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Ren X Zhao L Sivashanmugam A Miao Y Korando L Yang Z Reardon CA Getz GS Brouillette CG Jerome WG Wang J 《Biochemistry》2005,44(45):14907-14919
Apolipoprotein AI (apoAI), the major protein component of HDL, is one of the best predictors of coronary artery disease (CAD), with high apoAI and HDL levels being correlated with low occurrences of CAD. The primary function of apoAI is to recruit phospholipid and cholesterol for assembly of HDL particles. Like other exchangeable apolipoproteins, lipid-free apoAI forms a mixture of different oligomers even at 1.0 mg/mL. This self-association property of the exchangeable apolipoproteins is closely associated with the lipoprotein-binding activity of this protein family. It is unclear if the self-association property of apolipoprotein is required for its lipoprotein-binding activity. We developed a novel method for engineering an oligomeric protein to a monomeric, biologically active protein. Using this method, we generated a monomeric mouse apoAI mutant that is active. This mutant contains the first 216 residues of mouse apoAI and replaces six hydrophobic residues with either polar or smaller hydrophobic residues at the defined positions (V118A/A119S/L121Q/T191S/T195S/T199S). Cross-linking results show that this mutant is greater than 90% monomeric at 8 mg/mL. CD, DSC, and NMR results indicate that the mutant maintains an identical secondary, tertiary structure and stability as those of the wild-type mouse apoAI. Lipid-binding assays suggest that the mutant shares an equal lipoprotein-binding activity as that of the wild-type apoAI. In addition, both the monomeric mutant and the wild-type protein make nearly identical rHDL particles. With this monomeric mouse apoAI, high-quality NMR data has been collected, allowing for the NMR structural determination of lipid-free apoAI. On the basis of these results, we conclude that this apoAI mutant is a monomeric, active apoAI useful for structural determination. 相似文献
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Heather F. Armitage Andrea J. Britton René van der Wal Imogen S. K. Pearce Des B. A. Thompson Sarah J. Woodin 《Global Change Biology》2012,18(1):290-300
Ecosystems are subject to multiple, natural and anthropogenic environmental influences, including nitrogen (N) deposition, land use and climate. Assessment of the relative importance of these influences on biodiversity and ecosystem functioning is crucial for guiding policy and management decisions to mitigate global change; yet, few studies consider multiple drivers. In the UK, ongoing loss of the internationally important arctic/alpine moss‐sedge community, Racomitrium heath, has been linked to elevated N deposition, high grazing pressures and their combination; however, the relative importance of these drivers remains unclear. We used environmental gradients across the habitat's European distribution (UK, Faroes, Norway and Iceland) to investigate the relative impact of N deposition and grazing pressure, as well as climate, on the condition of the dominant moss species, Racomitrium lanuginosum. Key variables including tissue chemistry, growth and cover were measured at 36 sites, and multiple linear regressions were used to examine the relative importance of the drivers across sites. Our results clearly show that regional variation in the condition of R. lanuginosum across Europe is primarily associated with the impacts of N deposition, with climate (air temperature) and grazing pressure