Regulation of Gene Expression Chapter 18

About This Presentation

Title:

Regulation of Gene Expression Chapter 18

Description:

Regulation of Gene Expression Chapter 18 – PowerPoint PPT presentation

Number of Views:363

Avg rating:3.0/5.0

Slides: 116

Provided by: PatB172

Learn more at: https://www.lancasterschools.org

Category:

more less

Transcript and Presenter's Notes

Title: Regulation of Gene Expression Chapter 18

1
Regulation of Gene ExpressionChapter 18
2

3
(No Transcript)
4
Gene expression

Flow of genetic information
Genotype to phenotype
Genes to proteins
Proteins not made at random
Specific purposes
Appropriate times

5
Control of gene expression

Selective expression of genes
All genes are not expressed at the same time
Expressed at different times

6
Prokaryote regulation
7
Control of gene expression

Regulate at transcription
Gene expression responds to
Environmental conditions
Type of nutrients
Amounts of nutrients
Rapid turn over of proteins

8
Fig. 18-2
Precursor
Feedback inhibition
trpE gene
Enzyme 1
trpD gene
Regulation of gene expression
trpC gene
Enzyme 2
trpB gene
Enzyme 3
trpA gene
Tryptophan
(b) Regulation of enzyme production
(a) Regulation of enzyme activity
9
Prokaryote

Anabolism
Building up of a substance
Catabolism
Breaking apart a substance

10
Prokaryote

Operon
Section of DNA
Enzyme-coding genes
Promoter
Operator
Sequence of nucleotides
Overlaps promoter site
Controls RNA polymerase access to the promoter

11
(No Transcript)
12
Prokaryote

Multiple genes are expressed in a single gene
expression
trp operon
Trytophan
Synthesis
Lac operon
Lactose
Degradation

13
Prokaryote

trp Operon
Control system to make tryptophan
Several genes that make tryptophan
Regulatory region

14
Fig. 18-3a
trp operon
Promoter
Genes of operon
trpD
trpA
trpE
trpC
trpB
Operator
Stop codon
Start codon
mRNA 5?
RNA polymerase
mRNA
5?
A
B
C
D
E
Polypeptide subunits that make up enzymes for
tryptophan synthesis
15
Prokaryote

?tryptophan present
Bacteria will not make tryptophan
Genes are not transcribed
Enzymes will not be made
Repression

16
Prokaryote

Repressors
Proteins
Bind regulatory sites (operator)
Prevent RNA polymerase attaching to promoter
Prevent or decrease the initiation of
transcription

17
Prokaryote

Repressors
Allosteric proteins
Changes shape
Active or inactive

18
Prokaryote

?tryptophan
Tryptophan binds the trp repressor
Repressor changes shape
Active shape
Repressor fits DNA better
Stops transcription
Tryptophan is a corepressor

19
Fig. 18-3b-2
DNA
No RNA made
mRNA
Protein
Active repressor
Tryptophan (corepressor)
(b) Tryptophan present, repressor active, operon
off
20
(No Transcript)
21
Prokaryote

?tryptophan
Nothing binds the repressor
Inactive shape
RNA polymerase can transcribe

22
Fig. 18-3a
trp operon
Promoter
Promoter
Genes of operon
DNA
trpD
trpA
trpR
trpE
trpC
trpB
Operator
Regulatory gene
Stop codon
Start codon
3?
mRNA 5?
RNA polymerase
mRNA
5?
A
B
C
D
E
Protein
Inactive repressor
Polypeptide subunits that make up enzymes for
tryptophan synthesis
(a) Tryptophan absent, repressor inactive, operon
on
23
(No Transcript)
24
Prokaryote

Lactose
Sugar used for energy
Enzymes needed to break it down
Lactose present
Enzymes are synthesized
Induced

25
Prokaryote

lac Operon
Promoter
Operator
Genes to code for enzymes
Metabolize (break down) lactose

26
Prokaryote

Lactose is present
Repressor released
Genes expressed
Lactose absent
Repressor binds DNA
Stops transcription

27
(No Transcript)
28
Prokaryote

Allolactose
Binds repressor
Repressor releases from DNA
Inducer
Transcription begins
Lactose levels fall
Allolactose released from repressor
Repressor binds DNA blocks transcription

29
Fig. 18-4b
lac operon
DNA
lacY
lacZ
lacA
lacI
RNA polymerase
3?
mRNA
mRNA 5?
5?
Permease
Transacetylase
?-Galactosidase
Protein
Inactive repressor
Allolactose (inducer)
(b) Lactose present, repressor inactive, operon on
30
Fig. 18-4a
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
31
(No Transcript)
32
(No Transcript)
33
Prokaryote

