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921.
Céline E. Géneau Felix L. Wäckers Henryk Luka Claudia Daniel Oliver Balmer 《Basic and Applied Ecology》2012,13(1):85-93
Habitat management is an important element in sustainable agriculture and can be used to maximize a range of ecosystem services that support crop production. An important example of such ecosystem services is biological control of pests which can be enhanced by providing arthropod natural enemies with suitable floral resources. The potential risk of this approach, however, is that flowering plants may enhance the fitness of the targeted pests as well. We conducted experiments to identify selective plant species that would improve the longevity and parasitization rate of the parasitoid wasp Microplitis mediator without benefiting its host pest, the cabbage moth Mamestra brassicae. Effects on longevity were also assessed for Diadegma fenestrale, a generalist parasitoid wasp attacking lepidopteran pests. Additionally, we compared the effects of floral and extrafloral nectar, the latter being formed in some plant species and can significantly prolong the duration of nectar availability for natural enemies. Longevity of M. mediator and D. fenestrale as well as parasitization rates of M. mediator were significantly increased by the presence of Fagopyrum esculentum (floral nectar), Centaurea cyanus (floral and extrafloral nectar) and non-flowering Vicia sativa (extrafloral nectar). M. mediator parasitized 202.3 ± 29.7 M. brassicae larvae during its lifetime when presented F. esculentum, compared to 14.4 ± 3.4 larvae in the absence of floral resources. Extrafloral nectar of C. cyanus and V. sativa was as suitable for M. mediator as floral nectar and significantly increased longevity and parasitization rates. Longevity and fecundity of M. brassicae were not supported by the plant species tested. These results stress the importance of plant screening to achieve plant selectivity and to maximize biological control. F. esculentum, C. cyanus and V. sativa are recommended as selective plant species to enhance parasitoids of M. brassicae. 相似文献
922.
923.
Marxen Julia C.; Prymak Oleg; Beckmann Felix; Neues Frank; Epple Matthias 《Journal of Molluscan Studies》2008,74(1):19-26
Embryos of different developmental stages and newly hatchedjuveniles of the freshwater snail Biomphalaria glabrata wereinvestigated by synchrotron radiation micro computer tomography(SRµCT). Because this method is sensitive for objectswith a high X-ray density, it is ideally suited to study mineralizedtissues without the need for dissection of the sample, i.e.removal of the soft tissue. This is a clear advantage over scanningelectron microscopy (SEM). However, the resolution is inferiorto SEM (about 1–2 µm compared to a few nm).After the measurement, computer-processed handling (virtualturning, cutting and measuring) of the object is possible. Thedevelopment of the calcified shell in embryos before hatching(age 60, 72, 96 and 120 h after oviposition) was investigatedand both methods were compared. While it was not possible tofind a calcified shell in 60 h old embryos, the shell in72 h old embryos was almost fully mineralized. By SRµCT,the weight of the calcified shell was estimated to 0.64, 9.59and 30.3 µg for embryos of 72, 96 and 120 h.All juvenile snails, of 5 days and 4 weeks after hatching, containedconcretions in the stomach, mostly consisting of calcium phosphate. (Received 10 May 2007; accepted 20 September 2007) 相似文献
924.
