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971.
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974.
Resveratrol (trans-3,4N-trihydroxystilbene), a phytoalexin present in grapes and red wine is emerging as a natural compound with anticancer properties. However, the physiological and molecular effects of resveratrol on normal uterine cells are poorly understood. In the present study we evaluated the effects of resveratrol on normal uterine cells and the mechanisms involved in vivo. Healthy immature rats were treated s.c. with resveratrol (0, 0.5, 5, and 50 mg/kg body weight) for 7 consecutive days and euthanized on the eighth day. Uteri were collected and weighed, and endometrium was recovered for total protein extraction, followed by Western blot analysis. Estrogen receptor alpha 1 (ESR1) and beta 2 (ESR2) affinity and activation by resveratrol were also determined by in vitro ESR-binding assays. Immunohistochemistry (IHC) studies were performed to visualize the proliferation marker, proliferating cell nuclear antigen (PCNA), and immunofluorescence (IF) studies were done to study the localization of PTGS2. The results showed that resveratrol increased uterine wet weight and uterine body weight ratios significantly. This local cellular proliferation in terms of the thickening of the columnar epithelial cells and an increase in the number of glands was accompanied by an increase of AKT 16 phosphorylation and PTGS2 and XIAP protein expression. These results were further supported by IF and IHC analyses. Total AKT, ESR1, and ESR2 protein expression levels were not modulated by the treatment; however, resveratrol showed moderate estrogenicity for both ESR isoforms. Expression of progesterone receptor A (PGR) was induced in the presence of resveratrol. These data support the hypothesis that resveratrol can act in a prosurvival or antiapoptotic way through AKT, XIAP, and PTGS2 regulation in the endometrium and could positively affect the outcome of pregnancy and favor fertility. 相似文献
975.
Substitution reaction of chloro η6-arene ruthenium N∩O-base complexes [(η6-arene)Ru(N∩O)Cl] [N∩O = pyrazine-2-carboxylic acid (pca-H), 8-hydroxyquinoline (hq-H); arene = p-iPrC6H4Me, N∩O = hq (1); arene = C6Me6, N∩O = hq (2)] with NaN3 yield the neutral arene ruthenium azido complexes of the general formula [(η6-arene)Ru(N∩O)N3] [N∩O = pca, arene = p-iPrC6H4Me (3), arene = C6Me6 (4); N∩O = hq, arene = p-iPrC6H4Me (5), arene = C6Me6 (6)]. These complexes undergo [3 + 2] dipolar cycloaddition reaction with activated alkynes dimethyl and diethyl acetylenedicarboxylates to yield the arene triazole complexes [(η6-arene)Ru(N∩O){N3C2(CO2R)2}] [N∩O = pca, R = Me, arene = p-iPrC6H4Me (7), C6Me6 (8); R = Et, arene = p-iPrC6H4Me (9), C6Me6 (10); N∩O = hq, R = Me, arene = p-iPrC6H4Me (11) C6Me6 (12); R = Et, arene = p-iPrC6H4Me (13), C6Me6 (14)]. On the bases of proton NMR study, in the above triazole complexes N(2) isomers are assigned with dimethylacetylenedicarboxylate whereas N(1) isomers with diethylacetylenedicarboxylate. All complexes have been characterized by IR and NMR spectroscopy as well as by elemental analysis. The molecular structures of the azido complexes [(η6-p-iPrC6H4Me)Ru(pca)N3] (3), [(η6-p-iPrC6H4Me)Ru(hq)N3] (5) and [(η6-C6Me6)Ru(hq)N3] (6) have been established by single crystal X-ray diffraction studies. 相似文献
976.
977.
