首页 | 本学科首页   官方微博 | 高级检索  
文章检索
  按 检索   检索词:      
出版年份:   被引次数:   他引次数: 提示:输入*表示无穷大
  收费全文   38694篇
  免费   3591篇
  国内免费   5394篇
  47679篇
  2024年   126篇
  2023年   529篇
  2022年   1246篇
  2021年   1992篇
  2020年   1433篇
  2019年   1833篇
  2018年   1695篇
  2017年   1308篇
  2016年   1799篇
  2015年   2592篇
  2014年   3086篇
  2013年   3207篇
  2012年   3871篇
  2011年   3523篇
  2010年   2239篇
  2009年   1974篇
  2008年   2249篇
  2007年   2038篇
  2006年   1762篇
  2005年   1468篇
  2004年   1191篇
  2003年   1124篇
  2002年   943篇
  2001年   624篇
  2000年   529篇
  1999年   485篇
  1998年   320篇
  1997年   295篇
  1996年   269篇
  1995年   214篇
  1994年   209篇
  1993年   145篇
  1992年   176篇
  1991年   128篇
  1990年   123篇
  1989年   112篇
  1988年   87篇
  1987年   79篇
  1986年   77篇
  1985年   85篇
  1984年   45篇
  1983年   41篇
  1982年   48篇
  1981年   32篇
  1979年   37篇
  1978年   22篇
  1977年   23篇
  1974年   22篇
  1973年   29篇
  1971年   21篇
排序方式: 共有10000条查询结果,搜索用时 19 毫秒
991.
A useful strategy for identifying ligand binding domains of G protein-coupled receptors has been the exploitation of species differences in antagonist potencies. We have used this approach for the CCR1 chemokine receptor with a novel series of antagonists, the 4-hydroxypiperidines, which were discovered by high throughput screening of human CCR1 and subsequently optimized. The structure-activity relationships for a number of different 4-hydroxypiperidine antagonists for human and mouse CCR1 were examined by receptor binding and functional assays. These compounds exhibit major differences in their rank order of potency for the human and mouse chemokine receptor CCR1. For example, the initial lead template, BX 510, which was a highly potent functional antagonist for human CCR1 (K(i) = 21 nM) was >400-fold less active on mouse CCR1 (K(i) = 9150 nM). However, increasing the length of the linker between the piperidine and dibenzothiepine groups by one methylene group generated a compound, BX 511, which was equipotent for both human and mouse CCR1. These and other analogs of the lead template BX 510, which have major differences in potency for human and mouse CCR1, are described, and a model for their interaction with human CCR1 is presented.  相似文献   
992.
In mouse and human, precursors of NK cell lineage home to decidualizing uteri. To assess the requirement for IL-15, an essential cytokine for NK differentiation in lymphoid tissue, on uterine NK (uNK) cell differentiation, implantation sites from IL-15(-/-) mice were analyzed histologically. IL-15(-/-) implantation sites had no uNK cells, no spiral-artery modification, and lacked the decidual integrity found in normal mice. IL-15(-/-) recipients of C57BL/6 marrow displayed similar pathology. However, implantation sites from recombination-activating gene-2(-/-)gamma(c)(-/-) (alymphoid) recipients of IL-15(-/-) marrow showed normal uNK cells, modified spiral arteries, and well-developed decidua basalis. Deletion of the IFN-regulatory factor (IRF)-1, but not IRF-2 (factors important in peripheral NK cell differentiation) limited but did not prevent uNK cell development. In situ hybridization localized IRF-1 largely to placental trophoblast cells. IRF-1(-/-) marrow transplanted into recombination-activating gene-2(-/-)gamma(c)(-/-) displayed competence for full uNK cell differentiation. IL-15 mRNA expression at implantation sites of IRF-1(-/-) and C57BL/6 was similar, suggesting that, unlike in bone marrow and spleen, IRF-1 does not regulate IL-15 in the pregnant uterus. Terminal differentiation of uNK cells was not promoted in pregnant IRF-1(-/-) mice by 5-day infusion of murine rIL-15, suggesting that IRF-1 deficiency rather than IL-15 deficiency limits uNK cell differentiation in these mice. Further, IRF-1 regulates placental growth, birth weight, and postnatal growth of offspring. These studies indicate that uNK cell development and maturation share some aspects with NK cell development in other tissues, but also display distinctive tissue-specific regulation.  相似文献   
