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61.
Henri Cappetta 《Geobios》1981,14(5):563-575
Recent researches in the phosphat-bearing basins ofMorocco have allowed to collect new selachian forms. In this paper, three Ypresian genera from Ouled Abdoun basin, new for Morocco, are described: Heptranchias howellii (Reed, 1946), Alopias denticulatus nov. sp. and Odontorhytis pappenheimiBöhm, 1926. The re-discovery of the genus Odontorhytis allows to state precisely its morphological dental features and to affirm that it is well a selachian and not a teleostean, as it was thought. The stratigraphic distribution of some species is stated precisely.  相似文献   
62.
Thirty-two species of Cladocera and 27 species of free-living copepods were identified in a series of samples collected in 25 localities in and around the Fouta Djalon mountains, West Africa. Beside great richness in numbers of species, the nature of the fauna is noteworthy: at least 20% of the Cladocera and 50% of the copepods are endemic to West Africa. Possible palaeoclimatological reasons for this are discussed. The cladoceran genus Streblocerus is recorded from Africa for the first time. It is an element of northern origin in the fauna of West Africa. More examples of this kind are documented among the Copepoda Cyclopoida and Harpacticoida, but the bulk of the fauna is evidently of tropical origin. In particular, great adaptive radiation is occurring in the local representatives of the genus Tropocyclops. Three new species of Parastenocaris are described; they are the first representatives of this genus found in West Africa.  相似文献   
63.
In the immature rat uterus, high concentrations of androgens competed specifically with estradiol on the estrogen receptor (RE). This competition was stereospecific for C19 steroids bearing a 17β and/or 3 hydroxyl group. Very low affinity ligands, such as testosterone, could not compete with estradiol at equilibrium but decreased the association rate of estradiol on its receptor. High doses (> 0.4mg) of 5 α aihydrotestosterone provoked in vivo as in vitro the nuclear translocation of RE. The nuclear receptor thus formed displayed the same 5.2 S sedimentation constant as that induced by estradiol. We conclude that the weak affinity binding of androgens to the estrogen receptor is sufficient to induce its nuclear translocation in vivo provided androgen concentration is high enough in uterus to occupy the estradiol binding site. Conversely, progesterone which does not bind RE could not provoke its nuclear translocation.  相似文献   
64.
Dirk Nolf  Henri Cappetta 《Geobios》1976,9(3):251-277
An important new collection of otoliths from theCalcaire Grossier of the Paris Basin, as well as a critical review of already published material is studied and reveals the presence of 56 species. Five of these are new: Muraenesox spatulus, Genus Synodontidarum intermedius, Genus Ophidiidarum spinosus, Chanda bohlkei and Mene sekharani. The assemblage is indicative of tropical to subtropical marine and neritic environment with solid bottom. Biogeographically, it shows affinities with the recent Indo-pacific fauna. The association of the sites at Fercourt and Château-Rouge is clearly different from the one found at the sites of Condé-en-Brie and Damery, as it is less littoral than the second association mentioned.  相似文献   
65.
The growth of Chinese hamster somatic cells was inhibited by 0.2 mg/cc of 2-deoxygalactose. Mutants partially or fully resistant to 2-deoxygalactose were isolated in a single-step or two-step selection. Some of them did not grow as well as the wild type; one of them which lacked galactokinase(EC.2.7.1.6) activity did not grow at all in galactose medium. The galactokinase kinetic properties (Vmax & kmax of the other mutants and of the wild type were different. Therefore resistance resulted either from the possible absence of galactokinase synthesis or from a structural mutation, possible a missence mutation, in the galactokinase gene.- A simple diagnostic test for juvenile cataract is proposed.  相似文献   
66.
Unstable clones excreting L-lysine into their growth medium are obtained at a very high frequency following UV irradiation in both haploid and diploid strains of Saccharomycopsis lipolytica, provided they carry a mutation affecting the first enzyme of the lysine pathway and confering resistance to end product inhibition. The phenotype can be stabilized in some sublines; it appears as dominant and coupled with a decrease in spore viability. Excretion in batch cultures is confined to the end of the exponential phase, and seems not to consist in a simple release of the lysine pool content.  相似文献   
67.
The specific activity of carbons 1 and 2 of plasma acetoacetate has been used as a measure of the specific activity of liver mitochondrial acetyl-CoA in tracer studies. To test whether or not acetoacetate actually reflects acetyl-CoA, livers were perfused with a mixture of substrates that are converted to mitochondrial acetyl-CoA: 1 mM lactate, 0.2 mM pyruvate, 0.2 mM acetate, and, where indicated, 0.2 mM octanoate or 0.2 mM alpha-ketoisocaproate. In each experiment, one of these substrates was 13C-labeled. Labeling of mitochondrial acetyl-CoA was assessed by three methods: (i) molar percent enrichment of total tissue acetyl-CoA; (ii) molar percent enrichment of carbons 4 and 5 of tissue citrate, the precursor of which is acetyl-CoA; and (iii) molar percent enrichment of carbons 1 and 2 of perfusate ketone bodies. Nonhomogeneous labeling of liver mitochondrial acetyl-CoA occurred under most conditions, i.e. the enrichments of carbons 4 and 5 of citrate were different from enrichments of carbons 1 and 2 of ketone bodies. Thus, based upon our results obtained in perfused livers, we question the validity of measuring the labeling of carbons 1 and 2 of acetoacetate as a noninvasive probe of liver mitochondrial acetyl-CoA.  相似文献   
68.
Plasmodium falciparum is responsible for severe malaria which is one of the most prevalent and deadly infectious diseases in the world. The antimalarial therapeutic arsenal is hampered by the onset of resistance to all known pharmacological classes of compounds, so new drugs with novel mechanisms of action are critically needed. Albitiazolium is a clinical antimalarial candidate from a series of choline analogs designed to inhibit plasmodial phospholipid metabolism. Here we developed an original chemical proteomic approach to identify parasite proteins targeted by albitiazolium during their native interaction in living parasites. We designed a bifunctional albitiazolium-derived compound (photoactivable and clickable) to covalently crosslink drug–interacting parasite proteins in situ followed by their isolation via click chemistry reactions. Mass spectrometry analysis of drug–interacting proteins and subsequent clustering on gene ontology terms revealed parasite proteins involved in lipid metabolic activities and, interestingly, also in lipid binding, transport, and vesicular transport functions. In accordance with this, the albitiazolium-derivative was localized in the endoplasmic reticulum and trans-Golgi network of P. falciparum. Importantly, during competitive assays with albitiazolium, the binding of choline/ethanolamine phosphotransferase (the enzyme involved in the last step of phosphatidylcholine synthesis) was substantially displaced, thus confirming the efficiency of this strategy for searching albitiazolium targets.  相似文献   
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