QUESTIONS: 1. Name the DNA for which transcription requires SP1. 2. What is the evidence as seen in the autoradiogram? 3. What type of transcription factor is SP1? METHOD 1. Set up in vitro transcription reaction with DNA template, 32P-UTP, plus or minus transcription factor SP1 2. Separate transcripts by gel electrophoresis
QUESTIONS: Based on the results shown in the autoradiogram, we see a band in lane 1 (from transfection with plasmid 1) with but not in lane 2 (from transfection with plasmid 2). 1. What does the band in the autoradiogram represent? 2. What do these results tell us about the nature of the extra piece of DNA included in plasmid 1 and absent in plasmid 2? (What is the “name” for this extra piece of DNA?)
Lecture 9 Transcription Termination, mRNA processing, & post- transcriptional control Reading: Chapter 12 Molecular Biology syllabus web siteweb site
Transcription termination Several mechanisms exist to regulate the termination of transcription in bacteria and eukaryotic cells In bacteria, the two principle mechanisms involve RNA polymerase and one of these also requires the termination factor Rho In eukaryotes, the mechanisms for terminating transcription differ for each of the three types of RNA polymerase
Rho-independent termination occurs at characteristic sequences in E. coli DNA
Premature termination by attenuation helps regulate expression of some bacterial operons
Mechanism of attenuation of trp-operon transcription
Rho-dependent termination sites are present in some -phage and E. coli genes Figure 11-4 The Rho factor is a hexameric protein around which a 70- to 80-base segment of the growing RNA transcript wraps Rho then moves along the RNA in the 3 direction until it eventually unwinds the RNA-DNA hybrid at the active site of RNA polymerase Whether transcription is terminated or not depends on whether Rho “catches up” to RNA polymerase Rho-dependent sites have no clear consensus sequence and Rho-dependent termination operates at relatively few operons
Three eukaryotic RNA polymerases employ different termination mechanisms RNA polymerase I is terminated by a mechanism that requires a polymerase-specific termination factor, which binds downstream of the transcription unit RNA polymerase II is terminated in a region kb beyond the poly(A) addition site, and termination is coupled to the process that cleaves and polyadenylates the 3 end of a transcript RNA polymerase III is terminated after polymerizing a series of U residues
Transcription of HIV genome is regulated by an antitermination mechanism
Processing of eukaryotic mRNA
The 5-cap is added to nascent RNAs after initiation by RNA polymerase II
Pre-mRNAs are cleaved at specific 3 sites and rapidly polyadenylated
During the final step in formation of mature, functional mRNA, introns are removed and exons are spliced together
Splicing occurs at short, conserved sequences Consensus sequences around 5 and 3 splice sites in vertebrate pre-mRNA
Analysis of RNA products formed in an in vitro splicing reaction
Splicing proceeds via two sequential transesterfication reactions
Small nuclear RNAs (snRNAs) assist in the splicing reaction
Self-splicing introns-evolutionary models of trans-acting snRNAs?
Other post-transcriptional regulatory mechanisms Alternative splicing (e.g. ion channels affecting auditory cells; affecting wiring/neuronal connections in the brain) mRNA 3’ ends that target mRNA to cytoplasmic location (resulting in protein gradients across cell) mRNA stability affected by 3’ untranslated sequences Regulation of antisense transcripts and siRNA RNA editing (common in mt in protozoa/plants and chloroplasts; rarer in higher eukaryotes) Post-transcriptional modification (e.g. tRNA) Translational activation of mRNAs (cytoplasmic polyadenylation of stored mRNAs with short polyA tails- induced upon fertilization of xenopus oocytes or synaptic activity in neuronal dendrites)