993.
A procedure for the high-performance liquid chromatographic determination of vertilmicin in rat serum was described using pre-column derivatization. The serum proteins were precipitated with acetonitrile and vertilmicin in the supernatant was derivatized with 1-fluoro-2,4-dinitrobenzene. Etimicin was selected as the internal standard. The mobile phase consisted of methanol--20mM ammonium acetate (80:20, v/v), and flow-rate was 0.9 ml/min. Ultraviolet detection was set at 365 nm. The reaction products were chromatographed on a C(18) column kept at 40 degrees C. A good linearity was found in the range of 0.5-250 microg/ml. Both intra- and inter-day precisions of vertilmicin, expressed as the relative standard deviation, were less than 7.4%. Accuracy, expressed as the relative error, ranged from -0.1 to 3.6%. The mean absolute recovery of vertilmicin at three different concentrations was 92.5%. Serum volumes of 50 microl were sufficient for the determination of vertilmicin. The method was proved suitable for the pharmacokinetic study of vertilmicin in rats.  相似文献   
994.
To date, the association of coral–bacteria and the ecological roles of bacterial symbionts in corals remain largely unknown. In particular, little is known about the community components of bacterial symbionts of corals involved in the process of denitrification and ammonia oxidation. In this study, the nitrite reductase (nirS and nirK) and ammonia monooxygenase subunit A (amoA) genes were used as functional markers. Diverse bacteria with the potential to be active as denitrifiers and ammonia-oxidizing bacteria (AOB) were found in two East China Sea corals: stony coral Alcyonium gracillimum and soft coral Tubastraea coccinea. The 16S rRNA gene library analysis demonstrated different communities of bacterial symbionts in these two corals of the same location. Nitrite reductase nirK gene was found only in T. coccinea, while both nirK and nirS genes were detected in A. gracillimum, which might be the result of the presence of different bacterial symbionts in these two corals. AOB rather than ammonia-oxidizing archaea were detected in both corals, suggesting that AOB might play an important role in the ammonia oxidation process of the corals. This study indicates that the coral bacterial symbionts with the potential for nitrite reduction and ammonia oxidation might have multiple ecological roles in the coral holobiont, which promotes our understanding of bacteria-mediated nitrogen cycling in corals. To our knowledge, this study is the first assessment of the community structure and phylogenetic diversity of denitrifying bacteria and AOB in corals based on nirK, nirS, and amoA gene library analysis.  相似文献   
995.
不同干扰对黄土区典型草原物种多样性和生物量的影响   总被引:3,自引:0,他引:3  
对黄土区典型草原进行封育+施肥(EF)、封育+火烧(EB)、封育(E)和放牧(G)处理,实地调查分析群落盖度、高度、密度、地上现存量和物种多样性,以研究不同干扰对黄土区典型草原群落物种多样性和生物量的影响.结果表明:在4种干扰类型中,施肥+封育草地群落盖度和地上生物量最高,且优势度指数最高,这与禾本科草占优势地位有关,群落均匀度指数和多样性指数最低,符合“生态位理论”;放牧地群落高度、盖度、密度和地上现存量最低,群落丰富度指数和多样性指数最高,支持“中度干扰理论”;封育地密度和均匀度指数最高;具体表现为:4种干扰类型地上生物量的变化趋势为封育+施肥>封育+火烧>封育>放牧;说明长时间的封育对草地是一种严重干扰.群落丰富度指数(R和Ma)的排列顺序为放牧>封育+施肥>封育+火烧>封育,群落物种多样性指数(H'和D)的排列顺序为放牧>封育>封育+火烧>封育+施肥,优势度指数与多样性指数相反,群落均匀度指数(Jsw和Ea)的排列顺序为封育>放牧>封育+火烧>封育+施肥.不同干扰样地群落生产力与Shannon-Wiener和Simpson 多样性指数间呈负相关关系,这个结论可以用地上/地下竞争的相互作用来解释.  相似文献   
996.
光照和生长阶段对菖蒲根系泌氧的影响   总被引:1,自引:0,他引:1  
王文林  王国祥  万寅婧  夏劲  唐晓燕  陈昕  梁斌  庄巍 《生态学报》2013,33(12):3688-3696
以自然湖泊沉积物为研究基质,利用微型电机控制溶氧微电极实现纵向精确微位移,在照光与遮光条件下,对典型湿地植物菖蒲幼苗、成株根系根基部起总根长1/4处(根1/4)、根系中部(根1/2)、从根基部起总根长3/4处(根3/4)及根尖(根1)处根系微界面径向溶氧浓度变化进行原位精确测定。结果表明:无论有无光照,菖蒲幼苗、成株根系不同部位均存在从根表面至沉积物氧饱和度由高到低的氧扩散层,其厚度0.18—0.68 mm;根1/2、3/4、1处氧扩散能力菖蒲成株较幼苗显著增强(P<0.01),根1/4处二者则无显著差异(P>0.05);光照对菖蒲幼苗、成株根系不同部位氧扩散能力的影响存在差异,光照对菖蒲幼苗根1/2及菖蒲成株根1/2、根3/4处影响显著(照光组显著高于遮光组,P<0.01),而对菖蒲幼苗根1/4、根3/4、根1及菖蒲成株根1/4、根1处无显著影响(P>0.05);从根系泌氧空间差异上看,照光条件下菖蒲幼苗、成株分别表现为根1/2>根3/4≈根1≈根1/4(P<0.01,P>0.05)和根1/2>根3/4>根1>根1/4(P<0.01),遮光条件下菖蒲幼苗、成株分别表现为根1/2≈根3/4≈根1≈根1/4(P>0.05)和根1/2>根3/4≈根1>根1/4(P<0.01,P>0.05)。  相似文献   
997.