The IL1alpha-S100A13 heterotetrameric complex structure: a component in the non-classical pathway for interleukin 1alpha secretion 总被引:1,自引:0,他引:1
Interleukin 1α (IL1α) plays an important role in several key biological functions, such as angiogenesis, cell proliferation, and tumor growth in several types of cancer. IL1α is a potent cytokine that induces a wide spectrum of immunological and inflammatory activities. The biological effects of IL1α are mediated through the activation of transmembrane receptors (IL1Rs) and therefore require the release of the protein into the extracellular space. IL1α is exported through a non-classical release pathway involving the formation of a specific multiprotein complex, which includes IL1α and S100A13. Because IL1α plays an important role in cell proliferation and angiogenesis, inhibiting the formation of the IL1α-S100A13 complex would be an effective strategy to inhibit a wide range of cancers. To understand the molecular events in the IL1α release pathway, we studied the structure of the IL1α-S100A13 tetrameric complex, which is the key complex formed during the non-classical pathway of IL1α release. 相似文献
978.
Biocatalyst behavior was comparatively evaluated under diverse microenvironments viz., self-induced electrogenic (bioelectrochemical treatment, BET) and anaerobic treatment (AnT) microenvironments, with real-field pharmaceutical wastewater. Relatively higher treatment efficiency was observed with BET (COD removal, 78.70%) over AnT (32%) along with the power output. Voltammetric profiles of AnT showed persistent reduction behavior, while BET depicted simultaneous redox behavior. BET operation documented significantly higher bio-electrocatalytic activity (kapp, 245.22 s−1) than AnT (kapp, 7.35 s−1). The electron accepting conditions due to the presence of electrode in the BET might contributed to higher electrogenesis leading to enhanced substrate degradation along with the removal of multiple pollutants accounting for the effective reduction of toxicity levels of wastewater. Even at higher organic loads, BET operation showed good treatment efficiency without process inhibition. Introduction of electrode-membrane assembly in anaerobic microenvironment showed significant change in the electrocatalytic behavior of biocatalyst resulting in enhanced treatment of complex wastewater. 相似文献
979.
Balasubramanyam M Aravind S Gokulakrishnan K Prabu P Sathishkumar C Ranjani H Mohan V 《Molecular and cellular biochemistry》2011,351(1-2):197-205
Molecular and Cellular Biochemistry - Type 2 diabetes patients exhibit subclinical inflammation but the regulatory mechanisms are poorly understood. We sought to evaluate the role of miR-146a... 相似文献
980.
A. Kiran KumarP. Chiranjeevi G. MohanakrishnaS. Venkata Mohan 《Ecological Engineering》2011,37(10):1555-1562
Natural attenuation of estrogenic endocrine disrupting compounds (EDCs) such as estriol (E3, natural) and 17α-ethinylestradiol (EE2, synthetic) were evaluated in a designed ecologically engineered treatment system (EETS) along with domestic sewage. These two estrogens are the major contaminants of sewage and found to cause adverse effects on the endocrine system of humans and animals when exposed even in nanogram concentrations. The EETS consisted of three tanks containing diverse biota, viz., aquatic macrophytes, submerged plants, emergent plants, algae and bacteria present in the system mimic the natural cleansing functions of wetlands and help in the treatment of pollutants present in wastewater. During operation, 22 μg/l of E3 and EE2 were separately fed for 10 days each and operated in continuous mode (20 l/day). The floating macrophytes system (Tank 1) was more effective in removing estrogens [E3 - 61.77% (13.59 μg/l); EE2 - 69.09% (15.20 μg/l)] compared to the submerged-emergent macrophytes-based integrated system (Tank 2) [E3 - 16.58% (3.65 μg/l); EE2 - 18.52% (4.08 μg/l)] and submerged-rooted microphytes system (Tank 3) [E3 - 15.20%, (3.35 μg/l); EE2 - 7.72%, (1.70 μg/l)]. On the whole, EETS can effectively treat EDCs [E3 93.56% (20.59 μg/l); EE2 95.34% (20.97 μg/l)]. Removal of COD (68.06%), nitrates (60.02%) and turbidity (83.43%) was also observed simultaneously during EETS operation. The designed EETS is ecologically complex and mechanically simple and has very low energy consumption and function based on a natural cleansing mechanism (attenuation) with esthetic value. 相似文献