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151.
R A Segal  H Takahashi  R D McKay 《Neuron》1992,9(6):1041-1052
Neurotrophins and their receptors are widespread in the developing and mature CNS. Identifying the differentiation state of neurotrophin-responsive cells provides a basis for understanding the developmental functions of these factors. Studies using dissociated and organotypic cultures of rat cerebellum demonstrated that the neurotrophins brain-derived neurotrophic factor (BDNF) and neurotrophin-3 (NT-3) affect developing granule cells at distinct stages in differentiation. While early granule neurons in the external germinal layer responded to BDNF, more mature granule cells responded to NT-3. BDNF, but not NT-3, enhanced survival of granule cells in cultures of embryonic cerebella. Thus, BDNF and NT-3 have distinct sequential functions that are likely to be critical in the development of the cerebellum. BDNF may promote the initial commitment, while NT-3 may direct the subsequent maturation of granule cells.  相似文献   
152.
153.
E Korkotian  M Segal 《Neuron》2001,30(3):751-758
Dendritic spines have long been known to contain contractile elements and have recently been shown to express apparent spontaneous motility. Using high-resolution imaging of dendritic spines of green-fluorescent protein (GFP)-expressing, patch-clamped hippocampal neurons in dissociated culture, we find that bursts of action potentials, evoked by depolarizing current pulses, cause momentary contractions of dendritic spines. Blocking calcium currents with cobalt prevented these twitches. In additional experiments with neurons loaded via a micropipette with calcium-sensitive and insensitive dyes, spontaneous calcium transients were associated with a rapid contraction of the spine head. The spine twitch was prolonged by tetraethylammonium or bicuculline, which enhance calcium transients, and was blocked by the actin polymerization antagonist latrunculin-B. The spine twitch may be instrumental in modulating reactivity of the NMDA receptor to afferent stimulation, following back-propagating action potentials.  相似文献   
154.
The present study compared bereavement responses of 325 monozygotic (MZ) and 176 dizygotic (DZ) adolescent and adult twins following the loss of their co-twins. A subset of twins completed the Grief Experience Inventory using a retrospective time frame, while a second subset completed it using a current time frame. It was hypothesized that MZ twins (in both retrospective and current groups) would report higher levels of grief-related behavior than DZ twins, consistent with Hamilton's (1964) concept of inclusive fitness. Discriminant function and profile analyses yielded supportive findings, but only for the retrospective MZ and DZ twin comparisons. Females in both groups expressed higher levels of bereavement-related behavior than males. Findings are discussed with reference to theoretical aspects of grief and mourning.  相似文献   
155.
In this paper, we explore modeling overlapping biological processes. We discuss a probabilistic model of overlapping biological processes, gene membership in those processes, and an addition to that model that identifies regulatory mechanisms controlling process activation. A key feature of our approach is that we allow genes to participate in multiple processes, thus providing a more biologically plausible model for the process of gene regulation. We present algorithms to learn each model automatically from data, using only genomewide measurements of gene expression as input. We compare our results to those obtained by other approaches and show that significant benefits can be gained by modeling both the organization of genes into overlapping cellular processes and the regulatory programs of these processes. Moreover, our method successfully grouped genes known to function together, recovered many regulatory relationships that are known in the literature, and suggested novel hypotheses regarding the regulatory role of previously uncharacterized proteins.  相似文献   
156.
Studies were carried out to test whether the induction of a primary production of antibodies is determined by DNA replication. An in vitro system for the induction of antibody to dinitrophenyl (DNP) determinants following immunization with α-DNP-poly-l-lysine was employed. Cytosine arabinoside (CA), at doses which inhibited DNA synthesis, yet did not affect viability of cells, was applied at different time intervals following antigenic stimulation. Inhibition of DNA synthesis during 36–48 hr following antigenic stimulation prevented the appearance of antibody producing cells. On the other hand, CA applied during the first 36 hr or at 48 hr did not prevent antibody production. Thus, one critical cycle of DNA replication seems to determine antibody production. The lag period prior to the CA-sensitive period is antigen determined.  相似文献   
157.
The kinetics of α-methyl-d-glucoside accumulation by rat kidney cortex slices under conditions of varying extracellular sodium concentration were investigated. Extracellular sodium reduction below 144 mequivi/l resulted in a diminished initial uptake and reduced influx calculated by steady-state analysis of a two-compartment system. At 72 mequiv/l extracellular sodium efflux was decreased to the same extent as influx resulting in the same steady state concentration that was observed at 144 mequiv/l sodium. At 36 mequiv/l the steady state concentration was below that observed at 144 mequiv/l sodium because of a disproportionate decrease of influx. In the complete absence of extracellular sodium, no concentration gradient was achieved and efflux had become increased. Low extracellular sodium was associated with an increase in the apparent Km of transport without affecting the V. The apparent Ki for sodium appeared to be in th e 40 to 59 mequiv/l range. The presence of 20 mM α-methyl-d-glucose prompted the accelerated efflux of the sugar from the tubule cells in a normal fashion despite a low extracellular sodium concentration.  相似文献   
158.
Summary The uptake, incorporation and distribution of tritiated thymidine and uridine into visceral organs of immature female and male rats was studied. Radioautographs of various organs were prepared 5, 15 and 30 min after intraperitoneal administration. The distribution of the radioactivity was compared with sections obtained 30 min after intravenous injection of the same amount of nucleotides.The intraperitoneal injection was performed by directing the needle toward the right side of the abdominal cavity. Visceral organs from the injected side contained consistently more silver grains than those from the opposite side. Sections of the abdominal organs showed a decreasing concentration gradient of reduced silver grains extending from the serosal part of the organ to the deeper layers. In addition, initial labeling was observed in sectors of organs which protruded into the peritoneal cavity. In contrast, following intravenous administration of nucleotides a concentration gradient was not observed in any of the visceral organs.The results of the present study suggest that nucleotides administered intraperitoneally may penetrate the abdominal organs directly via the serosal surface without prior entry into the general circulation.  相似文献   
159.
160.
α-Methyl-d-glucoside has been shown to be a non-metabolizable sugar which is accumulated against a concentration gradient by a Na+-dependent and phlorizin inhibited process by adult rat renal cortical slices incubatedin vitro at 37 °C. (2) The velocity of accumulation increased linearly with substrate concentrations up to 1.5 mM, but at higher concentrations obeyed saturable kinetics with an apparentKm of about 6 mM. (3) Uptake was enhanced as Na+ was increased from 0 to 100 mequiv/l. Higher Na+ concentrations caused no further effect. (4) A pH maximum of transport occurred between 7.35 and 8.0. (5) Glucoside uptake was inhibited byd-glucose,d-galactose,d-fructose,d-mannose andd-ribose. The inhibition byd-glucose andd-galactose was competitive with apparentKt of 24 and 53 mM, respectively. (6) Bothd-glucose andd-galactose accelerated the efflux of α-methyl-d-glucoside from preloaded cells. (7) Kidney cortex slices from 1-day-old rats were unable to accumulate α-methyl-d-glucoside to form a concentration gradient. The ability to concentrate the glucoside increased progressively after birth, reaching near normal in tissue from 15-day-old animals. The data indicate that the transport process in the newborn is rudimentary, failing also to display accelerated efflux phenomenon. (8) α-Methyl-d-glucoside is transported in rat kidney cortex by a mechanism similar in many ways to that ofd-galactose.  相似文献   
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