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991.
Fatemeh Eini Arash Bidadkosh Hamid Nazarian Abbas Piryaei Marefat Ghaffari Novin Khojasteh Joharchi 《Molecular reproduction and development》2019,86(8):1053-1066
Although in‐vitro maturation (IVM) of oocytes has been presented as an alternative treatment to traditional stimulated in‐vitro fertilization, the culture condition can be improved by natural antioxidants. Thus, we investigated the protective effect of Thymoquinone (TQ) during IVM in the polycystic ovary syndrome (PCOS) mice model. The induction of PCOS was made by dehydroepiandrosterone via subcutaneous injection, in prepubertal female B6D2F1‐mice. After 21 days later, germinal vesicle (GV)‐stage‐oocytes were extracted and incubated in IVM media containing 0, 1.0, 10.0, and 100.0 μM of TQ. To assess fertilization and blastulation rates, after 22–24 hr, the treated oocytes were fertilized in‐vitro with epididymal spermatozoa. Some other oocytes were evaluated for maturation, epigenetic, and oxidative stress markers. Similarly, the mRNA expression of epigenetic enzymes genes (Dnmt1 and Hdac1), three maternally derived genes (Mapk, CyclinB, and Cdk1) and apoptosis‐related genes (Bax and Bcl2) were assessed. Our results showed that the maturation, fertilization, and blastulation rates were significantly higher in the 10.0 μM TQ‐treated group compared with the untreated group and likewise with in‐vivo matured oocytes. The Bax expression was reduced in 10.0 μM TQ matured oocytes, but Bcl2, Dnmt1, Hdac1, Cdk1, and Mapk were upregulated in this group compared to other groups. Furthermore, dimethylation of histone‐3 at lysine‐9 (H3K9m2) and DNA methylation were significantly increased whereas H4K12 acetylation (H4K12ac) was decreased in the 10.0 μM TQ‐treated group in comparison with control and in‐vivo matured oocytes. Therefore, our results are suggesting that 10.0 μM TQ may enhance the developmental competence of PCOS oocytes via the modulation of oxidative stress and epigenetic alterations. 相似文献
992.
翻译后修饰如磷酸化、乙酰化、甲基化、泛素化和SUMO化调节不同蛋白质的不同功能。磷酸化可能是最常见的修饰之一,蛋白质磷酸化通过一系列的激酶和磷酸酶催化,从而改变蛋白质功能。SUMO修饰是一种类泛素化修饰。SUMO修饰包括活化、结合、连接和解离,涉及多个酶多个步骤的催化过程。SUMO化可调节蛋白质相互作用、亚细胞定位、蛋白质稳定性和转录活性。关于磷酸化和SUMO化的蛋白质翻译后修饰,已有广泛研究报道。但很少关注于磷酸化和SUMO化之间的相互作用,以及它们对蛋白质的共同修饰。本文综述了蛋白质磷酸化和SUMO化之间的相互作用,以及共同修饰对细胞生理和肿瘤的影响。 相似文献
993.
Mrinal Kalita Archana Archana Astha Dimri Prema G. Vasudev Ramesh Ramapanicker 《Journal of peptide science》2019,25(3)
An isolated uncharged hydrogen bond acceptor such as the carbonyl functionality of an aldehyde or a keto group is absent in natural amino acids. Although glutamine and asparagine are known to hydrogen bond through the amide carbonyl group in their side chains, they also possess the amide ? NH2 group, which can act as a hydrogen bond donor. This makes the structural study of peptides containing an oxo residue, with an isolated carbonyl group in the side chain, interesting. Here, we report the synthesis of δ‐ and ε‐oxo amino acids and their incorporation into oligopeptides as the N‐terminal residue. The resultant oxo peptides were extensively studied using X‐ray crystallography to understand the interactions offered by the oxo group in peptide crystals. We find that the oxo groups are capable of providing additional hydrogen bonding opportunities to the peptides, resulting in increased intermolecular interactions in crystals. The study thus offers avenues for the utilization of oxo residues to introduce intermolecular interactions in synthetic peptides. 相似文献
994.
Extracellular NAD and ATP: Partners in immune cell modulation 总被引:3,自引:2,他引:1
Friedrich Haag Sahil Adriouch Anette Braß Caroline Jung Sina Möller Felix Scheuplein Peter Bannas Michel Seman Friedrich Koch-Nolte 《Purinergic signalling》2007,3(1-2):71-81
Extracellular NAD and ATP exert multiple, partially overlapping effects on immune cells. Catabolism of both nucleotides by extracellular enzymes keeps extracellular concentrations low under steady-state conditions and generates metabolites that are themselves signal transducers. ATP and its metabolites signal through purinergic P2 and P1 receptors, whereas extracellular NAD exerts its effects by serving as a substrate for ADP-ribosyltransferases (ARTs) and NAD glycohydrolases/ADPR cyclases like CD38 and CD157. Both nucleotides activate the P2X7 purinoceptor, although by different mechanisms and with different characteristics. While ATP activates P2X7 directly as a soluble ligand, activation via NAD occurs by ART-dependent ADP-ribosylation of cell surface proteins, providing an immobilised ligand. P2X7 activation by either route leads to phosphatidylserine exposure, shedding of CD62L, and ultimately to cell death. Activation by ATP requires high micromolar concentrations of nucleotide and is readily reversible, whereas NAD-dependent stimulation begins at low micromolar concentrations and is more stable. Under conditions of cell stress or inflammation, ATP and NAD are released into the extracellular space from intracellular stores by lytic and non-lytic mechanisms, and may serve as ‘danger signals–to alert the immune response to tissue damage. Since ART expression is limited to naïve/resting T cells, P2X7-mediated NAD-induced cell death (NICD) specifically targets this cell population. In inflamed tissue, NICD may inhibit bystander activation of unprimed T cells, reducing the risk of autoimmunity. In draining lymph nodes, NICD may eliminate regulatory T cells or provide space for the preferential expansion of primed cells, and thus help to augment an immune response. 相似文献
995.