Lactose tryptophan metabolism
Adjustment by bacteria
Regulates protein synthesis
Response to environment
Negative control of genes
Operons turned off by active repressors
Tryptophan repressible operon
Lactose inducible operon

34
Prokaryote
35
Prokaryote

Activators
Bind DNA
Stimulate transcription
Involved in glucose metabolism
lac operon

36
Prokaryote

Activator
Catabolite activator protein (CAP)
Stimulates transcription of operons
Code for enzymes to metabolize sugars
cAMP helps CAP
cAMP binds CAP to activate it
CAP binds to DNA (lac Operon)

37
Prokaryote

Glucose elevated cAMP low
cAMP not available to bind CAP
Does not stimulate transcription
Bacteria use glucose
Preferred sugar over others.

38
(No Transcript)
39
Prokaryote

lac operon
Regulated by positive negative control
Low lactose
Repressor blocks transcription
High lactose
Allolactose binds repressor
Transcription happens

40
Prokaryote

lac operon
Glucose also present
CAP unable to bind
Transcription will proceed slowly
Glucose absent
CAP binds promoter
Transcription goes quickly

41
(No Transcript)
42
Eukaryote gene expression

All cells in an organism have the same genes
Some genes turned on
Others remain off
Leads to development of specialized cells
Cellular differentiation

43
Eukaryote gene expression

Gene expression assists in regulating development
Homeostasis
Changes in gene expression in one cell helps
entire organism

44
Control of gene expression

Chromosome structure
Transcriptional control
Posttranscriptional control

45
Fig. 18-6
Signal
NUCLEUS
Chromatin
Chromatin modification
DNA
Gene available for transcription
Gene
Transcription
Exon
RNA
Primary transcript
Intron
RNA processing
Tail
mRNA in nucleus
Cap
Transport to cytoplasm
CYTOPLASM
mRNA in cytoplasm
Translation
Degradation of mRNA
Polypeptide
Protein processing
Active protein
Degradation of protein
Transport to cellular destination
Cellular function
46
Eukaryotes

1. DNA is organized into chromatin
2. Transcription occurs in nucleus
3. Each gene has its own promoter

47
(No Transcript)
48
Chromatin structure

DNA is tightly packaged
Heterochromatin
Tightly packed
Euchromatin
Less tightly packed
Influences gene expression
Promoter location
Modification of histones

49
Chromatin structure

Histone acetylation
Acetyl groups (-COCH3)
Attach to Lysines in histone tails
Loosen packing
Histone methylation
Methyl groups (-CH3)
Tightens packing

50
Fig. 18-7
Histone tails
Amino acids available for chemical modification
DNA double helix
(a) Histone tails protrude outward from a
nucleosome
Acetylated histones
Unacetylated histones
(b) Acetylation of histone tails promotes loose
chromatin structure that permits transcription
51
Chromatin structure

Methylation of bases (cytosine)
Represses transcription
Embryo development

52
Eukaryotes

Epigenetic change
Chromatin modifications
Change in gene expression
Passed on to the next generation
Not a DNA sequence change

53
Transcription control

RNA polymerase must bind DNA
Proteins regulate by binding DNA
RNA polymerase able to bind or not
Stimulates transcription or blocks it

54
Fig. 18-8-3
Poly-A signal sequence
Enhancer (distal control elements)
Proximal control elements
Termination region
Exon
Exon
Exon
Intron
Intron
DNA
Downstream
Upstream
Promoter
Transcription
Exon
Exon
Exon
Intron
Intron
Primary RNA transcript
Cleaved 3? end of primary transcript
5?
RNA processing
Poly-A signal
Intron RNA
Coding segment
mRNA
3?
Start codon
Stop codon
Poly-A tail
3? UTR
5? Cap
5? UTR
55
Eukaryotes

Transcription
RNA Polymerase
Transcription factors (regulatory proteins)
General transcription factors (initiation
complex)
Specific transcription factors

56
Eukaryotes

Initiation of transcription
Activator proteins
Activator binds the enhancers
Enhancers (DNA sequences)
Interacts with the transcription factors
Binds to the promoter
RNA polymerase binds and transcription begins

57
Fig. 18-9-2
Promoter
Activators
Gene
DNA
Distal control element
Enhancer
TATA box
General transcription factors
DNA-bending protein
Group of mediator proteins
58
Fig. 18-9-3
Promoter
Activators
Gene
DNA
Distal control element
Enhancer
TATA box
General transcription factors
DNA-bending protein
Group of mediator proteins
RNA polymerase II
RNA polymerase II
Transcription initiation complex
RNA synthesis
59
(No Transcript)
60
Eukaryotes
D\Chapter_18\A_PowerPoint_Lectures\18_Lecture_Pre
sentation\1809TranscripInitiationA.html
61
Fig. 18-10
Enhancer
Promoter
Albumin gene
Control elements
Crystallin gene
LENS CELL NUCLEUS
LIVER CELL NUCLEUS
Available activators
Available activators
Albumin gene not expressed
Albumin gene expressed
Crystallin gene not expressed
Crystallin gene expressed
(b) Lens cell
(a) Liver cell
62
Post transcriptional control

