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Biol 568 Advanced Topics in Molecular Genetics

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Title: Biol 568 Advanced Topics in Molecular Genetics

1
Biol 568Advanced Topics in Molecular Genetics

2
Oncogenes and Cancer

Genes cell phenotypes
Transforming viruses
Retroviral oncogenes

3
Cancer Cell Phenotypes

Immortalization
indefinite growth (no other phenotype changes)
Transformation
independence of factors normally required for
growth
Metastasis
cells are mobile invade normal tissue

4
Terminology

Primary cells
immediate descendants of cells taken from an
organism
mimic in vivo phenotype
generally survive for only a short period of time
in culture

5
Terminology

Crisis
primary cell cultures enter into senescence
majority of the cells die
Established cell line
cells that have passed through crisis
non-tumorigenic
immortal, and other phenotypic changes

6
Primary cell culture
Primary Cell Culture
Crisis
Established Cell Line
CELLS
TIME
7
Fig 30.4 Cancer Cell Properties
8
Cell Properties

Anchorage dependence
Serum (growth factor) dependence
Density dependent inhibition
Cytoskeletal organization

9
Cell Properties

Anchorage dependence
cells need a solid or firm surface to stick to
Serum (growth factor) dependence
growth factors in serum are essential for growth
of cells in culture

10
Cell Properties

Density-dependent inhibition
cells grow only to a certain density, then stop
may involve cell - cell contacts
Cytoskeletal organization
cells are flat extended
elongated network of actin filaments
Cells also grow as a monolayer

11
in vitro vs. in vivo
Established cell lines provide only an
approximation of in vivo control -changes in
the chromosomal complement -not true diploids/
aneuploids
12
Cell Properties

Transformed cells show altered phenotypes
no anchorage dependence
no dependence on serum (growth factors)
no density-dependent inhibition of growth
altered cytoskeleton

Form tumors

13
Fig 30.6 EM of normal and transformed cells
NORMAL
TRANSFORMED
14
Genetic Basis

What genetic events convert normal cells to
transformed cells?
multiple events
6-7 events over 20-40 years
propensity to cancer may be inherited
Single genetic change
exposure to carcinogens increases risk

15
Genetic Basis

Two classes of genes which can cause
transformation when mutated
Oncogenes
Tumor suppressor genes

16
Oncogenes

Initially identified as genes carried by viruses
which transform cells
viral oncogenes have cellular counterparts
proto-oncogenes
about 100 oncogenes have been identified
many different functions
transmembrane proteins, TFs, etc.

17
Oncogenes

Oncogene mutations
Gain of Function mutation
mutational change of protein
constitutive activation
overexpression
failure to shut off expression

18
Tumor suppressor genes

Loss of function mutation
detected by deletion or inactivating mutation
common in hereditary cancers
patients lack both alleles
about 10 tumor suppressor genes known
genes normally constrain cell cycle

19
Transformation of Cells

may occur
spontaneously
through exposure to carcinogens
by viral infection
transforming virus or tumor virus

20
Fig 30.4 Transforming viruses may carry
oncogenes
HPV human papillomaviruses gt60 known warts,
cervical cancers Adeno Adenoviruses gt 80
known mouse cells transformed (not
human) Herpes Epstein-Barr assoc. with variety
of diseases (lymphoma)
21
Fig 30.9 Permissive vs. nonpermissivecells
Two cellular responses to viral infection -
infection - transformation
22
Permissive vs. Non-Permissive

Permissive cells
Productive infection cycle
Release of new viral progeny
Cell death
Non permissive cells
Abortive infection cycle
Transformed cells
Phenotypic changes

23
Fig 30.10 Transformation by virusesadenovirus
or polyomavirus
Product of early gene required for transformation
24
Fig 30.11 Genetic transfer by
retroviruseshorizontal or vertical transfer of
genetic info
Both RNA and DNA forms of viral genome
25
Transforming Retroviruses

Two general groups
Non-defective viruses
Acute transforming viruses

26
Transforming Retroviruses

Acute transforming viruses
have a viral oncogene
derived from a cellular proto-oncogene
replication defective (needs helper virus)

27
Fig 30.12 Acute transforming retrovirus
28
Fig 30.14 Oncogenes of transforming retroviruses
Each transforming retrovirus caries an oncogene
29
Difference in v-onc and c-onc

v-onc viral oncogene
c-onc cellular proto-oncogene
More than 30 c-onc genes identified
Same oncogene present in several viruses

30
Expression of the v-onc sequence is capable of
transformation

RSV, temp sensitive mutations of v-src
Transformed phenotype reverted or regained
v-src gene needed for both initiation and
maintenance of transformation