playing secondary roles. In contrast to previous experimental studies, we found moss growth to be stimulated by elevated N deposition; this apparent discrepancy may result from the use of artificially high N concentrations in many experiments. Despite increased growth rates, we found that moss mat depth and cover declined in response to N deposition. Our results suggest that this is due to increased decomposition of material in the moss mat, which ultimately leads to loss of moss cover and habitat degradation. This study clearly demonstrates both the key role of N deposition in degradation of Racomitrium heath and the importance of observational studies along natural gradients for testing predictions from experimental studies in the real world. 相似文献
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该研究以宁夏贺兰山东麓酿酒葡萄种植区栽培面积最大的‘赤霞珠’为材料,在前期完成从果实形成至成熟不同发育时期的转录组测序以及关键有机酸含量测定基础上,进一步通过转录因子结合位点预测、差异表达基因分析、加权基因共表达网络关联分析(WGCNA),逐步筛选出与‘赤霞珠’果实苹果酸生物合成相关功能基因特异结合的、影响苹果酸生物合成的相应转录因子,并对其进行qRT PCR验证,以揭示这些关键功能基因及其关键转录因子在葡萄不同种植区、果实不同发育时期存在的相互调控作用机制,为以后培育优质酿酒葡萄提供新的理论依据与思路。结果表明:(1)GC/MS分析发现, ‘赤霞珠’果实在4个发育时期的延胡索酸和苹果酸含量变化趋势基本一致,两种酸含量均从果实硬果期到绿果期逐步升至最高(3.63和626.53 μg/g),之后缓慢下降,经转色期到成熟期后逐渐降至最低(2.14和244.26 μg/g),而草酰乙酸的变化趋势却相反,在硬果期含量最高(315.54 μg/g),经绿果期、转色期到成熟期逐渐降至最低值(126.11 μg/g)。(2)‘赤霞珠’果实发育时期样本转录组测序共获得可能与苹果酸生物合成途径12种功能基因结合的转录因子6 411个,其中延胡索酸水化酶(FH)的3个功能基因有86个转录因子,苹果酸脱氢酶(MDH)的10个功能基因有717个转录因子。(3)转录组测序数据及其与有机酸含量WGCNA关联结果的Veen分析确定了‘赤霞珠’果实成熟过程中与苹果酸生物合成相关度最高的3个FH基因(VIT_14s0060g01700、VIT_13s0019g03330、VIT_07s0005g00880)、2个MDH基因(VIT_10s0003g01000、VIT_13s0019g05250)及相应的18个关键转录因子。(4)qRT PCR验证及相关性分析表明, FH基因VIT_13s0019g03330与其转录因子VIT_01s0011g06200、VIT_08s0056g01230以及MDH基因VIT_13s0019g05250与其转录因子VIT_06s0004g04960、VIT_10s0003g02070的表达水平与苹果酸的积累存在显著正相关关系,推测这4个关键转录因子可能通过调控功能基因的转录,综合影响‘赤霞珠’果实苹果酸的生物合成。 相似文献
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Salvador promotes both cell cycle exit and apoptosis through the modulation of both cyclin E and Drosophila inhibitor of apoptosis protein in Drosophila. However, the cellular function of human Salvador (hSav1) is rarely reported. To screen for novel binding proteins that interact with hSav1, the cDNA of hSav1 was cloned into a bait protein plasmid, and positive clones were screened from a human fetal liver cDNA library by the yeast two-hybrid system. hSav1 mRNA was expressed in yeast and there was no self-activation and toxicity in the yeast strain AH109. Twenty proteins were found to interact with hSav1, including HS1 (haematopoietic cell specific protein1)-associated protein X-1 (HAX-1); neural precursor cell expressed, developmentally down-regulated 9, pyruvate kinase, liver and RBC, cytochrome c oxidase subunit Vb, enoyl coenzyme A hydratase short chain 1, and NADH dehydrogenase (ubiquinone) 1 beta subcomplex, demonstrating that the yeast two-hybrid system is an efficient method for investigating protein interactions. Among the identified proteins, there were many mitochondrial proteins, indicating that hSav1 may play a role in mitochondrial function. We also confirmed the interaction of HAX-1 and hSav1 in mammalian cells. This investigation provides functional clues for further exploration of potential apoptosis-related proteins in disease biotherapy. 相似文献
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设计合成了两个分别互补于乙肝病毒2.1kb mRNA起始区(片段A)和增强子区(片段B)的硫代磷酸的DNA片段,在经克隆HBV DNA转染HepG2细胞建立的HBV短暂表达系统及稳定产生HBV的2215细胞中研究二者对HBsAg及HBeAg表达的抑制作用。结果表明反义寡聚物能不同程序抑制乙肝抗原表达,并与剂量呈一定正相关。在HepG2细胞HBV短暂表达系统中,6μmol/L浓度时,片段A、B对HB 相似文献
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