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81.
82.
The origin of nucleic acid template replication is a major unsolved problem in science. A novel stochastic model of nucleic acid chemistry was developed to allow rapid prototyping of chemical experiments designed to discover sufficient conditions for template replication. Experiments using the model brought to attention a robust property of nucleic acid template populations, the tendency for elongation to outcompete replication. Externally imposed denaturation-renaturation cycles did not reverse this tendency. For example, it has been proposed that fast tidal cycling could establish a TCR (tidal chain reaction) analogous to a PCR (polymerase chain reaction) acting on nucleic acid polymers, allowing their self-replication. However, elongating side-reactions that would have been prevented by the polymerase in the PCR still occurred in the simulation of the TCR. The same finding was found with temperature and monomer cycles. We propose that if cycling reactors are to allow template replication, oligonucleotide phenotypes that are capable of favorably altering the flux ratio between replication and elongation, for example, by facilitating sequence-specific cleavage within templates, are necessary; accordingly the minimal replicase ribozyme may have possessed restriction functionality. 相似文献
83.
84.
Raffaella Di Lisi Anne Picard Simonetta Ausoni Stefano Schiaffino 《BMC molecular biology》2007,8(1):78
Background
We reported previously that the cardiac troponin I (cTnI) promoter drives cardiac-specific expression of reporter genes in cardiac muscle cells and in transgenic mice, and that disruption of GATA elements inactivates the cTnI promoter in cultured cardiomyocytes. We have now examined the role of cTnI promoter GATA elements in skeletal muscle cells. 相似文献85.
86.
Debra L Fisk Leigh C LattaIV Roland A Knapp Michael E Pfrender 《BMC evolutionary biology》2007,7(1):22
Background
Introduced species can have profound effects on native species, communities, and ecosystems, and have caused extinctions or declines in native species globally. We examined the evolutionary response of native zooplankton populations to the introduction of non-native salmonids in alpine lakes in the Sierra Nevada of California, USA. We compared morphological and life-history traits in populations of Daphnia with a known history of introduced salmonids and populations that have no history of salmonid introductions. 相似文献87.
The sequencing of the genome of a female rhesus macaque (Macaca mulatta) of Indian origin will provide us with biomedical and evolutionary insights into both humans and Old World monkeys. 相似文献
88.
Amanda Ferreira da Silva Mendes Luciana Cardoso Cidade Maria Luiza Peixoto de Oliveira Wagner Campos Otoni Walter Dos Santos Soares-Filho Marcio Gilberto Cardoso Costa 《Plant Cell, Tissue and Organ Culture》2009,97(3):331-336
Identification of beta-lactam antibiotics that have negligible effects on plant regeneration is a critical step towards the
establishment of a reliable Agrobacterium-mediated transformation protocol for perennial trees. In the present report, we have evaluated the effects of the novel beta-lactam
antibiotics meropenem and timentin on plant regeneration of a perennial woody fruit plant, Citrus sinensis, in comparison with the commonly used beta-lactam cefotaxime. It was observed that, in contrast to cefotaxime, meropenem
and timentin had a positive or no detrimental effect on the shoot regeneration from epicotyl explants. Residual effects of
the beta-lactams from shoot regeneration medium also affected the subsequent ability of the roots to elongate. The addition
of meropenem and/or timentin in the rooting medium mostly improved or did not affect the rooting ability of the adventitious
shoots. These data indicated that meropenem and timentin can positively replace cefotaxime in Agrobacterium-mediated transformation of C. sinensis. 相似文献
89.
During an adaptive immune response, lymphocytes proliferate for five to twenty-five cell divisions, then stop and die over
a period of weeks. Based on extensive flow cytometry data, Hawkins et al. (Proc Natl Acad Sci USA 104:5032–5037, 2007) introduced
a cell-level stochastic model of lymphocyte population dynamics, called the Cyton Model, that accurately captures mean lymphocyte
population size as a function of time. In Subramanian et al. (J Math Biol 56(6):861–892, 2008), we performed a branching process
analysis of the Cyton Model and deduced from parameterizations for in vitro and in vivo data that the immune response is predictable
despite each cell’s fate being highly variable. One drawback of flow cytometry data is that individual cells cannot be tracked,
so that it is not possible to investigate dependencies in the fate of cells within family trees. In the absence of this information,
while the Cyton Model abandons one of the usual assumptions of branching processes (the independence of lifetime and progeny
number), it adopts another of the standard branching processes hypotheses: that the fates of progeny are stochastically independent.
However, new experimental observations of lymphocytes show that the fates of cells in the same family tree are not stochastically
independent. Hawkins et al. (2008, submitted) report on ciné lapse photography experiments where every founding cell’s family
tree is recorded for a system of proliferating lymphocytes responding to a mitogenic stimulus. Data from these experiments
demonstrate that the death-or-division fates of collaterally consanguineous cells (those in the same generation within a founding
cell’s family tree) are strongly correlated, while there is little correlation between cells of distinct generations and between
cells in distinct family trees. As this finding contrasts with one of the assumptions of the Cyton Model, in this paper we
introduce three variants of the Cyton Model with increasing levels of collaterally consanguineous correlation structure to
incorporate these new found dependencies. We investigate their impact on the predicted expected variability of cell population
size. Mathematically we conclude that while the introduction of correlation structure leaves the mean population size unchanged
from the Cyton Model, the variance of the population size distribution is typically larger. Biologically, through comparison
of model predictions for Cyton Model parameterizations determined by in vitro and in vivo experiments, we deduce that if collaterally
consanguineous correlation extends beyond cousins, then the immune response is less predictable than would be concluded from
the original Cyton Model. That is, some of the variability seen in data that we previously attributed to experimental error
could be due to intrinsic variability in the cell population size dynamics.
相似文献
90.
Liu Y Yu Y Yang S Zeng B Zhang Z Jiao G Zhang Y Cai L Yang R 《Cancer immunology, immunotherapy : CII》2009,58(5):687-697
An elevated number of Gr-1+CD11b+ myeloid-derived suppression cells (MDSCs) has been described in mice and human bearing tumor and associated with immune suppression.
Arginase I production by MDSCs in the tumor environment may be a central mechanism for immunosuppression and tumor evasion.
In this study and before, we found that Gr-1+CD11b+ MDSCs from ascites and spleen of mice bearing ovarian 18D carcinoma express a high level of PD-1, CTLA-4, B7-H1 and CD80
while other co-stimulatory molecules, namely CD40, B7-DC and CD86 are not detected. Further studies showed that PD-1 and CTLA-4
on the Gr-1+CD11b+ MDSCs regulated the activity and expression of arginase I. The blockage and silencing of PD-1, CTLA-4 or both PD-1 and CTLA4
molecules could significantly reduce arginase I activity and expression induced with tumor-associated factor. Similar results
were also observed while their ligands B7-H1 and/or CD80 were blocked or silenced. Furthermore, CD80 deficiency also decreased
the arginase I expression and activity. Antibody blockade or silencing of PD-1, CTLA-4 or both reduced the suppressive potential
of PD-1+CTLA-4+MDSCs. Blockade of PD-1, CTLA-4 or both also slowed tumor growth and improved the survival rate of tumor-bearing
mice. Thus, there may exist a coinhibitory and costimulatory molecules-based immuno-regulating wet among MDSCs.
This research was supported by Nankai University grant, NSFC grant “30771967”, “985” grant,The Ministry of Science and Technology
grant “2006AA020502”“06C26211200695”, Tianjin Grant “07JCZDJC03300” and “06ZHCXSH04800”. 相似文献