31
2 Models for Oncogenicity

Quantitative model
Qualitative model

32
Difference in v-onc and c-onc

Quantitative model
v-onc and c-onc are indistinguishable
v-onc is oncogenic
more highly expressed
expressed in inappropriate cell types
expression cannot be switched off

33
Difference in v-onc and c-onc

Qualitative model
c-onc lacks oncogenic properties
v-onc is mutated version
Gain of function

34
v-onc vs. c-onc genes
Gene Changes Identity v-onc region
missing mos 11 / 369 97 None H-ras 3 /
189 98 None K-ras 7 / 189
96 None sis 18 / 220 92 None myc 2 /
417 99 None src 16 / 514 97 C-term
19 aa fms 20 / 930 98 C-term 50 aa erbB 99
/ 600 83 N-term half C-term erbA 22 / 396
95 N-term 12 aa myb 11 / 372 97 N C
termini (268 aa)
35
Level of Expression also Important
Oncogenicity when overexpressed
36
Fig 30.15 Transfection assay
Tumor
Extract DNA
Transfect
Detection of oncogenes from transformed cell
lines (not normal cells)
Integration
colony of transformed cells
37
Transforming Activity

DNA Isolated only from tumorigenic cells
Transfection with DNA
Appearance of foci
Indicator for transforming ability of DNA
Genomic DNA
Specific genes

38
Isolated Transforming Genes

Closely related sequences in DNA of normal cells
May have counterparts in the oncogenes carried
by known transforming viruses

39
ras transforming gene

multiple genes
H-ras, N-ras, K-ras
collectively known as p21ras
H-ras and K-ras have v-ras counterparts
very similar

40
ras oncogenes

Single base mutations can covert proto-oncogene
into oncogene
most commonly at aa12 or aa 61
Glycine at 12 (Gly G)
any other aa except Pro makes oncogenic
Glutamine at 61 (Gln Q)
alteration makes oncogenic some less effective

41
ras proto-oncogene

monomeric guanine nucleotide-binding protein
active with GTP bound
inactive with GDP bound
Two proteins influence ras activity
GAP - stimulate ras to hydrolyze GTP
GEF - stimulates replacement of GDP with GTP
See Fig 30.16

42
signal transduction pathway
EGF
EGFR
Sos
GAP
Grb
Pi
MAPKK
fos
jun
Transcription
43
signal transduction pathway
Cdc25
Ira 1, 2
Pi
GDP
S. cerevisiae
44
Fig 30.16 Ras Activity
(GEF)
45
Fig 30.16 Ras Activity
46
Fig 30.16 Ras Activity
47
Activation of protooncogenes

Insertion of retroviruses
Translocation
Amplification

48
Oncogene Amplification

Established cell lines
Susceptible to karyotypic changes
Presence of known oncogenes in the amplified
regions
In Tumors
Amplification of particular oncogenes

49
Activation by Retroviral Insertion

Insertion of a non-defective virus
First noticed in bursal lymphomas
T-cell lymphomas
Ability of LTRs to cause expression of cellular
genes

50
Fig 30.17 Insertion of ALV at c-myc locus
51
Fig 30.17 Insertion of ALV at c-myc locus
52
Fig 30.17 Insertion of ALV at c-myc locus
53
Coding sequence of c-myc does not change

Oncogenicity
caused by loss of normal control
increased expression of the gene
Other oncogenes activated by the same mechanism
c-erb, c-myb, c-mos, c-raf

54
Activation by Translocation

Translocation to a new chromosomal location
Reciprocal translocation
Illegitimate recombination between two
chromosomes
Known examples
Oncogenes brought by translocation to the
proximity of Ig or TCR locuses

55
Fig 30.18Reciprocal chromosomal translocation
B cells
T cells
56
c-myc activation by translocation

In B cells
c-myc is translocated to Ig locus (H)
c-myc brought to actively expressed region
2- to 10-fold increase in expression
structure of c-myc may be changed
In T cells
c-myc is translocated to TCR locus

57
c-myc and tumorigenic phenotypes

Continued high expression of c-myc is oncogenic
Expression of c-myc must be switched off to allow
immature lymphocytes to differentiate into T and
B-cells

58
c-myc and tumorigenic phenotypes

c-myc linked to Ig enhancer
Transgenic mice develop lymphomas
Present in both mature and immature B-cells
Over-expression of c-myc is tumorigenic
throughout the B-cell lineage

59
c-myc and tumorigenic phenotypes

c-myc linked to LTR ( mmtv)
Transgenic mice develop variety of cancers
Over-expression of c-myc transforms the cell into
corresponding tumor

60
c-myc activation

Activation of c-myc via
retroviral insertion
chromosomal translocation
gene amplification
Activation by increased/altered expression
NOT by altered amino acid sequence