RNA processing
Primary transcript
Exact copy of the entire gene
RNA splicing
Introns removed from the mRNA
snRNPs (small nuclear ribonulceoproteins)

63
(No Transcript)
64
(No Transcript)
65
Post transcriptional control

Splicing plays a role in gene expression
Exons can be spliced together in different ways.
Leads to different polypeptides
Originated from same gene

66
Post transcriptional control

Example in humans
Calcitonin CGRP
Hormones released from different organs
Derived from the same transcript

67
Fig. 18-11
Exons
DNA
Troponin T gene
Primary RNA transcript
RNA splicing
or
mRNA
68
Post transcriptional control
D\Chapter_18\A_PowerPoint_Lectures\18_Lecture_Pre
sentation\1811RNAProcessingA.html
69
Post transcriptional control

Transport of transcript
Passes through nuclear pores
Active transport
Cannot pass until all splicing is done

70
Post transcriptional control

mRNA degradation
Life span
Some can last hours, a few weeks
mRNA for hemoglobin survive awhile

D\Chapter_18\A_PowerPoint_Lectures\18_Lecture_Pre
sentation\1813mRNADegradationA.html
71
Post transcriptional control

Translation of RNA
Translation factors are necessary
Regulate translation
Translation repressor proteins
Stop translation
Bind transcript
Prevents it from binding to the ribosome

72
Post transcriptional control

Ferritin (iron storage)
Aconitase
Translation repressor protein
Binds ferritin mRNA
Iron will bind to aconitase
Aconitase releases the mRNA
Ferritin production increases

73
Post transcriptional control

Protein modification
Phosphorylation
Other alterations can affect the activity of
protein
Insulin
Starts out as a larger molecule
Cut into more active sections

74
Post transcriptional control

Protein modification
Degradation
Protein is marked by small protein
Protein complex then breaks down proteins
Proteasomes

75
Post transcriptional control
D\Chapter_18\A_PowerPoint_Lectures\18_Lecture_Pre
sentation\1812ProteinDegradationA.html
D\Chapter_18\A_PowerPoint_Lectures\18_Lecture_Pre
sentation\1812ProteinProcessingA.html
76
Fig. 18-UN4
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
Translation
mRNA degradation
or
mRNA
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.
77
Post transcriptional control

Most gene regulation-transcription
New discovery
Small RNAs
21-28 nucleotides long
Play a role in gene expression
New transcript before leaving the nucleus

78
Post transcriptional control

RNA interference
RNA forming double stranded loops from newly
formed mRNA
Loops are formed
Halves have complementary sequences
Loops inhibit expression of genes
Where double RNA came from

79
Post transcriptional control

Dicer
Cuts double stranded RNA into smaller RNAs
called
microRNA (miRNA)
Small interfering RNA (siRNAs)

80
Fig. 18-13
Hairpin
miRNA
Hydrogen bond
Dicer
miRNA
miRNA- protein complex
3?
5?
(a) Primary miRNA transcript
Translation blocked
mRNA degraded
(b) Generation and function of miRNAs
81
Post transcriptional control

miRNAs bind mRNA
Prevents translation
siRNAs breaks apart mRNA before its translated

82
Post transcriptional control

siRNAs play a role in heterochromatin formation
Block large regions of the chromosome
Small RNAs may also block transcription of
specific genes

83
Fig. 18-UN5
Chromatin modification
Small RNAs can promote the formation
of heterochromatin in certain regions, blocking
transcription.
Chromatin modification
Transcription
Translation
RNA processing
miRNA or siRNA can block the translation of
specific mRNAs.
Translation
mRNA degradation
Protein processing and degradation
mRNA degradation
miRNA or siRNA can target specific mRNAs for
destruction.
84
Embryonic development

Zygote gives rise to many different cell types
Cells ?tissues ?
organs ? organ systems
Gene expression
Orchestrates developmental programs of animals

85
Fig. 18-14a
(a) Fertilized eggs of a frog
86
(No Transcript)
87
(No Transcript)
88
Embryonic development

Zygote to adult results
Cell division
Cell differentiation
Cells become specialized in structure function
Morphogenesis
creation of from
Body arrangement

89
Fig. 47-6
(a) Fertilized egg
(b) Four-cell stage
(c) Early blastula
(d) Later blastula
90
Fig. 47-1
1 mm
91
Fig. 46-17
(c) 20 weeks
(a) 5 weeks
(b) 14 weeks
92
Embryonic development

