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Transcription stages

In allosteric enzymes, the activity of the enzyme is modulated by a non-covalently bound metabolite at a site on a protein other than the catalytic site. Normally, this results in a conformational change, which makes the catalytic site inactive or less active. Covalent modulated enzymes are interconverted between active and inactive forms by the action of other enzymes, some of which are modulated by allosteric-type control. Both of these control mechanisms are responsive to changes in cell conditions and typically the response time in allosteric control is a matter of seconds as compared with minutes in covalent modulation. A third type of control, the control of enzyme synthesis at the transcription stage of protein synthesis (see Appendix 5.6), can take several hours to take effect. [Pg.328]

Section 27.28 In the transcription stage of protein biosynthesis a molecule of messenger RNA (mRNA) having a nucleotide sequence complementary to that of DNA is assembled. Transcription is followed by translation, in... [Pg.1105]

Genes are DNA and carry the inheritable characteristics of an organism and these characteristics are normally expressed at the molecular level via protein synthesis Gene expression consists of two stages transcription and translation, both of which involve RNAs Sections 28 11 and 28 12 describe these RNAs and their roles m transcription and translation... [Pg.1172]

Both amantadiae and rknantadiae have been found to reduce the duration of influenza A-iaduced fever and malaise, and to lessen viral shedding. Prophylactic treatment has been recommended for high risk patients (95). It has been suggested that, ia the presence of amantadine, the influenza vims attaches normally to cells, but once iaside the ceU the vims fails to initiate repHcation. Thus amantadine appears to inhibit the initiation of transcription at an early stage between uncoating and viral-specific RNA synthesis (96). [Pg.310]

TFIIA and TFIIB are two basal transcription factors that are involved in the nucleation stages of the preinitiation complex by binding to the TBP-TATA box complex. Crystal structures of the ternary complex TFIIA-TBP-TATA box have been determined by the groups of Paul Sigler, Yale University, and Timothy Richmond, ETH, Zurich, and that of the TFIIB-TBP-TATA box by Stephen Burley and collaborators. The TBP-DNA interactions and the distortions of the DNA structure are essentially the same in these ternary complexes as in the binary TBP-TATA complex. [Pg.159]

Documentation checks are vital at this stage since you are being judged on your on-time shipment performance. A delay caused by an error in the ASN will jeopardize all your hard work to meet the shipment date. The system that prints the container labels should therefore use the same data that is entered onto the ASN in order to avoid error. Eliminate human transcription errors and you are halfway there. The only other action is making sure that what s in the box is what it says on the label. [Pg.488]

In addition to those described above, some of the newest compounds emerging in SERM development are ER 3-selective ligands and pathway-selective modulators that target the interaction of the ERs with the transcription factor NFkB. While such compounds are in the early stages of clinical evaluation, thus far they demonstrate great potential for use in the treatment of inflammatory disorders such as arthritis, inflammatory bowel disease, and like other SERMs, cancer [4]. [Pg.1116]

Since the SUMO pathway affects multiple pathways ranging from transcription, DNA repair, and intracellular trafficking over cell signaling and cell cycle control to basic metabolism, it is not suiprising that links to diseases and viral assaults are emerging. However, the field is not yet at a stage sufficiently developed for pharmacological intervention. Below we will describe selected examples for links of the SUMO pathway to diseases and viral functions. [Pg.1166]

Evidence for the involvement of a Cdc2/Cyc B complex in the mitotic stages of germ cell development comes from studies in Drosophila. Cyc B transcripts are abundant and uniformly distributed in the early Drosophila embryo (Whitfield et al., 1989, 1990 Lehner and O Farrell, 1990b). Maternally derived Cyc B transcripts are also concentrated at the posterior pole of the oocyte. Later, during embryogenesis, Cyc B tran-... [Pg.17]

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See also in sourсe #XX -- [ Pg.822 ]



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