Properties of RNA polymerase
- Completely processive – single enzyme transcribes complete RNA
- Catalyses both initiation and elongation of RNA – no primer needed
- No proof reading mechanism
Different types of RNA polymerase where are they found
1: nucleolus
2+3: nucleoplasm
What do RNA polymerase 1 2 and 3 make
1) rRNA
2) mRNA, snRNA, snoRNA,miRNA
3) tRNA, rRNA, some snRNAs
What happens in initiation in transcription
- Specific GTFs that bind to correct promoter and recruit polymerase
- Binding of TATA box binding protein (TBP) and TBP associated factors to TATA box
- Causes sequential recruitment of other TFs for RNA polymerase 2 (TFIIs) e.g. TBII1,TF11B,TFIIF .
- Forms preinitiation complex: protein scaffold onto which polymerase is recruited
- On completion, the initiation complex/basal transcription apparatus unwinds stretch of double helix to reveal single stranded DNA that it will transcribe
What happens in elongation
- RNA polymerase 2 selects correct ribonucleotide triphosphate and catalyses formation of phosphodiester bond.
- RNA molecule doesn’t require primer and is synthesised in 5’3’ direction
- Normal base pairing but U not T, so mRNA strand complementary to DNA template
In what direction does polymerase move
- RNA pol 2 move unidirectionally away from promoter region along DNA
What happens in protein dependent termination
self-complementary RNA in palindromic GC-rich region forms hair pin in RNA structure due to base pairing, this hair pin followed by oligo (U) sequence (caused by T rich region). This complex destabilises weak association between RNA and DNA so they dissociate
What happens in protein independent termination
Rho protein binds to newly made RNA at C rich, G poor region scanning along RNA towards RNA polymerase (needs ATP). When it reaches RNA polymerase, it breaks DNA-RNA association, terminating transcription.
Where is the signal for termination of RNA pol
Newly transcribed RNA
How is preMrna processed
capping, polyadenylation and splicing.
What happens in capping
- A GMP nucleotide/G residue is added to the 5’ end of preMRNA by 5’-5’ triphosphate bond ; G residue is methylated and binds to cap binding complex. (methyl guanosine cap
What is the role of capping
protects the 5’ terminal of the mRNA against degradation (exonucleases can’t recognise 5’ end due to 5’-5’ linkage)
- improves ribosomal recognition for translation (recruits small ribosomal subunit)
- Provides scope for regulation of translation.
- Export machinery recognises and uses cap to help mRNA move out of nucleus
What end does capping protect
5’ END
How does splicing occur
- snRNA-mediated transesterification reaction results in 2 sequential breakages and rejoining of sugar phosphate backbone in RNA excision of introns and fusion of exons.
What does a splicesome consist of
snRNA, (bound to) splicing factor, in complex known as snRNPs
And, premRNA being processed
Describe importance of snRNAs
have complementary sequences to splice sites at each exon-intron junction so can hybridise with them in RNA-RNA interactions
What are splice sites
there are 5’ and 3’ splice sites at border of each exon/intron
Dinucletode found at 3’ and 5’ end of intron
5’ = GU
3’=AG
What is nonsense mediated decay
surveillance mechanism in which exon junction proteins act as markers to identify faulty Mrna. Exon junction complex downstream of stop codon is recognised and indicates that it’s a premature stop codon so faulty mRNA containing premature stop codons are degraded.
True of false, after normal stop codon, no more EJC complexes form
True
What happens after splicing at exon exon junctions
marked by deposition of exon junction proteins/complex.
Why is alternate splicing important
cells to generate several different proteins (i.e. exon skipping so many transcripts made) from a gene – enables tissue specific gene expression.
The more introns per gene…
Increased complexity of organism and greater regulation of splicing
How can alternatve splicing be enhanced
enhancer proteins, which bind to enhancer sequences packed into exons. Make splice site more attractive, provide binding site for components of spliceosome so more likely to include exon X in final mRNA.
