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《Journal of enzyme inhibition and medicinal chemistry》2013,28(1):80-86
Glycosidases play an important role in a wide range of physiological and pathological conditions, and have become potential targets for the discovery and development of agents useful for the treatment of diseases such as diabetes, cancer, influenza, and even AIDS. In this study, several benzimidazole derivatives were prepared from o-phenylenediamine and aromatic and heteroaromatic carboxaldehydes in very good yields, using PdCl2(CH3CN)2 as the most efficient catalyst. Synthesized compounds were assayed for their activity on yeast and rat intestinal α-glucosidase inhibition and cytotoxic activity against colon carcinoma cell line HT-29. Compound 3e exhibited 95.6% and 75.3% inhibition of yeast and rat intestinal α-glucosidase enzyme, while showing 74.8% cytotoxic activity against the HT-29 cell line at primary screening concentrations of 2.1?mM for yeast and rat intestinal α-glucosidase enzyme and 0.2?mM for cytotoxic activity against the HT-29 cell line, respectively. Compound 3c displayed 76% and 34.4% inhibition of yeast and rat intestinal α-glucosidase enzyme, and 80.4% cytotoxic activity against the HT-29 cell line at similar primary screening concentrations. The IC50 value for the most potent intestinal α-glucosidase inhibitor compound 3e was found to be 99.4?μM. The IC50 values for the most active cytotoxic compounds 3c and 3e were 82?μM and 98.8?μM, respectively. Both compounds displayed significant antihyperglycemic activity in starch-induced postprandial hyperglycemia in rats. This is the first report assigning yeast and rat intestinal α-glucosidase enzyme inhibition, cytotoxic activity against the HT-29 cell line, and antihyperglycemic activity to benzimidazole compounds 3c and 3e. 相似文献
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YSY-01A是一种新型蛋白酶体抑制剂,前期研究已经证实其对肿瘤细胞的增殖有抑制作用.但是它对肿瘤血管生成是否有影响尚不明确.本研究旨在探明YSY-01A阻碍肿瘤细胞促进血管生成的作用及机制.我们首先将磺酰罗丹明B(sulforhodamine B,SRB)法与细胞共培养(Transwell)模型相结合,探讨YSY-01A抑制人结肠癌细胞(HT-29 cells)对人脐静脉内皮细胞(human umbilical vein endothelial cells,HUVECs)的增殖促进作用;运用高内涵筛选(high content screening,HCS)法研究YSY-01A对HT-29细胞中NF-κB核转位的影响;利用Western blot法检测YSY-01A对HT-29细胞中缺氧诱导因子-1α(hypoxia- inducible factor-1α,HIF-1α)及血管内皮生长因子(vascular endothelial growth factor,VEGF)的表达调控.为了观察YSY-01A对HUVEC增殖和运动有无直接抑制作用,我们采用SRB法观察YSY-01A对HUVEC的增殖抑制作用;运用HCS法分别考察YSY-01A对HUVEC的运动抑制和细胞毒作用.结果证实,YSY-01A可以阻碍HT-29细胞对HUVEC的增殖促进作用并具有浓度依赖性.YSY-01A还可抑制HT-29细胞中NF-κB的核转位,下调HIF-1α及VEGF的表达.进一步研究证实,YSY-01A能够浓度依赖地抑制HUVECs的增殖和运动,而不伴有明显的细胞毒作用.上述结果表明,YSY-01A可以通过抑制蛋白酶体活性下调肿瘤细胞中促血管生成因子的表达,进而在血管内皮细胞中发挥抗血管生成作用. 相似文献
546.
Fouchier F Penel C Pierre Montero M Bremond P Champion S 《European journal of cell biology》2007,86(3):143-160
Mn(2+) was found to induce adhesion of HT29-D4 adenoma carcinoma cells to fibrinogen (Fb). This was independent of the expression of the beta3 integrin subunit and involved endogenous alphavbeta6 but not alphavbeta5 integrin. Thus, addition of Mn(2+) led to a change in integrin alphavbeta6 specificity. Furthermore, Mn(2+) was found to strongly activate the extracellular signal-regulated kinase/mitogen-activated protein kinase (ERK/MAPK) pathway in the HT29-D4 cell line. As a MAPK inhibitor strongly reduced the Mn(2+)-induced cell adhesion to Fb, it is suggested that a link between MAPK activation and cell adhesion to Fb exists. Both expression and activity of matrix metalloproteinase-9 (MMP-9) were enhanced by Mn(2+) and this led to Fb processing. MMP inhibitors prevented Mn(2+)-mediated cell adhesion to Fb, leading us to suggest that Mn(2+) promoted convergent changes in integrin alphavbeta6 conformation and Fb structure through activation of ERK/MAPK and MMP-9. Finally, we found that Mn(2+) and activators of the ERK pathway cooperated in HT29-D4 cell adhesion to Fb. Such a process may be involved in bone metastasis of some cancer cells. 相似文献
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Carla R. Angelani Lucrecia M. Curto Inés S. Cabanas Julio J. Caramelo Vladimir N. Uversky José M. Delfino 《Biochimica et Biophysica Acta - Proteins and Proteomics》2014,1844(9):1599-1607
Δ78Δ is a second generation functional all-β sheet variant of IFABP (intestinal fatty acid binding protein) corresponding to the fragment 29–106 of the parent protein. This protein and its predecessor, Δ98Δ (segment 29–126 of IFABP), were initially uncovered by controlled proteolysis. Remarkably, although IFABP and Δ98Δ are monomers in solution, Δ78Δ adopts a stable dimeric structure. With the aim of identifying key structural features that modulate the aggregation of β-proteins, we evaluate here the structure and aggregation propensity of Δ78Δ. The 2,2,2-trifluoroethanol (TFE) induced aggregation of this protein shows a primary nucleation–elongation mechanism, characterized by the stabilization of a dimeric nucleus. Its rate of production from the co-solvent induced aggregation prone state governs the kinetics of polymerization. In this context, the value of Δ78Δ lies in the fact that – being a stable dimeric species – it reduces an otherwise bimolecular reaction to a unimolecular one. Interestingly, even though Δ78Δ and IFABP display similar conformational stability, the abrogated form of IFABP shows an enhanced aggregation rate, revealing the ancillary role played on this process by the free energy of the native proteins. Δ78Δ share with IFABP and Δ98Δ a common putative aggregation-prone central peptide. Differences in the exposure/accessibility of this segment dictated by the environment around this region might underlie the observed variations in the speed of aggregation. Lessons learnt from this natural dimeric protein might shed light on the early conformational events leading to β-conversion from barrels to amyloid aggregates. 相似文献
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