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911.
912.
Impacts of Community-based Conservation on Local Communities in the Annapurna Conservation Area, Nepal 总被引:1,自引:0,他引:1
Siddhartha B. Bajracharya Peter A. Furley Adrian C. Newton 《Biodiversity and Conservation》2006,15(8):2765-2786
Approaches to the management of protected areas that involve the participation of local communities are now being widely promoted.
However, the impacts of such community-based conservation initiatives on local communities remain poorly defined. This research
examines the socio-economic impacts of community-based conservation within the Annapurna Conservation Area (ACA), Nepal, through
semi-structured interviews and a questionnaire survey with local residents, situated both within and outside the protected
area. Results indicate that local communities have received a number of benefits from conservation, including improvements
in access to forest resources, improved basic infrastructure such as drinking water, trails and bridges, and improvements
in health, sanitation and social services. However, relatively few people (14.9%) within ACA receive direct financial income
from tourism. Local communities also experience a number of costs of being involved in conservation, the most significant
of which is increased crop damage by wildlife. Eighty-four percent of respondents within ACA have experienced problems of
crop damage, accounting for 6% (rice) to 23% (maize) of total production. Depredation of livestock by wildlife is also experienced;
mean losses per household being the equivalent of £3.9 (Rs. 479.70) each year. However, 66% of respondents within ACA reported
that they had never experienced this problem. These results indicate that the socio-economic benefits of community-based approaches
to conservation can outweigh the costs, even though the latter are significant. However, a participatory approach to management
of problematic animal species will need to be developed within ACA, if conflicts between local communities and protected area
management are to be avoided in future. 相似文献
913.
Lycium barbarum, a famous Chinese medicinal herb, has a long history of use as a traditional remedy for male infertility. Polysaccharides are the most important functional constituent in L. barbarum fruits. We systematically investigated the effect of L. barbarum polysaccharides (LBP) on rat testis damage induced by a physical factor (43 degrees C heat exposure), on DNA damage of mouse testicular cells induced by a chemical factor (H2O2), and on sexual behavior and reproductive function of hemicastrated male rats. The results showed that LBP provided a protective effect against the testicular tissue damage induced by heat exposure. When compared with negative control, a suitable concentration of LBP significantly increased testis and epididymis weights, improved superoxide dismutase (SOD) activity, and raised sexual hormone levels in the damaged rat testes. LBP had a dose-dependent protective effect against DNA oxidative damage of mouse testicular cells induced by H2O2. LBP improved the copulatory performance and reproductive function of hemicastrated male rats, such as shortened penis erection latency and mount latency, regulated secretion of sexual hormones and increased hormone levels, raised accessory sexual organ weights, and improved sperm quantity and quality. The present findings support the folk reputation of L. barbarum fruits as an aphrodisiac and fertility-facilitating agent, and provide scientific evidence for a basis for the extensive use of L. barbarum fruits as a traditional remedy for male infertility in China. 相似文献
914.
Joshua Schroeder Janina Kueper Kaplan Leon Meir Liebergall 《World journal of stem cells》2015,7(1):186-194
In the past few years, stem cells have become the focus of research by regenerative medicine professionals and tissue engineers. Embryonic stem cells, although capable of differentiating into cell lineages of all three germ layers, are limited in their utilization due to ethical issues. In contrast, the autologous harvest and subsequent transplantation of adult stem cells from bone marrow, adipose tissue or blood have been experimentally utilized in the treatment of a wide variety of diseases ranging from myocardial infarction to Alzheimer’s disease. The physiologic consequences of stem cell transplantation and its impact on functional recovery have been studied in countless animal models and select clinical trials. Unfortunately, the bench to bedside translation of this research has been slow. Nonetheless, stem cell therapy has received the attention of spinal surgeons due to its potential benefits in the treatment of neural damage, muscle trauma, disk degeneration and its potential contribution to bone fusion. 相似文献
915.
《Saudi Journal of Biological Sciences》2017,24(6):1418-1423
Schistosomiasis is still one of the main parasitic diseases that affect human health in tropical regions. Whilst praziquantel (PZQ) is the main classic antischistosomal drug, the need for new drugs is still a must due to the low effectiveness of the drug on the schistosome young worms, and the evolving of PZQ resistant strains. Nanotechnology is one of the most important recent and current methods used to treat human diseases including parasitic ones. Therefore, the present study aimed to examine the curative role of gold nanoparticles (GNPs) on splenic tissue of mice infected with Schistosoma mansoni Sambon, 1907. High-resolution transmission electron microscopy was used for characterization of nanoparticles (NP). GNPs of 1 mg/kg mice body weight were inoculated into mice infected with S. mansoni. The parasite caused deteriorations in histological architecture of the spleen tissue, and splenomegaly. Additionally, the parasite induced a significant reduction in splenic tissue glutathione levels; however, the concentrations of nitric oxide and malondialdehyde were significantly increased. Treatment of mice with GNPs reduced the extent of histological impairment and oxidative stress in spleen tissue. Therefore, our results demonstrate the protective role of GNPs against splenic damage in mice infected with S. mansoni. 相似文献
916.
