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We compared histochemical and immunohistochemical staining as well as fluorochrome labeling in murine bone specimens that were fixed with 10% neutral buffered formalin to those fixed with HistoChoice®. We showed that sections from undecalcified tibiae fixed for 4 h in HistoChoice® resulted in enhanced toluidine blue and Von Kossa histochemical staining compared to formalin fixation. HistoChoice® produced comparable or improved staining for alkaline phosphatase. Acid phosphatase localization was better in formalin fixed specimens, but osteoclasts were visuralized more easily in HistoChoice® fixed specimens. As expected, immunohistochemical labeling was antibody dependent; some antibodies labeled better in HistoChoice® fixed specimens while others were better in formalin fixed specimens. Toluidine blue, Von Kossa, and alkaline phosphatase staining of sections fixed for 12 h produced sections that were similar to 4 h fixed sections. Fixation for 12 h preserved acid phosphatase activity better. Increasing fixation to 12 h affected immunolocalization differentially. Bone sialoprotein labeling in HistoChoice® fixed specimens was comparable to formalin fixed samples. On the other hand, after 12 h formalin fixation, osteocalcin labeling was comparable to HistoChoice®. For most histochemical applications, fixing murine bone specimens for 4 h with HistoChoice® yielded superior staining compared to formalin fixation. If immunohistochemical localization is desired, however, individual antibodies must be tested to determine which fixation process retains antigenicity better. In addition, there was no detectable difference in the intensity of fluorochrome labeling using either fixative. Finally, fixation duration did not alter the intensity of labeling. 相似文献
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Synthesis of some nucleotides derived from 3'-deoxythymidine 总被引:2,自引:0,他引:2
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Genome-wide scan on total serum IgE levels identifies FCER1A as novel susceptibility locus 下载免费PDF全文
Weidinger S Gieger C Rodriguez E Baurecht H Mempel M Klopp N Gohlke H Wagenpfeil S Ollert M Ring J Behrendt H Heinrich J Novak N Bieber T Krämer U Berdel D von Berg A Bauer CP Herbarth O Koletzko S Prokisch H Mehta D Meitinger T Depner M von Mutius E Liang L Moffatt M Cookson W Kabesch M Wichmann HE Illig T 《PLoS genetics》2008,4(8):e1000166
High levels of serum IgE are considered markers of parasite and helminth exposure. In addition, they are associated with allergic disorders, play a key role in anti-tumoral defence, and are crucial mediators of autoimmune diseases. Total IgE is a strongly heritable trait. In a genome-wide association study (GWAS), we tested 353,569 SNPs for association with serum IgE levels in 1,530 individuals from the population-based KORA S3/F3 study. Replication was performed in four independent population-based study samples (total n = 9,769 individuals). Functional variants in the gene encoding the alpha chain of the high affinity receptor for IgE (FCER1A) on chromosome 1q23 (rs2251746 and rs2427837) were strongly associated with total IgE levels in all cohorts with P values of 1.85 x 10(-20) and 7.08 x 10(-19) in a combined analysis, and in a post-hoc analysis showed additional associations with allergic sensitization (P = 7.78 x 10(-4) and P = 1.95 x 10(-3)). The "top" SNP significantly influenced the cell surface expression of FCER1A on basophils, and genome-wide expression profiles indicated an interesting novel regulatory mechanism of FCER1A expression via GATA-2. Polymorphisms within the RAD50 gene on chromosome 5q31 were consistently associated with IgE levels (P values 6.28 x 10(-7)-4.46 x 10(-8)) and increased the risk for atopic eczema and asthma. Furthermore, STAT6 was confirmed as susceptibility locus modulating IgE levels. In this first GWAS on total IgE FCER1A was identified and replicated as new susceptibility locus at which common genetic variation influences serum IgE levels. In addition, variants within the RAD50 gene might represent additional factors within cytokine gene cluster on chromosome 5q31, emphasizing the need for further investigations in this intriguing region. Our data furthermore confirm association of STAT6 variation with serum IgE levels. 相似文献
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Impacts of land use on riparian forest along an urban – rural gradient in southern Manitoba 总被引:3,自引:0,他引:3
Extensive landscape modification by humans has led to the fragmentation of riparian forests across North America. We compared
the vegetation of extant riparian forest along an urban-rural disturbance gradient. In 1999, twenty-five sites along Assiniboine
River in Manitoba, Canada were categorized according to land use: urban, suburban, high intensity rural, low intensity rural,
and relatively high quality reference forest. Differences in herbaceous, shrub, and tree species composition and diversity
were related to the proportion of surrounding land use, forest patch size, connectivity, and area:perimeter ratio. Urban riparian
forests were more disturbed and isolated. They were smaller and characterized by drier, more alkaline soils. Moreover, they
had significantly lower native and overall understorey species diversity, and had a higher proportion of exotics including
Solanum dulcamara and Hesperis matronalis. Suburban forests were less disturbed, faced greater development pressure, and had sandier soils. Although suburban understorey
diversity was similar to that of rural forests, suburban sites had a higher proportion of exotic species, especially escaped
horticultural and invasive species including Caragana arborescens and Rhamnus cathartica. Reference sites were relatively large and exhibited greater connectivity, but there was little difference in species composition
and diversity among high intensity rural, low intensity rural, and reference sites. These site types were less disturbed than
either urban or suburban forests, and reference sites were characterized by hydrophilic species including Scirpus fluviatilis and Carex aquatilis. Our results suggest that landscape measures of disturbance, and related changes in environment, may be confidently used
to assess impacts of land use on vegetation along urban-rural gradients.
This revised version was published online in June 2006 with corrections to the Cover Date. 相似文献