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71.
Foxl2 gene and the development of the ovary: a story about goat, mouse, fish and woman 总被引:2,自引:0,他引:2
Baron D Batista F Chaffaux S Cocquet J Cotinot C Cribiu E De Baere E De Baeree E Guiguen Y Jaubert F Pailhoux E Pannetier M Vaiman D Vigier B Veitia R Fellous M 《Reproduction, nutrition, development》2005,45(3):377-382
In this review, we describe recent results concerning the genetics of sex determination in mammals. Particularly, we developed the study of the FOXL2 gene and its implication in genetic anomalies in goats (PIS mutation) and humans (BPES). We present the expression of FOXL2 in the ovaries of different species. 相似文献
72.
Bernice Wright Trevor Gibson Jeremy Spencer Julie A. Lovegrove Jonathan M. Gibbins 《PloS one》2010,5(3)
Background
Flavonoid metabolites remain in blood for periods of time potentially long enough to allow interactions with cellular components of this tissue. It is well-established that flavonoids are metabolised within the intestine and liver into methylated, sulphated and glucuronidated counterparts, which inhibit platelet function.Methodology/Principal Findings
We demonstrate evidence suggesting platelets which contain metabolic enzymes, as an alternative location for flavonoid metabolism. Quercetin and a plasma metabolite of this compound, 4′-O-methyl quercetin (tamarixetin) were shown to gain access to the cytosolic compartment of platelets, using confocal microscopy. High performance liquid chromatography (HPLC) and mass spectrometry (MS) showed that quercetin was transformed into a compound with a mass identical to tamarixetin, suggesting that the flavonoid was methylated by catechol-O-methyl transferase (COMT) within platelets.Conclusions/Significance
Platelets potentially mediate a third phase of flavonoid metabolism, which may impact on the regulation of the function of these cells by metabolites of these dietary compounds. 相似文献73.
Kyle J. Nakamura Johannes S. Gach Laura Jones Katherine Semrau Jan Walter Frederic Bibollet-Ruche Julie M. Decker Laura Heath William D. Decker Moses Sinkala Chipepo Kankasa Donald Thea James Mullins Louise Kuhn Michael B. Zwick Grace M. Aldrovandi 《PloS one》2010,5(3)
Human antibody 4E10 targets the highly conserved membrane-proximal external region (MPER) of the HIV-1 transmembrane glycoprotein, gp41, and has extraordinarily broad neutralizing activity. It is considered by many to be a prototype for vaccine development. In this study, we describe four subjects infected with viruses carrying rare MPER polymorphisms associated with resistance to 4E10 neutralization. In one case resistant virus carrying a W680G substitution was transmitted from mother to infant. We used site-directed mutagenesis to demonstrate that the W680G substitution is necessary for conferring the 4E10-resistant phenotype, but that it is not sufficient to transfer the phenotype to a 4E10-sensitive Env. Our third subject carried Envs with a W680R substitution causing variable resistance to 4E10, indicating that residues outside the MPER are required to confer the phenotype. A fourth subject possessed a F673L substitution previously associated with 4E10 resistance. For all three subjects with W680 polymorphisms, we observed additional residues in the MPER that co-varied with position 680 and preserved charged distributions across this region. Our data provide important caveats for vaccine development targeting the MPER. Naturally occurring Env variants described in our study also represent unique tools for probing the structure-function of HIV-1 envelope. 相似文献
74.
Liu WM Li R Sun JZ Wang J Tsai J Wen W Kohlmann A Williams PM 《Journal of theoretical biology》2006,243(2):273-278
An ideal expression algorithm should be able to tell truly different expression levels with small false positive errors and be robust to assay changes. We propose two algorithms. PQN is the non-central trimmed mean of perfect match intensities with quantile normalization. DQN is the non-central trimmed mean of differences between perfect match and mismatch intensities with quantile normalization. The quantiles for normalization can be either empirical or theoretical. When array types and/or assay change in a study, the normalization to common quantiles at the probe set level is essential. We compared DQN, PQN, RMA, GCRMA, DCHIP, PLIER and MAS5 for the Affymetrix Latin square data and our data of two sets of experiments using the same bone marrow but different types of microarrays and different assay. We found the computation for AUC of ROC at affycomp.biostat.jhsph.edu can be improved. 相似文献
75.
