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41.
42.
Roger L. Snowden 《Tetrahedron letters》1984,25(35):3835-3836
An efficient synthesis of dienediester 3, a key intermediate for drimane-related sesquiterpenes, is described starting from enal 4. 相似文献
43.
A synthesis of 1,2-cis-configurated, non-isosteric phosphonate analogues of aldose-1-phosphates is described. Treatment of 1-O-acyl-glycoses 1 , 7 , 13 , and 19 with trialkyl phosphite in the presence of trimethylsilyl trifluoromethanesulfonate gave the 1,2-cis-configurated glycosylphosphonates 2 , 4 , 8 , 10 , 14 , 16 , 20 , and 22 as the major anomers and the 1,2-trans-configurated glycosylphosphonates 3 , 5 , 9 , 11 , 15 , 17 , 21 , and 23 as the minor anomers. The 1,2-cis-configurated phosphonates 4 , 10 , 16 , and 22 were deprotected to give the (β-D -glucopyranosyl)phosphonate 6 , the (β-D -mannopyranosyl)phosphonate 12 , the (β-D -ribofuranosyl)phosphonate 18 , and the (β-D -arabinofuranosyl)phosphonate 24 , respectively, in high yields. The preferred formation of 1,2-cis-configurated phosphonates is explained by postulating an equilibrium between the anomeric phosphonium-salt intermediates (such as 25 and 26 ) and a stabilization of the cis-configurated salts through formation of a pentacoordinated species (such as 28 ). 相似文献
44.
Roger M. Smith 《Chromatographia》1982,16(1):155-157
Summary The pungent principles of ginger and grains of paradise are examined using a reversed-phase HPLC column. An electrochemical detector is used to selectively detect the phenolic gingerols and shogaols. The retention indices of the compounds are compared using methanowater and acetonitrile-water as eluents.Presented at the 14th International Symposium on Chromatography London, September, 1982 相似文献
45.
Chemical fourling on the unit-cell level is introduced as a structure-building operation in the solid state. A chemical fourling structure is achieved when two twin planes are perpendicular to each other. Each fourling unit has infinite extension in only one direction and can be related to a well-known structure type or packing of atoms. The structures of the tetragonal tungsten bronzes MxWO3 and Pd(NH3)4Cl · H2O are presented as examples of chemical fourlings of cubic close packing. The structures of SeO2, Mn2Hg5, and Zr2F7O are shown to be a sequence of chemical fourlings of primitive cubic packing. Chemical fourling units of hexagonal close packing are found in the structures of tetragonal Ti3Sb, α-V3S and Sb6O7(SO4)2. The structures of CuAl2, SeTl, NbTe4, Ti3Sb, and MnU6 all have the same chemical fourling unit. Cr23C6 is described as a bounded chemical fourling of cubic close packing. 相似文献
46.
Christian Bellec Daniel Bertin Roger Colau StPhane Deswarte Pierre Maitte Claude Viel 《Journal of heterocyclic chemistry》1979,16(8):1611-1616
Z α-Cyano-β-nitrostyrenes were prepared by nitration with dinitrogentetroxide of the corresponding α-cyanostyrenes. Elsomers were obtained by photoirradiation of Z isomers. The electrochemical reduction of these cyanonitro compounds generates the α-cyanooximes which lead, according to the experimental conditions(ring closure or hydrolysis), either to 5-aminoisoxazoles or to β-ketonitriles. 相似文献
47.
Douglas X. West Robert D. Profilet John C. Severns Roger K. Bunting 《Transition Metal Chemistry》1988,13(1):29-34
Summary A series of cobalt(II), nickel(II) and copper(II) complexes of 2-picolinamineN-oxide, HA, has been prepared. Solids of formula [M(HA)3](BF4)2 (M=cobalt(II) or nickel(II); [Cu(HA)2]X2 (X=BF
4
–
, NO
3
–
); [Co(HA)2X2] (X=Cl– or Br–); [Ni(HA)2Cl2] and [Cu(HA)X2] (X=Cl– or Br–] have been isolated and characterized by partial elemental analyses, molar conductivities, magnetic susceptibilities, DSC-TGA, and spectral methods. All complexes were found to be monomeric, and their spectral parameters are compared with those of the metal ion complexes ofN-alkyl-2-picolinamineN-oxides, 2-dialkylaminopyridineN-oxides and 2-picolinamine. The cobalt(II) and nickel(II) halide complexes spectrally show a mixture of octahedral and tetrahedral centres. 相似文献
48.
In vitro high throughput screening of compounds for favorable metabolic properties in drug discovery
Masimirembwa CM Thompson R Andersson TB 《Combinatorial chemistry & high throughput screening》2001,4(3):245-263
Drug metabolism can have profound effects on the pharmacological and toxicological profile of therapeutic agents. In the pharmaceutical industry, many in vitro techniques are in place or under development to screen and optimize compounds for favorable metabolic properties in the drug discovery phase. These in vitro technologies are meant to address important issues such as: (1) is the compound a potent inhibitor of drug metabolising enzymes (DMEs)? (2) does the compound induce the expression of DMEs? (3) how labile is the compound to metabolic degradation? (4) which specific enzyme(s) is responsible for the compound's biotransformation? and (5) to which metabolites is the compound metabolized? Answers to these questions provide a basis for judging whether a compound is likely to have acceptable pharmacokinetic properties in vivo. To address these issues on the increasing number of compounds inundating the drug discovery programs, high throughput assays are essential. A combination of biochemical advances in the understanding of the function and regulation of DMEs (in particular, cytochromes P450, CYPs) and automated analytical technologies are revolutionizing drug metabolism research. Automated LC-MS based metabolic stability, fluorescence, radiometric and LC-MS based CYP inhibition assays are now in routine use. Automatible models for studying CYP induction based on enzyme activity, quantitative RT-PCR and reporter gene systems are being developed. We will review the utility and limitations of these HTS approaches and highlight on-going developments and emerging technologies to answer metabolism questions at the different stages of the drug discovery process. 相似文献
49.
(±)-α and β-Himachalene, 5 and 6 , have been synthesized in a convergent manner from 3,3-dimethylacrolein ( 9 ), the ester enolate 10 and the silyloxypentadienyllithium 7 . The key steps are the regioselective γ-addition of the dienal 13 to 7 and the intramolecular Diels-Alder addition 15 → 16 . Hydrogenolysis of the diethylphosphate group and functionalization at C (5) completed the synthesis of 5 and 6 . 相似文献
50.
Roger N. F. Thorneley 《Journal of organometallic chemistry》1974,70(3):C37-C39
The kinetic isotope effect for β-hydride elimination from alkyliridium(I) complexes has bee found to be kH/kD = 2.28 ± 0.20. 相似文献