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991.
Blood flow distribution and tissue allometry in channel catfish 总被引:2,自引:0,他引:2
I. R. Schultz ¶ M. G. Barron ‡ M. C. Newman ‡ A. M. Vick § 《Journal of fish biology》1999,54(6):1275-1286
Blood flow (as percentage of cardiac output) in fasted channel catfish acclimated to 21°C was directed primarily to white muscle (72%) followed by head kidney (5·7%), red muscle (5·5%), trunk kidney (3·1%), liver (2·2%), swim bladder (1·4%) and skin (1·1%). The stomach, intestines, pyloric caeca, gonads, brain, abdominal fat and spleen contained <0·5% of blood flow. There was considerable interfish variation among blood flow distribution to visceral organs with substantial spatial heterogeneity of blood flow to white muscle. The spatial heterogeneity of flow to muscle prevented accurate estimation of total flow to this tissue based on the microsphere deposition of a few sub-samples. Instead, a novel approach, based on the whole animal counting of the eviscerated carcass was used to measure blood flow to white muscle. The scaling relationships for tissue mass in catfish (63–1873 g) followed the allometric equation (aWb ) and tended to exhibit negative allometry, with organ weight decreasing in proportion to body weight. The b values for most tissues ranged between 0·83 and 1·0. The relative mass of the brain showed the greatest decline and with a b value of 0·32. The results, together with previous data on cardiac output, permitted calculation of organ blood flow rates in channel catfish. © 1999 The Fisheries Society of the British Isles 相似文献
992.
John H. Leamon Eric T. Schultz Joseph F. Crivello 《Environmental Biology of Fishes》2000,57(4):451-458
Variation among four commonly used health indices was examined in the mummichog, Fundulus heteroclitus. The four indices were liver glycogen content (LGC), liver-somatic index (LSI), condition index (K) and RNA–DNA ratio. Fish were collected from five coastal locations in southeastern Connecticut. Fish health, as determined by these four indices, varied considerably among estuaries and between sexes. The relationship between each index and specimen length was significantly different among estuaries for either sex. When regressed against length, the slopes for the indices ranged from positive to negative. For each index, significant differences existed among some of the length-centered means at each estuary for either sex. Estuary rank for one index did not necessarily correlate with the estuary rank for another index. The significance of this variability and its impact on the use of the indices as bioindicators of environmental perturbation is discussed. 相似文献
993.
J F Kameni Tcheudji L Lebeau N Virmaux C G Maftei R H Cote C Lugnier P Schultz 《Journal of molecular biology》2001,310(4):781-791
Phosphodiesterase 6 (PDE6), a multisubunit (alphabetagamma(2)delta) enzyme, plays a major role in visual function by hydrolysing cGMP in response to a light stimulus. Solubilized bovine rod PDE6 molecules depleted of their gamma subunits were purified to homogeneity from bovine retinal rods and their molecular organization was investigated by electron microscopy. Image analysis of single particles revealed the three-dimensional dimeric arrangement of the purified alphabetadelta complex, and the internal organization of each catalytic subunit into three distinct domains at a resolution of 2.8 nm. The relative volume of each domain is consistent with sequence analysis and functional data, which suggest that these domains correspond to the catalytic and two GAF domains. This hypothesis was confirmed by immunolabelling experiments, which located the N-terminal part of the catalytic subunit where the major interaction between the two alphabeta subunits was found to occur. The 3D molecular organization of human platelet PDE5 appears highly homologous to that of bovine rod PDE6, as predicted by similarities in their primary sequences. These observations describe the quaternary organization of the catalytic PDE6 alphabeta complex, and place the catalytic and regulatory domains on a structural model. 相似文献
994.
Paruch K Dwyer MP Alvarez C Brown C Chan TY Doll RJ Keertikar K Knutson C McKittrick B Rivera J Rossman R Tucker G Fischmann TO Hruza A Madison V Nomeir AA Wang Y Lees E Parry D Sgambellone N Seghezzi W Schultz L Shanahan F Wiswell D Xu X Zhou Q James RA Paradkar VM Park H Rokosz LR Stauffer TM Guzi TJ 《Bioorganic & medicinal chemistry letters》2007,17(22):6220-6223
Properly substituted pyrazolo[1,5-a]pyrimidines are potent and selective CDK2 inhibitors. Compound 15j is orally available and showed efficacy in a mouse A2780 xenograft model. 相似文献
995.
