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311.
IMMUNOGLOBULIN polypeptide chains consist of two well defined regions designated the “variable region” and the “constant region”. Whereas great diversity exists in amino-acid sequences of variable regions, the constant regions of a given subclass of heavy chains (CH)* are essentially invariant in sequence1, 2. Exceptions are the allelic forms, such as the rabbit allotypes A14 and A153, 4, where a threonine-alanine interchange occurs in the constant region of γ chains (Appella, Chersi, R. G. M. and Dubiski, in preparation). The markers unique to a chains (for example, A14-A15) are closely linked to allotypic markers at the a locus (a1, a2, a3)3, 4 which seem to be present on four different Ig heavy chain classes (α, γ, ε, µ)5–7. These puzzling observations can be explained if the a locus determinants are variable region markers which reflect genetically controlled differences in some relatively constant residues within the VH region sequences7. 相似文献
312.
Insulin like growth factor-1 (IGF-1) plays an important role in the proliferation and differentiation of neural progenitor
cells. The effects of IGF-1 can be regulated by insulin like growth factor binding protein-3 (IGFBP-3) which can either inhibit
or stimulate the proliferation of cells depending on the expression of proteases that can release IGF-1 from IGF1-IGFBP3 complex.
Although IGF-1 is essential for the development of brain, both IGFBP-3 and IGF-1 are elevated in the brains of children younger
than 6 months of age. Likewise, IGFBP-3 is also upregulated following cerebral ischemia and hypoxia. However, the role of
IGFBP-3 in neurogenesis is not clear. Using an in vitro culture system of rat neural progenitor cells, we demonstrate that
IGFBP-3 specifically regulates the IGF-1 mediated neural progenitor cell proliferation via down regulation of phopho-Akt,
and cyclin D1. In addition, IGFBP-3 also decreased the content of nestin in the neural progenitor cells indicating its potential
role in neurogenesis. 相似文献
313.
314.
Jessica L. Gaines Kathleen E. Finn Julia P. Slopsema Lane A. Heyboer Katharine H. Polasek 《Journal of computational neuroscience》2018,45(1):29-43
Surface electrical stimulation has the potential to be a powerful and non-invasive treatment for a variety of medical conditions but currently it is difficult to obtain consistent evoked responses. A viable clinical system must be able to adapt to variations in individuals to produce repeatable results. To more fully study the effect of these variations without performing exhaustive testing on human subjects, a system of computer models was created to predict motor and sensory axon activation in the median nerve due to surface electrical stimulation at the elbow. An anatomically-based finite element model of the arm was built to accurately predict voltages resulting from surface electrical stimulation. In addition, two axon models were developed based on previously published models to incorporate physiological differences between sensory and motor axons. This resulted in axon models that could reproduce experimental results for conduction velocity, strength-duration curves and activation threshold. Differences in experimentally obtained action potential shape between the motor and sensory axons were reflected in the models. The models predicted a lower threshold for sensory axons than motor axons of the same diameter, allowing a range of sensory axons to be activated before any motor axons. This system of models will be a useful tool for development of surface electrical stimulation as a method to target specific neural functions. 相似文献
315.
316.
Melissa B. Rooney Michael J. Honeychurch Fabiola M. Selvaraj Robert E. Blankenship Alan M. Bond Hans C. Freeman 《Journal of biological inorganic chemistry》2003,8(3):306-317
The reversible formal potentials of auracyanin A and auracyanin B, two closely related "blue" copper proteins from the photosynthetic bacterium Chloroflexus aurantiacus, have been determined by protein film voltammetry in the range 4相似文献
317.
