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141.
Claudia Sassenrath Kai Sassenberg Devin G. Ray Katharina Scheiter Halszka Jarodzka 《PloS one》2014,9(11)
Two studies examined an unexplored motivational determinant of facial emotion recognition: observer regulatory focus. It was predicted that a promotion focus would enhance facial emotion recognition relative to a prevention focus because the attentional strategies associated with promotion focus enhance performance on well-learned or innate tasks - such as facial emotion recognition. In Study 1, a promotion or a prevention focus was experimentally induced and better facial emotion recognition was observed in a promotion focus compared to a prevention focus. In Study 2, individual differences in chronic regulatory focus were assessed and attention allocation was measured using eye tracking during the facial emotion recognition task. Results indicated that the positive relation between a promotion focus and facial emotion recognition is mediated by shorter fixation duration on the face which reflects a pattern of attention allocation matched to the eager strategy in a promotion focus (i.e., striving to make hits). A prevention focus did not have an impact neither on perceptual processing nor on facial emotion recognition. Taken together, these findings demonstrate important mechanisms and consequences of observer motivational orientation for facial emotion recognition. 相似文献
142.
Mircea Winter Mirjam A Moser Dominique Meunier Katharina Mattes Christina Murko Christina Humer Tina Meischel Gerald Brosch Patrick Matthias Maria Sibilia Christian Seiser 《The EMBO journal》2013,32(24):3176-3191
The histone deacetylases HDAC1 and HDAC2 remove acetyl moieties from lysine residues of histones and other proteins and are important regulators of gene expression. By deleting different combinations of Hdac1 and Hdac2 alleles in the epidermis, we reveal a dosage‐dependent effect of HDAC1/HDAC2 activity on epidermal proliferation and differentiation. Conditional ablation of either HDAC1 or HDAC2 in the epidermis leads to no obvious phenotype due to compensation by the upregulated paralogue. Strikingly, deletion of a single Hdac2 allele in HDAC1 knockout mice results in severe epidermal defects, including alopecia, hyperkeratosis, hyperproliferation and spontaneous tumour formation. These mice display impaired Sin3A co‐repressor complex function, increased levels of c‐Myc protein, p53 expression and apoptosis in hair follicles (HFs) and misregulation of HF bulge stem cells. Surprisingly, ablation of HDAC1 but not HDAC2 in a skin tumour model leads to accelerated tumour development. Our data reveal a crucial function of HDAC1/HDAC2 in the control of lineage specificity and a novel role of HDAC1 as a tumour suppressor in the epidermis. 相似文献
143.
Krysko DV Diez-Fraile A Criel G Svistunov AA Vandenabeele P D'Herde K 《Apoptosis : an international journal on programmed cell death》2008,13(9):1065-1087
The vertebrate ovary is an extremely dynamic organ in which excessive or defective follicles are rapidly and effectively eliminated
early in ontogeny and thereafter continuously throughout reproductive life. More than 99% of follicles disappear, primarily
due to apoptosis of granulosa cells, and only a minute fraction of the surviving follicles successfully complete the path
to ovulation. The balance between signals for cell death and survival determines the destiny of the follicles. An abnormally
high rate of cell death followed by atresia can negatively affect fertility and eventually lead irreversibly to premature
ovarian failure. In this review we provide a short overview of the role of programmed cell death in prenatal differentiation
of the primordial germ cells and in postnatal folliculogenesis. We also discuss the issue of neo-oogenesis. Next, we highlight
molecules involved in regulation of granulosa cell apoptosis. We further discuss the potential use of scores for apoptosis
in granulosa cells and characteristics of follicular fluid as prognostic markers for predicting the outcome of assisted reproduction.
Potential therapeutic strategies for combating premature ovarian failure are also addressed. 相似文献
144.
