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A perivascular origin for mesenchymal stem cells in multiple human organs   总被引:4,自引:0,他引:4  
Mesenchymal stem cells (MSCs), the archetypal multipotent progenitor cells derived in cultures of developed organs, are of unknown identity and native distribution. We have prospectively identified perivascular cells, principally pericytes, in multiple human organs including skeletal muscle, pancreas, adipose tissue, and placenta, on CD146, NG2, and PDGF-Rbeta expression and absence of hematopoietic, endothelial, and myogenic cell markers. Perivascular cells purified from skeletal muscle or nonmuscle tissues were myogenic in culture and in vivo. Irrespective of their tissue origin, long-term cultured perivascular cells retained myogenicity; exhibited at the clonal level osteogenic, chondrogenic, and adipogenic potentials; expressed MSC markers; and migrated in a culture model of chemotaxis. Expression of MSC markers was also detected at the surface of native, noncultured perivascular cells. Thus, blood vessel walls harbor a reserve of progenitor cells that may be integral to the origin of the elusive MSCs and other related adult stem cells.  相似文献   
64.
于永光  赵斌 《微生物学报》2008,27(2):209-216
设计在不同pH水平(4.3、5.1、5.8、6.8)下两种VA菌根真菌Glomus mosseae和Gigaspora margarita对紫云英Astragalus sinicus进行单接种、混合接种及无接种对照的盆栽实验。对紫云英地上和地下部分生物量、根部侵染率、SDH和ALP酶活进行了检测。实验结果表明:紫云英的生长效应与VA菌根真菌的侵染率及两种酶活成明显相关性。土壤pH升高,单接种Glomus mosseae和混合接种的侵染率也随之升高,而单接种Gigaspora margarita的侵染率呈现  相似文献   
65.
Huo X  Qi X  Tang F  Zu R  Li L  Wu B  Qin Y  Ji H  Fu J  Wang S  Tian H  Hu Z  Yang H  Zhou M  Wang H  Zhu F 《PloS one》2011,6(3):e17995

Background

We investigated the seropositive rates and persistence of antibody against pandemic (H1N1) 2009 virus (pH1N1) in pregnant women and voluntary blood donors after the second wave of the pandemic in Nanjing, China.

Methodology/Principal Findings

Serum samples of unvaccinated pregnant women (n = 720) and voluntary blood donors (n = 320) were collected after the second wave of 2009 pandemic in Nanjing. All samples were tested against pH1N1 strain (A/California/7/2009) with hemagglutination inhibition assay. A significant decline in seropositive rates, from above 50% to about 20%, was observed in pregnant women and voluntary blood donors fifteen weeks after the second wave of the pandemic. A quarter of the samples were tested against a seasonal H1N1 strain (A/Brisbane/59/2007). The antibody titers against pH1N1 strain were found to correlate positively with those against seasonal H1N1 strain. The correlation was modest but statistically significant.

Conclusions and Significance

The high seropositive rates in both pregnant women and voluntary blood donors suggested that the pH1N1 virus had widely spread in these two populations. Immunity derived from natural infection seemed not to be persistent well.  相似文献   
66.
同尾酶技术在构建疟疾多价重组DNA疫苗中的应用   总被引:6,自引:0,他引:6  
同尾酶是一类识别不同核苷酸序列但能酶切产生相同粘性末端的限制性内切酶,依靠同尾酶的这种特性,可以根据需要将不同的DNA 片段进行灵活组合,获得各种排列顺序的多价表位重组疫苗.将这种方法用于疟疾多价重组DNA 疫苗的研制;BALB/c 小鼠免疫实验对所得重组疫苗PU286的免疫原性进行了测定.  相似文献   
67.

Background

Cancer stem cells (CSCs) are highly proliferative and tumorigenic, which contributes to chemotherapy resistance and tumor occurrence. CSCs specific therapy may achieve excellent therapeutic effects, especially to the drug-resistant tumors.

