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71.
F. Vogel 《Clinical genetics》1984,25(5):381-415
Heterozygotes of autosomal-recessive diseases can often be recognized by special heterozygote tests, since enzyme activities are normally reduced in comparison with the normal homozygote state. In Drosophila, the majority of recessive lethal mutations shows a reduction of fitness in heterozygotes, whereas in a strong minority fitness of heterozygotes is increased. This review will be devoted to a consideration of the extent to which heterozygotes for a wide variety of nominally recessive diseases are subject either to an increased liability for common diseases or slight shifts of behavioral characteristics. The available evidence has been collected and will be discussed in three steps: Most studies are available for phenylketonuria. For this group of diseases, a slight reduction of average--especially verbal--I.Q. in heterozygotes has been reported together with signs of a slightly increased cerebral irritability, a possible slight increase of risk for mental disease, and an increase of blood phenylalanine levels in stress situations. The PKU example is used to discuss methodological problems involved in such studies. Other conditions for which relevant deviations in heterozygotes are possible or even likely include among others lipid storage diseases, microcephaly, myoclonus epilepsy, Wilson's disease, galaktokinase deficiency, homocystinuria, recessive myotonia and ataxia- teleangiectasia (increased cancer risk). Since heterozygotes for autosomal recessive diseases are common, it is possible that an appreciable fraction of "multifactorial" genetic liabilities for common, "constitutional" or mental disease might simply be due to heterozygosity for genes whose homozygous affects are already well known. By the same token, much of the "normal" genetic variability influencing cognitive performance (I.Q.)--especially in the lower range--and personality characteristics could also be caused by recessive genes in the heterozygous state.  相似文献   
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Summary The static ocular counterrolling (OCR) of the four scientific crew members in the first Spacelab mission was measured during baseline-data-collection before and after the flight of SL-1. It was presumed that the modification of otolithic responses during spaceflight will be reflected in specific changes of the OCR-gain on the first days after recovery. The magnitude of OCR was determined analysing colour-transparencies of subjects right eyes that were produced in different positions of lateral body tilt. In general, one subject did not show any changes at all; three subjects exhibited a significant decrease of OCR-gain after exposure to weightlessness, whereby differences could be found between the responses for small and large angles of lateral body tilt. Moreover, asymmetrical effects of OCR-gain were found between body tilt to the left and tilt to the right side. Two subjects already demonstrated such an asymmetry before the flight with the higher gain on left-tilt (or right eye up), and three subjects exhibited left-right asymmetries after the spaceflight with the higher gain tilting to the right (or right eye down). A possible correlation between these vestibular asymmetries and space-sickness susceptibility is discussed.  相似文献   
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Goncharov I  Weiner L  Vogel Z 《Neuroscience》2005,134(2):567-574
(-)Delta9-tetrahydrocannabinol is a scavenger of free radicals. However, the activation of the CB1 receptor in cultured C6 glioma cells by (-)delta9-tetrahydrocannabinol in the presence of reagents generating reactive oxygen species leads to amplification of the cellular damage from oxidative stress. This was evident by increased loss of cell wall integrity, impaired mitochondrial function and reduction of glucose uptake. In addition, (-)delta9-tetrahydrocannabinol treatment was also found to be deleterious to the cells under conditions of glucose starvation. Free radicals have been implicated in various conditions leading to cell death and, as a routine, the Fenton reaction is utilized for modeling reactive oxygen species production. Our study was performed using a cell permeating Fe(III) chelating quinone that provides more physiological conditions for mimicking the naturally occurring oxidative stress within the cell and thus serves as a better model for natural reactive oxygen species formation.  相似文献   
76.
Mimotope and anti-idiotypic vaccines to induce an anti-IgE response   总被引:1,自引:0,他引:1  
We have defined epitopes on human IgE by screening different phage display random peptide libraries with a monoclonal anti-IgE antibody termed BSW17. The selected mimotopes and epitopes within the Cepsilon3 and Cepsilon4 region of IgE induced antibodies that were nonanaphylactogenic and had biological activity similar to BSW17. The chemically synthesized and KLH-coupled IgE epitopes or mimotopes were used to induce an anti-IgE response in rhesus monkeys. The immunized rhesus monkeys were subsequently protected in a PCA test when sensitized with human IgE and triggered with the corresponding allergen. Furthermore, using the same monoclonal anti-IgE antibody, we also generated an anti-idiotypic antibody that showed sequence homology with the IgE epitope in the Cepsilon3 domain. This anti-idiotypic antibody as well as the mimotopes were then used in a mouse model to induce orally an anti-IgE immune response. For this purpose mice were fed by intragastric gavages with bacteriophages displaying the small IgE-homologous structures. Orally immunized mice produced serum anti-IgE antibodies that were inhibited by BSW17 suggesting that it may be possible to induce a systemic anti-IgE response orally.  相似文献   
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Poly(epichlorohydrin) and poly(epichlorohydrin-co-ethylene oxide) were modified by reaction with potassium thiocyanate (KSCN), tetrabutylammonium p-toluenesulfinate (NBu4SO2C7H7) and tetrabutylammonium benzenesulfinate (NBu4SO2C6H5). Though the substitution of chlorine in the polymers with these nucleophilic reagents in most cases is accompanied by side reactions, appropriate reaction conditions allow degrees of substitution higher than 90% to be obtained. The glass transition temperature (Tg) of the thiocyanate-modified homo- and copolymer exhibits only a small increase with increasing degree of substitution. While the Tg of the original homo- and copolymer is observed at ?20°C and ?38°C, respectively, the glass transition of the highly substituted homopolymer occurs at ?12°C and for the copolymer at ?31°C. On the other hand, the thiocyanate-modified polymers show a remarkably higher decomposition temperature of about 250°C as compared with that of the unmodified polymers (160–180°C). In addition, the solubility is markedly influenced by the substitution. While the original homo- and copolymers are soluble in, e.g., benzene and toluene, the highly modified products are only soluble in polar solvents such as THF, acetone, DMSO and diglyme. Introducing sulfonyl groups, the resulting polymers exhibit a glass transition temperature increased to a greater extent. For the homopolymer with the highest degree of substitution (98,3%), a Tg of 73°C is observed. Concerning the decomposition temperature, a drastical increase up to 370°C occurs. Finally the influence of phase transfer catalysts on the described reactions was investigated.  相似文献   
80.
This paper describes the development of a murine bank of monoclonal antibodies against Bordetella pertussis toxin, filamentous hemagglutinin (FHA), pili, lipopolysaccharide (LPS), or outer membrane proteins (OMPs). Subunits S1, S2, S3 of pertussis toxin (PT) bound immunoglobulins and glycoproteins such as fetuin and haptoglobin in an unspecific manner. The specificity of monoclonal antibodies towards subunits S1, S2, S3 or S4 of PT could be demonstrated by using purified immunoglobulins or their Fab2 fragments. A set of FHA-specific monoclonal antibodies could be differentiated on the basis of their binding to the various breakdown products present in FHA preparations. Pili-specific monoclonal antibodies reacted with either native pili or denatured pilin, and both demonstrated serotype specificity. Monoclonal antibodies to Bordetella pertussis OMPs were directed to either the virulent phase-regulated trypsin-sensitive, detergent-extractable OMPs 92 kDa, 32 kDa, and 30 kDa or the non-virulent phase-expressed, not-trypsin sensitive OMPs 38 kDa, 33kDa, and 18 kDa.  相似文献   
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