A systemic Pasteurella multocida toxin aggravates cardiac hypertrophy and fibrosis in mice 下载免费PDF全文
Markus Weise Christiane Vettel Katharina Spiger Ralf Gilsbach Lutz Hein Kristina Lorenz Thomas Wieland Klaus Aktories Joachim H. C. Orth 《Cellular microbiology》2015,17(9):1320-1331
Pasteurella multocida toxin (PMT) persistently activates heterotrimeric G proteins of the Gαq/11, Gα12/13 and Gαi family without interaction with G protein‐coupled receptors (GPCRs). We show that PMT acts on heart tissue in vivo and on cardiomyocytes and cardiac fibroblasts in vitro by deamidation of heterotrimeric G proteins. Increased normalized ventricle weights and fibrosis were detected after intraperitoneal administration of PMT in combination with the GPCR agonist phenylephrine. In neonatal rat cardiomyocytes, PMT stimulated the mitogen‐activated protein kinase pathway, which is crucial for the development of cellular hypertrophy. The toxin induced phosphorylation of the canonical phosphorylation sites of the extracellular‐regulated kinase 1/2 and, additionally, caused phosphorylation of the recently recognized autophosphorylation site, which appears to be important for the development of cellular hypertrophy. Moreover, PMT stimulated the small GTPases Rac1 and RhoA. Both switch proteins are involved in cardiomyocyte hypertrophy. In addition, PMT stimulated RhoA and Rac1 in neonatal rat cardiac fibroblasts. RhoA and Rac1 have been implicated in the regulation of connective tissue growth factor (CTGF) secretion and expression. Accordingly, we show that PMT treatment increased secretion and expression of CTGF in cardiac fibroblasts. Altogether, the data indicate that PMT is an inducer of pathological remodelling of cardiac cells and identifies the toxin as a promising tool for studying heterotrimeric G protein‐dependent signalling in cardiac cells. 相似文献
145.
Monz K Maas-Kück K Schumacher U Schulz T Hallmann R Schnäker EM Schneider SW Prehm P 《Journal of cellular biochemistry》2008,105(5):1260-1266
When secreted from malignant cells, hyaluronan facilitates tumor invasion and metastasis, as inhibition of its export by zaprinast inhibited metastasis formation in mice. However, the precise steps of the metastatic cascade, which were influenced by zaprinast, have not been identified as yet. Here we analyzed the cell biological effects of the inhibitor on three human melanoma cell lines that differed in their hyaluronan production and their metastatic capability when xenografted into SCID mice. We measured the influence of zaprinast on cellular hyaluronan export, surface coat formation, proliferation, random migration, colony formation in soft agar, adhesion, and transepithelial resistance. Concentrations of zaprinast not affecting cell proliferation, adhesion and transepithelial resistance, nevertheless reduced hyaluronan export by 50%, surface coat formation, random migration, and colony formation in soft agar. These results indicate that hyaluronan enhances metastasis formation primarily in those steps of the metastatic cascade, which involves tumor cell migration. 相似文献
146.
Katharina Gryksa Laura Mittmann Angelika Bauer Daniel Peterlik Peter J. Flor Nicole Uschold‐Schmidt Oliver J. Bosch 《Genes, Brain & Behavior》2020,19(1)
The group III metabotropic glutamate receptor subtype 7 (mGlu7) is an important regulator of glutamatergic and GABAergic neurotransmission and known to mediate emotionality and male social behavior. However, a possible regulatory role in maternal behavior remains unknown to date. Adequate expression of maternal behavior is essential for successful rearing and healthy development of the young. By understanding genetic and neural mechanisms underlying this important prosocial behavior, we gain valuable insights into possible dysregulations. Using genetic ablation as well as pharmacological modulation, we studied various parameters of maternal behavior in two different mouse strains under the influence of mGlu7. We can clearly show a regulatory role of mGlu7 in maternal behavior. Naïve virgin female C57BL/6 mGlu7 knockout mice showed more often nursing postures and less spontaneous maternal aggression compared to their heterozygous and wildtype littermates. In lactating C57BL/6 wildtype mice, acute central activation of mGlu7 by the selective agonist AMN082 reduced arched back nursing and accelerated pup retrieval without affecting maternal aggression. In addition, in lactating CD1 wildtype mice the selective mGlu7 antagonist XAP044 increased both pup retrieval and maternal aggression. With respect to receptor expression levels, mGlu7 mRNA expression was higher in lactating vs virgin C57BL/6 mice in the prefrontal cortex, but not hypothalamus or hippocampus. In conclusion, these findings highlight a significant role of the mGlu7 receptor subtype in mediating maternal behavior in mice. Region‐dependent studies are warranted to further extend our knowledge on the specific function of the brain glutamate system in maternal behavior. 相似文献
147.
