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101.
摘要 目的:建立植入了骨修复材料小型猪腰椎椎体骨组织标本的不脱钙病理组织切片制备方法。方法:将含骨修复材料的腰椎椎体骨组织标本进行分割暴露组织切面,梯度浓度乙醇脱水后经Technovit 7200 VLC光聚树脂浸润,经黄蓝光共同辐照进行光聚合包埋,借助硬组织病理切磨系统制备含骨修复材料不脱钙病理组织切片。结果:结果显示通过上述方法制备的病理组织切片,经苏木精-伊红(HE)染色及甲苯胺蓝染色后光学显微镜下观察能较好地显示骨的各种组织细胞结构,可清晰的观察到骨小梁的走向及连接情况。结论:研究建立了含骨修复材料骨组织标本病理组织切片制备方法,实现了含骨修复材料不脱钙骨组织病理切片的制备,经病理染色后实现了带植入物的组织学观察,为生物材料及医疗器械动物试验研究提供了新的病理检测手段及组织学评价途径。  相似文献   
102.
摘要 目的:探讨参苓白术散联合针刺对溃疡性结肠炎大鼠内质网应激、炎症反应的作用机制。方法:采用三硝基苯磺酸的方法构建溃疡性结肠炎大鼠模型。给予大鼠参苓白术散联合针刺干预。采用ELISA法检测大鼠病变结肠的炎症反应和氧化应激水平;采用肉眼观察各组结肠组织形态学评分;采用Western blot 检测大鼠内质网应激相关蛋白的表达。结果:与空白组相比,模型组、针刺组、参苓白术散、参苓白术散组联合针刺组大鼠体质量更低(P<0.05);与模型组相比,针刺组、参苓白术散、参苓白术散组联合针刺组溃疡指数评分和大鼠体质量更低(P<0.05),且参苓白术散组联合针刺组明显低于针刺组和参苓白术散组;与空白组相比,模型组、针刺组、参苓白术散、参苓白术散组联合针刺组ROS、GSH-Px、MDA更高(P<0.05);与模型组相比,针刺组、参苓白术散、参苓白术散组联合针刺组ROS、GSH-Px、MDA更低(P<0.05),且参苓白术散组联合针刺组明显低于针刺组和参苓白术散组;与空白组相比,模型组、针刺组、参苓白术散、参苓白术散组联合针刺组TNF-α、IL-1β、IL-18更高(P<0.05);与模型组相比,针刺组、参苓白术散、参苓白术散组联合针刺组TNF-α、IL-1β、IL-18更低(P<0.05),且参苓白术散组联合针刺组低于针刺组和参苓白术散组;与空白组相比,模型组、针刺组、参苓白术散、参苓白术散组联合针刺组GRP78、p-PERK、p-eIF2α更高(P<0.05);与模型组相比,针刺组、参苓白术散、参苓白术散组联合针刺组GRP78、p-PERK、p-eIF2α更低(P<0.05),且参苓白术散组联合针刺组明显低于针刺组和参苓白术散组。结论:参苓白术散组联合针刺可有效抑制溃疡性结肠炎大鼠内质网应激,进而抑制炎症反应和氧化应激反应,并促进溃疡性结肠炎大鼠病变病情转归。  相似文献   
103.
The action of rotameric probes introduced either in position 7 or 8 in the sequence of substance P (SP) was investigated, i.e. -tetrahydroisoquinoleic acid (Tic), -fluorenylglycine (Flg), -diphenylalanine (Dip), the diastereoisomers of -1-indanylglycine (Ing) and -benz[ƒ]indanylglycine (Bfi), the Z- and E-isomers of dehydrophenylalanine and dehydronaphthylalanine (ΔZPhe, ΔEPhe, ΔZNal, ΔENal) and (Dmp). The aim of this study was the topographical characterization of the binding subsites of human NK-1 receptor expressed in CHO cells, especially the S7 and S8 subsites, corresponding to residues Phe7 and Phe8 of substance P. According to the binding potencies of these substituted-SP analogues, the S7 binding subsite is smaller than the S8 subsite: the S7 subsite accepts only one aromatic nucleus, while the S8 can accommodate three coplanar nuclei altogether. These findings are compatible with the idea that the S8 binding subsite may reside in the extracellular loops of the hNK-1 receptor. NK-1 agonists bind to human NK-1 receptor and activate the production of both inositol phosphates and cyclic AMP. As already quoted for septide, [pGlu6, Pro9]SP(6–11), discrepancies are observed between affinity (Ki) and activity (EC50) values for IPs production. While a weak correlation between Ki and EC50 values for IPs production could be found (r = 0.70), an excellent correlation could be demonstrated between their affinities (Ki) and their potencies (EC50) for cAMP production (r = 0.97). The high potency (EC50) observed for ‘septide-like’ molecules on PI hydrolysis, compared to their affinity is not an artefact related to the high level of NK-1 receptors expressed on CHO cells since a good correlation was found between EC50 values obtained for PI hydrolysis and those measured for spasmogenic activity in guinea pig ileum bioassay (r = 0.94).

