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91.
Sixteen newH-2 haplotypes derived from wild mice 总被引:2,自引:1,他引:1
Wild mice captured in Texas, Scotland, Federal Republic of Germany, Denmark, Spain, Greece, Israel, Egypt, and Chile were mated to inbred strains and through successive backcross matings and H-2 typing lines homozygous for wild-derived H-2, haplotypes were established. The lines, which are neither congenic nor inbred, were then typed with antibodies defining known H-2 alleles at class I and class II loci. In addition, antisera were produced by the immunization of inbred strains with tissues of the new lines. Sixteen of the lines were characterized in this manner. The characterization resulted in the identification of 16 new H-2 haplotypes, 11 new K alleles, 10 new D alleles, and 21 new class I antigenic determinants, most of them of the private type. Most of the haplotypes represent natural recombinants sharing segments of the H-2 complex with previously identified haplotypes. A number of haplotypes are recombinants between the K and the A loci, which in genetic studies have proved difficult to separate. The lines, however, also provide evidence for preservation of blocks of genes in the H-2 complex, particularly in the class II region. Some of class I alleles previously found in wild mice from Michigan have now been found again in these mice. Several class II alleles of these lines appear to be the same as those found in inbred strains. Identical or nearly identical class I and class II alleles thus commonly occur in different populations. These findings strengthen the argument that in populations, H-2 alleles are relatively stable. 相似文献
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93.
Zofia Lenkiewicz Barbara Dabrowska Zofia Schiffer 《International journal of biometeorology》1989,33(4):251-258
The motor activity of Syrian hamsters (Mesocricetus auratus Waterhouse) under the influence of negative ionization of the atmosphere applied for 10, 20 or 30 min per day was investigated. An ionizer with output of 14000 light negative ions per 1 cm3 of air was used. Studies carried out in the light phase of a 1212 h light/dark regime revealed a relation between the reaction of the animal and the time of day at which ionization was applied. Ionization for 20 or 30 min in the light phase decreased motor activity, while 10 min of ionization increased it compared to control animals. Ionization in the dark phase gave a more distinct rise in activity than that applied in the light phase for all three durations of ionization.This work was supported by RP-II-12 (A1)-Investigations concerning regulation mechanisms of biorhythms by animals and humans in the basic conditions and under stress 相似文献
94.
We recently reported the first molecular genetic evidence that Dictyostelium Ca2+ responses to chemoattractants include a contribution from the endoplasmic reticulum (ER) – responses are enhanced in mutants lacking calreticulin or calnexin, two major Ca2+ -binding proteins in the ER, even though the influx of Ca2+ into the mutants is reduced. Compared with wild-type cells, the ER in the mutants contributes at least 30–70 nM additional Ca2+ to the responses. Here we report that this additional ER contribution to the cytosolic Ca2+ signal depends upon extracellular Ca2+ – it does not occur in the absence of extracellular Ca2+ , increases to a maximum as the extracellular Ca2+ levels rise to 10 μM and then remains constant at extracellular Ca2+ concentrations up to at least 250 μM. These results suggest that Ca2+ influx causes the intracellular release, in the simplest scenario by a mechanism involving Ca2+ -induced Ca2+ release from the ER. By way of contrast, we show that Ca2+ responses to mechanical stimulation are reduced, but still occur in the absence of extracellular Ca2+ . Unlike the responses to chemoattractants, mechanoresponses thus include contributions from the ER that are independent of extracellular Ca2+ . 相似文献
95.
Zofia F. Bielecka Kamila Maliszewska‐Olejniczak Ilan J. Safir Cezary Szczylik Anna M. Czarnecka 《Biological reviews of the Cambridge Philosophical Society》2017,92(3):1505-1520
Three‐dimensional (3D) cell culture models are becoming increasingly popular in contemporary cancer research and drug resistance studies. Recently, scientists have begun incorporating cancer stem cells (CSCs) into 3D models and modifying culture components in order to mimic in vivo conditions better. Currently, the global cell culture market is primarily focused on either 3D cancer cell cultures or stem cell cultures, with less focus on CSCs. This is evident in the low product availability officially indicated for 3D CSC model research. This review discusses the currently available commercial products for CSC 3D culture model research. Additionally, we discuss different culture media and components that result in higher levels of stem cell subpopulations while better recreating the tumor microenvironment. In summary, although progress has been made applying 3D technology to CSC research, this technology could be further utilized and a greater number of 3D kits dedicated specifically to CSCs should be implemented. 相似文献
96.
