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991.
Lipoprotein oxidation is a process thought to be involved in atherogenesis. Dietary antioxidants that prevent or inhibit oxidative damage to lipoproteins may help to prevent atherosclerosis. Both black and green teas can be major dietary sources of flavonoids and other phenolics with antioxidant activity. Results of previous studies suggest that green tea may have a greater antioxidant potential than black tea. The aim of this study was to assess and compare the effects of black and green tea on in vitro lipoprotein oxidation. The tea extracts were prepared using a method similar to that used to prepare infusions of tea for drinking. Antioxidant activities of seven black teas and four green teas were assessed using an in vitro assay that measures Cu2+ ‐induced oxidation of lipoproteins in human serum. All tea extracts inhibited in vitro lipoprotein oxidation in human serum to a similar extent. No significant difference in antioxidant activity was found between black and green tea. Caffeine prepared to a comparable concentration to that found in tea had no effect on lipoprotein oxidation. Further studies are required to determine the importance of these findings in relation to possible protective effects of black and green tea consumption against atherogenesis and cardiovascular disease. © 1999 Society of Chemical Industry  相似文献   
992.
A highly deacetylated chitosan from shrimp with a degree of deacetylation of 95 ± 3% was prepared and spun into a monofilament fiber using a solution of 5% by weight chitosan in 5% by volume aqueous acetic acid. Samples of the spun fibers were immersed in separate solutions containing phosphate ions and phthalate ions, and subsequently washed and dried. The various solutions ranged in pH from 4.12 to 7.75. The highest dry mechanical properties resulted from solutions containing phthalate ions between 4.5–5.5 pH, and from solutions containing phosphate ions at pH 5.4. Immersion time was varied between 1 and 60 min at 25.8°C, and temperature was varied between 25.8 and 70.0°C, in the phosphate ion solutions at a pH of 5.8. Dry mechanical properties were highest at 25.8°C and after 1 h of treatment. Chitosan films were subjected to similar treatments in phosphate and phthalate ion solutions. Fourier transform infrared data (FTIR) on the films suggest that some interaction is occurring between the phosphate ions and the amine group on the chitosan backbone. An additional experiment was performed whereby the same chitosan was used to prepare a dope of 4% by weight chitosan in 4% by volume aqueous acetic acid with 30% by volume methanol. This solution was spun into fibers, but was subjected to a “final draw” by increasing the speed of the winder. With increasing the final draw, denier and elongation‐at‐break decreased, while the other mechanical properties showed a marked increase. © 1999 John Wiley & Sons, Inc. J Appl Polym Sci 72: 1721–1732, 1999  相似文献   
993.
994.
In this paper, we propose an approach to reusing requirements specification, called task-based specifications in conceptual graphs (TBCG). In TBCG, task-based specification methodology is used to serve as the mechanism to structure the knowledge captured in conceptual models, and conceptual graphs are adopted as the formalism to express requirements specification. TBCG provides several mechanisms to facilitate the reuse of formal specifications: a contextual retrieval mechanism to support context-sensitive specifications retrieval and incremental context acquisition, a graph matching mechanism to compute the similarity between two graphs based on the semantic match and fuzzy logic, and a paraphraser to serve as an explanation mechanism for the retrieval specifications. ©1999 John Wiley & Sons, Inc.  相似文献   
995.
