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991.
Pelletier JP Boileau C Boily M Brunet J Mineau F Geng C Reboul P Laufer S Lajeunesse D Martel-Pelletier J 《Arthritis research & therapy》2005,7(5):R1091-R1102
This study sought to evaluate the levels of mRNA expression and protein synthesis of MMP-13, cathepsin K, aggrecanase-1 (ADAMTS-4),
aggrecanase-2 (ADAMTS-5) and 5-lipoxygenase (5-LOX) in cartilage in the experimental anterior cruciate ligament (ACL) dog
model of osteoarthritis (OA), and to examine the effects of treatment with licofelone, a 5-lipoxygenase (LOX)/cyclooxygenase
(COX) inhibitor, on the levels of these catabolic factors. Sectioning of the ACL of the right knee was performed in three
experimental groups: group 1 received no active treatment (placebo group); and groups 2 and 3 received therapeutic concentrations
of licofelone (2.5 or 5.0 mg/kg/day orally, respectively) for 8 weeks, beginning the day following surgery. A fourth group
consisted of untreated dogs that were used as normal controls. Specimens of cartilage were selected from lesional areas of
OA femoral condyles and tibial plateaus, and were processed for real-time quantitative PCR and immunohistochemical analyses.
The levels of MMP-13, cathepsin K, ADAMTS-4, ADAMTS-5 and 5-LOX were found to be significantly increased in OA cartilage.
Licofelone treatment decreased the levels of both mRNA expression and protein synthesis of the factors studied. Of note was
the marked reduction in the level of 5-LOX gene expression. The effects of the drug were about the same at both tested dosages.
In vivo treatment with therapeutic dosages of licofelone has been found to reduce the degradation of OA cartilage in experimental
OA. This, coupled with the results of the present study, indicates that the effects of licofelone are mediated by the inhibition
of the major cartilage catabolic pathways involved in the destruction of cartilage matrix macromolecules. Moreover, our findings
also indicate the possible auto-regulation of 5-LOX gene expression by licofelone in OA cartilage. 相似文献
992.
Studies have shown that both carbon dioxide (CO?) and octenol (1-octen-3-ol) are effective attractants for mosquitoes. The objective of the present study was to evaluate the attractiveness of 1-octen-3-ol and CO? for diurnal mosquitoes in the southeastern Atlantic forest. A Latin square experimental design was employed with four treatments: CDC-light trap (CDC-LT), CDC-LT and 1-octen-3-ol, CDC-LT and CO? and CDC-LT with 1-octen-3-ol and CO?. Results demonstrated that both CDC-CO? and CDC-CO?-1-octen-3-ol captured a greater number of mosquito species and specimens compared to CDC-1-octen-3-ol; CDC-LT was used as the control. Interestingly, Anopheles (Kerteszia) sp. was generally attracted to 1-octen-3-ol, whereas Aedes serratus was the most abundant species in all Latin square collections. This species was recently shown to be competent to transmit the yellow fever virus and may therefore play a role as a disease vector in rural areas of Brazil. 相似文献
993.
Pedro Henrique Monteiro Torres Gabriel Limaverde Soares Costa Sousa Pedro Geraldo Pascutti 《Proteins》2011,79(9):2684-2692
Endostatin is a potent antiangiogenic protein derived from the noncollagenous domain 1 (NC1) of collagen XVIII. The mechanism by which endostatin exerts its antiangiogenic effect is still incompletely understood. It has been shown that the 27 amino acid N‐terminal fragment of murine endostatin has antitumor, antimigration, and antipermeability activities comparable to the full soluble protein. To understand how this peptide can exert such elaborate function, we performed structural analysis using molecular dynamics to evaluate the behavior of this fragment in aqueous environment. Here, we show that the N‐terminal peptide of murine endostatin is able to assume a well‐defined structure, folding into a zinc‐dependent β‐hairpin conformation. Analyzing the folding mechanism, we were able to understand why the N‐terminal peptide of human endostatin with the same length failed to acquire a stable conformation. Conversely, we were able to predict the successful folding of the R4Q mutant and of a shorter form of the human peptide with 25 residues. Finally, we show that the β‐hairpin conformation assumed by the zinc‐bound peptide of murine endostatin has a high structural similarity with fragments of another family of angiogenesis inhibitors: the integrin‐binding portion of the NC1 domain of collagen IV. Indeed, our docking simulations show that arresten, canstatin, and the endostatin peptide bind to the same spot of αVβ3 integrin, suggesting similar interactions via a common binding site on this receptor. Proteins 2011;. © 2011 Wiley‐Liss, Inc. 相似文献
994.
995.