Marie GB Hansen Mette Christoffersen Line R Thuesen Morten R Petersen Anders M Bojesen 《Acta veterinaria Scandinavica》2010,52(1):3
Background
Borrelia burgdorferi sensu lato and Anaplasma phagocytophilum are able to infect horses. However, the extend to which Danish horses are infected and seroconvert due to these two bacteria is unknown. The aim of the present study was to evaluate the seroprevalence of B. burgdorferi sensu lato and A. phagocytophilum in Danish horses.Methods
A total of 390 blood samples collected from all major regions of Denmark and with a geographical distribution corresponding to the density of the Danish horse population were analyzed. All samples were examined for the presence of antibodies against B. burgdorferi sensu lato and A. phagocytophilum by the use of the SNAP®4DX ® ELISA test.Results
Overall, 29.0% of the horses were seropositive for B. burgdorferi sensu lato whereas 22.3% were seropositive for A. phagocytophilum.Conclusions
Antibodies against B burgdorferi sensu lato and A. phagocytophilum are commonly found among Danish horses thus showing that Danish horses are frequently infected by these organisms.318.
Real-time Investigation of SV40 Large T-antigen Helicase Activity Using Surface Plasmon Resonance 总被引:1,自引:0,他引:1
Jason Plyler Karl Jasheway Bodin Tuesuwan Jessica Karr Jarryd S. Brennan Sean M. Kerwin Wendi M. David 《Cell biochemistry and biophysics》2009,53(1):43-52
The simian virus 40 (SV40) genome is a model system frequently employed for investigating eukaryotic replication. Large T-antigen
(T-ag) is a viral protein responsible for unwinding the SV40 genome and recruiting necessary host factors prior to replication.
In addition to duplex unwinding T-ag possesses G-quadruplex DNA helicase activity, the physiological consequence of which
is unclear. However, formation of G-quadruplex DNA structures may be involved in genome maintenance and function, and helicase
activity to resolve these structures may be necessary for efficient replication. We report the first real-time investigation
of SV40 T-ag helicase activity using surface plasmon resonance (SPR). In the presence of ATP, T-ag was observed to bind to
immobilized single-stranded DNA, forked duplex DNA, and the human telomeric foldover quadruplex DNA sequence. Inhibition of
T-ag duplex helicase activity was observable in real-time and the intramolecular quadruplex was unwound.
相似文献
Wendi M. DavidEmail: |
319.
Gunnar W. Schade Sheena J. Solomon Ebba Dellwik Kim Pilegaard Annette Ladstätter-Weissenmayer 《Biogeochemistry》2011,106(3):337-355
In-canopy mixing ratio gradients and above-canopy fluxes of several volatile organic compounds (VOCs) were measured using
a commercial proton transfer reaction mass spectrometer (PTR-MS) in a European beech (Fagus sylvatica) forest in Denmark. Fluxes of methanol were bidirectional: Emission occurred during both day and night with highest fluxes
(0.2 mg C m−2 h−1) during a warm period; deposition occurred dominantly at daytime. Confirming previous branch-level measurements on beech,
the forest’s monoterpene emissions (0–0.5 mg C m−2 h−1), and in-canopy mixing ratios showed a diurnal cycle consistent with light-dependent emissions; a result contrasting temperature-only
driven emissions of most conifer species. Also emitted was acetone, but only at ambient temperatures exceeding 20°C. Slow
deposition dominated at lower temperatures. Our in-canopy gradient measurements contrast with earlier results from tropical
and pine forest ecosystems in that they did not show this beech ecosystem to be a strong sink for oxygenated VOCs (OVOCs).
Instead, their gradients were flat and only small deposition velocities (<0.2 cm s−1) were observed to the onsite soil. However, as methanol soil uptake was consistent and possibly related to soil moisture,
more measurements are needed to evaluate its soil sink strength. In turn, as canopy scale fluxes are net fluxes with stomatal
emissions from photosynthesizing leaves potentially affecting non-stomatal oxygenated VOC uptake, only independent, controlled
laboratory experiments may be successful in separating gross fluxes. 相似文献
320.
Julio A. Camarero Youngeun Kwon 《International journal of peptide research and therapeutics》2008,14(4):351-357
Many experimental approaches in biology and biophysics, as well as applications in diagnosis and drug discovery, require proteins
to be immobilized on solid supports. Protein microarrays, for example, provide a high-throughput format to study biomolecular
interactions. The technique employed for protein immobilization is a key to the success of these applications. Recent biochemical
developments are allowing, for the first time, the selective and traceless immobilization of proteins generated by cell-free
systems without the need for purification and/or reconcentration prior to the immobilization step. 相似文献