Genetic containment of forest plantations 总被引:2,自引:0,他引:2
Amy M. Brunner Jingyi Li Stephen P. DiFazio Olga Shevchenko Brooke E. Montgomery Rozi Mohamed Hao Wei Cathleen Ma Ani Anna Elias Katherine VanWormer Steven H. Strauss 《Tree Genetics & Genomes》2007,3(2):75-100
Dispersal of pollen, seeds, or vegetative propagules from intensively bred, exotic, or recombinant DNA modified forest plantations
may cause detrimental or beneficial ecological impacts on wild or managed ecosystems. Insertion of genes designed to prevent
or substantially reduce dispersal could reduce the risk and extent of undesired impacts. Containment measures may also be
required by law or marketplace constraints, regardless of risks or benefits. We discuss: (1) the context for when genetic
containment or mitigation systems may be needed; (2) technology approaches and mechanisms; (3) the state of knowledge on genes/genomics
of sexual reproduction in forest trees; (4) stability of transgene expression during vegetative growth; (5) simulation studies
to define the level of containment needed; and (6) needed research to deliver effective containment technologies. We illustrate
progress with several examples from our research on recombinant DNA modified poplars. Our simulations show that even partial
sterility can provide very substantial reductions in gene flow into wild trees. We conclude that it is impossible to define
the most effective containment approaches, nor their reliability, based on current genomic knowledge and technological tools.
Additional genomic and technological studies of a wide variety of options are needed. Studies in field environments are essential
to provide data relevant to ecological analysis and regulatory decisions and need to be carried out in phylogenetically diverse
representatives of the economically most important taxa of forest trees.
相似文献
Steven H. StraussEmail: |
996.
A new method for immobilization of acetylcholinesterase (AChE) to alginate gel beads by activating the carbonyl groups of
alginate using carbodiimide coupling agent has been successfully developed. Maximum reaction rate (V
max) and Michaelis–Menten constant (K
m) were determined for the free and binary immobilized enzyme. The effects of pH, temperature, storage stability, reuse number
and thermal stability on the free and immobilized AChE were also investigated. For the free and binary immobilized enzyme
on the Ca–alginate gel beads, optimum pH values were found to be 7 and 8, respectively. Optimum temperatures for the free
and immobilized enzyme were observed to be 30 and 35 °C, respectively. Upon 60 days of storage the preserved activity of free
and immobilized enzyme were found as 4 and 68%, respectively. In addition, reuse number, and thermal stability of the free
AChE were increased by as a result of binary immobilization. 相似文献
997.
The 20S proteasome of Schistosoma mansoni: a proteomic analysis 总被引:1,自引:0,他引:1
Castro-Borges W Cartwright J Ashton PD Braschi S Guerra Sa R Rodrigues V Wilson RA Curwen RS 《Proteomics》2007,7(7):1065-1075
998.
Rajbir Singh Sean W. Harshman Amy S. Ruppert Amir Mortazavi David M. Lucas Jennifer M. Thomas-Ahner Steven K. Clinton John C. Byrd Michael A. Freitas Mark R. Parthun 《Clinical proteomics》2015,12(1):22
Background
Chromatin is an extraordinarily complex structure. Much of this complexity results from the presence of numerous histone post-translational modifications and histone variants. Alterations in the patterns of histone post-translational modifications are emerging as a feature of many types of cancer and have been shown to have prognostic value.Results
We have applied a liquid chromatography/mass spectrometry-based approach to comprehensively characterize the histone proteome in primary samples from chronic lymphocytic leukemia (CLL) patients, as well as bladder and breast cancer cell culture models. When compared to non-malignant CD19+ B cells from healthy donors, the CLL histone proteome showed a distinct signature of differentially expressed species, spanning all the histones studied and including both post-translationally modified species and unmodified, non-allelic replication-dependent histone isoforms. However, the large changes in histone H3 and H4 that are characteristic of many cancer types were not observed. One of species of H2A (mass = 14,063 Da) was the most strongly associated with time to treatment in CLL patients. CLL patient samples also demonstrated histone profiles that were distinct from those of the bladder and breast cancer cells.Conclusions
Signatures of histone profiles are complex and can distinguish between healthy individuals and CLL patients and may provide prognostic markers. In addition, histone profiles may define tissue specific malignancies.999.
1000.