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51.
The knockout mouse project 总被引:1,自引:0,他引:1
Austin CP Battey JF Bradley A Bucan M Capecchi M Collins FS Dove WF Duyk G Dymecki S Eppig JT Grieder FB Heintz N Hicks G Insel TR Joyner A Koller BH Lloyd KC Magnuson T Moore MW Nagy A Pollock JD Roses AD Sands AT Seed B Skarnes WC Snoddy J Soriano P Stewart DJ Stewart F Stillman B Varmus H Varticovski L Verma IM Vogt TF von Melchner H Witkowski J Woychik RP Wurst W Yancopoulos GD Young SG Zambrowicz B 《Nature genetics》2004,36(9):921-924
Mouse knockout technology provides a powerful means of elucidating gene function in vivo, and a publicly available genome-wide collection of mouse knockouts would be significantly enabling for biomedical discovery. To date, published knockouts exist for only about 10% of mouse genes. Furthermore, many of these are limited in utility because they have not been made or phenotyped in standardized ways, and many are not freely available to researchers. It is time to harness new technologies and efficiencies of production to mount a high-throughput international effort to produce and phenotype knockouts for all mouse genes, and place these resources into the public domain. 相似文献
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H. P. von Hahn 《Cellular and molecular life sciences : CMLS》1962,18(11):509-511
Zusammenfassung Die Michaelis-KonstanteKm der katheptischen Aktivität im Schwanzgewebe von Xenopuslarven wird durch das stark regenerationshemmende leucinanaloge Aminoketon E 9 nicht beeinflusst, obwohl nach 5 Tagenin vivo-Behandlung der Larven mit 3 · 10–3
M E 9 ein starker Anstieg der spezifischen Kathepsinaktivität im Schwanzgewebe zu beobachten ist. Das leucinanaloge-Bromallylglycin (BAG) hemmt die Regeneration wenig, erhöht jedoch dieKm deutlich. Es wird postuliert, dass E 9 eine Zunahme der Kathepsine im Schwanzgewebe bewirkt, ohne die kinetischen Eigenschaften dieser Enzyme zu beeinflussen, während BAG an den aktiven Zentren der Kathepsine wirkt und die Affinität zum Substrat herabsetzt.
With the aid of a grant from the Schweizerischer Nationalfonds zur Förderung der wissenschaftlichen Forschung. — Author's present address: Institut für experimentelle Gerontologie, Nonnenweg 7, Basel (Switzerland). 相似文献
With the aid of a grant from the Schweizerischer Nationalfonds zur Förderung der wissenschaftlichen Forschung. — Author's present address: Institut für experimentelle Gerontologie, Nonnenweg 7, Basel (Switzerland). 相似文献
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Boyartchuk VL Broman KW Mosher RE D'Orazio SE Starnbach MN Dietrich WF 《Nature genetics》2001,27(3):259-260
We have used a novel quantitative trait locus model to study the genetics of survival of F2 progeny of susceptible BALB/cByJ and resistant C57BL/6ByJ mice that have been infected with Listeria monocytogenes. This allowed us to map modifiers of L. monocytogenes susceptibility to chromosomes 5 and 13. 相似文献
57.
'Inverse' melting of a vortex lattice 总被引:1,自引:0,他引:1
Avraham N Khaykovich B Myasoedov Y Rappaport M Shtrikman H Feldman DE Tamegai T Kes PH Li M Konczykowski M van der Beek K Zeldov E 《Nature》2001,411(6836):451-454
Inverse melting is the process in which a crystal reversibly transforms into a liquid or amorphous phase when its temperature is decreased. Such a process is considered to be very rare, and the search for it is often hampered by the formation of non-equilibrium states or intermediate phases. Here we report the discovery of first-order inverse melting of the lattice formed by magnetic flux lines in a high-temperature superconductor. At low temperatures, disorder in the material pins the vortices, preventing the observation of their equilibrium properties and therefore the determination of whether a phase transition occurs. But by using a technique to 'dither' the vortices, we were able to equilibrate the lattice, which enabled us to obtain direct thermodynamic evidence of inverse melting of the ordered lattice into a disordered vortex phase as the temperature is decreased. The ordered lattice has larger entropy than the low-temperature disordered phase. The mechanism of the first-order phase transition changes gradually from thermally induced melting at high temperatures to a disorder-induced transition at low temperatures. 相似文献
58.
van der Marel D Molegraaf HJ Zaanen J Nussinov Z Carbone F Damascelli A Eisaki H Greven M Kes PH Li M 《Nature》2003,425(6955):271-274
Quantum criticality is associated with a system composed of a nearly infinite number of interacting quantum degrees of freedom at zero temperature, and it implies that the system looks on average the same regardless of the time- and length scale on which it is observed. Electrons on the atomic scale do not exhibit such symmetry, which can only be generated as a collective phenomenon through the interactions between a large number of electrons. In materials with strong electron correlations a quantum phase transition at zero temperature can occur, and a quantum critical state has been predicted, which manifests itself through universal power-law behaviours of the response functions. Candidates have been found both in heavy-fermion systems and in the high-transition temperature (high-T(c)) copper oxide superconductors, but the reality and the physical nature of such a phase transition are still debated. Here we report a universal behaviour that is characteristic of the quantum critical region. We demonstrate that the experimentally measured phase angle agrees precisely with the exponent of the optical conductivity. This points towards a quantum phase transition of an unconventional kind in the high-T(c) superconductors. 相似文献
59.
Rawat UB Zavialov AV Sengupta J Valle M Grassucci RA Linde J Vestergaard B Ehrenberg M Frank J 《Nature》2003,421(6918):87-90
Protein synthesis takes place on the ribosome, where genetic information carried by messenger RNA is translated into a sequence of amino acids. This process is terminated when a stop codon moves into the ribosomal decoding centre (DC) and is recognized by a class-1 release factor (RF). RFs have a conserved GGQ amino-acid motif, which is crucial for peptide release and is believed to interact directly with the peptidyl-transferase centre (PTC) of the 50S ribosomal subunit. Another conserved motif of RFs (SPF in RF2) has been proposed to interact directly with stop codons in the DC of the 30S subunit. The distance between the DC and PTC is approximately 73 A. However, in the X-ray structure of RF2, SPF and GGQ are only 23 A apart, indicating that they cannot be at DC and PTC simultaneously. Here we show that RF2 is in an open conformation when bound to the ribosome, allowing GGQ to reach the PTC while still allowing SPF-stop-codon interaction. The results indicate new interpretations of accuracy in termination, and have implications for how the presence of a stop codon in the DC is signalled to PTC. 相似文献
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