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1.
The objective of the present paper is to develop an analytic theory of cylindrical low-power RF plasma sources operating at an industrial frequency (f=13.56 MHz, ω=8.52×107 s?1). Inductive surface exciters of electromagnetic fields (exciting antennas) are considered that are positioned either at the side surface of the cylinder or at one of its end surfaces. In the latter case, the plasma flows out of the source through the opposite end surface of the cylinder. A study is made of elongated systems in which the length L of the cylinder exceeds its diameter 2R and of planar disk-shaped systems with L<2R. Simple analytic expressions are derived for electromagnetic fields excited by the antenna in the source plasma. The equivalent plasma resistance and the equivalent RF power deposited in the plasma are calculated for systems with prescribed parameters, i.e., in a non-self-consistent model. Up to now, such sources have been investigated mainly through the numerical solution of the complicated general electrodynamic equations. In the Introduction, the problem is formulated in general terms and the geometry of the sources, as well as the characteristic parameters of the source plasma, is discussed. In Section 2, plasma sources operating without an external magnetic field are investigated. In Section 3, helicon plasma sources in a sufficiently strong external magnetic field are considered. Analytic predictions are compared with the results from solving the problem numerically without using the helicon approximation. Section 4 gives a brief discussion of an electron cyclotron resonance-based RF plasma source. In the Conclusion, the main results of the paper are summarized and the technological efficiency of the sources under consideration is estimated at a qualitative level.  相似文献   
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The development of a high-voltage discharge above the water surface is considered. The peculiarity of the observed type of discharge is explained by the process of water evaporation.  相似文献   
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Modeling a sialic acid binding pocket in the external loops of JC virus VP1   总被引:1,自引:0,他引:1  
JC virus (JCV) is a common human polyomavirus that infects over 70% of the population worldwide. JCV has a restricted cell tropism that is caused partly by the initial interaction between the virus and sialic acid-containing host cell receptors. To identify the molecular interactions between the virus and its cellular receptor, we used a combined approach of site-directed mutagenesis and homology-based molecular modeling. A model of the major viral capsid protein VP1 based on sequence alignment with other closely related polyomaviruses allowed us to target specific amino acids in the extracellular loops of VP1 for mutagenesis. An analysis of the growth rates of 17 point mutants led to the identification of VP1 amino acids that are critical in virus-host cell receptor interactions. Molecular dynamics simulations were then used to build and confirm a model of the interaction between VP1 and the sialic acid component of the JCV receptor.  相似文献   
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A mechanism is proposed that can lead to radial ion acceleration in a plasma discharge excited by an electron beam in a relatively weak longitudinal magnetic field. The mechanism operates as follows. The beam generates an azimuthally asymmetric slow potential wave, which traps electrons. Trapped magnetized electrons drift radially with a fairly high velocity under the combined action of the azimuthal wave field (which is constant for them) and a relatively weak external longitudinal magnetic field. The radial electron flux generates a radial charge-separation electric field, which accelerates unmagnetized plasma ions in the radial direction. The ion flux densities and energies achievable in experiments with kiloelectronvolt electron beams in magnetic fields of up to 100 G are estimated.  相似文献   
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Hydrogen sulfide (H(2)S) has recently been identified as a regulator of various physiological events, including vasodilation, angiogenesis, antiapoptotic, and cellular signaling. Endogenously, H(2)S is produced as a metabolite of homocysteine (Hcy) by cystathionine β-synthase (CBS), cystathionine γ-lyase (CSE), and 3-mercaptopyruvate sulfurtransferase (3MST). Although Hcy is recognized as vascular risk factor at an elevated level [hyperhomocysteinemia (HHcy)] and contributes to vascular injury leading to renovascular dysfunction, the exact mechanism is unclear. The goal of the current study was to investigate whether conversion of Hcy to H(2)S improves renovascular function. Ex vivo renal artery culture with CBS, CSE, and 3MST triple gene therapy generated more H(2)S in the presence of Hcy, and these arteries were more responsive to endothelial-dependent vasodilation compared with nontransfected arteries treated with high Hcy. Cross section of triple gene-delivered renal arteries immunostaining suggested increased expression of CD31 and VEGF and diminished expression of the antiangiogenic factor endostatin. In vitro endothelial cell culture demonstrated increased mitophagy during high levels of Hcy and was mitigated by triple gene delivery. Also, dephosphorylated Akt and phosphorylated FoxO3 in HHcy were reversed by H(2)S or triple gene delivery. Upregulated matrix metalloproteinases-13 and downregulated tissue inhibitor of metalloproteinase-1 in HHcy were normalized by overexpression of triple genes. Together, these results suggest that H(2)S plays a key role in renovasculopathy during HHcy and is mediated through Akt/FoxO3 pathways. We conclude that conversion of Hcy to H(2)S by CBS, CSE, or 3MST triple gene therapy improves renovascular function in HHcy.  相似文献   
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Pseudomonas aeruginosa is an important cause of infections, especially in patients with immunodeficiency or diabetes. Antibiotics are effective in preventing morbidity and mortality from Pseudomonas infection, but because of spreading multidrug-resistant bacterial strains, bacteriophages are being explored as an alternative therapy. Two newly purified broad host range Pseudomonas phages, named vB_Pae-Kakheti25 and vB_Pae-TbilisiM32, were characterized as candidates for use in phage therapy. Morphology, host range, growth properties, thermal stability, serology, genomic sequence, and virion composition are reported. When phages are used as bactericides, they are used in mixtures to overcome the development of resistance in the targeted bacterial population. These two phages are representative of diverse siphoviral and podoviral phage families, respectively, and hence have unrelated mechanisms of infection and no cross-antigenicity. Composing bactericidal phage mixtures with members of different phage families may decrease the incidence of developing resistance through a common mechanism.  相似文献   
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Exogenous hydrogen sulfide (H2S) leads to down-regulation of inflammatory responses and provides myocardial protection during acute ischemia/reperfusion injury; however its role during chronic heart failure (CHF) due to myocardial infarction (MI) is yet to be unveiled. We previously reported that H2S inhibits antiangiogenic factors such, as endostatin and angiostatin, but a little is known about its effect on parstatin (a fragment of proteinase-activated receptor-1, PAR-1). We hypothesize that H2S inhibits parstatin formation and promotes VEGF activation, thus promoting angiogenesis and significantly limiting the extent of MI injury. To verify this hypothesis MI was created in 12 week-old male mice by ligation of left anterior descending artery (LAD). Sham surgery was performed except LAD ligation. After the surgery mice were treated with sodium hydrogen sulfide (30 μmol/l NaHS, a donor for H2S, in drinking water) for 4 weeks. The LV tissue was analyzed for VEGF, flk-1 and flt-1, endostatin, angiostatin and parstatin. The expression of VEGF, flk-1 and flt-1 were significantly increased in treated mice while the level of endostatin, angiostatin and parstatin were decreased compared to in untreated mice. The echocardiography in mice treated with H2S showed the improvement of heart function compared to in untreated mice. The X-ray and Doppler blood flow measurements showed enhancement of cardiac-angiogenesis in mice treated with H2S. This observed cytoprotection was associated with an inhibition of anti-angiogenic proteins and stimulation of angiogenic factors. We established that administration of H2S at the time of MI ameliorated infarct size and preserved LV function during development of MI in mice. These results suggest that H2S is cytoprotective and angioprotective during evolution of MI.  相似文献   
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