Structural determinants of the anti-HIV activity of a CCR5 antagonist derived from Toxoplasma gondii
Yarovinsky F Andersen JF King LR Caspar P Aliberti J Golding H Sher A 《The Journal of biological chemistry》2004,279(51):53635-53642
The protozoan parasite Toxoplasma gondii possesses a protein, cyclophilin-18 (C-18), which binds to the chemokine receptor CCR5, induces interleukin-12 production from murine dendritic cells, and inhibits fusion and infectivity of human immunodeficiency virus 1 (HIV-1) R5 viruses by co-receptor antagonism. Site-directed mutagenesis was employed to identify the domains in C-18 responsible for its CCR5 binding and antiviral functions. To do so we focused on amino acid differences with Plasmodium falciparum cyclophilin, which, although 53% identical with C-18, has minimal binding activity for CCR5, and we generated 22 mutants with substitutions in the regions of non-homology located on the putative surface of the molecule. Two mutations situated on the face of C-18, predicted to be involved in its interaction with the ligand cyclosporin A, were shown to be critical for CCR5-binding and the inhibition of HIV-1 fusion and infectivity. In contrast, four mutations in C-18 specifically designed to abolish the peptidyl-prolyl cis-trans-isomerase activity of the protein failed to inactivate its CCR5 binding and HIV inhibitory activities. Interleukin-12 induction by C-18, on the other hand, was abrogated by mutations effecting either the CCR5 binding or enzymatic function of the molecule. These findings shed light on the structural basis of the molecular mimicry of the chemokine function by a pathogen-derived protein and provide a basis for further modification of C-18 into an antiviral agent. 相似文献
925.
Franks F 《Biophysical chemistry》2003,105(2-3):251-261
The physical nature of a glass, as related to stable liquid and crystalline solid phases was defined by Kauzmann in 1948. Since then, glass research has been almost exclusively confined to inorganic materials. This review aims to demonstrate that many substances, not falling into the category of classical 'materials', can be rendered into amorphous states. In particular, water itself, but also water soluble and water sensitive organic molecules, some of them biomolecules, can be rendered into supersaturated and solid solutions. New ways of studying and applying amorphisation processes have led to major advances in food and pharmaceutical processing aimed mainly at the stabilisation of labile materials. Because of their molecular similarities to water, polyhydroxy compounds are attracting particular interest as potential matrix elements in the preparation of glassy products. 相似文献
926.
Claverie-Martin F González-Acosta H Flores C Antón-Gamero M García-Nieto V 《Human genetics》2003,113(6):480-485
Dent's disease is an X-linked renal tubular disorder characterized by low-molecular-weight proteinuria, hypercalciuria, nephrocalcinosis, nephrolithiasis, and eventual renal failure. Various types of mutations in the renal chloride channel gene, CLCN5, have been identified in patients with this disease. We studied a Spanish patient with Dent's disease and found, by polymerase chain reaction amplification of the CLCN5 exons, an abnormally large exon 11. Sequencing analysis revealed that this was attributable to the insertion in codon 650 of an Alu element of the "young" Ya5 subfamily. The Alu element was inserted with the same orientation as the CLCN5 gene and arose de novo on the maternal chromosome. Polymorphism analysis indicated that the insertion occurred in the germline of the maternal grandfather. The presence of a long poly(A) tract and evidence for a 16-bp target-site duplication implied that the Alu element was integrated by retrotransposition. This mutation predicts a truncated ClC-5 protein that lacks part of the carboxy-terminus and is likely to result in loss of function of the chloride channel. Insertions of Alu sequences, which are rarely found in coding regions, have occasionally been reported to cause other genetic diseases. However, this is the first report of a retrotransposon insertion in the CLCN5 gene associated with Dent's disease.Electronic Supplementary Material Supplementary material is available in the online version of this article at 相似文献
927.
Two Brevibacterium linens strains and the cheese-ripening yeast Geotrichum candidum were compared with regard to their ability to produce volatile sulfur compounds (VSCs) from three different precursors namely L-methionine, 4-methylthio-2-oxobutyric acid (KMBA) and 4-methylthio-2-hydroxybutyric acid (HMBA). All microorganisms were able to convert these precursors to VSCs. However, although all were able to produce VSCs from L-methionine, only G. candidum accumulated KMBA when cultivated on this amino acid, contrary to B. linens suggesting that the transamination pathway is not active in this microorganism. Conversely, a L-methionine gamma-lyase activity--which catalyses the one step L-methionine to methanethiol (MTL) degradation route--was only found in B. linens strains. Several other enzymatic activities involved in the catabolism of the precursors tested were investigated. KMBA transiently accumulated in G. candidum cultures, and was then reduced to HMBA by a KMBA dehydrogenase (KDH) activity. This activity was not detected in B. linens. Despite no HMBA dehydrogenase (HDH) was found in G. candidum, a strong HMBA oxidase (HOX) activity was measured in this microorganism. This latter activity was weakly active in B. linens. KMBA and HMBA demethiolating activities were found in all the microorganisms. Our results illustrate the metabolic diversity between cheese-ripening microorganisms of the cheese ecosystem. 相似文献
928.