Dana M. Blumenthal Julie A. Kray William Ortmans Lewis H. Ziska Elise Pendall 《Global Change Biology》2016,22(9):3026-3038
Elevated CO2 and warming may alter terrestrial ecosystems by promoting invasive plants with strong community and ecosystem impacts. Invasive plant responses to elevated CO2 and warming are difficult to predict, however, because of the many mechanisms involved, including modification of phenology, physiology, and cycling of nitrogen and water. Understanding the relative and interactive importance of these processes requires multifactor experiments under realistic field conditions. Here, we test how free‐air CO2 enrichment (to 600 ppmv) and infrared warming (+1.5 °C day/3 °C night) influence a functionally and phenologically distinct invasive plant in semi‐arid mixed‐grass prairie. Bromus tectorum (cheatgrass), a fast‐growing Eurasian winter annual grass, increases fire frequency and reduces biological diversity across millions of hectares in western North America. Across 2 years, we found that warming more than tripled B. tectorum biomass and seed production, due to a combination of increased recruitment and increased growth. These results were observed with and without competition from native species, under wet and dry conditions (corresponding with tenfold differences in B. tectorum biomass), and despite the fact that warming reduced soil water. In contrast, elevated CO2 had little effect on B. tectorum invasion or soil water, while reducing soil and plant nitrogen (N). We conclude that (1) warming may expand B. tectorum's phenological niche, allowing it to more successfully colonize the extensive, invasion‐resistant northern mixed‐grass prairie, and (2) in ecosystems where elevated CO2 decreases N availability, CO2 may have limited effects on B. tectorum and other nitrophilic invasive species. 相似文献
76.
An obligate intermediate along the slow folding pathway of a group II intron ribozyme 总被引:4,自引:1,他引:4
Most RNA molecules collapse rapidly and reach the native state through a pathway that contains numerous traps and unproductive intermediates. The D135 group II intron ribozyme is unusual in that it can fold slowly and directly to the native state, despite its large size and structural complexity. Here we use hydroxyl radical footprinting and native gel analysis to monitor the timescale of tertiary structure collapse and to detect the presence of obligate intermediates along the folding pathway of D135. We find that structural collapse and native folding of Domain 1 precede assembly of the entire ribozyme, indicating that D1 contains an on-pathway intermediate to folding of the D135 ribozyme. Subsequent docking of Domains 3 and 5, for which D1 provides a preorganized scaffold, appears to be very fast and independent of one another. In contrast to other RNAs, the D135 ribozyme undergoes slow tertiary collapse to a compacted state, with a rate constant that is also limited by the formation D1. These findings provide a new paradigm for RNA folding and they underscore the diversity of RNA biophysical behaviors. 相似文献
77.
78.
Julie A. Woods John A. Hadfield Alan T. McGown Brian W. Fox 《Bioorganic & medicinal chemistry》1993,1(5)
Bis(2-bromo-4,5-dimethoxyphenyl)sulfide (5) and bis(2-bromo-4,5-dimethoxyphenyl) selenide (7) have been shown to block cells in the G2/M phase of the cell cycle, whereas the debromo (4, 6) equivalents do not. The dibromoselenide (7) is cytotoxic to tumour cells in vitro and has been shown to increase the mitotic index of treated cells. These biological effects are consistent with disruption of the mitotic apparatus. This agent does not inhibit microtubule assembly in vitro, but does bind to tubulin. Molecular modelling of these structures indicates that their spatial and electronic structures may make an important contribution to the biological activity. 相似文献
79.
Jacklyn N. Hellwege Nicholette D. Palmer W. Mark Brown Julie T. Ziegler S. Sandy An Xiuqing Guo Y.-D. Ida Chen Kent Taylor Gregory A. Hawkins Maggie C. Y. Ng Elizabeth K. Speliotes Carlos Lorenzo Jill M. Norris Jerome I. Rotter Lynne E. Wagenknecht Carl D. Langefeld Donald W. Bowden 《Human genetics》2015,134(2):215-215
80.
Joanne Blanchfield Julie Dutton Ron Hogg David Craik David Adams Richard Lewis Paul Alewood Istvan Toth 《Letters in Peptide Science》2001,8(3-5):235-239
The -conotoxin MII is a 16 amino acid long peptide toxinisolated from the marine snail, Conus magus. This toxinhas been found to be a highly selective and potent inhibitorof neuronal nicotinic acetylcholine receptors of the subtype32. To improve the bioavailability of this peptide, we havecoupled to the N-terminus of conotoxin MII, 2-amino-D,L-dodecanoic acid (Laa) creating a lipidic linear peptide whichwas then successfully oxidised to produce the correctly foldedconotoxin MII construct. 相似文献