61
Philadelphia Translocation

Creates a hybrid oncogene
Philadelphia chromosome
present in patients with CML
Translocation of 5000 kb region from chr 9
carrying c-abl gene to the bcr gene of chr 22

62
Figure 30.19
Chr22
Chr9
bcr-abl fusion
Philadelphia Chromosomes
63
Why is Bcr-Abl fusion oncogenic?

Bcr-Abl protein activates Ras pathway via Grb2
and Shc
c-abl codes for a tyrosine kinase activity
In v-abl changes in N-terminal region activate
kinase activity and transforming capacity
Lack of N-terminal region may cause inappropriate
activation of kinase activity in bcr-abl fusion

64
Oncogenes

Components of signal transduction cascades
Growth factor receptor kinases
Cytoplasmic kinases
Regulators of gene expression

65
Signal Transduction Cascade
Growth Factor
Growth factor receptor
membrane
Adaptor (Ras)
Kinase Cascade (serine threonine kinases)
Transcription Factors
nucleus
66
Fig 30.20 Different Types of Oncogenes
67
Fig 30.20 Different Types of Oncogenes
68
Fig 30.20 Different Types of Oncogenes
69
Common feature

Trigger changes in cell phenotypes
initiating or responding to changes related to
cell growth
direct changes in gene expression

70
Oncogenes

Components of signal transduction cascades
Growth factor receptor kinases
Cytoplasmic kinases
Regulators of gene expression

71
Transmembrane receptors Initiate signal
trasduction pathways
Tyrosine Kinases Targets Tyrosine residues of
target proteins
Cytoplasmic enzymes Provide catalytic functions
for receptors that lack kinase activity
72
Transmembrane receptors

Extra-, Intra-cellular regions
Kinase activity
Activated upon dimerization
Autophosphorylation reaction

73
Ligand binding induces receptor dimerization
74
Fig 30.21 Activation of GF receptor
Ligand binding induces dimerization Dimers
are active
Mutant is constitutively active - not repressed
Spontaneously forms dimers Constitutively
active
75
v-erb

Truncated version of c-erb/EGF receptor
lacks N- and C-terminal domains
N-terminal deletion causes spontaneous
dimerization
C-terminal deletion removes inhibitory domain
Contain activating mutations in the catalytic
domain
Oncogenicity Deletions/ mutations that
constitutively activate the receptor

76
v-erb

erb2 closely related to EGF receptor
mutations in transmembrane region
Dimer-formation increased
c-fms CSF-I receptor
mutations in extracellular domain
Dimer-formation increased, constitutively active
point mutations in C-terminal domain
Inhibitory effect of c-terminal domain abolished

77
Oncogenes

Components of signal transduction cascades
Growth factor receptor kinases
Cytoplasmic tyrosine kinases
Regulators of gene expression

78
src as prototype cytoplasmic tyrosine kinase

first kinase oncoproteins characterized
first tyrosine kinase
multiple viral oncogenes in this group
v-src, v-yes, v-fgr, v-fps/fes, v-abl, v-ros
N-terminus is modified
amino acid removed, end myristoylated

79
Fig 30.22 Src protein domains
80
Comparison of c-src and v-src
c-Src
v-Src
Property
Phosphorylate target tyrosine residues

20X
Attached to the membrane via myristylation

Autophosphorylated at Tyr-416
-

Phosphorylated at Tyr-527

-
C-terminal sequence replaced including Tyr-527
-

81
Src Phosphorylation see Fig 30.23
82
Control of src activity by phosphorylation

Mutation at Tyr527
activates the transforming potential of c-Src
c-Src-Phe527
becomes phosphorylated at Tyr-416
kinase activity increased 10X,
transforms target cells
Mutation at Tyr416
eliminates ability of c-Src to transform
c-SrcPhe 416, Phe 527
Kinase activity reduced

83
Control of src Activity by Phosphorylation

Tyr416 activates oncogenicity of Src
Tyr527 represses oncogenicity of c-Src

84
Fig 30.24 Receptor tyrosine kinase (src)
activation
85
Control of src Activation

Tyr 527-SH2 interaction required for inactivation
of c-Src
Tyr 527-SH2 binding critical for oncogenicity
inactivated by polyoma middle T antigen
inactivated by SH2-SH3 mutations
SH2-SH3 domains required for proper activation
of c-Src

86
Oncogenes

Components of signal transduction cascades
Growth factor receptor kinases
Cytoplasmic kinases
Regulators of gene expression

87
Oncogenes

Regulators of gene expression
Act directly at the level of expression
Oncogenes
rel, jun, fos erbA, myc, myb

88
v-Oncogenes

Quantitative or qualitative changes
changes in the level of expression
modifications, defective TFs, dominant negatives
alter expression of target genes
acquire specificity for new targets (less likely)

