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排序方式: 共有341条查询结果,搜索用时 187 毫秒
1.
Relationships between Activators and Inhibitors of Plasminogen, and the Progression of Small Abdominal Aortic Aneurysms 总被引:1,自引:0,他引:1
J. S. Lindholt B. Jrgensen G. -P. Shi E. W. Henneberg 《European journal of vascular and endovascular surgery》2003,25(6):546-551
OBJECTIVE: plasmin is a common activator of the known proteolytic systems involved in the aneurysmal degradation, and is reported to be associated with the expansion of abdominal aortic aneurysms (AAA). The aim of this study was to study the activating pathways of plasminogen as predictors of the progression of AAA. MATERIALS AND METHODS: one hundred and twelve of 122 male patients with a small AAA (def.: +3cm) were interviewed, examined, had blood samples taken at diagnosis, and scanned annually for 1-5 years (mean 3.5 years), and referred for surgery if the AAA exceeded 5cm in diameter.A random sample of 70 of the 112 cases had plasma levels of urokinase-like-plasminogen activator (uPA), tissue-type-plasminogen activator (tPA), plasminogen-activator-inhibitor-1 (PAI-1), macrophage inhibiting factor (MIF), tumour-growth-factor-beta1 (TGF-beta1), homocysteine, and serum levels of IgA-antibodies against Chlamydia pneumoniae (IgA-CP) and Cotinine (a nicotine metabolite) measured. Spearmans correlation analysis was used for statistics. RESULTS: the annual expansion rate correlated positively with tPA, IgA-CP and S-Cotinine; r =0.37 (p=0.002), 0.29 (p=0.006) and 0.24 (p=0.038), while PAI1, uPA, TGF-beta1, homocysteine, and MIF did not. S-Cotinine did also correlate positively with tPA, r=0.24 (p=0.049). CONCLUSION: the aortic matrix degradation in AAA may be partly caused by an activation of plasminogen by tPA, but apparently not by uPA, which usually dominates matrix degradation. Smoking seems to be a factor for this pathway, while the pathways of IgA-CP and MIF, a new marker of aneurysmal progression, seem different. The latter observations suggest that other proteolytic pathways are involved in the aortic wall degradation in AAA. 相似文献
2.
检测切应力作用下肾近端小管上皮细胞纤溶酶原激活物tPA和uPA mRNA表达的变化,探讨糖尿病肾病早期小管间质细胞外基质重塑的可能机制.用5 dyn/cm2和10 dyn/cm2的切应力处理肾近端小管上皮细胞(NRK-52E),作用时间分别为1、3和6 h,用RT-PCR法检测tPA及uPA mRNA的表达.结果表明:切应力呈大小和时间依赖性下调肾小管上皮细胞tPA及uPA mRNA的表达.在糖尿病肾病早期,高滤过引起的切应力增加可抑制肾近端小管上皮细胞tPA和uPA mRNA表达,导致肾小管间质纤维蛋白溶解活性降低,参与小管间质细胞外基质的重塑. 相似文献
3.
tPA信号肽和鼠疫杆菌保护性抗原V融合基因的构建及免疫效果鉴定 总被引:1,自引:0,他引:1
获得含有鼠疫杆菌V抗原编码基因以及tPA信号肽编码序列的重组质粒,并测定其诱导特异性免疫应答的能力。采用PCR扩增鼠疫菌杆菌V基因构建到pVAX1质粒中产生pVAX1/V重组质粒,PCR扩增tPA信号肽编码序列片段并将其插入到pVAX1/V中V基因的上游,构建tPA-pVAX1/V重组质粒;转染COS-7细胞,免疫细胞化学方法鉴定V蛋白的表达;二重组质粒分别加mGM-CSF质粒免疫BALB/c小鼠,观察免疫应答反应;以400个LD50强毒鼠疫杆菌皮下攻击免疫小鼠观察保护效率。结果显示,tPA-pVAX1/V在COS-7细胞中表达了V蛋白;免疫小鼠血清产生了特异性抗体和细胞免疫应答;攻毒保护率达80%。成功构建了分泌型V蛋白的真核表达质粒载体,具有诱导特异性细胞免疫和体液免疫应答的能力,对强毒鼠疫杆菌攻毒有一定的保护效力,为鼠疫杆菌新型疫苗研制奠定了基础。 相似文献
4.
Komai S Matsuyama T Matsumoto K Kato K Kobayashi M Imamura K Yoshida S Ugawa S Shiosaka S 《The European journal of neuroscience》2000,12(4):1479-1486
We found that neuropsin, an extracellular matrix serine protease, has a regulatory effect on Schaffer-collateral long-term potentiation (LTP) in the mouse hippocampus. Bath application of 1-170 nM recombinant neuropsin modulated early phase LTP in the Schaffer-collateral pathway with a 'bell-shape' dose-response curve. The maximum enhancing activity (134% of control LTP) was found at approximately 2.5 nM. Bath application of a neutralizing antibody against neuropsin in the hippocampal slice resulted in a marked inhibition of the tetanus-induced early phase of LTP. The in vivo continuous intraventricular infusion of an antisense oligonucleotide against neuropsin significantly reduced the amplitude of the tetanus-induced early phase of LTP in vitro. Neuropsin did not directly change the N-methyl D-aspartate (NMDA) current. Thus, neuropsin appears to act as a regulatory molecule in the early phase of LTP via its proteolytic function on extracellular matrix rather than affecting NMDA receptor-mediated calcium increase. 相似文献
5.
