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101.
102.

Representational analysis is used to examine the interplay between Fermi surface nesting and local moment effects in the formation of the magnetically ordered states of the rare-earth nickel borocarbides, RNi2B2C. We derive compatibility tables for the propagation wavevector k, the local moment anisotropy and the ordered moment direction μ k for materials with this tetragonal crystal structure. The magnetic structures observed in the rare-earth nickel borocarbides are discussed in this context.  相似文献   
103.
Here, we report a novel “CyClick” strategy for the macrocyclization of peptides that works in an exclusively intramolecular fashion thereby precluding the formation of dimers and oligomers via intermolecular reactions. The CyClick chemistry is highly chemoselective for the N‐terminus of the peptide with a C‐terminal aldehyde. In this protocol, the peptide conformation internally directs activation of the backbone amide bond and thereby facilitates formation of a stable 4‐imidazolidinone‐fused cyclic peptide with high diastereoselectivity (>99 %). This method is tolerant to a variety of peptide aldehydes and has been applied for the synthesis of 12‐ to 23‐membered rings with varying amino acid compositions in one pot under mild reaction conditions. The reaction generated peptide macrocycles featuring a 4‐imidazolidinone in their scaffolds, which acts as an endocyclic control element that promotes intramolecular hydrogen bonding and leads to macrocycles with conformationally rigid turn structures.  相似文献   
104.
Matrix‐assisted laser desorption/ionization imaging mass spectrometry (MALDI IMS) is a molecular imaging technology uniquely capable of untargeted measurement of proteins, lipids, and metabolites while retaining spatial information about their location in situ. This powerful combination of capabilities has the potential to bring a wealth of knowledge to the field of molecular histology. Translation of this innovative research tool into clinical laboratories requires the development of reliable sample preparation protocols for the analysis of proteins from formalin‐fixed paraffin‐embedded (FFPE) tissues, the standard preservation process in clinical pathology. Although ideal for stained tissue analysis by microscopy, the FFPE process cross‐links, disrupts, or can remove proteins from the tissue, making analysis of the protein content challenging. To date, reported approaches differ widely in process and efficacy. This tutorial presents a strategy derived from systematic testing and optimization of key parameters, for reproducible in situ tryptic digestion of proteins in FFPE tissue and subsequent MALDI IMS analysis. The approach describes a generalized method for FFPE tissues originating from virtually any source.  相似文献   
105.
Real-time imaging in the terahertz (THz) spectral range was achieved using a milliwatt-scale, 2.8 THz quantum cascade laser and an uncooled, 160 x 120 pixel microbolometer camera modified with Picarin optics. Noise equivalent temperature difference of the camera in the 1-5 THz frequency range was estimated to be at least 3 K, confirming the need for external THz illumination when imaging in this frequency regime. Despite the appearance of fringe patterns produced by multiple diffraction effects, single-frame and extended video imaging of obscured objects show high-contrast differentiation between metallic and plastic materials, supporting the viability of this imaging approach for use in future security screening applications.  相似文献   
106.
In this paper, we prove the existence and uniqueness of the entropy solution for a first-order stochastic conservation law with a multiplicative source term involving a Q-Brownian motion. After having defined a measure-valued weak entropy solution of the stochastic conservation law, we present the Kato inequality, and as a corollary, we deduce the uniqueness of the measure-valued weak entropy solution, which coincides with the unique weak entropy solution of the problem. The Kato inequality is proved by a doubling of variables method; to that purpose, we prove the existence and the uniqueness of the strong solution of an associated stochastic nonlinear parabolic problem by means of an implicit time discretization scheme; we also prove its convergence to a measure-valued entropy solution of the stochastic conservation law, which proves the existence of the measure-valued entropy solution.  相似文献   
107.
Current biomimetics for medical applications use a single biomimetic approach to imitate natural structures, which can be insufficient for reconstructing structurally complex natural systems. Multipronged efforts may resolve these complexities. To achieve interesting nanostructure‐driven optical properties, a dual‐biomimetic system contained within a single nanoagent was engineered to recapitulate chlorosomes, efficient light‐harvesting organelles that have unique dye assemblies and tunable photonic properties. A series of chlorin dyes was synthesized, and these hydrophobic assemblies were stabilized inside a high‐density lipoprotein, a second biomimetic that enabled in vivo utility. This system resulted in tunable tumor imaging of intact (photoacoustic) and disrupted (activatable fluorescence) nanostructures. The successful demonstration of this multipronged biomimetic approach opens the door for reconstruction of complex natural systems for biomedical applications.  相似文献   
108.
A new heterogeneous catalyst composed of copper and nickel oxide particles supported within charcoal has been developed. It catalyzes cross-couplings that traditionally use palladium, nickel, or copper, including Suzuki-Miyaura reactions, Buchwald-Hartwig aminations, vinylalane alkylations, etherifications of aryl halides, aryl halide reductions, asymmetric conjugate reductions of activated olefins, and azide-alkyne "click" reactions.  相似文献   
109.
Cell-based screening using phenotypic assays is a useful means of identifying bioactive chemicals for use as tools to elucidate complex cellular processes. However, the chemicals must display sufficient selectivity and their targets have to be identified. We describe how cell-based screening assays can be designed to maximize the likelihood of discovering selective compounds through the choice of positive readouts, low chemical concentrations and long incubation periods. Examining the potency, efficacy and activity range of chemicals can further help set apart those likely to act more specifically. Identifying the cellular targets of active chemicals can be especially demanding. Secondary screens and the cautious use of the candidate approach can help narrow down their mechanisms of action, but biased approaches may lead to the identification of secondary or even irrelevant targets. We discuss strategies for unbiased target identification by sampling potential targets at the genome-wide and proteome-wide levels.  相似文献   
110.
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