89
v-Rel

Transforming function of avian reticuloendothelios
is virus
B-cell lymphomas in chicken
c-Rel, family of NF-kB
Lacks 100 a.a. from C-terminal
Small point mutations in remaining sequence

90
Fig 30.26 Function of oncogenic factors

v-Rel, blocks NF-kB pleiotropic functions
v-Rel-NFkB dimers are inactive

91
AP1

Mediates transcription induced by phorbol esters
Activates promoters with AP1- binding sites
Dimer subunits coded by c-jun and c-fos
bZip TFs basic region leucine zippers
v-jun and v-fos
truncated versions of c-jun and c-fos
point mutations

92
Fig 30.26 Function of oncogenic factors
93
v-erbA

c-erbA
Thyroid hormone receptor, family of steroid
receptors
Located in the nucleus
binds to response elements in promoters with or
without ligand
Binds to triiodothyronine with high affinity
Hormone binding needed to activate txn of
previously bound receptor

94
v-erbA

Truncated form of c-erbA
point mutations
T3 affinity abolished
v-erbA independent of hormone binding, cannot
stimulate transcription

95
Fig 30.26 Function of oncogenic factors
v-erbA, dominant negative, blocks functioning of
its normal cellular counterpart
96
c-jun, c-rel, c-fos, c-myc

Immediate early genes
may be involved in cascades that initiate cycling
Target genes may be involved in growth initiation

97
Transformation by Adenovirus E1A oncogene

E1A
Three transcripts, alternative splicing
13S, 12S, closely related
Posess ability to immortalize cells
Cooperate with other oncogenes for transformation
Different activates/ represses host gene
expression
Different domains required

98
Fig 30.27 Adenovirus E1A region is spliced to
form three transcripts
99
Adenovirus E1A Oncogene

Activates RNA polymerase II and III loci (domain
3)
Regulates host gene expression via protein
interactions (domains 1, 2)
Targets CBP/p300, TBP, RB, p 27

100
Tumor Suppressor Genes

Loss of both alleles is tumorigenc
Best known
Rb
p53

101
Retinoblastoma (Rb)

Childhood disease
Tumor of the retina
Inherited or sporadic (somatic mutation)
Associated with deletions of band q14 of
chromosome 13
Loss of function of Rb mutation/deletions that
abolish gene expression

102
Fig 30.28 Retinoblastoma
103
Rb protein

Nuclear phosphoprotein
influences cell cycle
Phosphorylated by cyclin/cdk at end of G1
Dephosphorylated during mitosis
Binds to specific targets
phosphorylation releases target proteins

104
Target proteins of Rb

E2F group of transcription factors
activate genes essential for S phase
Rb binding inhibits target activation
Rb represses gene expression via E2F
Rb prevents cell from entering S phase

105
Fig 30.29 Rb and the cell cycle
106
Tumor Suppressor Rb

Overexpression of Rb impedes cell growth
Rb- osteosarcoma cell lines
transfected with Rb
growth is impeded
Effect of Rb reverted by D cyclins
form cdk-cyclins that phosphorylate Rb
Other Rb type proteins
p107, p130

107
Fig 30.30 Tumor suppressors and cell cycle
control

108
Other cell cycle control proteins

Also tumor suppressor proteins
Small inhibitory proteins
p16, p21, p27
inhibit activity of cyclins in the quiescent
state ( G0)
inactivating mutations in tumors

109
Tumor Suppressor p53

Nuclear phosphoprotein
Associates with T antigen in SV40 transformed
cells
In early experiments, found to immortalize cells
these were mutant versions of p53!

110
Fig 30.32 p53 Activity
Dominant Negative Mutants
111
p53

Wild type p53 restrains growth
p53 mutations accumulate in many types of cancer
Deletion of both alleles or point mutations
produce the same phenotype
Unrestrained cell growth
p53 is involved in general/common control of cell
proliferation

112
p53 - tumor suppressor

mutant p53 cells have a tendency to amplify DNA
p53- mice are viable, develop variety of tumors
at early stages
wt p53 inhibits transformation of cells in culture

113
p53 mutations

Li Fraumeni syndrome
cancer predisposition syndrome
autosomal dominant
heterozygotes for p53
p53 mutations
Dominant negatives

114
Tumor suppressor p53

Normal cells have low levels of p53
p53 activated by irradation/DNA damage
functions in growth arrest and/or apoptosis?
depends on the stage of cell cycle!
see Fig 30.33

115
Fig 30.33 DNA damage activates p53
116
Activated p53 Function

In early G1, p53 triggers a checkpoint that
blocks further progression through the cell cycle
If the cell is committed to division, p53
triggers apoptosis

117
Fig 30.34 p53functional domains
118
p53 functional domains