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21.
The specific substance from Pneumococcus type 34 (41). The phosphodiester linkages 总被引:6,自引:5,他引:1
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G. J. F. Chittenden W. K. Roberts J. G. Buchanan J. Baddiley 《The Biochemical journal》1968,109(4):597-602
1. The phosphate groups in the type-specific substance S.34 from Pneumococcus type 34 (U.S. type 41) were shown to join the hydroxyl group at position 1 or 5 of ribitol and the hydroxyl group at position 3 of a d-galactofuranosyl residue in the next repeating unit. 2. A partial structure of the type-specific substance was derived. 3. New syntheses of d-galactose 2-phosphate and d-galactose 3-phosphate are described. 相似文献
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Structure and function of amylases. I. The subunit structure of porcine pancreatic -amylase 总被引:1,自引:0,他引:1
The isozymes of porcine pancreatic α-amylase were reduced with dithiothreitol to two enzymatically active subunits which had molecular weights of 25,000 daltons each. These subunits could be isolated and separated from each other by chromatography on DEAE-cellulose. Subsequent treatment of the subunits with EDTA, DTT, and iodoacetamide gave derivatives that emerged in identical elution volumes from DEAE-cellulose columns and that migrated very rapidly and identically on disc-gel electrophoresis. These latter experiments suggested that the subunits might have similar primary structures. This hypothesis was tested by preparing tryptic peptide maps of the subunits. The results indicated that the subunits had very similar, if not identical, primary structures. 相似文献
24.
The phosphorylation of thymidine has been studied in a model evaporating pond environment. Evaporation of dilute solutions of thymidine and ammonium oxalate in the presence of apatite leads to the synthesis of nucleotides. The presence of organic compounds such as cyanamide or urea substantially increases the yields of products. Solutions of cyanogen, when heated and evaporated in the presence of nucleoside and apatite, produce similarly high yields of nucleotide without added condensing agents. The mechanism of the reaction appears to involve the hydrolysis of cyanogen to produce ammonium oxalate and urea, among other products. An evolutionary continuum leading from the cosmically abundant CN moiety to the establishment of conditions favorable for phosphorylation on the primitive earth is suggested. 相似文献
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The synthesis of 2(R),3-dihydroxypropyl and 2(R),3(R)-dihydroxybutyl β-d-fructopyranosides, and some derivatives, employing Sharpless-type catalytic asymmetric dihydroxylation procedures is described. Some aspects of the reactions, including stereoselectivities and chemical evidence for the assigned stereochemistry of the main products are reported. 相似文献
27.
Chittenden TW Pak J Rubio R Cheng H Holton K Prendergast N Glinskii V Cai Y Culhane A Bentink S Schwede M Mar JC Howe EA Aryee M Sultana R Lanahan AA Taylor JM Holmes C Hahn WC Zhao JJ Iglehart JD Quackenbush J 《PloS one》2010,5(12):e15581
GIPC1 is a cytoplasmic scaffold protein that interacts with numerous receptor signaling complexes, and emerging evidence suggests that it plays a role in tumorigenesis. GIPC1 is highly expressed in a number of human malignancies, including breast, ovarian, gastric, and pancreatic cancers. Suppression of GIPC1 in human pancreatic cancer cells inhibits in vivo tumor growth in immunodeficient mice. To better understand GIPC1 function, we suppressed its expression in human breast and colorectal cancer cell lines and human mammary epithelial cells (HMECs) and assayed both gene expression and cellular phenotype. Suppression of GIPC1 promotes apoptosis in MCF-7, MDA-MD231, SKBR-3, SW480, and SW620 cells and impairs anchorage-independent colony formation of HMECs. These observations indicate GIPC1 plays an essential role in oncogenic transformation, and its expression is necessary for the survival of human breast and colorectal cancer cells. Additionally, a GIPC1 knock-down gene signature was used to interrogate publically available breast and ovarian cancer microarray datasets. This GIPC1 signature statistically correlates with a number of breast and ovarian cancer phenotypes and clinical outcomes, including patient survival. Taken together, these data indicate that GIPC1 inhibition may represent a new target for therapeutic development for the treatment of human cancers. 相似文献
28.
Chittenden TW Claes F Lanahan AA Autiero M Palac RT Tkachenko EV Elfenbein A Ruiz de Almodovar C Dedkov E Tomanek R Li W Westmore M Singh JP Horowitz A Mulligan-Kehoe MJ Moodie KL Zhuang ZW Carmeliet P Simons M 《Developmental cell》2006,10(6):783-795
Branching morphogenesis is a key process in the formation of vascular networks. To date, little is known regarding the molecular events regulating this process. We investigated the involvement of synectin in this process. In zebrafish embryos, synectin knockdown resulted in a hypoplastic dorsal aorta and hypobranched, stunted, and thin intersomitic vessels due to impaired migration and proliferation of angioblasts and arterial endothelial cells while not affecting venous development. Synectin(-/-) mice demonstrated decreased body and organ size, reduced numbers of arteries, and an altered pattern of arterial branching in multiple vascular beds while the venous system remained normal. Murine synectin(-/-) primary arterial, but not venous, endothelial cells showed decreased in vitro tube formation, migration, and proliferation and impaired polarization due to abnormal localization of activated Rac1. We conclude that synectin is involved in selective regulation of arterial, but not venous, growth and branching morphogenesis and that Rac1 plays an important role in this process. 相似文献
29.
Background
Alcoholism presents widespread social and human health problems. Alcohol sensitivity, the development of tolerance to alcohol and susceptibility to addiction vary in the population. Genetic factors that predispose to alcoholism remain largely unknown due to extensive genetic and environmental variation in human populations. Drosophila, however, allows studies on genetically identical individuals in controlled environments. Although addiction to alcohol has not been demonstrated in Drosophila, flies show responses to alcohol exposure that resemble human intoxication, including hyperactivity, loss of postural control, sedation, and exposure-dependent development of tolerance. 相似文献30.
Most bacteria in the ocean can be motile. Chemotaxis allows bacteria to detect nutrient gradients, and hence motility is believed to serve as a method of approaching sources of food. This picture is well established in a stagnant environment. In the ocean a shear microenvironment is associated with turbulence. This shear flow prevents clustering of bacteria around local nutrient sources if they swim in the commonly assumed "run-and-tumble" strategy. Recent observations, however, indicate a "back-and-forth" swimming behavior for marine bacteria. In a theoretical study we compare the two bacterial swimming strategies in a realistic ocean environment. The "back-and-forth" strategy is found to enable the bacteria to stay close to a nutrient source even under high shear. Furthermore, rotational diffusion driven by thermal noise can significantly enhance the efficiency of this strategy. The superiority of the "back-and-forth" strategy suggests that bacterial motility has a control function rather than an approach function under turbulent conditions. 相似文献