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11.
Haruo Nagayama Koji Nagano Akira Ikezaki Tetsuo Tashiro 《Chronobiology international》1991,8(3):203-209
To investigate the possibility of chronotherapy with antidepressants for patients with depression, we gave single daily doses of clomipramine 150 mg/day to 30 patients with depression at three different times of day, i.e., morning, noon, or before bedtime, using a double-blind method over a 4-week period. Beneficial effects differed according to the administration time of day, with the most effective result being found for the administration at noon. Time-dependent differences in side effects were observed in tremors and dryness of mouth. An additional 10 patients were administered their medications three times a day by traditional, equally divided doses, and the efficacy was inferior than daily single doses at noon. The study results showed the significance of the administration time of day for the benefits and side effects of antidepressant therapy for depression. 相似文献
12.
A possible clinical application of multicytokine-producing cytotoxic mononuclear cell (MCCM) therapy
Mitsuo Katano Eiro Kubota Hiroshi Yamamoto Mitsunari Nakamura Tatsuya Matsuo Takeharau Hisatsugu Takeshi Katsuki Hisao Koga Kiyonobu Ikezaki Kazuo Tabuchi Fumio Nagumo Jutaro Tadano 《Biotherapy》1991,3(4):373-379
When peripheral blood mononuclear cells (PBMC) were incubated with a streptococcal preparation, OK-432, for 24 h, PBMC acquired cytolytic activity against cultured and fresh human tumor cells. Such PBMC were called OK-432-activated mononuclear cells (OK-MC). OK-MC produce several kinds of cytokines such as interferon (IFN), IFN, and tumor growth inhibitory factor (TGIF) bothin vitro andin vivo. OK-MC-produced cytokines also inhibited the growth of cultured and fresh human tumor cells. The growth inhibition was examined by human tumor clonogenic assay using a double-layer agar technique. The results indicate that two pathways of anti-tumor activity are induced in OK-MC, i.e., cell-mediated and cytokine-mediated. 相似文献
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15.
Inhibition of epidermal growth factor-induced DNA synthesis by tyrosine kinase inhibitors 总被引:10,自引:0,他引:10
Kazuo Umezawa Takashi Hori Hirohisa Tajima Masaya Imoto Kunio Isshiki Tomio Takeuchi 《FEBS letters》1990,260(2):201-205
We prepared methyl 2,5-dihydroxycinnamate as a stable analogue of erbstatin, a tyrosine kinase inhibitor. This analogue was about 4 times more stable than erbstatin in calf serum. It inhibited epidermal growth factor receptor-associated tyrosine kinase in vitro with an IC50 of 0.15 μg/ml. It also inhibited in situ autophosphorylation of epidermal growth factor receptor in A431 cells. Methyl 2,5-dihydroxycinnamate was shown to delay the S-phase induction by epidermal growth factor in quiescent normal rat kidney cells, without affecting the total amount ofDNA synthesis. The effect of erbstatin on S-phase induction was smaller, possibly because of its shorter life time. 相似文献
16.
The rates of the utilization of glucose and mannose in Schizosaccharomycespombe were determined using glucose-grown cells. The rate ofaerobic fermentation in the medium containing glucose was notaffected by the addition of mannose. In contrast, CO2 evolutionin the mannose medium was greatly enhanced by the addition ofglucose, showing nearly the same rate as the glucose medium.The rate of glucose consumption was much higher than that ofmannose. In a medium containing both sugars, the rates of consumptionof glucose and mannose interfered with each other, the mannoseconsumption rate being more seriously affected by glucose. Intracellularaccumulation of the reducing sugar from the mannose containingmedium proceeded much more rapidly and reached a higher levelthan with the glucose medium. However, trehalose accumulatedat a much higher rate with the glucose medium. Consequently,the net increase in cellular carbohydrates, as calculated fromthe amount of reducing sugar and trehalose, proceeded much morerapidly in the glucose medium. We concluded that the differencein the rates of utilization of glucose and mannose might bedue to the difference in the rates of uptake of both sugars.
