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Transcription Biology Review. Bios 691 – Systems Biology January 2008. Outline. Gene structure Chromatin structure & modifications Transcription apparatus Transcription factors and cofactors Elongation and termination RNA capping, splicing, and adenylation RNA processing and miRNA’s.
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Transcription Biology Review Bios 691 – Systems Biology January 2008
Outline • Gene structure • Chromatin structure & modifications • Transcription apparatus • Transcription factors and cofactors • Elongation and termination • RNA capping, splicing, and adenylation • RNA processing and miRNA’s
Chromosome Organization • Mammalian chromosomes tend to fill discrete regions within the nucleus • An elaborate network of fibrils maintains these arrangements • RNA ‘factories’ at distinct locations do most of the transcription work • Nucleoli are factories for rRNA
Chromatin Structure • Protein scaffolds anchor the DNA • Within the scaffold there are loops • Most transcription happens on the loops • Much chromatin is wrapped in 30nm ‘heterochromatin’
Fine Structure of Chromatin • Heterochromatin – inaccessible • Bound with many proteins • Centromeres; telomeres; some other areas • Euchromatin – accessible • Still needs to be opened Telomeric Heterochromatin and Sirtuins Euchromatin: 30 nm & open
Gene Structure – Exons & Introns Exon Size distribution
Gene Structure – Initiation Sites • Most (~2/3) genes have multiple promoters • Most promoters are either ‘sharp’: • Very narrow range • Usually TATA + Inr • Often tissue specific • or ‘broad’: • Typically 70 bp range • Rarely TATA / Inr • Often widespread
Histones and Modifications Histone tails can be modified DNA contacts histones on their tails Histones can stay loose or assemble tightly
DNA Methylation Adding a Methyl to Cytosine Cytosine methylation is passed on to daughter cells
DNA-Binding Proteins • All proteins interact weakly with DNA • Proteins with projecting amino acids interact with the DNA major groove • Hydrogen bonds stabilize position of proteins on DNA • Proteins that line up several amino acid contacts bind strongly to specific DNA sequences
Transcription Factor Families • Several structures line up amino acids • Helix-turn-Helix (Homeodomain) • Helix-loop-helix • Zinc Finger • Mostly dimers • These families have proliferated because of their role in attracting transcription apparatus
Cofactors • Frequently the effect of DNA-binding proteins depends on co-factors • E.g. ER sits on the DNA but requires estrogen as a co-factor to function • Myc requires Max as a co-factor to stimulate transcription • If Max is coupled with Mad instead, the genes are repressed
Kick-starting Pol II & Elongation • Mediator protein bridges TF proteins and RNA Pol II • Contains kinase domains – may phosphorylate CTD of RNA Pol II
Initiating Transcription TBP on a TATA Box
RNA Polymerase II The cycle of adding nucleotides RNA Polymerase II Structure RNA (red) copied from DNA (blue) by RNA Polymerase II
RNA Processing Steps • Nucleus • capped, • spliced, • cleaved, • polyadenylated • Exported • Cytoplasm • stored • translated • degraded
Capping mRNA The RNA factory
Poly-adenylating RNA • Poly-A Polymerase adds ~100-150 Adenines to 3’ end • After export to cytoplasm, nucleases chop off ~10-20 A’s at a bite • Nucleases compete with ribosomes for mRNA’s • When ~30 A’s left degradation speeds up
RNA Export • RNA has to be passed through nuclear pores to show up in the cytoplasm (where we measure it)
P-Bodies • Loci where RNA • accumulates and • is degraded • Have their own structural proteins
Implications for Systems Biology • Levels of TF’s on a promoter may not predict levels of transcripts • Rate of transcription may not predict level of mRNA in the cytoplasm • Levels of mRNA in cytoplasm may not predict levels of protein