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11.
Reliable processes by use of vacuum components with specified outgassing rates Contamination of vacuum components cannot be avoided in the manufacturing process. In order to significantly reduce particulate and organic impurities, a multi-stage cleaning process and proof of cleanliness are essential. In order to guarantee a reproducible quality of the cleanliness of vacuum components, uniform standards for defined outgassing rates are necessary. The development of Vacom Purity Classes serves the generally accessible specification of components and characterises their vacuum and cleanroom suitability. Vacom Vacuum Classes guarantee the suitability of vacuum components for use in UHV/XHV. In this article, the importance of cleaning of vacuum chambers and components is examined as well as the need to establish a uniform method for the quantitative measurement of the outgassing rate is highlighted. The systematic division into Vacom Purity and Vacuum Classes provides the basis for a cross-industry standard for the defined quality of vacuum processes. 相似文献
12.
Industry 4.0 – Challenges for constructions of vacuum systems Vacuum systems are finding their way into branches and belonging modern process chains which were hardly in contact with UHV technology in the past. Besides an automatic operation and a flawless processing of parts, vacuum systems and their peripheral devices have to feature options for data output and analysis for subsequent processing in e.g. MES to come up with Industry 4.0 requirements. Subcomponents in vacuum technology partly comply with these requirements in a insufficient way because of their unchanged demands over the last decades. This makes integration into an automatic system more difficult. Despite of that, Industry 4.0 compliant vacuum systems are already producible when there's access to high-level experiences in vacuum and automation technology. This is shown by the examples of residual gas analysis and cleanliness measurement systems and the vacuum bake out oven. A cooperation of vacuum system manufacturers and manufacturers of components is necessary in the future to be able to produce automated vacuum systems in a more efficient way. 相似文献
13.
14.
Matthias Schulz Ute Pippardt Lutz Kiesel Katrin Ritter Ralf Kriegel 《American Institute of Chemical Engineers》2012,58(10):3195-3202
Ba0.5Sr0.5Co0.8Fe0.2O3‐δ tubes, capillaries, capillary modules, and asymmetric membranes were prepared and tested for oxygen permeation in a dead‐end vacuum operation mode at temperatures up to 850°C. The capillary module was built up by reactive air brazing using seven capillaries and a supply tube. Two machined discs were used as an end cap and as a connector plate. The oxygen permeation behaves according to Wagner at small driving forces, but significant negative deviations were observed for asymmetric membranes and single capillaries at higher ones. This is caused by pressure drops at the vacuum side for single capillaries. The highest oxygen flux was revealed for the capillary module with 175.5 mL(STP)/min at a low‐vacuum pressure of 0.042 bar at 850°C, but the asymmetric membrane showing a little bit higher flux at moderate vacuum pressures above 0.07 bar. © 2012 American Institute of Chemical Engineers AIChE J, 58: 3195–3202, 2012 相似文献
15.
The radical polymerization of N‐isopropylacrylamide was carried out in toluene at low temperatures in the presence of silyl alcohols, such as triethylsilanol. Poly(N‐isopropylacrylamide) with a racemo dyad content of 75% was obtained at ? 80 °C with a 4:1 triethylsilanol to monomer ratio loading. NMR analysis suggests that the mechanism for syndiotactic induction, in the presence of silyl alcohols, may be similar to that observed with alkyl alcohols. In this case, a 1:2 complex formation, via hydrogen bonding interactions, leads to the induction of syndiotactic specificity. Copyright © 2012 Society of Chemical Industry 相似文献
16.
Proteases are important targets for the treatment of human disease. Several protease inhibitors have failed in clinical trials due to a lack of in vivo specificity, indicating the need for studies of protease function and inhibition in complex, disease-related models. The tight post-translational regulation of protease activity complicates protease analysis by traditional proteomics methods. Activity-based protein profiling is a powerful technique that can resolve this issue. It uses small-molecule tools-activity-based probes-to label and analyze active enzymes in lysates, cells, and whole animals. Over the last twelve years, a wide variety of protease activity-based probes have been developed. These synthetic efforts have enabled techniques ranging from real-time in vivo imaging of protease activity to high-throughput screening of uncharacterized proteases. This Review introduces the general principles of activity-based protein profiling and describes the recent advancements in probe design and analysis techniques, which have increased the knowledge of protease biology and will aid future protease drug discovery. 相似文献
17.