Differentiation of micronuclei (MN) caused by ionizing radiation from those caused by chemicals is a crucial step for managing treatment of individuals exposed to radiation. MN in binucleated lymphocytes in peripheral blood are widely used as biomarkers for estimating dose of radiation, but they are not specific for ionizing radiation. MN induced by ionizing radiation originate predominantly as a result of chromosome breaks (clastogenic action), whereas MN caused by chemical agents are derived from the loss of entire chromosomes (aneugenic action). C-banding highlights centromeres, which might make it possible to distinguish radiation induced MN, i.e., as a byproduct of acentric fragments, from those caused by the loss of entire chromosomes. To test the use of C-banding for identifying radiation induced MN, a blood sample from a healthy donor was irradiated with 3 Gy of Co-60 gamma rays and cultured. Cells were harvested and dropped onto slides, divided into a group stained directly with Giemsa and another processed for C banding, then stained with Giemsa. The frequency of MN in 500 binucleated cells was scored for each method. In preparations stained with Giemsa directly, the MN appeared as uniformly stained structures, whereas after C banding, some MN exhibited darker regions corresponding to centromeres that indicated that they were not derived from acentric fragments. The C-banding technique enables differentiation of MN from acentric chromosomal material. This distinction is useful for improving the specificity of the MN assay as a biomarker for ionizing radiation. 相似文献
917.
Vicente Planelles 《Cell cycle (Georgetown, Tex.)》2017,16(11):1020-1021
918.
Liang-Yu Fu Guang-Zhong Wang Bin-Guang Ma Hong-Yu Zhang 《Biochemical and biophysical research communications》2011,(3):367
Recently, numerous genome analyses revealed the existence of a universal G:C → A:T mutation bias in bacteria, fungi, plants and animals. To explore the molecular basis for this mutation bias, we examined the three well-known DNA mutation models, i.e., oxidative damage model, UV-radiation damage model and CpG hypermutation model. It was revealed that these models cannot provide a sufficient explanation to the universal mutation bias. Therefore, we resorted to a DNA mutation model proposed by Löwdin 40 years ago, which was based on inter-base double proton transfers (DPT). Since DPT is a fundamental and spontaneous chemical process and occurs much more frequently within GC pairs than AT pairs, Löwdin model offers a common explanation for the observed universal mutation bias and thus has broad biological implications. 相似文献
919.
Objective
To investigate the mechanism for the dual effects of estrogen on vascular smooth muscle cells (VSMCs).Methods
Cultured rat VSMCs were exposed to gradient concentrations (10−9-10−5 M) of 17β-estradiol (E2) with or without pre-administration of a broad-spectrum CYP450 inhibitor 1-aminobenzotriazole (ABT) (10 × 10−6 M) and an estrogen receptor (ER) antagonist ICI 182,780 (10−6 M), respectively. The growth, cell cycle progression, premature senescence, estrogen metabolites, reactive oxygen species (ROS) and DNA damage of the cells were analyzed with cell counting assay, flow cytometry, Western blot, liquid chromatography-mass spectrometry and comet assay, respectively.Results
E2 in its physiological levels from 10−9 M to 10−8 M had a concentration-dependent promoting effect on growth of VSMCs. However, when the concentration increased over 10−8 M, the growth-promoting effect gradually reversed to a growth-inhibiting action. When the activity of CYP450s was blocked by ABT, the growth-promoting effect of E2 increased and did not reverse at high concentrations. Whereas when the ERs were blocked by ICI 182,780, E2 showed a pure growth-inhibiting effect. The E2 metabolites 2- and 4-hydroxyestradiols accumulated with the increase of E2 over 10−8 M, which accompanied by increased ROS, DNA damage and cellular senescence. All of these changes were eliminated by block of CYP450s, indicating that the VSMC growth inhibition by E2 is due to an increased production of ROS from accumulated E2 metabolites which induces DNA damage, leading to VSMC premature senescence.Conclusion
The complex effect of E2 is due to two opposite actions: one ER-mediated and proliferative, and the other estrogen metabolite-induced and pro-senescent. 相似文献920.