1. Regulation of Gene Expression
Chapter 18
Regulation of Gene Expression

2. activity production Feedback inhibition Regulation of gene expression
Precursor
Feedback
inhibition
trpE gene
Enzyme 1
trpD gene
Regulation
of gene
expression
Enzyme 2
trpC gene
trpB gene
Figure 18.2 Regulation of a metabolic pathway
Enzyme 3
trpA gene
Tryptophan
(a) Regulation of enzyme
activity
(b) Regulation of enzyme
production

3. Polypeptide subunits that make up enzymes for tryptophan synthesis
trp Operon - Repressible trp operon
Promoter
Promoter
Genes of operon
DNA
trpR
trpE
trpD
trpC
trpB
trpA
Regulatory
gene
Operator
Start codon
Stop codon 3
mRNA 5
mRNA
RNA
polymerase 5 E D C B A
Protein
Inactive
repressor
Polypeptide subunits that make up
enzymes for tryptophan synthesis
(a) Tryptophan absent, repressor inactive, operon on.
DNA
No RNA made
Figure 18.3 The trp operon in E. coli: regulated synthesis of repressible enzymes
mRNA
Protein
Active
repressor
Tryptophan
(corepressor)
(b) Tryptophan present, repressor active, operon off.

4. Allolactose inducer lac Operon - inducible Regulatory gene Promoter
Operator
DNA
lacI
lacZ No
RNA
made 3
mRNA
RNA
polymerase 5
Active
repressor
Protein
(a) Lactose absent, repressor active, operon off.
lac operon
DNA
lacI
lacZ
lacY
lacA
RNA
polymerase
Figure 18.4 The lac operon in E. coli: regulated synthesis of inducible enzymes
For the Cell Biology Video Cartoon Rendering of the lac Repressor from E. coli, go to Animation and Video Files. 3
mRNA
mRNA 5 5
-Galactosidase
Permease
Protein
Transacetylase
Allolactose
inducer
Inactive
repressor
(b) Lactose present, repressor inactive, operon on.

5. Positive Gene Regulation
Promoter
Operator
DNA
lacI
lacZ
CAP-binding site
RNA
polymerase
binds and
transcribes
Active
CAP
cAMP
Inactive lac
repressor
Inactive
CAP
Allolactose
(a) Lactose present, glucose scarce (cAMP level
high): abundant lac mRNA synthesized
Promoter
Operator
DNA
lacI
lacZ
Figure 18.5 Positive control of the lac operon by catabolite activator protein (CAP)
CAP-binding site
RNA
polymerase less
likely to bind
Inactive
CAP
Inactive lac
repressor
(b) Lactose present, glucose present (cAMP level
low): little lac mRNA synthesized

6. Histone Modifications Acetylation Promotes Transcription
tails
Amino
acids
available
for chemical
modification
DNA
double helix
(a) Histone tails protrude outward from a
nucleosome.
Figure 18.7 A simple model of histone tails and the effect of histone acetylation
Unacetylated histones
Acetylated histones
(b) Acetylation of histone tails promotes loose chromatin structure that permits transcription.

7. distal control elements
Control Elements = Transcription Factors
Poly-A signal
sequence
Enhancer
distal control elements
Proximal
control elements
Termination
region
Exon
Intron
Exon
Intron
Exon
DNA
Upstream
Downstream
Promoter
Transcription
Primary RNA
transcript
Exon
Intron
Exon
Intron
Exon
Cleaved 3 end
of primary
transcript 5
RNA processing
Intron RNA
Poly-A
signal
Figure 18.8 A eukaryotic gene and its transcript
Coding segment
mRNA 3
Start
codon
Stop
codon
5 Cap
5 UTR
3 UTR
Poly-A
tail

8. Activators Enhancer General transcription factors Transcription
Promoter
Gene
DNA
Distal control
element
Enhancer
TATA
box
General
transcription
factors
DNA-bending
protein
Group of
mediator proteins
RNA
polymerase II
Figure 18.9 A model for the action of enhancers and transcription activators
RNA
polymerase II
Transcription
initiation complex
RNA synthesis

9. Alternative RNA Processing
Exons
DNA
Troponin T gene
Primary
RNA
transcript
Figure Alternative RNA splicing of the troponin T gene
RNA splicing
mRNA or

10. Proteasome - Protein Degradation
and ubiquitin
to be recycled
Ubiquitin
Proteasome
Protein to
be degraded
Ubiquitinated
protein
Protein
fragments
(peptides)
Protein entering a
proteasome
Figure Degradation of a protein by a proteasome

11. Modifiers of Translation
Hairpin
miRNA
Hydrogen
bond
Dicer
miRNA
miRNA-
protein
complex 5 3
(a) Primary miRNA transcript
Figure Regulation of gene expression by miRNAs
mRNA degraded
Translation blocked
(b) Generation and function of miRNAs

12. (a) Fertilized eggs of a frog (b) Newly hatched tadpole
Fig
Figure From fertilized egg to animal: What a difference four days makes
(a) Fertilized eggs of a frog
(b) Newly hatched tadpole

13. Differential Gene Expression
Unfertilized egg cell
Sperm
Nucleus
Fertilization
Two different
cytoplasmic
determinants
NUCLEUS
Early embryo
(32 cells)
Zygote
Signal
transduction
pathway
Mitotic
cell division
Signal
receptor
Figure Sources of developmental information for the early embryo
Two-celled
embryo
Signal
molecule
(inducer)
(a) Cytoplasmic determinants in the egg
(b) Induction Signals by
nearby cells