996.
997.
JB Poell RJ van Haastert T de Gunst IJ Schultz WM Gommans M Verheul F Cerisoli PI van Noort GP Prevost RQ Schaapveld E Cuppen 《PloS one》2012,7(8):e43569
Malignant melanoma is an aggressive form of skin cancer with poor prognosis. Despite improvements in awareness and prevention of this disease, its incidence is rapidly increasing. MicroRNAs (miRNAs) are a class of small RNA molecules that regulate cellular processes by repressing messenger RNAs (mRNAs) with partially complementary target sites. Several miRNAs have already been shown to attenuate cancer phenotypes, by limiting proliferation, invasiveness, tumor angiogenesis, and stemness. Here, we employed a genome-scale lentiviral human miRNA expression library to systematically survey which miRNAs are able to decrease A375 melanoma cell viability. We highlight the strongest inhibitors of melanoma cell proliferation, including the miR-15/16, miR-141/200a and miR-96/182 families of miRNAs and miR-203. Ectopic expression of these miRNAs resulted in long-term inhibition of melanoma cell expansion, both in vitro and in vivo. We show specifically miR-16, miR-497, miR-96 and miR-182 are efficient effectors when introduced as synthetic miRNAs in several melanoma cell lines. Our study provides a comprehensive interrogation of miRNAs that interfere with melanoma cell proliferation and viability, and offers a selection of miRNAs that are especially promising candidates for application in melanoma therapy. 相似文献
998.
999.
Hellwig N Plant TD Janson W Schäfer M Schultz G Schaefer M 《The Journal of biological chemistry》2004,279(33):34553-34561
The low extracellular pH of inflamed or ischemic tissues enhances painful sensations by sensitizing and activating the vanilloid receptor 1 (TRPV1). We report here that activation of TRPV1 results in a marked intracellular acidification in nociceptive dorsal root ganglion neurons and in a heterologous expression system. A characterization of the underlying mechanisms revealed a Ca(2+)-dependent intracellular acidification operating at neutral pH and an additional as yet unrecognized direct proton conductance through the poorly selective TRPV1 pore operating in acidic extracellular media. Large organic cations permeate through the activated TRPV1 pore even in the presence of physiological concentrations of Na(+), Mg(2+), and Ca(2+). The wide pore and the unexpectedly high proton permeability of TRPV1 point to a proton hopping permeation mechanism along the water-filled channel pore. In acidic media, the high relative proton permeability through TRPV1 defines a novel proton entry mechanism in nociceptive neurons. 相似文献
1000.
Paullones are potent inhibitors of glycogen synthase kinase-3beta and cyclin-dependent kinase 5/p25. 总被引:5,自引:0,他引:5
M Leost C Schultz A Link Y Z Wu J Biernat E M Mandelkow J A Bibb G L Snyder P Greengard D W Zaharevitz R Gussio A M Senderowicz E A Sausville C Kunick L Meijer 《European journal of biochemistry》2000,267(19):5983-5994
Paullones constitute a new family of benzazepinones with promising antitumoral properties. They were recently described as potent, ATP-competitive, inhibitors of the cell cycle regulating cyclin-dependent kinases (CDKs). We here report that paullones also act as very potent inhibitors of glycogen synthase kinase-3beta (GSK-3beta) (IC50: 4-80 nM) and the neuronal CDK5/p25 (IC50: 20-200 nM). These two enzymes are responsible for most of the hyperphosphorylation of the microtubule-binding protein tau, a feature observed in the brains of patients with Alzheimer's disease and other neurodegenerative 'taupathies'. Alsterpaullone, the most active paullone, was demonstrated to act by competing with ATP for binding to GSK-3beta. Alsterpaullone inhibits the phosphorylation of tau in vivo at sites which are typically phosphorylated by GSK-3beta in Alzheimer's disease. Alsterpaullone also inhibits the CDK5/p25-dependent phosphorylation of DARPP-32 in mouse striatum slices in vitro. This dual specificity of paullones may turn these compounds into very useful tools for the study and possibly treatment of neurodegenerative and proliferative disorders. 相似文献