This study deals with the process of optimization and synthesis of Poly(3-hydroxybutyrate) microspheres with encapsulated Cl-amidine. Cl-amidine is an inhibitor of peptidylarginine deiminases (PADs), a group of calcium-dependent enzymes, which play critical roles in a number of pathologies, including autoimmune and neurodegenerative diseases, as well as cancer. While Cl-amidine application has been assessed in a number of in vitro and in vivo models; methods of controlled release delivery remain to be investigated. P(3HB) microspheres have proven to be an effective delivery system for several compounds applied in antimicrobial, wound healing, cancer, and cardiovascular and regenerative disease models. In the current study, P(3HB) microspheres with encapsulated Cl-amidine were produced in a size ranging from ~4–5 µm and characterized for surface morphology, porosity, hydrophobicity and protein adsorption, in comparison with empty P(3HB) microspheres. Cl-amidine encapsulation in P(3HB) microspheres was optimized, and these were found to be less hydrophobic, compared with the empty microspheres, and subsequently adsorbed a lower amount of protein on their surface. The release kinetics of Cl-amidine from the microspheres were assessed in vitro and expressed as a function of encapsulation efficiency. There was a burst release of ~50% Cl-amidine in the first 24 h and a zero order release from that point up to 16 days, at which time point ~93% of the drug had been released. As Cl-amidine has been associated with anti-cancer effects, the Cl-amidine encapsulated microspheres were assessed for the inhibition of vascular endothelial growth factor (VEGF) expression in the mammalian breast cancer cell line SK-BR-3, including in the presence of the anti-proliferative drug rapamycin. The cytotoxicity of the combinatorial effect of rapamycin with Cl-amidine encapsulated P(3HB) microspheres was found to be 3.5% more effective within a 24 h period. The cells treated with Cl-amidine encapsulated microspheres alone, were found to have 36.5% reduction in VEGF expression when compared with untreated SK-BR-3 cells. This indicates that controlled release of Cl-amidine from P(3HB) microspheres may be effective in anti-cancer treatment, including in synergy with chemotherapeutic agents. Using controlled drug-delivery of Cl-amidine encapsulated in Poly(3-hydroxybutyrate) microspheres may be a promising novel strategy for application in PAD-associated pathologies.  相似文献   
996.
The polymeric coating used in metal packaging such as cans for foods and beverages may contain residual amounts of monomers used in the production of the coating, as well as unreacted linear and cyclic oligomers. Traditionally, although designed for use with plastic food contact materials, food simulants have been used to determine the migration of monomers from coatings into foodstuffs. More recently, food simulants have also been used to determine oligomeric species migrating from can coatings. In the work reported here, the migration of both monomers and oligomers from polyester-based can coatings into food simulants and foodstuffs, some of which were towards the end of their shelf-life, is compared. The concentrations of monomers and selected oligomers in canned foods at the end of their shelf life were found to be significantly lower than those in food simulants, which in turn was lower than those in the extraction solvent acetonitrile.  相似文献   
997.
运用热丝化学气相沉积(HFCVD)的方法制备了以多孔钛为基体的掺杂硼金刚石(porous Ti/BDD)薄膜电极,并测试了它的主要物理性质,SEM表明金刚石相生长良好并且能均匀地分布在基体表面和孔内,Raman光谱表明电极的金刚石相纯而且质量很高。采用循环伏安法研究了酸性条件下茜素红在多孔Ti/BDD电极上的电氧化行为。通过改变阳极电流密度、支持电解质Na2SO4的浓度来研究茜素红在多孔Ti/BDD电极上的电化学氧化降解的效果影响。结果表明:电流密度40 mA/cm2、支持电解质浓度0.5 mol/L为较理想的工艺参数,总电流效率达到30.2%。在相同条件下,发现多孔Ti/BDD薄膜电极氧化降解茜素红与平板Ti/BDD薄膜电极相比具有更高的电流效率。紫外可见光光谱证实了多孔Ti/BDD电极能够有效地电氧化降解茜素红。  相似文献   
998.
