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991.
Zhou P Cowled C Todd S Crameri G Virtue ER Marsh GA Klein R Shi Z Wang LF Baker ML 《Journal of immunology (Baltimore, Md. : 1950)》2011,186(5):3138-3147
Bats are known to harbor a number of emerging and re-emerging zoonotic viruses, many of which are highly pathogenic in other mammals but result in no clinical symptoms in bats. The ability of bats to coexist with viruses may be the result of rapid control of viral replication early in the immune response. IFNs provide the first line of defense against viral infection in vertebrates. Type III IFNs (IFN-λs) are a recently identified IFN family that share similar antiviral activities with type I IFNs. To our knowledge, we demonstrate the first functional analysis of type III IFNs from any species of bat, with the investigation of two IFN-λ genes from the pteropid bat, Pteropus alecto. Our results demonstrate that bat type III IFN has similar antiviral activity to type I and III IFNs from other mammals. In addition, the two bat type III IFNs are differentially induced relative to each other and to type I IFNs after treatment or transfection with synthetic dsRNA. Infection with the bat paramyxovirus, Tioman virus, resulted in no upregulation of type I IFN production in bat splenocytes but was capable of inducing a type III IFN response in three of the four bats tested. To our knowledge, this is the first report to describe the simultaneous suppression of type I IFN and induction of type III IFN after virus infection. These results may have important implications for the role of type III IFNs in the ability of bats to coexist with viruses. 相似文献
992.
993.
McCarthy JS Sekuloski S Griffin PM Elliott S Douglas N Peatey C Rockett R O'Rourke P Marquart L Hermsen C Duparc S Möhrle J Trenholme KR Humberstone AJ 《PloS one》2011,6(8):e21914
Background
Critical to the development of new drugs for treatment of malaria is the capacity to safely evaluate their activity in human subjects. The approach that has been most commonly used is testing in subjects with natural malaria infection, a methodology that may expose symptomatic subjects to the risk of ineffective treatment. Here we describe the development and pilot testing of a system to undertake experimental infection using blood stage Plasmodium falciparum parasites (BSP). The objectives of the study were to assess the feasibility and safety of induced BSP infection as a method for assessment of efficacy of new drug candidates for the treatment of P. falciparum infection.Methods and Findings
A prospective, unblinded, Phase IIa trial was undertaken in 19 healthy, malaria-naïve, male adult volunteers who were infected with BSP and followed with careful clinical and laboratory observation, including a sensitive, quantitative malaria PCR assay. Volunteers were randomly allocated to treatment with either of two licensed antimalarial drug combinations, artemether–lumefantrine (A/L) or atovaquone-proguanil (A/P). In the first cohort (n = 6) where volunteers received ∼360 BSP, none reached the target parasitemia of 1,000 before the day designated for antimalarial treatment (day 6). In the second and third cohorts, 13 volunteers received 1,800 BSP, with all reaching the target parasitemia before receiving treatment (A/L, n = 6; A/P, n = 7) The study demonstrated safety in the 19 volunteers tested, and a significant difference in the clearance kinetics of parasitemia between the drugs in the 13 evaluable subjects, with mean parasite reduction ratios of 759 for A/L and 17 for A/P (95% CI 120–4786 and 7–40 respectively; p<0.01).Conclusions
This system offers a flexible and safe approach to testing the in vivo activity of novel antimalarials.Trial Registration:
ClinicalTrials.gov NCT01055002相似文献994.
Jean-Marie Burel Sébastien Besson Colin Blackburn Mark Carroll Richard K. Ferguson Helen Flynn Kenneth Gillen Roger Leigh Simon Li Dominik Lindner Melissa Linkert William J. Moore Balaji Ramalingam Emil Rozbicki Aleksandra Tarkowska Petr Walczysko Chris Allan Josh Moore Jason R. Swedlow 《Mammalian genome》2015,26(9-10):441-447
995.
Using miniaturized radiotelemetry to discover the breeding grounds of the endangered New Zealand Storm Petrel Fregetta maoriana 下载免费PDF全文
Matt J. Rayner Chris P. Gaskin Neil B. Fitzgerald Karen A. Baird Martin M. Berg David Boyle Leigh Joyce Todd J. Landers Graeme G. Loh Sue Maturin Lyndon Perrimen R. Paul Scofield Joanna Simm Ian Southey Graeme A. Taylor Alan J. D. Tennyson Bruce C. Robertson Megan Young Richard Walle Stefanie M. H. Ismar 《Ibis》2015,157(4):754-766
Identification of breeding sites remains a critical step in species conservation, particularly in procellariiform seabirds whose threat status is of global concern. We designed and conducted an integrative radiotelemetry approach to uncover the breeding grounds of the critically endangered New Zealand Storm Petrel Fregetta maoriana (NZSP), a species considered extinct before its rediscovery in 2003. Solar‐powered automated radio receivers and hand‐held telemetry were used to detect the presence of birds on three island groups in the Hauraki Gulf near Auckland, New Zealand. At least 11 NZSP captured and radiotagged at sea were detected at night near Te Hauturu‐o‐Toi/Little Barrier Island with the detection of an incubating bird leading to the discovery of the first known breeding site for this species. In total, four NZSP breeding burrows were detected under mature forest canopy and three adult NZSP and two NZSP chicks were ringed. Telemetry data indicated NZSP showed strong moonlight avoidance behaviour over the breeding site, had incubation shifts of approximately 5 days and had a breeding season extending from February to June/July, a different season from other Procellariiformes in the region. Radiotelemetry, in combination with rigorously collected field data on species distribution, offers a valuable technique for locating breeding grounds of procellariiform seabirds and gaining insights into breeding biology while minimizing disturbance to sensitive species or damage to fragile habitat. Our study suggests an avenue for other breeding ground searches in one of the most threatened avian Orders, and highlights the general need for information on the location of breeding sites and understanding the breeding biology in data‐deficient birds. 相似文献
996.