Background

Treatment for children with high-risk neuroblastoma with anti-disialoganglioside mAb ch14.18, IL-2, and GM-CSF plus 13-cis-retinoic acid after myeloablative chemotherapy improves survival, but 40 % of patients still relapse during or after this therapy. The microenvironment of high-risk neuroblastoma tumors includes macrophages, IL-6, and TGFβ1. We hypothesized that this microenvironment suppresses anti-tumor functions of natural killer (NK) cells and that lenalidomide, an immune-modulating drug, could overcome suppression.

Methods

Purified NK cells were cultured with IL-2, neuroblastoma/monocyte-conditioned culture medium (CM), IL-6, TGFβ1, and lenalidomide in various combinations and then characterized using cytotoxicity (direct and antibody-dependent cell-mediated cytotoxicity), cytokine, flow cytometry, and Western blotting assays. Anti-tumor activity of NK cells with lenalidomide, ch14.18, or both was evaluated with a xenograft model of neuroblastoma.

Results

CM from neuroblastoma/monocyte co-cultures contains IL-6 and TGFβ1 that suppress IL-2 activation of NK cell cytotoxicity and IFNγ secretion. IL-6 and TGFβ1 activate the STAT3 and SMAD2/3 pathways in NK cells and suppress IL-2 induction of cytotoxicity, granzymes A and B release, perforin expression, and IFNγ secretion. Lenalidomide blocks IL-6 and TGFβ1 activation of these signaling pathways and inhibits their suppression of NK cells. Neuroblastoma cells in NOD/SCID mice exhibit activated STAT3 and SMAD2/3 pathways. Their growth is most effectively inhibited by co-injected peripheral blood mononuclear cells (PBMC) containing NK cells when mice are treated with both ch14.18 and lenalidomide.