Zofia Ksikiewicz‐Parulska 《Invertebrate Biology》2019,138(2)
The aim of this study was to investigate vertical migration behaviors in two species of hygrophilous micro‐snails, Vertigo moulinsiana and Vertigo angustior, in relation to the time of the year (spring and summer) at two sites that differ in ground water level (periodically inundated site and non‐inundated site). The study shows different patterns of vertical migrations in the studied species. Vertigo angustior demonstrated a strong affinity to the litter layer (a weak tendency for vertical movements), independent of the time of year and site studied. By contrast, V. moulinsiana showed a clear tendency for vertical migrations, which differed depending on the time of year and site. These differences may be related to the spatial segregation of microhabitats used by these two species at the sites studied and to differences in the ability to resist inundation. Vertigo angustior is associated with microhabitats which are not subjected to prolonged inundation and tolerates a brief submersion. The periodic character of vertical migrations may suggest the effect of endogenous factors related to reproduction in V. moulinsiana. Some plasticity of this behavior in relation to habitat conditions demonstrated by this species may be an adaptation to live in unpredictably flooded environments. 相似文献
97.
Almost 30 years ago, neuropeptide Y (NPY) was discovered as a sympathetic co-transmitter and one of the most evolutionarily conserved peptides abundantly present all over the body. Soon afterward, NPY's multiple receptors were characterized and cloned, and the peptide's role in stress was first documented. NPY has proven to be pivotal for maintaining many stress responses. Most notably, NPY is known for activating long-lasting vasoconstriction in many vascular beds, including coronary arteries. More recently, NPY was found to play a role in stress-induced accretion of adipose tissue which many times can lead to detrimental metabolic changes. It is however due to its prominent actions in the brain, one of which is its powerful ability to stimulate appetite as well as its anxiolytic activities that NPY became a peptide of importance in neuroscience. In contrast, its actions in the rest of the body, including its role as a stress mediator, remained, surprisingly underappreciated and not well understood. Our research has focused on that other, "peripheral" side of NPY. In this review, we will discuss those actions of NPY on the cardiovascular system and metabolism, as they relate to adaptation to stress, and attempt to both distinguish NPY's effects from and integrate them with the effects of the classical stress mediators, glucocorticoids, and catecholamines. To limit the bias of someone (ZZ) who has viewed the world of stress through the eyes of NPY for over 20 years, fresh insight (DH) has been solicited to more objectively assess NPY's contributions to stress-related diseases and the body's ability to adapt to stress. 相似文献
98.
Pye D Kyriakouli DS Taylor GA Johnson R Elstner M Meunier B Chrzanowska-Lightowlers ZM Taylor RW Turnbull DM Lightowlers RN 《Nucleic acids research》2006,34(13):e95
The human mitochondrial genome (mtDNA) encodes polypeptides that are critical for coupling oxidative phosphorylation. Our detailed understanding of the molecular processes that mediate mitochondrial gene expression and the structure–function relationships of the OXPHOS components could be greatly improved if we were able to transfect mitochondria and manipulate mtDNA in vivo. Increasing our knowledge of this process is not merely of fundamental importance, as mutations of the mitochondrial genome are known to cause a spectrum of clinical disorders and have been implicated in more common neurodegenerative disease and the ageing process. In organellar or in vitro reconstitution studies have identified many factors central to the mechanisms of mitochondrial gene expression, but being able to investigate the molecular aetiology of a limited number of cell lines from patients harbouring mutated mtDNA has been enormously beneficial. In the absence of a mechanism for manipulating mtDNA, a much larger pool of pathogenic mtDNA mutations would increase our knowledge of mitochondrial gene expression. Colonic crypts from ageing individuals harbour mutated mtDNA. Here we show that by generating cytoplasts from colonocytes, standard fusion techniques can be used to transfer mtDNA into rapidly dividing immortalized cells and, thereby, respiratory-deficient transmitochondrial cybrids can be isolated. A simple screen identified clones that carried putative pathogenic mutations in MTRNR1, MTRNR2, MTCOI and MTND2, MTND4 and MTND6. This method can therefore be exploited to produce a library of cell lines carrying pathogenic human mtDNA for further study. 相似文献
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100.