According to the binding potencies of constrained analogues of phenylalanine, the S7 binding subsite of human NK-1 receptor is small, whereas the S8, which can accommodate three coplanar nuclei, might probably reside in the extracellular loop. The discrepancies observed between affinity (Ki) and activity (EC50) values for IPs production are not an artefact of CHO cells since a good correlation was found between EC50 for PI hydrolysis and those measured in guinea pig ileum bioassay.  相似文献   

104.
提出神经元胞浆转运的两相流模型,对胞浆快转运和慢转运进行统一的流体力学描述,给出微粒转运与胞浆流动的定量关系。  相似文献   
105.
建立了多组多滞后区间系数定常非线性控制系统的结构概念,采用鲁棒镇定的等价法,给出了具有扰动结构参数的多组多滞后区问系数定常非线性关联控制大系统的结构与关联鲁棒镇定,同时给出了扰动参数与滞后非线性项界线的估价公式。  相似文献   
106.
The cytoskeletal events that assist restitution of the native intestinal epithelium are poorly understood. To enhance our understanding of repair mechanisms in the native intestinal epithelium we assessed the functional role of actin and the temporal and spatial alterations in actin and villin that occur in native enterocytes migrating in response to injury. Using a well-characterizedin vitroUssing chamber model of native intestine epithelial restitution, the actin inhibitor cytochalasin D (CD) was applied to determine the functional importance of actin to restitution as assessed by sensitive electrophysiological means and structural techniques. Additionally we used phalloidin and indirect immunohistochemistry to localize and semi-quantitate F-actin and villin in migrating cells during restitution. We report new data that shows that when cytoskeletal changes were impaired with CD, the epithelial monolayer was re-established in fewer than 20% of CD-treated villi, cells bordering the epithelial defect did not assume the characteristic phenotype associated with migrating cells, and transepithelial resistance did not return to pre-injury levels. F-actin and villin were present at the leading edge of the migrating cells, basolateral F-actin was decreased, and cytoplasmic villin was increased as determined by phalloidin and immunohistochemical methods. We conclude thatin vitrorepair of the native intestinal epithelium is functionally and structurally dependent on major changes in the cytoskeleton of cells involved in re-establishing the epithelial monolayer over a complex extracellular matrix.  相似文献   
107.
旱地玉米农田棵间蒸发研究   总被引:3,自引:0,他引:3  
采用中子微区模拟装置测量旱地玉农田棵间蒸发,实验表明,本实验装置实用可行。晋西棵间蒸发量占降水量(510nm)的55%以上,棵间蒸发与蒸散的比值同时叶面积指数呈反相关,玉米产量与作物蒸腾呈正相关。  相似文献   
108.
Existing risk assessment procedures for carcinogens are intended to be “conservative” in the uncertainty dimension—giving estimates that are expected to be higher than true risks for typical people. However, these procedures do not consider the likely variability in susceptibility among individual people. This paper updates previous estimates of the likely extent of this variability for metabolically activated, genetically-acting carcinogens based on recent information on human interindividual variability in metabolic activation, detoxification, and DNA repair. The resulting expected skewness of cancer risk distributions is estimated using Monte Carlo simulations of both variability and uncertainty.

Some risk management implications are:

  1. When evaluating the fairness of a particular risk distribution, managers need to gain familiarity with a three-dimensional characterization—X level of risk, for the Yth percentile individual (addressing variability) with Z degree of confidence (addressing uncertainty).

  2. To the extent that variability distributions are skewed (e.g., with a long tail extending to high values) population mean risks will tend to exceed risks for median individuals. Together with the skewness in uncertainty distributions, this implies that “expected value” estimates of aggregate population risks—the estimates of interest for cost benefit analyses—are likely to be closer to traditional upper confidence limit risk estimates than has often been assumed in the past.

 

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