Conclusion

Immunotherapy with anti-tumor cell antibodies may be improved by lenalidomide, which enhances activation of NK cells and inhibits their suppression by IL-6 and TGFβ1.  相似文献   
998.
How to generate a non-zero first hyperpolarizability for a centrosymmetric molecule is a challenging question. In this paper, an external (pump) electric field is used to make a centrosymmetric benzene molecule generate a non-zero value of the electric field induced first hyperpolarizability (β F ). This comes from the centrosymmetry breaking of electron cloud. Two interesting rules are exhibited. (1) β F is anisotropic for different directional fields (F i, i?=?X, Y, Z). (2) The field dependence of β F is a non-monotonic function, and an optimum external electric field causes the maximum value of β F . The largest first hyperpolarizability β F reaches the considerable level of 3.9?×?105 a.u. under F Y?=?330?×?10?4 a.u. for benzene. The external electric field effects on non-centrosymmetric edge-modified graphene ribbon H2N-(3,3)ZGNR-NO2 was also studied in this work. The first hyperpolarizability reaches as much as 2.1?×?107 a.u. under F X?=?600?×?10?4 a.u. for H2N-(3,3)ZGNR-NO2. We show that the external electric field can not only create a non-zero first hyperpolarizability for centrosymmetric molecule, but also remarkably enhance the first hyperpolarizability for a non-centrosymmetric molecule.  相似文献   
999.
采用各种色谱对硬毛地笋(Lycopus lucidus Turcz.var.hirtus Regel)的化学成分进行分离,通过理化性质和波谱分析进行结构鉴定。从硬毛地笋全草甲醇提取物中分离鉴定了9个化合物:β-胡萝卜素(1),7,3’,4’-三羟基黄酮(2),β-谷甾醇(3),3’,4’,5-三羟基-3,7-二甲氧基黄酮(4),α-香树脂醇(5),β-香树脂醇(6),24-羟基-乌苏-12-烯-28-酸(7),β-胡萝卜苷(8),24-甲基-5α-胆甾-7,22-二烯-6α-醇-3β-O-葡萄糖苷(9)。化合物4,7和9为首次从该科植物中分离得到,化合物1~9均为首次从硬毛地笋中分离得到。  相似文献   
1000.
科尔沁沙地湖泊消涨对气候变化的响应   总被引:6,自引:0,他引:6  
常学礼  赵学勇  王玮  刘良旭 《生态学报》2013,33(21):7002-7012
湖泊是受气候变化影响显著的地理单元之一,不同地区湖泊消涨与气候变化关系的分析是理解陆地水文过程对未来气候变化响应的关键之一。对干旱、半干旱地区而言,湖泊消涨对气候变化的响应是干旱区生态保护和未来可持续发展的重要指征。气候变化对湖泊的影响研究在不同的区域已有较多的研究,但是针对湖泊群且基于湖泊大小分级和不同降水强度的对应研究还很鲜见。有鉴于此,作者在RS和GIS技术支持下,采用湖泊大小和降水强度分级的方法,分析了科尔沁沙地湖泊群消涨与气候变化的关系。在1971-2010年间,年均气温波动升高和降水量波动减少是该区域的主要气候变化特点。从5年移动平均分析来看,1990年是气温变化的转折点,1991-2010年的平均气温7.36(?0.55)℃,高于全球同期平均增温0.52℃。在1975-2009年间,科尔沁沙地湖泊面积和数量的变化趋势呈抛物线型减少,在1995年湖泊面积与数量最高。进入21世纪,湖泊面积萎缩、数量减少呈明显的加快趋势。到2009年,面积>0.05km2湖泊数量仅为81个,不足高峰期(1995年)的11%;湖泊总面积为4375.0hm2,不到1995年的26%。本研究表明,湖泊消涨主要受到年降水量波动影响,与年内降水分布格局无关,气温变化的影响不显著。  相似文献   
设为首页 | 免责声明 | 关于勤云 | 加入收藏

Copyright©北京勤云科技发展有限公司  京ICP备09084417号