Mechanisms regulating gene expression Flashcards
What is involved in the regulation of gene transcription?
Transcription- chromatin structure, histone modification (epigenetic), regulatory proteins (transcription factors)
DNA has non coding regions that regulate both transcription and translation.
List the gene regulatory regions
Promoter = core promoter and proximal promotor region
1) Core promotor comprises DNA sequence within -40 to +40 of start of transcription (contains TATA box)
2) promotor proximal region -200 to +50 bp relative to RNa start site (contains the CCAAT) box
3) reguatory elements- enhancers (positive regulation) or repressors/ silencers (negative regulation). Bind transcription factor proteins (non covalently) that interact through DNA looping with basal transcription machinery. these elements act independently of orientation and distance to RNA transcription start site. So if you take a sequence and invert it, regulatory elements will still bind.
4) boundary elements are DNA segments at the ends of a gene region that function as insulators and bloack the influence of positive or negative DNA elements from affect adjacent genes. ex: prevent spread of heterochromatin
What modifications can be made to histones and how do they affect transcription?
1) deacetylation - generates heterochromatin (condesnsed-inert chromatin) less transcription
2) acetylation - euchromatin (open active chromatin) more transcription
3) methylation- gene repression or expression depending on the residue methylated and the number of methy groups added.
Explain how regulation of chromatin strucure acts cooperatively with transcription factor proteins to regulate gene expression.
Histone acetylation/ deacetylation, methylation/demethylation, and ATP dependent chromatin remodeling enzymes (SWI/SNF proteins) act to either make DNA more or less accessible to the protein complexes involved in transcription to eith up-regulate or down-regulate DNA transcription. facilitates the assembly of general transcription factors, mediator, and RNA polymerase at the promoter.
Describe the order of events leading to transcription
Gene activator protein binds to chromatin → chromatin remodeling complex comes in and remodels chromatin → Histone modification enzymes covalently modify histones → Additional activator proteins bind to the gene regulatory region → mediator, general transcription factors, and RNA polymerase bind to assemble the pre-initiation complex at the promoter → binding of other activator proteins and rearrangement of proteins in the pre-initiation complex leads to transcription initiation.
Regulatory elements (enhancer or repressor)
1) short sequences of DNA that bind to the transcription factors
2) can be located up to 50kB from the start site of transcription
3) regulatory elements can be placed upstream or downstream from start of transcription
4) Each regulatory element may bind multiple trancription factors
histone acetylation
histone acetylation opens the chromatin. Lysines in the histone tails are acetylated, eliminating the side-chain positive charge (ammonium +) This breaks the charge interactions between adjacent nucelosomes allowing the chromatin structure to open.
done by histone acetyl transferases (HAT)
Histone deacetylation
generates heterochromatin. catalyzed by histone deacetylases HDACs
Histone tail modifications
Histone tails can be modified by histone methylases, adding a methyl group to lysines and arginines or histone kinases which ad phosphates to serine side chains
each modification type attracts proteins that specifically bind to the chemically modified site.
Chromodomains
Domains on proteins that specifically bind to methylated lysines and arginines.
bromodomains
domains of proteins that specifically bind to acetylated lysine.
Properties of transcription factors
1) have modular designs with an activation domain, dimerization domain, and a DNA binding domain
2) The DNA binding domain often contains a structural morif with amino acis that interact with a unique DNA element exposed by the major and/or minor groove of the DNA helix.
3) Commonly (but not always) transcription factors are homo- or hetero-dimers. (i.e. HTH, HLH, and bZIP TFs)
4) Dimers bind to a palindrome in the DNA, which contains a symmetry appropriate for dimer binding to two succesive turns in the DNA helix
Explain the modularity of TF proteins
Transcription factors can be divided into modules (domains). Usually have a dimerization module, have a DNA binding domain (module). Has an activation region (domain). Activation domain is the active part of the molecule can repress as well as activate. Never have observed the structure of an activation domain because they are dynamic and unobservable through crystallization technologies. These modules can be separated from one another. You can take a DNA binding domain and attach it to the domain of an activation domain.
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Characteristics of helix-turn-helix
1) Each monomer contains a recognition alpha-helix joined by a short turn to a second alpha helix. The second helix supports the recognition helix by hydrophobis interactions.
2) The HTH is embedded in a domain that may be all alpha, an all beta, or an alpha-beta type of domain. The type of dimer interface interaction will depend on the transcription factor protein
3) In dimer HTH proteins, the recognition helices from each monomer bind to adjacent turns to the major groove. The DNA site is palindromic
4) the two copies of the recognition helix are are seperated by exactly one turn (3.4 nm)
5) Each half of the paindrome sequence binds a monomer
Characteristics of the Helix loop helix proteins
1) Dimer structure. The two monomers are held together in a four helix bundle: each monomer contributes 2 alpha helices connected by a flexible loop of protein. A specific DNA sequence is bound by the two alpha helices that project from the frou-helix bundle.
2) each monomer contains a recognition helix joined by a loop to a second helix, which contins a leucine ziper motif.
3) The recognition helices from each monomer bind to adjacent turns of the major groove (usually a palindrome)
4) Myc, Max, Mad and MyoD