Glover CN Wood CM 《Journal of comparative physiology. B, Biochemical, systemic, and environmental physiology》2008,178(1):101-109
Bioavailability is integral in mediating the delicate balance between nutritive and potentially toxic levels of copper in
fish diets. Brush-border membrane vesicles isolated from freshwater rainbow trout intestine were used to characterise apical
copper absorption, and to examine the influence of the amino acid histidine on this process. In the absence of histidine,
a low affinity, high capacity copper uptake mechanism was described. However, when expressed as a function of ionic copper
(Cu2+), absorption was linear, rather than saturable, suggesting that the saturable curve was an artifact of copper speciation.
Conversely, in the presence of l-histidine (780 μM) saturable uptake was characterised. The uptake capacity discerned (J
max of 354 ± 81 nmol mg protein−1 min−1) in the presence of histidine indicated a significantly reduced capacity for copper transport than that in the absence of
histidine. To determine if copper uptake was achievable through putative histidine uptake pathways, copper and histidine were
incubated in the presence of tenfold greater concentrations of amino acids proposed to block histidine transporters. Accounting
for changes in copper speciation, significant inhibition of uptake by glycine and lysine were noted at copper levels of 699
and 1,028 μM. These results suggest that copper–histidine complexes may be transportable via specific amino acid-transporters
in the brush-border membrane. 相似文献
997.
Glucose-stimulated insulin release from rodent pancreatic B-cells is thought to be initiated by the closing of ATP-sensitive K+ channels in the plasma membrane as a consequence of glucose metabolism. We have identified an ATP-sensitive K+ channel in membrane patches excised from human B-cells which is similar to that found in rodent B-cells in conductance, kinetics, ATP sensitivity and its inhibition by sulphonylureas. In man, the ATP-sensitive K+ channel may also have a central role in glucose-stimulated insulin secretion and may be (linked to) the receptor for the hypoglycemic sulphonylureas. 相似文献
998.
I‐Ching Chen Jane K. Hill Hau‐Jie Shiu Jeremy D. Holloway Suzan Benedick Vun Khen Chey Henry S. Barlow Chris D. Thomas 《Global Ecology and Biogeography》2011,20(1):34-45
Aim To estimate whether species have shifted at equal rates at their leading edges (cool boundaries) and trailing edges (warm boundaries) in response to climate change. We provide the first such evidence for tropical insects, here examining elevation shifts for the upper and lower boundaries shifts of montane moths. Threats to species on tropical mountains are considered. Location Mount Kinabalu, Sabah, Malaysia. Methods We surveyed Lepidoptera (Geometridae) on Mount Kinabalu in 2007, 42 years after the previous surveys in 1965. Changes in species upper and lower boundaries, elevational extents and range areas were assessed. We randomly subsampled the data to ensure comparable datasets between years. Estimated shifts were compared for endemic versus more widespread species, and for species that reached their range limits at different elevations. Results Species that reached their upper limits at 2500–2700 m (n= 28 species, 20% of those considered) retreated at both their lower and upper boundaries, and hence showed substantial average range contractions (?300 m in elevational extent and ?45 km2 in estimated range area). These declines may be associated with changes in cloud cover and the presence of ecological barriers (geological and vegetation transitions) which impede uphill movement. Other than this group, most species (n= 109, 80% of the species considered) expanded their upper boundaries upwards (by an average of 152 m) more than they retreated at their lower boundaries (77 m). Main conclusions Without constraints, leading margins shifted uphill faster than trailing margins retreated, such that many species increased their elevational extents. However, this did not result in increases in range area because the area of land available declines with increasing elevation. Species close to a major ecological/geological transition zone on the mountain flank declined in their range areas. Extinction risk may increase long before species reach the summit, even when undisturbed habitats are available. 相似文献
999.
Plants are widely used in soil conservation to control and prevent erosion on hillslopes and on riverbanks. Previous research has shown the mechanical root reinforcement on soil stability can be considerable. However, land and forest managers still require information and simple tools to enable them to determine how and when a species becomes effective in terms of soil stabilisation. This paper uses root length data from a trial of young New Zealand trees and shrubs to develop a simple model to account for the spatial occupancy of a planting site by roots, and by implication their potential strength contribution to soil reinforcement. It is developed by calculating root surface area in contact with the soil to obtain an effective radius of the root spread about the stem. The approach generates a set of coefficients that are unique to a species for a given site which can then be used in the generalised model to predict root site occupancy, which is taken as a proxy for when soil reinforcement is attained. This information can then be used to assess effectiveness of different species mixes in planting plans. 相似文献
1000.
The extracellular secreted mucus and the cell surface glycocalyx prevent infection by the vast numbers of microorganisms that live in the healthy gut. Mucin glycoproteins are the major component of these barriers. In this Review, we describe the components of the secreted and cell surface mucosal barriers and the evidence that they form an effective barricade against potential pathogens. However, successful enteric pathogens have evolved strategies to circumvent these barriers. We discuss the interactions between enteric pathogens and mucins, and the mechanisms that these pathogens use to disrupt and avoid mucosal barriers. In addition, we describe dynamic alterations in the mucin barrier that are driven by host innate and adaptive immune responses to infection. 相似文献