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trans Activation of the simian virus 40 enhancer.   总被引:14,自引:4,他引:10       下载免费PDF全文
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We examined the effects of simian virus 40 infection on the temporal and spatial organization of initiation sites for DNA replication in Muntjac cells by means of light microscopic DNA fiber autoradiography. Initiation at multiple sites along the DNA fiber in virus-infected confluent Muntjac cells was more nearly synchronous than in serum-deprived controls, although temporal control in the infected cells did not reach the level observed in cells incubated in serum-enriched medium. Initiation sites in virus-infected cells appeared to be spatially closer together than in either uninfected serum-deprived or uninfected serum-enriched cells. This change did not appear to be the result of the induction or repression by simian virus 40 of clusters of replication units with new and different organizations.  相似文献   

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Do transcriptional enhancers also augment DNA replication?   总被引:5,自引:0,他引:5  
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The regulation of transformed phenotypes was studied in newly isolated preadipose cell lines which were established after infection with simian virus 40 tsA58 dl2009. The clonal cell lines isolated exhibited most of the characteristics typical of transformed cells. The transformants, however, were able to differentiate into adipocytes in the presence of low calf serum (0.5%) and a combination of several hormones, including hydrocortisone and insulin. Treatment with insulin alone stimulated the growth of these cells but did not induce lipid accumulation without added hydrocortisone. The effect of hydrocortisone was accompanied by a restoration of growth control in the transformants after they reached high cell density. The blot hybridization analysis of cellular DNAs digested by restriction enzymes revealed that simian virus 40 genomes were integrated at multiple separate sites at which a head-to-tail oligomeric insertion took place. Large T antigen was synthesized in growing cells but was regulated at high cell density when cells were committed to differentiate by glucocorticoids. These results suggest that the glucocorticoid hydrocortisone is capable of restoring growth regulation at high cell densities to simian virus 40-transformed preadipose cell lines.  相似文献   

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Complexes between simian virus 40 DNA and topoisomerase I (topo I) were isolated from infected cells treated with camptothecin. The topo I break sites were precisely mapped by primer extension from defined oligonucleotides. Of the 56 sites, 40 conform to the in vitro consensus sequence previously determined for topo I. The remaining 16 sites have an unknown origin and were detectable even in the absence of camptothecin. Only 11% of the potential break sites were actually broken in vivo. In the regions mapped, the pattern of break sites was asymmetric. Most notable are the clustering of sites near the terminus for DNA replication and the confinement of sites to the strand that is the template for discontinuous DNA synthesis. These asymmetries could reflect the role of topo I in simian virus 40 DNA replication and suggest that topo I action is coordinated spatially with that of the replication complex.  相似文献   

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