14. MyoD Protein - Muscle Cell Differentiation
Nucleus
Master regulatory gene myoD
Other muscle-specific genes
DNA
Embryonic
precursor cell
OFF
OFF
mRNA
OFF
MyoD protein
(transcription
factor)
Myoblast
(determined)
Figure Determination and differentiation of muscle cells
mRNA
mRNA
mRNA
mRNA
Myosin, other
muscle proteins,
and cell cycle–
blocking proteins
MyoD
Another
transcription
factor
Part of a muscle fiber
(fully differentiated cell)

15. BODY AXES Pattern Formation in Drosophila fruit fly
Head
Thorax
Abdomen
0.5 mm
BODY
AXES
Dorsal
Right
Anterior
Posterior
Left
Ventral
(a) Adult
Follicle cell 1
Egg cell
developing within
ovarian follicle
Nucleus
Egg
cell
Nurse cell 2
Unfertilized egg
Egg
shell
Depleted
nurse cells
Fertilization
Laying of egg 3
Fertilized egg
Figure Key developmental events in the life cycle of Drosophila
Embryonic
development 4
Segmented
embryo
0.1 mm
Body
segments
Hatching 5
Larval stage
(b) Development from egg to larva

16. Affects Polarity Development
Bicoid Protein
Affects Polarity Development
EXPERIMENT
Tail
Head T1 T2 A8 T3 A7 A1 A2 A6 A3 A4 A5
Wild-type larva
Tail
Tail A8 A8 A7 A6 A7
Mutant larva (bicoid)
RESULTS
Figure Is Bicoid a morphogen that determines the anterior end of a fruit fly?
Fertilization,
translation
of bicoid
mRNA
100 µm
Anterior end
Bicoid mRNA in mature
unfertilized egg
Bicoid protein in early
embryo
CONCLUSION
Nurse cells
Egg
bicoid mRNA
Developing egg
Bicoid mRNA in mature unfertilized egg
Bicoid protein in early embryo

17. within a control element within the gene
Proto-oncogene to Oncogene
Proto-oncogene
DNA
Translocation or
transposition:
Gene amplification:
Point mutation:
within a control element
within the gene
New
promoter
Oncogene
Oncogene
Figure Genetic changes that can turn proto-oncogenes into oncogenes
Normal growth-
stimulating
protein in excess
Normal growth-stimulating
protein in excess
Normal growth-
stimulating
protein in excess
Hyperactive or
degradation-
resistant protein

18. EFFECTS OF MUTATIONS Multi-Step Model of Cancer Development
Colon
EFFECTS OF MUTATIONS
Loss of tumor-
suppressor gene
APC (or other) 1
Activation of
ras oncogene 2
Loss of
tumor-suppressor
gene p53 4
Colon wall
Loss of
tumor-suppressor
gene DCC 3
Additional
mutations 5
Figure A multistep model for the development of colorectal cancer
Normal colon
epithelial cells
Small benign
growth (polyp)
Larger benign
growth (adenoma)
Malignant tumor
(carcinoma)

19. Genes not expressed Genes expressed Promoter Operator Genes
Review
Genes not expressed
Genes expressed
Promoter
Operator
Genes
Fig. 18-UN2
Active repressor:
no inducer present
Inactive repressor:
inducer bound
Fig. 18-UN3

20. Eukaryotic Differential Gene Expression
Signal
NUCLEUS
Chromatin
Chromatin modification
DNA
Gene available
for transcription
Gene
Transcription
RNA
Exon
Primary transcript
Intron
RNA processing
Tail
Cap
mRNA in nucleus
Transport to cytoplasm
CYTOPLASM
mRNA in cytoplasm
Degradation
of mRNA
Translation
Figure 18.6 Stages in gene expression that can be regulated in eukaryotic cells
Polypeptide
Protein processing
Active protein
Degradation
of protein
Transport to cellular
destination
Cellular function

21. Protein processing and degradation
Regulation of Gene Expression
Chromatin modification
Transcription
• Genes in highly compacted
chromatin are generally not
transcribed.
• Regulation of transcription initiation:
DNA control elements bind specific
transcription factors.
• Histone acetylation seems to
loosen chromatin structure,
enhancing transcription.
Bending of the DNA enables activators to
contact proteins at the promoter, initiating
transcription.
• DNA methylation generally
reduces transcription.
• Coordinate regulation:
Enhancer for
liver-specific genes
Enhancer for
lens-specific genes
Chromatin modification
Transcription
RNA processing
• Alternative RNA splicing:
RNA processing
Primary RNA
transcript
mRNA
degradation
Translation
mRNA or
Fig. 18-UN4
Protein processing
and degradation
Translation
• Initiation of translation can be controlled
via regulation of initiation factors.
mRNA degradation
• Each mRNA has a
characteristic life span,
determined in part by
sequences in the 5 and
3 UTRs.
Protein processing and degradation
• Protein processing and
degradation by proteasomes
are subject to regulation.

22. You should now be able to:
Explain the concept of an operon and the function of the operator, repressor, and corepressor.
Explain the adaptive advantage of grouping bacterial genes into an operon.
Explain how repressible and inducible operons differ and how those differences reflect differences in the pathways they control.

23. Explain how DNA methylation and histone acetylation affect chromatin structure and the regulation of transcription.
Define control elements and explain how they influence transcription.
Explain the role of promoters, enhancers, activators, and repressors in transcription control.

24. 7. Explain how maternal effect genes affect polarity and development in Drosophila embryos.
8. Explain how mutations in tumor-suppressor genes can contribute to cancer.