Results

In this study, we developed a kind of targeting nanoparticle system based on cationic albumin functionalized with hyaluronic acid (HA) to target the CD44 overexpressed CSCs. All-trans-retinoic acid (ATRA) was encapsulated in the nanoparticles with ultrahigh encapsulation efficiency (EE%) of 93% and loading content of 8.37%. TEM analysis showed the nanoparticles were spherical, uniform-sized and surrounded by a coating layer consists of HA. Four weeks of continuously measurements of size, PDI and EE% revealed the high stability of nanoparticles. Thanks to HA conjugation on the surface, the resultant nanoparticles (HA-eNPs) demonstrated high affinity and specific binding to CD44-enriched B16F10 cells. In vivo imaging revealed that HA-eNPs can targeted accumulate in tumor-bearing lung of mouse. The cytotoxicity tests illustrated that ATRA-laden HA-eNPs possessed better killing ability to B16F10 cells than free drug or normal nanoparticles in the same dose, indicating its good targeting property. Moreover, HA-eNPs/ATRA treatment decreased side population of B16F10 cells significantly in vitro. Finally, tumor growth was significantly inhibited by HA-eNPs/ATRA in lung metastasis tumor mice.

Conclusions

These results demonstrate that the HA functionalized albumin nanoparticles is an efficient system for targeted delivery of antitumor drugs to eliminate the CSCs.
  相似文献   
68.
核桃-小麦复合系统中细根生长动态及竞争策略   总被引:3,自引:0,他引:3  
以核桃(Juglans regia)-小麦(Triticum aestivum)间作复合系统为研究对象,用微根窗和根钻相结合的方法采样,研究复合系统中核桃和小麦细根年内年际的生长动态和竞争适应策略,为农林复合系统的经营管理和竞争模型的建立提供理论依据和技术支持。结果表明,间作核桃和小麦根系均在上半年有一个大的生长高峰(5月和4月),在下半年有一个小的生长高峰(9月和11月),二者的竞争主要发生在上半年的大生长高峰期。在各年份各土层,间作核桃的根长密度均低于单作核桃,且在从第7年开始存在显著差异。在0—20 cm土层间作小麦根长密度在第3—7年间获得迅速提高,从第7年开始显著高于单作小麦,但在20 cm以下土层则相反。间作使核桃和小麦细根生态位实现了分离,11年的观察期内间作核桃比单作核桃细根的垂直分布中心下移了6.59 cm,间作小麦比单作小麦的上移了8.59 cm。在根系竞争策略方面,小麦根系是通过短期内的快速生长,迅速占据土壤空间获得竞争优势;而核桃根系是通过根系的逐年积累,逐步占据土壤空间从而获得竞争优势。可以干扰核桃根系积累过程的"竞争-干扰-再平衡"农林复合经营管理策略可以让复合系统中核桃和小麦保持各自竞争优势的情况下实现共存。在根系形态方面,自身细根直径较小者小麦在剧烈竞争区域以增加细根直径减小比根长来适应竞争,而自身细根直径较大者核桃则相反。  相似文献   
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70.
Obesity and its associated metabolic disorders such as diabetes, hepatic steatosis and chronic heart diseases are affecting billions of individuals. However there is no satisfactory drug to treat such diseases. In this study, we found that alisol A, a major active triterpene isolated from the Chinese traditional medicine Rhizoma Alismatis, could significantly attenuate high‐fat‐diet‐induced obesity. Our biochemical detection demonstrated that alisol A remarkably decreased lipid levels, alleviated glucose metabolism disorders and insulin resistance in high‐fat‐diet‐induced obese mice. We also found that alisol A reduced hepatic steatosis and improved liver function in the obese mice model.In addition, protein expression investigation revealed that alisol A had an active effect on AMPK/ACC/SREBP‐1c pathway. As suggested by the molecular docking study, such bioactivity of alisol A may result from its selective binding to the catalytic region of AMPK.Therefore, we believe that Alisol A could serve as a promising agent for treatment of obesity and its related metabolic diseases.  相似文献   
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