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排序方式: 共有419条查询结果,搜索用时 15 毫秒
31.
目的探讨大黄酚对大鼠单侧输尿管梗阻模型(UUO)肾间质纤维化的影响。方法 27只SD大鼠随机分为假手术组、模型组、大黄酚组。用单侧输尿管梗阻术建立肾间质纤维化模型,大黄酚治疗14 d后检测血肌酐、尿素氮水平;采用免疫组织化学方法观察肾组织结缔组织生长因子(CTGF)、α-平滑肌肌动蛋白(α-SMA)、纤维连接蛋白(FN)的表达情况。结果与假手术组相比,模型组血肌酐、尿素氮的水平以及CTGF、α-SMA、FN的表达均显著增高。与模型组相比,大黄酚组血肌酐、尿素氮水平降低,CTGF、α-SMA、FN的阳性表达显著下调。结论大黄酚可能通过抑制UUO大鼠肾组织CTGF、α-SMA、FN的表达,从而缓解肾间质纤维化的发生发展。  相似文献   
32.
刘亮  周知午 《中南药学》2013,(12):890-892
目的 研究三七总苷对酒精性肝损伤大鼠肝脏TGF-β1/Smads和CTGF表达的影响。方法 大鼠灌服白酒-玉米油-吡唑混合液14周,建立酒精性肝损伤模型。成模大鼠随机分成模型组、三七总苷组(高、低剂量组)、水飞蓟素组,同时另设正常对照组,均治疗4周后,测定肝功能、大鼠肝组织TGF-β1、Smad3、Smad7、CTGFmRNA的表达量。结果 与模型组比较,三七总苷组能明显降低血清中谷丙转氨酶(ALT)、谷草转氨酶(AST)以及总胆红素(TB)水平,减少肝组织TGF-β1、Smad3、Smad7、CTGF mRNA的表达量;不同剂量组之间,差异有统计学意义(P〈0.05);高剂量三七总苷组与水飞蓟素组之间,差异无统计学意义(P〉0.05)。结论 三七总苷与对酒精性肝损伤大鼠肝脏TGF-β1/Smads、CTGF表达有抑制作用。  相似文献   
33.
Activation of proximal tubular cells by fibrotic and inflammatory mediators is an important hallmark of chronic kidney disease. We have developed a novel strategy to intervene in renal fibrosis, by means of locally delivered kinase inhibitors. Such compounds will display enhanced activity within tubular cells and reduced unwanted systemic effects. In our approach kinase inhibitors are linked to the renal carrier lysozyme using a platinum-based linker that binds drugs via a coordinative linkage. Many kinase inhibitors contain aromatic nitrogen atoms able to bind to this linker without the need of prior derivatization. The resulting drug-lysozyme conjugates are rapidly filtered in the glomerulus into the tubular lumen and subsequently reabsorbed via the endocytic pathway for clearance of low-molecular weight proteins. An important property of the formed conjugates is their in vivo stability and the sustained drug release profile within target cells. This review summarizes the state-of-the-art of drug targeting to the kidney. Furthermore, we will highlight recent results obtained with kinase inhibitor-lysozyme conjugates targeted to different kinases, i.e. the transforming growth factor (TGF)-beta-receptor kinase, p38 MAPkinase and Rho-associated kinase. Both in vitro and in vivo results demonstrated their efficient tubular uptake and beneficial therapeutic effects, superior to treatment with free kinase inhibitors. These proof-of-concept studies clearly indicate the feasibility of drug targeting for improving the renal specificity of kinase inhibitors.  相似文献   
34.
目的:探讨参地补肾胶囊对肾小球硬化大鼠BMP-7、CTGF表达的影响。方法:采用单侧肾脏切除同时尾静脉注射阿霉素的方法建立肾小球硬化大鼠模型,实验分为正常对照组、模型组、西药(洛汀新)对照组、中药(苏黄泄浊丸)组和参地补肾胶囊组,分组给药处理8周。检测各组大鼠24小时尿蛋白定量、血肌酐(SCr)、尿素氮(BUN)、血浆蛋白(ALB);光镜观察大鼠肾脏病理学变化;免疫组化法检测BMP-7、CTGF表达。结果:各治疗组大鼠24小时尿蛋白及血SCr、BUN、ALB较模型组明显改善(P0.05)。各给药组大鼠肾脏病理变化明显改善。各治疗组均能抑制CTGF的表达(P0.05),上调BMP-7表达(P0.05);参地补肾胶囊组作用明显优于两阳性对照组(P0.05)。结论:参地补肾胶囊对肾小球硬化大鼠肾功能具有保护作用,上调BMP-7表达、抑制CTGF表达可能是其部分作用机制。  相似文献   
35.
张新志  吴锋  何立群 《时珍国医国药》2011,22(12):2853-2855
目的 探讨抗纤灵冲剂防治肾间质纤维化可能的作用靶点及分子生物学机制.方法 将72只SPF级SD大鼠中54只行经典单侧输尿管结扎,制备UUO大鼠模型,造模成功后分为模型组、抗纤灵组、氯沙坦组.药物干预后分批于14d,21d,28d处死,留取左侧肾组织,运用PCR Array法,检测肾间质纤维化基因CTGF的阳性表达.结果 各时间点模型组CTGF基因水平分别较假手术组上调7.12倍、8.26倍及6.55倍,均>2倍,具有非常显著差异.各时间点抗纤灵组CTGF基因表达分别比模型组下调1.79倍、1.63倍、1.63倍,下调均>1.5倍,具有明显差异.结论 抗纤灵冲剂作用靶点及分子生物学机制之一是有效诱导CTGF基因表达下调而发挥抗肾间质纤维化效应.  相似文献   
36.
