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Regulation of eukaryotic genes
Gene silencing
Enhancers
Activators
Functional domains of activators
Idea for another extra credit project
Explore DNA binding domains of proteins.
1. Go to a web site with a Chime tutorial, e.g. GAL4 or Cro
2. Or use Kinemages
3. Write a roughly 2 page report on how a particular protein recognizes a DNA sequence
States of eukaryotic genes• Inactive:
– Closed chromatin– Open chromatin, but repressors or lack of
activators keep frequency of initiation low.– Open chromatin, transcription has initiated, but
polymerases will not elongate.
• Active:– Open chromatin, basal transcription: requires
TATA + Inr– Open chromatin, activated transcription:
requires enhancer or upstream activator sequences
Silent and open chromatin
Transcription initiation and pausing
Basal and activated transcription
Silencing Mechanism
Silencer
• Cis-acting sequences that cause a decrease in gene expression
• Similar to enhancer but has an opposite effect on gene expression
• Gene repression - inactive chromatin structure (heterochromatin)
• Examples– Telomeric silencing– a or genes - silent loci of mating type
switching in yeast
Silencer binding proteins
• Silencer binding protein serve as anchors for expansion of repressed chromatin
• Rap1 protein binds to silencer elements• SIR proteins (Silent Information Regulators)• Nucleates assembly of multi-protein complex
– hypoacetylated N-terminal tails of histones H3 and H4– methylated N-terminal tail of H3 (Lys 9)
• Experiments: Condensed chromatin– Resistant to DNaseI digestion– Delete silencer - genes are derepressed
Gene Silencing
Silencing Mechanism
Enhancers
• Cis-acting sequences that cause an increase in expression of a gene
• Act independently of position and orientation with respect to the gene.
• Can act to:– Increase the rate of initiation at a promoter– Increase the fraction of cells in which a
promoter is active
SV40 Control region
• Origin of replication
• Promoter and upstream activator sequences for early transcription
• Promoter for late transcription
• Enhancer
SV40 map
Many regulatory DNA sequences in SV40 control region
Stimulation of transcription by enhancer is independent of orientation and position
EarlyLate
T-Ag +
Enhancer
wt
Enh-
pos
orien
T-Ag +
T-Ag +T-Ag -
SV40:
Enhancers also regulate cellular genes
Enhancer contains multiple binding sites for transcriptional activators
EarlyLate
high level
Enhancer
wt
SV40:
A C B
low leveldeletion
revertant
T-Ag
C B
C BC high level
An enhanson
Enhancers can occur in a variety of positions with respect to genes
Transcription unitP
Ex1 Ex2
EnhancerEnhancer
Adjacent
Downstream
Internal
Distal
Upstream
Activator proteins
Modular nature of activator proteins
• DNA binding domain: recognition and binding to specific DNA sequences
• Multimerization domain: allows formation of homo- or hetero-multimers
• Activation domain: – Needed for increase in expression of
responding gene– Targets are still under investigation
• General transcription factors• Histone modifying enzymes• Nucleosome remodeling complexes, etc
Modular structure of GAL4
N C
1 98 148 196 768 881
Activation ActivationDNAbinding
DimerizationGAL80binding
Induction by galactose exposes an activation surface
• In the presence of galactose, GAL4 activates several genes whose products are required for galactose metabolism.
• GAL4 binds to a DNA sequence called UASG.
• In the absence of galactose, GAL80 blocks GAL4 activation.
• Binding of the sugar causes GAL80 to move.• This exposes the activation domain of GAL4.
Induction of GAL4
Domain swap experiments show the domains are interchangeable
• Fuse an DNA-binding domain (DBD) from one transcription factor to the activation domain (AD) of a different one.– DBD from LexA (E. coli)– AD from GAL4 (yeast)
• Now a target gene can be placed under control of the DNA binding site for the first factor
– GAL1 gene with oLex (LexA binding sites) can be
activated by the fusion protein.• Basis for 2-hybrid screen for any interacting proteins
Domain swap experiments: Diagram 1
Domain swap experiments: Diagram 2
Two Hybrid Screens (Interaction Cloning), part 1
Two Hybrid Screens (Interaction Cloning), part 2
