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Theoretical studies point to significant improvements in the performance of semiconductor laser amplifiers by injecting carriers with pulsed electric currents of sub-nanosecond duration. A pulsed Fabry-Perot amplifier (FPA) is most sensitive to input lightwave at the instant the carrier density is crossing the critical region, and gives a sharply pulsed sampling effect on the input lightwave signal. Compared with a FPA operating at subcritical electron density, the pulsed amplifier gives much higher gain, peak power, and bandwidth. In fact, pulsed operation of a FPA is also expected to give significantly higher gain and about the same peak output power as a traveling wave amplifier. Pulsed operation also improves the performance of a traveling wave amplifier by attenuating its internally reflected waves 相似文献
995.
A. Witvrouw K. Maex W. De Ceuninck G. Lekens J. D'Haen L. De Schepper 《Microelectronics Reliability》1998,38(6-8)
The degradation due to stress induced voiding of nitride passivated Al-1 wt.% Si and Ti/TN/ Al-1wt.% Si-0.5 wt. % Cu/Ti/TN interconnects with widths ranging between 0.4 and 1.2 μm was studied by in-situ conventional
high resolution resistance measurements (HRRM) during storage at temperatures between 168 and 240°C. The conventional measurements on Al-Si lines, which lasted more than one year, clearly showed that the interconnect lifetime decreases with decreasing line width. With HRRM the degradation due to stress induced voiding can be detected much sooner and with much more detail. From the HRRM it is clear that the resistance changes during storage often happen in jumps and that the degradation has a rather complex alloy, line width and temperature dependence. Both for 0.4 and 0.6 μm wide Al---Si lines more degradation occurred for storage at 175 °C compared to storage at 200 °C. For the Al---Si---Cu stacks the degradation of 0.4 μm wide lines was worse for storage at 240°C compared to storage at 200 °C, but the opposite was true for the 0.6 μm wide lines. 相似文献
996.
Bouchard Thomas J.; Arvey Richard D.; Keller Lauren M.; Segal Nancy L. 《Canadian Metallurgical Quarterly》1992,77(1):89
Responds to the points made by R. Cropanzano and K. James (see record 1991-00462-001) concerning the article by R. D. Arvey et al (1989). The authors acknowledge that the Arvey et al study is based on a single design, makes use of a small and special sample, and, as such, is vulnerable to threats of internal and external validity. Nevertheless, after providing a more comprehensive conceptual and empirical context for the study, and after reviewing a number of the issues raised by Cropanzano and James, the authors conclude that it is not premature to accept the idea that work attitudes are partially genetically influenced. Indeed, the authors use behavioral genetic theory, together with data gathered in the Arvey et al study, to make specific point predictions regarding the outcomes of an array of studies that easily can be undertaken. Finally, the authors acknowledge that the comments and issues raised by Cropanzano and James, along with the interchange, can offer directions for future research in this important area. (PsycINFO Database Record (c) 2010 APA, all rights reserved) 相似文献
997.
The method of layer-by-layer physicochemical analysis is used to study phase transformations in chromium-nickel steels of martensitic class after high-cycle fatigue tests and after thermal exposure at similar temperature and time conditions. The Laves phase is shown to be distributed nonuniformly over the cross section of specimens tested for fatigue resistance. The results of the tests are used to correct phase compositions. 相似文献
998.
KE Ensrud DM Black L Palermo DC Bauer E Barrett-Connor SA Quandt DE Thompson DB Karpf 《Canadian Metallurgical Quarterly》1997,157(22):2617-2624
BACKGROUND: The efficacy of antiresorptive therapy in preventing fractures in women at highest fracture risk, such as very elderly women or those with severe osteoporosis, is uncertain. PARTICIPANTS AND METHODS: Using data from a double-blind, randomized, placebo-controlled clinical trial that enrolled 2027 postmenopausal women aged 55 to 81 years with low femoral neck bone mineral density (BMD) and existing vertebral fractures, we examined the consistency of the effect of treatment with alendronate sodium in preventing fractures within a priori-specified risk subgroups defined at baseline by age, bone density, number of preexisting vertebral fractures, and history of postmenopausal fracture. The women were randomized to oral administration of alendronate or placebo and followed up for an average of 2.9 years. The initial dose of alendronate sodium was 5 mg/d; the dosage was increased from 5 to 10 mg/d at 24 months. New vertebral fractures, the primary end point of this arm of the trial, were defined by morphometry as a decrease of 20% and at least 4 mm in any vertebral height between baseline and a follow-up radiograph at 36 months. Incident clinical fractures, the secondary end point, included nonspine and clinical (symptomatic) vertebral fractures. All clinical fractures were confirmed with x-ray film reports or, in the case of clinical vertebral fractures, x-ray films. RESULTS: Overall, there was a 47% significant reduction in risk of new vertebral fractures in the alendronate group compared with the placebo group. The reduction in risk of new vertebral fracture was consistent across fracture risk categories including age (relative risk [RR], 0.49 in women < 75 years compared with 0.62 in those > or = 75 years), BMD (RR, 0.54 in women with a femoral neck BMD < 0.59 g/cm2 [median] compared with 0.53 in those with a BMD > or = 0.59 g/cm2), and number of preexisting vertebral fractures (RR, 0.58 in women with 1 vertebral fracture compared with 0.52 in those with > or = 2). The overall significant 28% reduction in risk of incident clinical fractures in the alendronate group compared with the placebo group was also observed within these subgroups. Compared with the number of lower-risk women, a similar or smaller number of high-risk women needed to be treated to prevent 1 fracture. For example, 8 women aged 75 years or older compared with 9 women younger than 75 years, or 4 women with 2 or more existing vertebral fractures compared with 16 women with 1 existing vertebral fracture, needed to be treated with alendronate for 5 years to prevent 1 new vertebral fracture. CONCLUSIONS: Alendronate effectively reduces fracture risk in postmenopausal women with vertebral fractures and low BMD, including those women at highest risk because of advanced age or severe osteoporosis. Since the risk reductions observed with alendronate treatment were consistent within fracture risk categories, more fractures were prevented by treating women at highest risk. 相似文献
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