268-277
Dynamic magnetic resonance (MR) imaging with contrast agents is a very promising technique for studying tissue perfusion in vivo. A temporal series of magnetic resonance images of the same slice are acquired following the injection of a contrast agent into the blood stream. The image intensity depends on the local concentration of the contrast agent, so that tissue perfusion can be studied by the image series. A new method of analyzing such series is described here. Nonparametric linear regression is used for modeling the image intensity along the series on a pixel by pixel basis. After modeling, some relevant quantities describing the time series are obtained and displayed as images. Due to its flexibility, this approach is preferred to parametric modeling when pathology is present since this can induce a wide spread of patterns for the pixel image intensity along time. Results of the application of the method to series of dynamic magnetic resonance images from ischaemic rat brains after the injection of the susceptibility agent Sprodiamide Inj. (Dy-DTPA-BMA) are shown and compared to results from a related known method. 相似文献
54.
Hagbi N Bergig O El-Sana J Billinghurst M 《IEEE transactions on visualization and computer graphics》2011,17(10):1369-1379
Nestor is a real-time recognition and camera pose estimation system for planar shapes. The system allows shapes that carry contextual meanings for humans to be used as Augmented Reality (AR) tracking targets. The user can teach the system new shapes in real time. New shapes can be shown to the system frontally, or they can be automatically rectified according to previously learned shapes. Shapes can be automatically assigned virtual content by classification according to a shape class library. Nestor performs shape recognition by analyzing contour structures and generating projective-invariant signatures from their concavities. The concavities are further used to extract features for pose estimation and tracking. Pose refinement is carried out by minimizing the reprojection error between sample points on each image contour and its library counterpart. Sample points are matched by evolving an active contour in real time. Our experiments show that the system provides stable and accurate registration, and runs at interactive frame rates on a Nokia N95 mobile phone. 相似文献
55.
(O)mür (O)cal 《国际自动化与计算杂志》2011,8(2):254-261
The coefficient diagram method (CDM) is one of the most effective control design methods. It creates control systems that
are very stable and robust with responses without the overshoot and small settling time. Furthermore, all control parameters
of the control systems are changed by varying some adjustment parameters in CDM depending on the demands. The model reference
adaptive systems (MRAS) are the systems that follow and change the control parameters according to a given model reference
system. There are several methods to combine the CDM with MRAS. One of these is to use the MRAS parameters as a gain of the
CDM parameters. Another is to directly use the CDM parameters as the MRAS parameters. In the industrial applications, the
system parameters can be changed frequently, but if the controller, by self-tuning, recalculates and develops its own parameters
continuously, the system becomes more robust. Also, if the poles of the controlled systems approach the jw axis, the response of the closed-loop MRAS becomes more and more insufficient. In order to obtain better results, CDM is
combined with a self-tuning model reference adaptive system. Systems controlled by a model reference adaptive controller give
responses with small or without overshoot, have small settling times, and are more robust. Thus, in this paper, a hybrid combination
of MRAS and CDM is developed and two different control structures of the control signal are investigated. The two methods
are compared with MRAS and applied to real-time process control systems. 相似文献
57.
In this letter, we propose a general framework for studying neural mass models defined by ordinary differential equations. By studying the bifurcations of the solutions to these equations and their sensitivity to noise, we establish an important relation, similar to a dictionary, between their behaviors and normal and pathological, especially epileptic, cortical patterns of activity. We then apply this framework to the analysis of two models that feature most phenomena of interest, the Jansen and Rit model, and the slightly more complex model recently proposed by Wendling and Chauvel. This model-based approach allows us to test various neurophysiological hypotheses on the origin of pathological cortical behaviors and investigate the effect of medication. We also study the effects of the stochastic nature of the inputs, which gives us clues about the origins of such important phenomena as interictal spikes, interictal bursts, and fast onset activity that are of particular relevance in epilepsy. 相似文献
58.
Intharathep P Laohpongspaisan C Rungrotmongkol T Loisruangsin A Malaisree M Decha P Aruksakunwong O Chuenpennit K Kaiyawet N Sompornpisut P Pianwanit S Hannongbua S 《Journal of molecular graphics & modelling》2008,27(3):342-348
To understand how antiviral drugs inhibit the replication of influenza A virus via the M2 ion channel, molecular dynamics simulations have been applied to the six possible protonation states of the M2 ion channel in free form and its complexes with two commercial drugs in a fully hydrated lipid bilayer. Among the six different states of free M2 tetramer, water density was present in the pore of the systems with mono-protonated, di-protonated at adjacent position, tri-protonated and tetra-protonated systems. In the presence of inhibitor, water density in the channel was considerably better reduced by rimantadine than amantadine, agreed well with the experimental IC(50) values. With the preferential position and orientation of the two drugs in all states, two mechanisms of action, where the drug binds to the opening pore and the histidine gate, were clearly explained, i.e., (i) inhibitor was detected to localize slightly closer to the histidine gate and can facilitate the orientation of His37 imidazole rings to lie in the close conformation and (ii) inhibitor acts as a blocker, binding at almost above the opening pore and interacts slightly with the three pore-lining residues, Leu26, Ala30 and Ser31. Here, the inhibitors were found to bind very weakly to the channel due to their allosteric hindrance while theirs side chains were strongly solvated. 相似文献
59.
The aim of this review is to provide an overview of proteomic studies in animal models of diabetes and to give some insight into the different methods available today in the rapidly developing field of proteomics. A summary of 31 papers published between 1997 and 2007 is presented. For instance, proteomics has been used to study the development of both type 1 and type 2 diabetes, diabetic complications in tissues like heart, kidney and retina and changes after treatment with anti-diabetic drugs like peroxisome proliferator-activated receptors agonists. Together, these studies give a good overview of a number of experimental approaches. Proteomics holds the promise of providing major contributions to the field of diabetes research. However, to achieve this, a number of issues need to be resolved. Appropriate data representation to facilitate data comparison, exchange, and verification is required, as well as improved statistical assessment of proteomic experiments. In addition, it is important to follow up the results with functional studies to be able to make biologically relevant conclusions. The potential of proteomics to dissect complex human disorders is now beginning to be realized. In the future, this will result in new important information concerning diabetes. 相似文献
60.
Gene expression changes in a transgenic mouse model overexpressing human wildtype and mutant torsinA
Grundmann K Hübener J Häbig K Reischmann B Poths S Hauser TK Magg J Riess O Bonin M Nguyen HP 《Proteomics. Clinical applications》2008,2(5):720-736
Primary torsion dystonia is an autosomal-dominantly inherited, neurodevelopmental movement disorder caused by a GAG deletion (ΔGAG) in the DYT1 gene, encoding torsinA. This mutation is responsible for approximately 70% of cases of early-onset primary torsion dystonia. The function of wildtype torsinA is still unknown, and it is unsolved how the deletion in the DYT1 gene contributes to the development of the disease. To better understand the molecular processes involved in torsinA pathology, we used genome-wide oligonucleotide microarrays to characterize gene expression patterns in the striatum of mouse models overexpressing the human wildtype and mutant torsinA. By this approach we were able to detect gene expression changes that seem to be specific for torsinA pathology. We found an impact of torsinA, independent from genotype, on vesicle trafficking, exocytosis, and neurotransmitter release in our mouse model. In addition, we were able to identify several new pathways and processes involved in the development of the nervous system that are affected by wildtype and mutant torsinA. Furthermore, we have striking evidence from our gene expression data that glutamate receptor mediated synaptic plasticity in the striatum is the affected underlying cellular process for impaired motor learning in human ΔGAG torsinA transgenic mice. 相似文献