All cells same genome
Differential gene expression
Genes regulated differently in each cell type

93
Fig. 18-10
Enhancer
Promoter
Albumin gene
Control elements
Crystallin gene
LENS CELL NUCLEUS
LIVER CELL NUCLEUS
Available activators
Available activators
Albumin gene not expressed
Albumin gene expressed
Crystallin gene not expressed
Crystallin gene expressed
(b) Lens cell
(a) Liver cell
94
Embryonic development

Specific activators
Materials in egg cytoplasm
Not homogeneous
Set up gene regulation
Carried out as cells divide

95
Embryonic development

Cytoplasmic determinants
Maternal substances in the egg
Influence early development
Zygote divides by mitosis
Cells contain different cytoplasmic determinants
Leads to different gene expression

96
Fig. 18-15a
Unfertilized egg cell
Sperm
Nucleus
Fertilization
Two different cytoplasmic determinants
Zygote
Mitotic cell division
Two-celled embryo
(a) Cytoplasmic determinants in the egg
97
Embryonic development

Environment around cell influences development
Induction
Signals from nearby embryonic cells
Cause transcriptional changes in target cells
Interactions between cells induce differentiation
of specialized cell types

98
Fig. 18-15b
NUCLEUS
Early embryo (32 cells)
Signal transduction pathway
Signal receptor
Signal molecule (inducer)
(b) Induction by nearby cells
99
G\Chapter_18\A_PowerPoint_Lectures\18_Lecture_Pre
sentation\1815bbCellSignalingA.html
100
Embryonic development

Determination
Observable differentiation of a cell
Commits a cell to its final fate
Cell differentiation is marked by the production
of tissue-specific proteins
Gives cell characteristic structure function

101
Embryonic development

Myoblasts
Produce muscle-specific proteins
Form skeletal muscle cells
MyoD
One of several master regulatory genes
Produces proteins
Commit cells to becoming skeletal muscle

102
Embryonic development

MyoD protein
Transcription factor
Binds to enhancers of various target genes
Causes expression

103
Fig. 18-16-1
Nucleus
Master regulatory gene myoD
Other muscle-specific genes
DNA
Embryonic precursor cell
OFF
OFF
104
Fig. 18-16-2
Nucleus
Master regulatory gene myoD
Other muscle-specific genes
DNA
Embryonic precursor cell
OFF
OFF
OFF
mRNA
MyoD protein (transcription factor)
Myoblast (determined)
105
Fig. 18-16-3
Nucleus
Master regulatory gene myoD
Other muscle-specific genes
DNA
Embryonic precursor cell
OFF
OFF
OFF
mRNA
MyoD protein (transcription factor)
Myoblast (determined)
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)
106
Embryonic development

Pattern formation
Development of spatial organization of tissues
organs
Begins with establishment of the major axes
Positional information
Molecular cues control pattern formation
Tells a cell its location relative to the body
axes neighboring cells

107
Fruit fly

Unfertilized egg contains cytoplasmic
determinants
Determines the axes before fertilization
After fertilization,
Embryo develops into a segmented larva with three
larval stages

108
Fig. 18-17a
Thorax
Head
Abdomen
0.5 mm
Dorsal
Right
BODY AXES
Posterior
Anterior
Left
Ventral
(a) Adult
109
Fig. 18-17b
Follicle cell
Egg cell developing within ovarian follicle
1
Nucleus
Egg cell
Nurse cell
Egg shell
Unfertilized egg
2
Depleted nurse cells
Fertilization Laying of egg
Fertilized egg
3
Embryonic development
Segmented embryo
4
0.1 mm
Body segments
Hatching
Larval stage
5
(b) Development from egg to larva
110
Fruit fly

Homeotic genes
Control pattern formation in late embryo,larva
and adult

111
Fig. 18-18
Eye
Leg
Antenna
Wild type
Mutant
112
Fruit fly

Maternal effect genes
Encode for cytoplasmic determinants
Initially establish the axes of the body of
Drosophila
Egg-polarity genes
Maternal effect genes
Control orientation of the egg
Consequently the fly

113
Fruit Fly

Bicoid gene
Maternal effect gene
Affects the front half of the body
An embryo whose mother has a mutant bicoid gene
Lacks the front half of its body
Duplicate posterior structures at both ends

114
Fig. 18-19a
EXPERIMENT
Tail
Head
A8
T1
T2
A7
T3
A6
A1
A5
A2
A3
A4
Wild-type larva
Tail
Tail
A8
A8
A7
A7
A6
Mutant larva (bicoid)
115
(No Transcript)

Write a Comment

User Comments (0)