Dr. Santina Maiorana Prof. Roberta Ettari Dr. Santo Previti Dr. Giorgio Amendola Dr. Annika Wagner Prof. Sandro Cosconati Prof. Ute A. Hellmich Prof. Tanja Schirmeister Prof. Maria Zappalà 《ChemMedChem》2020,15(16):1552-1561
In this paper, we report the design, synthesis and biological investigation of a series of peptidyl vinyl ketones obtained by modifying the P2 fragment of previously reported highly potent inhibitors of rhodesain, the main cysteine protease of Trypanosoma brucei rhodesiense. Investigation of the structure–activity relationship led us to identify new rhodesain inhibitors endowed with an improved selectivity profile (a selectivity index of up to 22 000 towards the target enzyme), and/or an improved antitrypanosomal activity in the sub-micromolar range. 相似文献
18.
Jonas Ort Benedikt Kremer Linda Grüßer Romy Blaumeiser-Debarry Hans Clusmann Mark Coburn Anke Hllig Ute Lindauer 《International journal of molecular sciences》2020,21(23)
Effective pharmacological neuroprotection is one of the most desired aims in modern medicine. We postulated that a combination of two clinically used drugs—nimodipine (L-Type voltage-gated calcium channel blocker) and amiloride (acid-sensing ion channel inhibitor)—might act synergistically in an experimental model of ischaemia, targeting the intracellular rise in calcium as a pathway in neuronal cell death. We used organotypic hippocampal slices of mice pups and a well-established regimen of oxygen-glucose deprivation (OGD) to assess a possible neuroprotective effect. Neither nimodipine (at 10 or 20 µM) alone or in combination with amiloride (at 100 µM) showed any amelioration. Dissolved at 2.0 Vol.% dimethyl-sulfoxide (DMSO), the combination of both components even increased cell damage (p = 0.0001), an effect not observed with amiloride alone. We conclude that neither amiloride nor nimodipine do offer neuroprotection in an in vitro ischaemia model. On a technical note, the use of DMSO should be carefully evaluated in neuroprotective experiments, since it possibly alters cell damage. 相似文献
19.
Robin C. E. Deutscher M. Safa Karagöz Dr. Patrick L. Purder Dr. Jürgen M. Kolos Dr. Christian Meyners Wisely Oki Sugiarto Patryk Krajczy Frederike Tebbe Thomas M. Geiger Dr. Can Ünal Prof. Dr. Ute A. Hellmich Prof. Dr. Michael Steinert Prof. Dr. Felix Hausch 《Chembiochem : a European journal of chemical biology》2023,24(21):e202300442
Legionella pneumophila is the causative agent of Legionnaires’ disease, a serious form of pneumonia. Its macrophage infectivity potentiator (Mip), a member of a highly conserved family of FK506-binding proteins (FKBPs), plays a major role in the proliferation of the gram-negative bacterium in host organisms. In this work, we test our library of >1000 FKBP-focused ligands for inhibition of LpMip. The [4.3.1]-bicyclic sulfonamide turned out as a highly preferred scaffold and provided the most potent LpMip inhibitors known so far. Selected compounds were non-toxic to human cells, displayed antibacterial activity and block bacterial proliferation in cellular infection-assays as well as infectivity in human lung tissue explants. The results confirm [4.3.1]-bicyclic sulfonamides as anti-legionellal agents, although their anti-infective properties cannot be explained by inhibition of LpMip alone. 相似文献
20.
The chain length and geometric isomerism of polyprenols from Eucommia ulmoides Oliver were analyzed using supercritical fluid chromatography. After intensive effort to establish separation conditions
for geometric isomers, a phenyl-bonded silica gel-packed column was found that cleanly separated poly-trans and-cis prenols. The presence of longchain poly-trans prenols (>9 mers) was confirmed for the first time in plants. Trans isomers were found in the leaf, seed coat, and root, but not in the bark and seed. Poly-trans prenols in this plant may act as intermediates for trans-polyisoprene biosynthesis. 相似文献