37.
目的通过检测脑胶质瘤患者肿瘤组织中血管内皮生长因子和结缔组织生长因子的表达水平,探讨其和肿瘤级别的关系及作用机制。方法应用免疫组化SP法检测49例胶质瘤手术标本中的VEGF和CTGF的表达水平,统计分析表达水平和肿瘤级别之间的关系。结果VEGF和CTGF在胶质瘤高级别组(Ⅲ-Ⅳ级)中的表达均明显高于低级别组(Ⅰ-Ⅱ级),说明随着肿瘤级别的升高VEGF和CTGF表达也增强。结论VEGF和CTGF在胶质瘤组织中高表达,而且表达水平和恶性程度有密切联系。VEGF和CTGF的检测可作为胶质瘤恶性程度判断的参考,为从基因水平上探讨胶质瘤的生物学行为、预后及治疗提供新的思路。  相似文献   
38.
目的:观察结缔组织生长因子(CTGF)在非小细胞肺癌(NSCLC)组织和正常肺组织中表达的差异性,并初步探讨CTGF表达与NSCLC恶性程度、侵袭和转移的关系。方法:采用免疫组织化学法(S-P法)检测50例NSCLC和10例正常肺组织中CTGF的表达情况,并分析CTGF与NSCLC患者临床病理特征之间的关系,以及CTGF在NSCLC组织中表达的相关性。结果:在50例NSCLC组织中有15例(30%)CTGF呈阳性表达,10例正常肺组织中有9例为阳性表达;统计结果显示,CTGF表达与NSCLC的临床分期(P=0.005)、淋巴结转移(P=0.04)有相关性。结论:CTGF在NSCLC组织中的表达较正常肺组织明显下调,与NSCLC的临床分期和淋巴结转移有相关性,提示CTG可能与NSCLC的侵润和转移有关。  相似文献   
39.
Tissue factor (TF) initiates the protease coagulation cascade in response to tissue injury. Homozygous deficiency of murine TF results in embryonic lethality, which is rescued by low-level expression of human TF. These low-TF mice have been shown to develop cardiac fibrosis. We tested the hypothesis that the development of cardiac fibrosis in low-TF mice results from dysregulated protease expression and is affected by gender. Mice were divided into the age groups 2-5, 6-12, 13-18 and 19+ weeks. Fibrosis was assessed by trichrome staining. Protease expression was measured in male and female mice by RT-PCR for mRNA and zymography, ELISA or immunoblot for protein. Urokinase plasminogen activator (uPA) activity was determined by zymography and chromogenic substrate assay. A marked gender effect was noted for the development of fibrosis, with interstitial collagen deposition occurring from 9 weeks in male low-TF mice, but not until 19 weeks in low-TF females. This delayed onset in females was accompanied by delayed up-regulation of molecular markers of injury. Matrix metalloproteinase (MMP)-3 and tissue inhibitor of metalloproteinase (TIMP)-1 expression were up-regulated in the hearts of male low-TF mice from 6 to 12 weeks and in females from 19 weeks. MMP/TIMP dysregulation was not seen prior to cardiac fibrosis and did not appear to explain the gender differences. However, uPA expression and activity were down-regulated prior to cardiac fibrosis in low-TF females, but were up-regulated in age-matched males. This suggests that the down-regulation of uPA in female low-TF mice protects them from more severe cardiac fibrosis.  相似文献   
40.
PURPOSE: To investigate whether pravastatin mitigates delayed radiation-induced enteropathy in rats, by focusing on the effects of pravastatin on acute cell death and fibrosis according to connective tissue growth factor (CTGF) expression and collagen inhibition. METHODS AND MATERIALS: Mitigation of delayed radiation-induced enteropathy was investigated in rats using pravastatin administered in drinking water (30 mg/kg/day) 3 days before and 14 days after irradiation. The ileum was irradiated locally after surgical exteriorization (X-rays, 19 Gy). Acute apoptosis, acute and late histologic alterations, and late CTGF and collagen deposition were monitored by semiquantitative immunohistochemistry and colorimetric staining (6 h, 3 days, 14 days, 15 weeks, and 26 weeks after irradiation). Pravastatin antitumor action was studied in HT-29, HeLa, and PC-3 cells by clonogenic cell survival assays and tumor growth delay experiments. RESULTS: Pravastatin improved delayed radiation enteropathy in rats, whereas its benefit in acute and subacute injury remained limited (6 h, 3 days, and 14 days after irradiation). Delayed structural improvement was associated with decreased CTGF and collagen deposition but seemed unrelated to acute damage. Indeed, the early apoptotic index increased, and severe subacute structural damage occurred. Pravastatin elicited a differential effect, protecting normal intestine but not tumors from radiation injury. CONCLUSION: Pravastatin provides effective protection against delayed radiation enteropathy without interfering with the primary antitumor action of radiotherapy, suggesting that clinical transfer is feasible.  相似文献   
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