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941.
Summary Golgi preparations were made by consecutive treatment of formalin-fixed brain and liver with potassium dichromate and silver nitrate. Impregnated tissue dissected from thin slices of the blocks were studied by X-ray powder diffraction methods, in a diffractometer and a Guinier camera. Such tissue proved to contain crystalline silver chromate, Ag2CrO4, both while still in the silver nitrate solution and after dehydration in ethanol and clearing in xylene and xylene-Dammar resin. No other compounds containing chromium or silver were detectable. Formalin-fixed tissue merely treated with silver nitrate contained silver chloride, but in impregnated tissue the amount was too scarce to be visible. Hence, silver chloride was no integral part of the Golgi precipitate.A number of mostly ethereal oils traditionally used for clearing histological sections, did not cause the appearance of metallic silver in detectable amount in the Golgi preparations. However, after treatment with clove oil and creosote metallic silver was detected in the tissue.This study was supported by U.S. P.H. S. Grant NS 07998. This aid is gratefully acknowledged.We are indebted to Miss I. Madsen and Mrs. K. Sörensen for technical assistance.  相似文献   
942.
Streptococcus pneumoniae is the leading causative agent of community-acquired pneumonia. Induction of apoptosis in pulmonary epithelial cells by bacteria during pneumonia might be harmful to the host. Interleukin-15 (IL-15) has been demonstrated as an effective inhibitor of apoptosis and is expressed in lung epithelium on the mRNA and protein level. Therefore, we characterized the sub-cellular expression pattern of the short and long IL-15 isoforms in lung epithelial cells in vitro as well as its role in pneumococci-related lung epithelial cell apoptosis. We found an expression pattern for both IL-15 signal peptides in the pulmonary epithelial cell lines A549 and Beas-2B. Moreover, a strong co-localization of IL-15 and IL-15Ralpha was detected on cell surfaces. Compared to pro-inflammatory cytokine stimulation, neither IL-15 nor its trimeric receptor complex was up-regulated after pneumococcal infection. However, overexpression of IL-15 isoforms revealed IL-15LSP and IL-15Vkl as inhibitors of pneumococci induced apoptosis in pulmonary epithelial cells. Thus, IL-15 may act as an anti-apoptotic molecule in pneumococci infection, thereby suggesting IL-15 as a benefical cytokine in pulmonary host defense against infection.  相似文献   
943.
Volatile metabolites controlling germination in buried weed seeds   总被引:3,自引:1,他引:3       下载免费PDF全文
Holm RE 《Plant physiology》1972,50(2):293-297
Velvetleaf (Abutilon theophrasti Medic), morning glory (Ipomoea purpurea [L.] Roth), and wild mustard (Brassica kaber [D.C.] L. C. Wheeler) seeds exhibited decreased germination with increased planting depth in soil. Flushing the soil for 2 minutes each day with air overcame the inhibition. A sealed in vitro system was used to sample the volatile components produced by weed seeds. Inhibition of seed germination was accompanied by decreased O2 levels and production of volatile metabolites identified as acetaldehyde, ethanol, and acetone. The effectiveness of these compounds in reducing germination was dependent on O2 levels.  相似文献   
944.
A portable hydraulic device has been developed for use in optimizing the design of brushes and cleaning units that may be employed to maintain fouling-release coatings. Laboratory tests showed that characteristics of experimental cleaning brushes, including bristle stiffness, density, and angle, significantly affected the shear and normal forces imparted to the surface and thus, to any encrusting organisms. The standoff distance between the cleaning unit and the surface also influenced the forces generated. The rate of rotation of the brush, however, had little effect on force. The hydraulic device, with its experimental brushes, can also be used to evaluate the cleanability of fouling-release surfaces in situ, or to assess wear of the coating system due to cleaning.  相似文献   
945.
Inherited diseases are the result of DNA sequence changes. In recessive diseases, the clinical phenotype results from the combined functional effects of variants in both copies of the gene. In some diseases there is often considerable variability of clinical presentation or disease severity, which may be predicted by the genotype. Additional effects may be triggered by environmental factors, as well as genetic modifiers which could be nucleotide polymorphisms in related genes, e.g. maternal ApoE or ABCA1 genotypes which may have an influence on the phenotype of SLOS individuals. Here we report the establishment of genotype variation databases for various rare diseases which provide individual clinical phenotypes associated with genotypes and include data about possible genetic modifiers. These databases aim to be an easy public access to information on rare and private variants with clinical data, which will facilitate the interpretation of genetic variants.  相似文献   
946.
Synaptotagmin is a multifunctional membrane protein that may regulate exo-endocytic cycling of synaptic vesicles at the presynaptic plasmalemma. Its C2B domain has been postulated to interact with a variety of effector molecules including acidic phospholipids, phosphoinositides, SNAREs (soluble N-ethylmaleimide-sensitive factor attachment protein receptors), calcium channels, and the clathrin adaptor complex AP-2. Here we report that a basic motif within the C2B domain is required and sufficient for binding to AP-2 via its mu2 subunit and that this interaction is dependent on multimerization of the AP-2 binding site. Moreover, we show that upon fusion to a plasma membrane reporter protein this sequence is sufficient to target the chimeric molecule for internalization. We hypothesize that basic motifs within multimeric membrane proteins may represent a novel type of clathrin/AP-2-dependent endocytosis signal.  相似文献   
947.
948.
949.
Endothelial nitric oxide synthase (eNOS) is essential for neovascularization. Here we show that the impaired neovascularization in mice lacking eNOS is related to a defect in progenitor cell mobilization. Mice deficient in eNOS (Nos3(-/-)) show reduced vascular endothelial growth factor (VEGF)-induced mobilization of endothelial progenitor cells (EPCs) and increased mortality after myelosuppression. Intravenous infusion of wild-type progenitor cells, but not bone marrow transplantation, rescued the defective neovascularization of Nos3(-/-) mice in a model of hind-limb ischemia, suggesting that progenitor mobilization from the bone marrow is impaired in Nos3(-/-) mice. Mechanistically, matrix metalloproteinase-9 (MMP-9), which is required for stem cell mobilization, was reduced in the bone marrow of Nos3(-/-) mice. These findings indicate that eNOS expressed by bone marrow stromal cells influences recruitment of stem and progenitor cells. This may contribute to impaired regeneration processes in ischemic heart disease patients, who are characterized by a reduced systemic NO bioactivity.  相似文献   
950.
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