148.
Schmidt-Bleek K Schell H Schulz N Hoff P Perka C Buttgereit F Volk HD Lienau J Duda GN 《Cell and tissue research》2012,347(3):567-573
Bone healing commences with an inflammatory reaction which initiates the regenerative healing process leading in the end to
reconstitution of bone. An unbalanced immune reaction during this early bone healing phase is hypothesized to disturb the
healing cascade in a way that delays bone healing and jeopardizes the successful healing outcome. The immune cell composition
and expression pattern of angiogenic factors were investigated in a sheep bone osteotomy model and compared to a mechanically-induced
impaired/delayed bone healing group. In the impaired/delayed healing group, significantly higher T cell percentages were present
in the bone hematoma and the bone marrow adjacent to the osteotomy gap when compared to the normal healing group. This was
mirrored in the higher cytotoxic T cell percentage detected under delayed bone healing conditions indicating longer pro-inflammatory
processes. The highly activated periosteum adjourning the osteotomy gap showed lower expression of hematopoietic stem cell
markers and angiogenic factors such as heme oxygenase and vascular endothelial growth factor. This indicates a deferred revascularization
of the injured area due to ongoing pro-inflammatory processes in the delayed healing group. Results from this study suggest
that there are unfavorable immune cells and factors participating in the initial healing phase. In conclusion, identifying
beneficial aspects may lead to promising therapeutical approaches that might benefit further by eliminating the unfavorable
factors. 相似文献
149.
Inferring species phylogenies is an important part of understanding molecular evolution. Even so, it is well known that an accurate phylogenetic tree reconstruction for a single gene does not always necessarily correspond to the species phylogeny. One commonly accepted strategy to cope with this problem is to sequence many genes; the way in which to analyze the resulting collection of genes is somewhat more contentious. Supermatrix and supertree methods can be used, although these can suppress conflicts arising from true differences in the gene trees caused by processes such as lineage sorting, horizontal gene transfer, or gene duplication and loss. In 2004, Huson et al. (IEEE/ACM Trans. Comput. Biol. Bioinformatics 1:151-158) presented the Z-closure method that can circumvent this problem by generating a supernetwork as opposed to a supertree. Here we present an alternative way for generating supernetworks called Q-imputation. In particular, we describe a method that uses quartet information to add missing taxa into gene trees. The resulting trees are subsequently used to generate consensus networks, networks that generalize strict and majority-rule consensus trees. Through simulations and application to real data sets, we compare Q-imputation to the matrix representation with parsimony (MRP) supertree method and Z-closure, and demonstrate that it provides a useful complementary tool. 相似文献
150.
Population dynamics of Gentiana pneumonanthe and Rhynchospora fusca during wet heathland restoration
Abstract. The population dynamics and reproductive strategies of two rare wet heathland species, Gentiana pneumonanthe and Rhynchospora, were studied in experimental permanent plots in a wet heathland near Bremen, NW Germany, to assess how effective sod cutting and mowing are in promoting these species. In one experiment, small plots (0.25 m2 - 4 m2) were sod-cut or mown; in the second, one large plot 30 mx 50m) was sod-cut. The development of the vegetation and the number of shoots of the two target species were recorded annually. Sod cutting lead to the highest shoot numbers of Gentiana in the long run, whilst mowing was more effective at the beginning of the experiment. Seedlings and adult shoots slowly became more and more abundant after sod cutting. In contrast, Rhynchospora soon formed closed stands after sod-cutting, first through seed germination and then through fast clonal growth of the established individuals. Moist soil or short inundations promoted the germination and seedling establishment of Gentiana, whereas drought negatively affected seedling recruitment. Long periods of inundation severely reduced the population at first, but high numbers of seedlings were found in the following growing season. For the disturbance-dependent Gentiana and Rhynchospora, the availability of gaps within the vegetation is of crucial importance. To promote existing populations, we suggest small-scale sod cuttings which create gaps without disturbing existing flowering individuals too much. For degenerated stands of wet heathland we recommend large-scale sod cutting to activate the seed bank. Additionally, seed introduction may be helpful to encourage the development of a wet heathland with characteristic floristic composition. 相似文献