1Present adress: Department of Biology, Faculty of Science,Osaka City University, Sumiyoshiku, Osaka 558. To whom reprintrequests should be adressed. (Received June 24, 1975; ) 相似文献
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Phylogeography of Fischer’s blue,Tongeia fischeri,in Japan: Evidence for introgressive hybridization
Ekgachai Jeratthitikul Takehiro Hara Masaya Yago Tateo Itoh Min Wang Shin-ichi Usami Tsutomu Hikida 《Molecular phylogenetics and evolution》2013,66(1):316-326
The widespread lycaenid butterfly Tongeia fischeri is distributed from eastern Europe to northeastern Asia and represented by three geographically isolated populations in Japan. In order to clarify the phylogeographic history of the species, we used sequences of three mitochondrial (COI, Cyt b and ND5) and two nuclear (Rpl5 and Ldh) genes of 207 individuals collected from 55 sites throughout Japan and five sites on the Asian continent. Phylogenetic trees and the median-joining network revealed six evolutionary mitochondrial haplotype clades, which corresponded to the geographic distribution of the species. Common ancestors of Japanese T. fischeri might have come to Japan during the mid-Pleistocene by multiple dispersals of continental populations, probably via a land bridge or narrow channel between western Japan and the Korean Peninsula. The geographical patterns of variation of mitochondrial and nuclear markers are discordant in northeastern Kyushu, possibly as a result of introgressive hybridization during the ancient contact between the Kyushu and Shikoku populations in the last glacial maximum. The phylogeographic pattern of T. fischeri in Japan are probably related to the geological history, Pleistocene climatic oscillations and distribution of the host plant. 相似文献
19.
Streptococcus pyogenes causes a broad spectrum of infectious diseases, including pharyngitis, skin infections and invasive necrotizing fasciitis. The initial phase of infection involves colonization, followed by intimate contact with the host cells, thus promoting bacterial uptake by them. S. pyogenes recognizes fibronectin (Fn) through its own Fn‐binding proteins to obtain access to epithelial and endothelial cells in host tissue. Fn‐binding proteins bind to Fn to form a bridge to α5β1‐integrins, which leads to rearrangement of cytoskeletal actin in host cells and uptake of invading S. pyogenes. Recently, several structural analyses of the invasion mechanism showed molecular interactions by which Fn converts from a compact plasma protein to a fibrillar component of the extracellular matrix. After colonization, S. pyogenes must evade the host innate immune system to spread into blood vessels and deeper organs. Some Fn‐binding proteins contribute to evasion of host innate immunity, such as the complement system and phagocytosis. In addition, Fn‐binding proteins have received focus as non‐M protein vaccine candidates, because of their localization and conservation among different M serotypes.Here, we review the roles of Fn‐binding proteins in the pathogenesis and speculate regarding possible vaccine antigen candidates. 相似文献
20.
Shigeyuki Fujimoto Naoya Itsumura Tokuji Tsuji Yasumi Anan Natsuko Tsuji Yasumitsu Ogra Tomoki Kimura Yusaku Miyamae Seiji Masuda Masaya Nagao Taiho Kambe 《PloS one》2013,8(10)
The activation process of secretory or membrane-bound zinc enzymes is thought to be a highly coordinated process involving zinc transport, trafficking, transfer and coordination. We have previously shown that secretory and membrane-bound zinc enzymes are activated in the early secretory pathway (ESP) via zinc-loading by the zinc transporter 5 (ZnT5)-ZnT6 hetero-complex and ZnT7 homo-complex (zinc transport complexes). However, how other proteins conducting zinc metabolism affect the activation of these enzymes remains unknown. Here, we investigated this issue by disruption and re-expression of genes known to be involved in cytoplasmic zinc metabolism, using a zinc enzyme, tissue non-specific alkaline phosphatase (TNAP), as a reporter. We found that TNAP activity was significantly reduced in cells deficient in ZnT1, Metallothionein (MT) and ZnT4 genes (ZnT1
−/−
MT
−/−
ZnT4
−/− cells), in spite of increased cytosolic zinc levels. The reduced TNAP activity in ZnT1
−/−
MT
−/−
ZnT4
−/− cells was not restored when cytosolic zinc levels were normalized to levels comparable with those of wild-type cells, but was reversely restored by extreme zinc supplementation via zinc-loading by the zinc transport complexes. Moreover, the reduced TNAP activity was adequately restored by re-expression of mammalian counterparts of ZnT1, MT and ZnT4, but not by zinc transport-incompetent mutants of ZnT1 and ZnT4. In ZnT1
−/−
MT
−/−
ZnT4
−/− cells, the secretory pathway normally operates. These findings suggest that cooperative zinc handling of ZnT1, MT and ZnT4 in the cytoplasm is required for full activation of TNAP in the ESP, and present clear evidence that the activation process of zinc enzymes is elaborately controlled. 相似文献