Lu S Yao Y Cheng X Mitchell S Leng S Meng S Gallagher JW Shelness GS Morris GS Mahan J Frase S Mansbach CM Weinberg RB Black DD 《The Journal of biological chemistry》2006,281(6):3473-3483
Intestinal apolipoprotein A-IV expression is highly regulated by dietary lipid in newborn swine, suggesting a role in lipid absorption. Constitutive overexpression of apoA-IV in newborn swine enterocytes enhances basolateral secretion of triacylglycerol (TG) in TG-rich lipoproteins 4.9-fold (Lu, S., Yao, Y., Meng, S., Cheng, X., and Black, D. D. (2002) J. Biol. Chem. 277, 31929-31937). To investigate the mechanism of this enhancement, IPEC-1 cells were transfected with a tetracycline-regulatable expression system (Tet-On). In cells incubated with oleic acid, a dose response relationship was observed between medium doxycycline concentration and basolateral apoA-IV and TG secretion. Similarly regulated expression of apoA-I did not enhance lipid secretion. The mean diameter of TG-rich lipoproteins secreted from doxycycline-treated cells was larger than from untreated cells (87.0 nm versus 53.4 nm). Basolateral apoB secretion decreased. Using the same expression system, full-length human apoA-IV (376 amino acids); a "pig-like" human apoA-IV, lacking the C-terminal EQQQ repeats (361 amino acids); and a "chicken-like" apoA-IV, further truncated to 343 amino acids, were expressed in IPEC-1 cells. With increasing protein secretion, cells expressing the full-length human apoA-IV displayed a 2-fold increase in TG secretion; in sharp contrast, cells expressing the pig-like human apoA-IV displayed a 25-fold increase in TG secretion and a 27-fold increase in lipoprotein diameter. When human apoA-IV was further truncated to yield a chicken-like protein, TG secretion was inhibited. We conclude that overexpression of swine apoA-IV enhances basolateral TG secretion in a dose-dependent manner by increasing the size of secreted lipoproteins. These data suggest that the region in the human apoA-IV protein from residues 344 to 354 is critical to its ability to enhance lipid secretion, perhaps by enabling the packaging of additional core TG into chylomicron particles. The EQQQ-rich region may play an inhibitory or modulatory role in chylomicron packaging in humans. 相似文献
996.
Background
Chow and Liu showed that the maximum likelihood tree for multivariate discrete distributions may be found using a maximum weight spanning tree algorithm, for example Kruskal's algorithm. The efficiency of the algorithm makes it tractable for high-dimensional problems. 相似文献997.
The Lagrangian stochastic model for estimating footprint and water vapor fluxes over inhomogeneous surfaces 总被引:5,自引:0,他引:5
This study investigated a two-dimensional Lagrangian stochastic dispersion model for estimating water vapor fluxes and footprint
over homogeneous and inhomogeneous surfaces. Over the homogeneous surface, particle trajectories were computed from a 2-D
Lagrangian model forced by Eulerian velocity statistics determined by Monin–Obukhov similarity theory (MOST). For an inhomogeneous
surface, the velocity and atmospheric stability profiles were computed using a second-order Eulerian closure model, and these
local profiles were then used to drive the Lagrangian model. The model simulations were compared with water vapor flux measurements
carried out above an irrigated bare soil site and an irrigated potato site. The inhomogeneity involved a step change in surface
roughness, humidity, and temperature. Good agreement between eddy-correlation-measured and Lagrangian-model-predicted water
vapor fluxes was found for both sites. Hence, this analysis demonstrates the practical utility of second-order closure models
in conjunction with Lagrangian analysis to estimate the scalar footprint in planar inhomogeneous flows. 相似文献
998.
Superoxide reductases (SORs) are superoxide (O2-)-detoxifying enzymes that catalyse the reduction of O2- into hydrogen peroxide. Three different classes of SOR have been reported on the basis of the presence or not of an additional N-terminal domain. They all share a similar active site, with an unusual non-heme Fe atom coordinated by four equatorial histidines and one axial cysteine residues. Crucial catalytic reaction intermediates of SOR are purported to be Fe(3+)-(hydro)peroxo species. Using resonance Raman spectroscopy, we compared the vibrational properties of the Fe3+ active site of two different classes of SOR, from Desulfoarculus baarsii and Treponema pallidum, along with their ferrocyanide and their peroxo complexes. In both species, rapid treatment with H2O2 results in the stabilization of a side-on high spin Fe(3+)-(eta(2)-OO) peroxo species. Comparison of these two peroxo species reveals significant differences in vibrational frequencies and bond strengths of the Fe-O2 (weaker) and O-O (stronger) bonds for the T. pallidum enzyme. Thus, the two peroxo adducts in these two SORs have different stabilities which are also seen to be correlated with differences in the Fe-S coordination strengths as gauged by the Fe-S vibrational frequencies. This was interpreted from structural variations in the two active sites, resulting in differences in the electron donating properties of the trans cysteine ligand. Our results suggest that the structural differences observed in the active site of different classes of SORs should be a determining factor for the rate of release of the iron-peroxo intermediate during enzymatic turnover. 相似文献
999.
1000.
Manuo-ocular coordination in target tracking. II. Comparing the model with human behavior 总被引:2,自引:0,他引:2
Several studies have shown that humans track a moving visual target with their eyes better if the movement of this target
is directly controlled by the observer's hand. The improvement in performance has been attributed to coordination control
between the arm motor system and the smooth pursuit (SP) system. In such a task, the SP system shows characteristics that
differ from those observed during eye-alone tracking: latency (between the target-arm and the eye motion onsets) is shorter,
maximum SP velocity is higher and the maximum target motion frequency at which the SP can function effectively is also higher.
The aim of this article is to qualitatively evaluate the behavior of a dynamical model simulating the oculomotor system and
the arm motor system when both are involved in tracking visual targets. The evaluation is essentially based on a comparison
of the behavior of the model with the behavior of human subjects tracking visual targets under different conditions. The model
has been introduced and quantitatively evaluated in a companion paper. The model is based on an exchange of internal information
between the two sensorimotor systems, mediated by sensory signals (vision, arm muscle proprioception) and motor signals (arm
motor command copy). The exchange is achieved by a specialized structure of the central nervous system, previously identified
as a part of the cerebellum. Computer simulation of the model yielded results that fit the behavior of human subjects observed
during previously reported experiments, both qualitatively and quantitatively. The parallelism between physiology and human
behavior on the one hand, and structure and simulation of the model on the other hand, is discussed.
Received: 6 March 1997 / Accepted in revised form: 15 July 1997 相似文献