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121.
Cornelia A. M. van de Weg Ralph M. H. G. Huits Cláudio S. Pannuti Rosalba M. Brouns Riemsdijk W. A. van den Berg Henk-Jan van den Ham Byron E. E. Martina Albert D. M. E. Osterhaus Mihai G. Netea Joost C. M. Meijers Eric C. M. van Gorp Esper G. Kallas 《PLoS neglected tropical diseases》2014,8(10)
Background
During a dengue outbreak on the Caribbean island Aruba, highly elevated levels of ferritin were detected in dengue virus infected patients. Ferritin is an acute-phase reactant and hyperferritinaemia is a hallmark of diseases caused by extensive immune activation, such as haemophagocytic lymphohistiocytosis. The aim of this study was to investigate whether hyperferritinaemia in dengue patients was associated with clinical markers of extensive immune activation and coagulation disturbances.Methodology/Principal Findings
Levels of ferritin, standard laboratory markers, sIL-2R, IL-18 and coagulation and fibrinolytic markers were determined in samples from patients with uncomplicated dengue in Aruba. Levels of ferritin were significantly increased in dengue patients compared to patients with other febrile illnesses. Moreover, levels of ferritin associated significantly with the occurrence of viraemia. Hyperferritinaemia was also significantly associated with thrombocytopenia, elevated liver enzymes and coagulation disturbances. The results were validated in a cohort of dengue virus infected patients in Brazil. In this cohort levels of ferritin and cytokine profiles were determined. Increased levels of ferritin in dengue virus infected patients in Brazil were associated with disease severity and a pro-inflammatory cytokine profile.Conclusions/Significance
Altogether, we provide evidence that ferritin can be used as a clinical marker to discriminate between dengue and other febrile illnesses. The occurrence of hyperferritinaemia in dengue virus infected patients is indicative for highly active disease resulting in immune activation and coagulation disturbances. Therefore, we recommend that patients with hyperferritinaemia are monitored carefully. 相似文献122.
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124.
Antigenic peptide binding to MHC class II molecules in the endocytic pathway occurs via a multifactorial process that requires the support of a specialized lysosomal chaperone called HLA-DM. DM shows both in primary amino acid sequence and quaternary structure a high homology to both MHC class I and class II molecules. Like the peptide presenting class II molecules, DM is expressed in all professional antigen presenting cells. DM catalyzes the dissociation of peptides that do not bind stably to the class II peptide-binding groove, thereby leading to the preferential presentation of stably binding antigenic peptides. The recently discovered HLA-DO molecule is mainly expressed in B cells and associates with DM, thereby markedly affecting DM function. Like DM, the genes encoding the HLA-DO heterodimer lie within the MHC class II region and exhibit strong homology to classical class II molecules. This review evaluates the unique effects of DO on DM-mediated antigen presentation by MHC class II molecules and discusses the possible physiological relevance for the B cell-specific expression of DO and its function. 相似文献
125.
Won Cheol Yim Mia L Swain Dongna Ma Hong An Kevin A Bird David D Curdie Samuel Wang Hyun Don Ham Agusto Luzuriaga-Neira Jay S Kirkwood Manhoi Hur Juan K Q Solomon Jeffrey F Harper Dylan K Kosma David Alvarez-Ponce John C Cushman Patrick P Edger Annaliese S Mason J Chris Pires Haibao Tang Xingtan Zhang 《The Plant cell》2022,34(11):4143
126.
Synopsis Vertical movements of bluegill were monitored in gradients of light intensity to assess this fish's photoregulatory ability and mechanisms. A computerized monitoring and control system created virtual gradients of light intensity by adjusting an overhead lamp's output in response to fish movements, in a vertical tube, to produce a programmed intensity at the fish's depth position. This approach separated the process of gradient formation from normal clues for photoregulation and allowed formation of light gradients incompatible with natural taxic responses to intensity. Hourly shifts in gradient position minimized the possibility of confounding photoregulation with position regulation. Observed patterns of movement reduced the extremes of light intensity to which bluegill were exposed, compared to no movement or random movement. Seven fish were tested, producing 10 experiments. In 4 of 10 experiments, the fish effectively photoregulated in gradients in which light intensity decreased with depth, as in natural habitats. In 1 of 10 experiments, the fish photoregulated in an inverse gradient, with intensity increasing with depth. Evidence of regulation in an inverse gradient suggests that normal taxic responses are not essential for photoregulation in bluegill. 相似文献
127.
Jun-Dae Kim Eunmi Kim Soonil Koun Hyung-Jin Ham Myungchull Rhee Myoung-Jin Kim Tae-Lin Huh 《Molecules and cells》2015,38(6):580-586
While increasing evidence indicates the important function of histone methylation during development, how this process influences cardiac development in vertebrates has not been explored. Here, we elucidate the functions of two histone H3 lysine 4 (H3K4) methylation enzymes, SMYD3 and SETD7, during zebrafish heart morphogenesis using gene expression profiling by whole mount in situ hybridization and antisense morpholino oligonucleotide (MO)-based gene knockdown. We find both smyd3 and setd7 are highly expressed within developing zebrafish heart and knock-down of these genes led to severe defects in cardiac morphogenesis without altering the expressions pattern of heart markers, including cmlc2, vmhc, and amhc. Furthermore, double knock-down by coinjection of smyd3 and setd7 MOs caused the synergistic defects in heart development. As similar to knock-down effect, overexpression of these genes also caused the heart morphogenesis defect in zebrafish. These results indicate that histone modifying enzymes, SMYD3 and SETD7, appear to function synergistically during heart development and their proper functioning is essential for normal heart morphogenesis during development. 相似文献
128.
129.
Activation of PPARδ attenuates neurotoxicity by inhibiting lipopolysaccharide‐triggered glutamate release in BV‐2 microglial cells
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130.
The addition of 2.8 g/ml algal extracts enhanced both scu-PA production and cell growth in a serum-free medium, compared to a conventional serum-free medium for the cultivation of recombinant CHO cells. The growth rate and scu-PA production were relatively lower in the serum-free medium than 5% serum containing medium: however, specific scu-PA production rate was higher in the serum-free medium due to the long-term period of cultivation (3.66×10–4 vs. 2.48×10–4 IU/cell/day). Overall scu-PA production rate was also greater in an enforced serum-free medium as 25,000 IU/day over 50 d of perfusion cultivation. The conversion ratio of scu-PA to tcu-PA was greatly reduced in the serum-free medium during perfusion cultivation (10% compared to 20% conversion in a serum containing medium). 相似文献