Pre-weaned porcine islets (PPIs) represent an unlimited source for islet transplantation but are functionally immature. We previously showed that necrostatin-1 (Nec-1) immediately after islet isolation enhanced the in vitro development of PPIs. Here, we examined the impact of Nec-1 on the in vivo function of PPIs after transplantation in diabetic mice. PPIs were isolated from pancreata of 8–15-day-old, pre-weaned pigs and cultured in media alone, or supplemented with Nec-1 (100 µM) on day 0 or on day 3 of culture (n = 5 for each group). On day 7, islet recovery, viability, oxygen consumption rate, insulin content, cellular composition, insulin secretion capacity, and transplant outcomes were evaluated. While islet viability and oxygen consumption rate remained high throughout 7-day tissue culture, Nec-1 supplementation on day 3 significantly improved islet recovery, insulin content, endocrine composition, GLUT2 expression, differentiation potential, proliferation capacity of endocrine cells, and insulin secretion. Adding Nec-1 on day 3 of tissue culture enhanced the islet recovery, proportion of delta cells, beta-cell differentiation and proliferation, and stimulation index. In vivo, this leads to shorter times to normoglycemia, better glycemic control, and higher circulating insulin. Our findings identify the novel time-dependent effects of Nec-1 supplementation on porcine islet quantity and quality prior to transplantation.  相似文献   
999.
A defined human microbiota‐associated (HMA) mouse model in BALB/c and immunodeficient Tgε26 mice was used to assess the ability of probiotic lactobacilli and bifidobacteria to enhance colonization resistance to gastrointestinal (GI) tract pathogens. Probiotic bacteria (1×108 colony forming unit (CFU)/mL) successfully excluded Campylobacter jejuni from both strains of mice 7 days after challenge. The probiotic bacteria also reduced the number of Salmonella in the large intestines of both mouse strains. The nylon wool fractionated spleen lymphocyte populations were incubated with Salmonella or C. jejuni antigens. The probiotic treatments did not affect lymphocyte proliferation to C. jejuni antigens, but significantly increased proliferation of lymphocytes to Salmonella antigens by 68 and 55%, respectively, over untreated mice. Caspase 3/7 activation was significantly reduced 33 and 38% in the T and B lymphocyte fractions, respectively, of probiotic‐treated, Salmonella‐challenged HMA BALB/c mice, suggesting that lymphocyte rescue from apoptosis was occurring as a result of probiotic bacteria activity. These results revealed an immunosuppressive activity by Salmonella that was inhibited by the presence of probiotic bacteria. In summary, lactobacilli and bifidobacteria competitively excluded C. jejuni from immunocompetent and immunodeficient mice and antagonized an observable Salmonella‐induced immunosuppression in immunocompetent mice.  相似文献   
1000.
The aim of this study was to evaluate the suitability of Methylene Blue (MB) and Vitamin B12 (Vit-B12) as water soluble inner aqueous phase (W1) markers for measuring the encapsulation efficiency and stability of water-in-oil-in-water (W1/O/W2) double emulsions stabilized by sodium caseinate (NaCN). The encapsulation efficiency and stability were determined by centrifugation of the double emulsion to separate the cream phase (W1/O) and the outer aqueous phase (W2) and measuring the concentration of marker in W2 by absorbance spectrophotometry. To validate this method the marker concentration measurable and the stability of the marker in W2 were measured. Both markers could be accurately measured in W2 and there was no change in the concentration of marker on storage of a W2 solution for 7 days at 45 °C. The recovery yields of MB and Vit-B12 in the recovered W2 of an oil-in-water (O/W2) emulsion, determined using the procedure normally used for measuring encapsulation efficiency and stability, were 78% and 99%, respectively, and 52 and 100%, respectively. Double emulsions had encapsulation efficiency of 61.9 ± 21.4% and 16.6 ± 1.1% and encapsulation stability of 62.0 ± 22.6% and 10.7 ± 0.7% for MB and Vit-B12, respectively. Recovery yield and encapsulation efficiency/stability data for MB indicate that it is not a suitable marker for measuring the encapsulation properties of NaCN stabilized double emulsions while similar data for Vit-B12 indicate that it is a suitable marker for studying the encapsulation properties of double emulsions stabilized with NaCN. Methods used in other studies to measure encapsulation properties of double emulsions are discussed in light of the results obtained in this study.  相似文献   
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