929.
Artificial chaperone-assisted refolding of bovine carbonic anhydrase using molecular assemblies of stimuli-responsive polymers 总被引:1,自引:0,他引:1
An artificial chaperone, which can decrease the protein aggregation and increase the reactivation yield of denatured protein in a fashion similar to natural chaperone, was newly developed using stimuli-responsive polymers. It has previously been reported that the addition of poly(propylene oxide)-phenyl-poly(ethylene glycol) (PPOn-Ph-PEG) with the unit number of PPO (n) 33 could enhance the refolding of bovine carbonic anhydrase (Kuboi et al. J. Chromatogr. B 2000, 243, 213). PPO-Ph-PEG with a large PPO chain (n = 50) was synthesized and the surface properties were characterized by both the relative fluorescence intensity of 1-anilino-8-naphthalene sulfonate (ANS) and the fluidity determined by diphenylhexatriene (DPH). The variation of ANS intensity and DPH fluidity is shown in a diagram as functions of temperature and polymer concentration. The high values of ANS intensity and fluidity of PPO50-Ph-PEG were obtained in a relatively wide conditional range (more than 0.08 mM and more than 15 degrees C) although the conditions showing the high values of PPO33-Ph-PEG were restricted (more than 0.1 mM and more than 40 degrees C). It was also found that molecular assemblies of PPOn-Ph-PEG with diameters of 7-18 nm were formed in the above conditions. On the basis of the surface properties of their polymer self-assemblies, the possibility of using them as an artificial chaperone was investigated. The effect of the addition of PPOn-Ph-PEG on the reactivation yield of a model protein, carbonic anhydrase from bovine (CAB), and the optical density of the solution was examined at various temperatures and concentrations. The reactivation yield of CAB was strongly enhanced and the aggregate formation (the optical density) was suppressed by adding PPOn-Ph-PEG in the above conditions, which show high ANS intensity and DPH fluidity. Especially in the presence of 0.1 mM PPO50-Ph-PEG, the reactivation yield of CAB reached approximately 100% at 40-55 degrees C. It was thus found that self-assemblies of the present polymer could be utilized as an artificial chaperone by selecting suitable stimuli conditions. 相似文献
930.
Random peptide libraries displayed on adeno-associated virus to select for targeted gene therapy vectors 总被引:20,自引:0,他引:20
Müller OJ Kaul F Weitzman MD Pasqualini R Arap W Kleinschmidt JA Trepel M 《Nature biotechnology》2003,21(9):1040-1046
Characterizing the molecular diversity of the cell surface is critical for targeting gene therapy. Cell type-specific binding ligands can be used to target gene therapy vectors. However, targeting systems in which optimum eukaryotic vectors can be selected on the cells of interest are not available. Here, we introduce and validate a random adeno-associated virus (AAV) peptide library in which each virus particle displays a random peptide at the capsid surface. This library was generated in a three-step system that ensures encoding of displayed peptides by the packaged DNA. As proof-of-concept, we screened AAV-libraries on human coronary artery endothelial cells. We observed selection of particular peptide motifs. The selected peptides enhanced transduction in coronary endothelial cells but not in control nonendothelial cells. This vector targeting strategy has advantages over other combinatorial approaches such as phage display because selection occurs within the context of the capsid and may have a broad range of applications in biotechnology and medicine. 相似文献