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排序方式: 共有163条查询结果,搜索用时 203 毫秒
31.
Tilman Ziegler Jan Horstkotte Claudia Schwab Vanessa Pfetsch Karolina Weinmann Steffen Dietzel Ina Rohwedder Rabea Hinkel Lisa Gross Seungmin Lee Junhao Hu Oliver Soehnlein Wolfgang M. Franz Markus Sperandio Ulrich Pohl Markus Thomas Christian Weber Hellmut G. Augustin Reinhard F?ssler Urban Deutsch Christian Kupatt 《The Journal of clinical investigation》2013,123(8):3436-3445
Septic shock is characterized by increased vascular permeability and hypotension despite increased cardiac output. Numerous vasoactive cytokines are upregulated during sepsis, including angiopoietin 2 (ANG2), which increases vascular permeability. Here we report that mice engineered to inducibly overexpress ANG2 in the endothelium developed sepsis-like hemodynamic alterations, including systemic hypotension, increased cardiac output, and dilatory cardiomyopathy. Conversely, mice with cardiomyocyte-restricted ANG2 overexpression failed to develop hemodynamic alterations. Interestingly, the hemodynamic alterations associated with endothelial-specific overexpression of ANG2 and the loss of capillary-associated pericytes were reversed by intravenous injections of adeno-associated viruses (AAVs) transducing cDNA for angiopoietin 1, a TIE2 ligand that antagonizes ANG2, or AAVs encoding PDGFB, a chemoattractant for pericytes. To confirm the role of ANG2 in sepsis, we i.p. injected LPS into C57BL/6J mice, which rapidly developed hypotension, acute pericyte loss, and increased vascular permeability. Importantly, ANG2 antibody treatment attenuated LPS-induced hemodynamic alterations and reduced the mortality rate at 36 hours from 95% to 61%. These data indicate that ANG2-mediated microvascular disintegration contributes to septic shock and that inhibition of the ANG2/TIE2 interaction during sepsis is a potential therapeutic target. 相似文献
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Julia Vogt Rabea Wagener Manuel Montesinos‐Rongen Ole Ammerpohl Werner Paulus Martina Deckert Reiner Siebert 《Genes, chromosomes & cancer》2019,58(1):66-69
Primary lymphomas of the central nervous system (PCNSL) are diffuse large B‐cell lymphomas (DLBCLs) confined to the central nervous system (CNS). We here performed array‐based DNA methylation analyses of 26 PCNSL and 78 DLBCL and validated our findings in an independent dataset. We identified 2847 CpGs differentially methylated between PCNSL and non‐CNS‐DLBCL. Neither a supervised analysis using these CpGs nor application of 3 CpG classifiers selected for class separation unambiguously separated PCNSL from non‐CNS‐DLBCL. Remarkably, 6/78 non‐CNS‐DLBCL consistently segregated with PCNSL, which displayed molecular features typical for PCNSL. Our findings suggest that a subset of non‐CNS‐DLBCL exists which molecularly resembles PCNSL. 相似文献
34.
The role played by various K+ channels during locomotor activity was studied using an in vitro neonatal rat spinal cord preparation. Locomotor-like activity was elicited by bath-applying serotonin (5-HT) and N-methyl-d-l-aspartate (NMA). Four different K+ channel blockers were tested by adding them to the superfusing saline. Each of the K+ channel blockers elicited a characteristic motor pattern with specific temporal parameters. Cs+ and tetraethyl ammonium both decreased the motor period, but had opposite effects on the burst amplitude. Apamin increased both the motor period and the burst amplitude. A dose-response relationship was established for the K+ channel blockers. The blockers elicited an unstable rhythmic activity, contrary to what occurred under control conditions. We also found that due to the specific changes that they elicit, the various blockers produce selective changes in the burst ratio. These results suggest that the various K+ channels contribute differently to the generation of locomotor activity. 相似文献
35.