目的:观察丹参注射液对糖尿病患者内皮tPA、NO储备和血管舒张功能的作用.方法:对32例Ⅱ型糖尿病患者和16例正常人,采用高频超声方法测定血管内皮依赖性和非依赖性舒张功能和颈总动脉内膜厚度,采用静脉闭塞试验测定tPA和NO储备释放.结果:糖尿病组内皮依赖性舒张功能降低,NO、tPA释放减少,且有高血压组比无高血压组降低更甚,与正常组相比,P<0.01或0.05,而三组非依赖性血管舒张功能差异无显著性.糖尿病组颈总动脉内膜厚度增加,无高血压组与正常人相比差异无显著性,但有高血压组与正常人相比,P<0.05.在应用丹参注射液治疗后,糖尿病组患者内皮依赖性舒张功能增强,NO、tPA释放水平升高,与治疗前相比,P<0.01或0.05,有显著性差异.结论:丹参注射液能有效地改善血管内皮细胞tPA、NO储备释放功能和内皮依赖性舒张功能,改善糖尿病微血管病变. 相似文献
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8.
Mark W. Gramling 《Thrombosis research》2010,125(5):377-381
In hemostasis, the serine protease inhibitor (serpin) plasminogen activator inhibitor-1 (PAI-1) functions to stabilize clots via inhibition of tissue plasminogen activator (tPA) with subsequent inhibition of fibrinolysis. In tissues, PAI-1 functions to inhibit extracellular matrix degradation via inhibition of urokinase plasminogen activator (uPA). Elevated levels of PAI-1 in the vasculature and in tissues have long been known to be associated with thrombosis and fibrosis, respectively. However, there is emerging evidence that PAI-1 may participate in the pathophysiology of a number of diseases such as atherosclerosis, restenosis, and cancer. In many of these disease states, the canonical view of PAI-1 as an inhibitor of tPA and uPA cannot fully account for a mechanism whereby PAI-1 contributes to the disease. In these cases, one must consider recent data, which indicates PAI-1 can directly promote pro-proliferative and anti-apoptotic signaling in a variety of cell types. Given the wide variety of inflammatory, hormonal, and metabolic signals that increase PAI-1 expression, it is important to consider mechanisms by which PAI-1 can directly participate in disease etiology. 相似文献
9.
Richard Camara Nathanael Matei John H Zhang 《Journal of cerebral blood flow and metabolism》2021,41(5):945
While the time window for reperfusion after ischemic stroke continues to increase, many patients are not candidates for reperfusion under current guidelines that allow for reperfusion within 24 h after last known well time; however, many case studies report favorable outcomes beyond 24 h after symptom onset for both spontaneous and medically induced recanalization. Furthermore, modern imaging allows for identification of penumbra at extended time points, and reperfusion risk factors and complications are becoming better understood. Taken together, continued urgency exists to better understand the pathophysiologic mechanisms and ideal setting of delayed recanalization beyond 24 h after onset of ischemia. 相似文献
10.
Cardiopulmonary dirofilariosis is a cosmopolitan disease caused by Dirofilaria immitis, a filaroid parasite whose adult worms live for years in the vascular system of its host. Previous studies have shown that D. immitis can use their excretory/secretory (ES) and surface antigens to enhance fibrinolysis, which could limit the formation of clots in its surrounding environment. Moreover, several isoforms of the glyceraldehyde 3-phosphate dehydrogenase (GAPDH) and galectin (GAL) were identified in both antigenic extracts as plasminogen-binding proteins. The aim of this work is to study the interaction of the GAPDH and GAL of D. immitis with the fibrinolytic system of the host. This study includes the cloning, sequencing and expression of the recombinant forms of the GAPDH and GAL of D. immitis (rDiGAPDH and rDiGAL) and the analysis of their capacity as plasminogen-binding proteins. The results indicate that rDiGAPDH and rDiGAL are able to bind plasminogen and stimulate plasmin generation by tissue plasminogen activator (tPA). This interaction needs the involvement of lysine residues, many of which are located externally in both proteins as have been shown by the molecular modeling of their secondary structures. In addition, we show that rDiGAPDH and rDiGAL enhance the expression of the urokinase-type plasminogen activator (uPA) on canine endothelial cells in culture and that both proteins are expressed on the surface of D. immitis in close contact with the blood of the host. These data suggest that D. immitis could use the associated surface GAPDH and GAL as physiological plasminogen receptors to shift the fibrinolytic balance towards the generation of plasmin, which might constitute a survival mechanism to avoid the clot formation in its intravascular habitat. 相似文献