Amara Khan Fernanda Ramos-Gomes Andrea Markus Matthias Mietsch Rabea Hinkel Frauke Alves 《Biomedical optics express》2021,12(11):7009
Heart failure is one of the most common causes of morbidity and mortality. Both maturational abnormalities and age-associated cardiac pathologies contribute to heart failure. Imaging-based assessment to discern detailed cardiac structure at various maturational stages is imperative for understanding mechanisms behind cardiac growth and aging. Using multiphoton nonlinear optical microscopy (NLOM) based label-free imaging, we investigated cardiac structural composition in a human-relevant aging model, the common marmoset monkey (Callithrix jacchus). Animals were divided into three different age groups including neonatal, young adult and old. By devising a unique strategy for segregating collagen and myosin emitted second harmonic generation (SHG) signals, we performed a volumetric assessment of collagen and total scattering tissue (collagen + myosin). Aged marmoset hearts exhibited an increase in collagen and total scattering tissue volume at the sites of severe tissue remodelling indicating age-related cardiac fibrosis. Significantly low scattering tissue volume in neonatal marmoset hearts was attributed to a lack of binding between the myofibrils in maturing cardiac tissue. Comprehensive quantitative assessment of structural composition during maturation and aging of marmoset hearts revealed significant differences in myofibril length, alignment, curvature and angular distribution. In conclusion, label-free high-resolution NLOM facilitates visualization and quantification of subcellular structural features for understanding vital age-related morphological alterations in the marmoset heart. 相似文献
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Elizabeth S. Fernandes Fiona A. Russell Domenico Spina Jason J. McDougall Rabea Graepel Clive Gentry Amelia A. Staniland David M. Mountford Julie E. Keeble Marzia Malcangio Stuart Bevan Susan D. Brain 《Arthritis \u0026amp; Rheumatology》2011,63(3):819-829
Objective
To investigate the involvement of transient receptor potential ankyrin 1 (TRPA1) in inflammatory hyperalgesia mediated by tumor necrosis factor α (TNFα) and joint inflammation.Methods
Mechanical hyperalgesia was assessed in CD1 mice, mice lacking functional TRP vanilloid 1 (TRPV1−/−) or TRPA1 (TRPA1−/−), or respective wild‐type (WT) mice. An automated von Frey system was used, following unilateral intraplantar injection of TNFα or intraarticular injection of Freund's complete adjuvant (CFA). Knee swelling and histologic changes were determined in mice treated with intraarticular injections of CFA.Results
TNFα induced cyclooxygenase‐independent bilateral mechanical hyperalgesia in CD1 mice. The selective TRPV1 receptor antagonist SB‐366791 had no effect on mechanical hyperalgesia when it was coinjected with TNFα, but intrathecally administered SB‐366791 attenuated bilateral hyperalgesia, indicating the central but not peripheral involvement of TRPV1 receptors. A decrease in pain sensitivity was also observed in TRPV1−/− mice. Intraplantar coadministration of the TRPA1 receptor antagonist AP‐18 with TNFα inhibited bilateral hyperalgesia. Intrathecal treatment with AP‐18 also reduced TNFα‐induced hyperalgesia. CFA‐induced mechanical hyperalgesia in CD1 mice was attenuated by AP‐18 (administered by intraarticular injection 22 hours after the administration of CFA). Furthermore, intraarticular CFA–induced ipsilateral mechanical hyperalgesia was maintained for 3 weeks in TRPA1 WT mice. In contrast, TRPA1−/− mice exhibited mechanical hyperalgesia for only 24 hours after receiving CFA.Conclusion
Evidence suggests that endogenous activation of peripheral TRPA1 receptors plays a critical role in the development of TNFα‐induced mechanical hyperalgesia and in sustaining the mechanical hyperalgesia observed after intraaarticular injection of CFA. These results suggest that blockade of TRPA1 receptors may be beneficial in reducing the chronic pain associated with arthritis.38.
Flachsbart F Ufer M Kleindorp R Nikolaus S Schreiber S Nebel A 《The journals of gerontology. Series A, Biological sciences and medical sciences》2011,66(11):1186-1191
Cytochrome P450 enzymes, especially the CYP2C subfamily, are involved in the generation of reactive oxygen species and are regarded as susceptibility factors for age-related diseases. Furthermore, the CYP2C-encoding genes are known to be highly polymorphic, with a number of variants leading to changes in enzyme activity. These observations prompted us to investigate whether allelic variation in the CYP2C-encoding genes was associated with human longevity. In a comprehensive haplotype tagging approach, we genotyped 56 single nucleotide polymorphisms located in the CYP2C gene family (CYP2C8, CYP2C9, CYP2C18, and CYP2C19) in our extensive collection of 1,384 long-lived individuals (centenarians and nonagenarians) and 945 younger controls. None of the tested single nucleotide polymorphisms showed a significant association with the longevity phenotype at the allele, genotype, or haplotype level. These results suggest that there is no notable influence of sequence variation in the CYP2C genes on longevity in the examined German population. 相似文献
39.
Radoui A Al Hamany Z Skalli Z Haddiya I Hamzaoui H Bouattar T Rhou H Benamar L Ezzaitouni F Bayahia R Ouzeddoun N 《Néphrologie & thérapeutique》2010,6(7):559-563
AimPregnancies in women with lupus nephritis (LN) are a high-risk situation. The aim of this study is to evaluate the impact of pregnancy on LN on either maternal and fetal prognosis.Patients and methodsIt is a retrospective study of 20 pregnancies in 12 women with lupus nephritis.ResultsThere were 19 live births and five fetal losses. LN flares were observed in 50 % of the cases during pregnancy and 25 % after delivery.ConclusionPregnancies in women with LN require a multidisciplinary monitoring and intense maternal and fetal care. 相似文献
40.
Kunert Kathleen S. Blum Marcus Duncker Gernot I. W. Sietmann Rabea Heichel Jens 《Albrecht von Graefes Archiv fur klinische und experimentelle Ophthalmologie》2011,249(9):1417-1424