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Molecular pathology: Physiopathology effect of Mutations

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Title: Molecular pathology: Physiopathology effect of Mutations

1
Molecular pathologyPhysiopathology effect of
Mutations

Dr Derakhshandeh, PhD

2
Mutations

changes to the either DNA or RNA
caused by copying errors in the genetic material
Cell division
Ultraviolet
Ionizing radiation
chemical mutagens
Viruses

3
Mutations In multicellular organisms

can be subdivided into
Germline mutations
can be passed on to descendants
Somatic mutations
cannot be transmitted to descendants in animals

4
Germ Somatic cell

a mutation is present in a germ cell
can give rise to offspring that carries the
mutation in all of its cells
Such mutations will be present in all descendants
of this cell
This is the case in hereditary disease
a mutation can occur in a somatic cell of an
organism
certain mutations can cause the cell to become
malignant
cause cancer

5
ClassificationBy effect on structure

Gene mutations have varying effects on health
where they occur
whether they alter the function of essential
proteins

6
Structurally, mutations can be classified as
7
Point mutations

caused by chemicals/malfunction of DNA
replication
exchange a single nucleotide for another
Most common is the transition that exchanges a
purine for a purine (A ? G)
or a pyrimidine for a pyrimidine, (C ? T)

8
Transition

caused by
Nitrous acid
base mispairing
5-bromo-2-deoxyuridine (BrdU)
mutagenic base analogs

9
Transversion

Less common
exchanges a purine for a pyrimidine
or a pyrimidine for a purine (C/T ? A/G)

10
Point mutations that occur within the protein
coding region of a gene

depending upon what the erroneous codon codes
for
Silent mutations
which code for the same amino acid
Missense mutations
which code for a different amino acid
Nonsense mutations
which code for a stop and can truncate the
protein

11
Insertions

add one or more extra nucleotides into the DNA
usually caused by transposable elements
or errors during replication of repeating
elements (e.g. AT repeats)
in the non/coding region of a gene may alter
splicing of the mRNA (splice site mutation)
or cause a shift in the reading frame (frame
shift)
significantly alter the gene product
Insertions can be reverted by excision of the
Transposable element

12
Deletion

remove one or more nucleotides from the DNA
Like insertions, these mutations can alter the
reading frame of the gene
Delitions of large chromosomal regions, leading
to loss of the genes within those regions
They are irreversible

13
Deletions/insertions/duplications

Out of frame
In frame

14
Deletions/insertions/duplications

Out of frame
result in frameshifts giving rise to stop codons.
no protein product or truncated protein product
deletions/insertions in DMD patients truncated
dystrophins of decreased stability
RB1 gene - usually no protein product in
retinoblastoma

15
Deletions/insertions/duplications

In frame
loss or gain of amino acid(s)
depending on the size and may give rise to
altered protein product with changed properties
eg CF Delta F508 loss of single amino acid
In some genes loss or gain of a single amino
acid mild

16
In frame

In some regions of RB1 a single amino acid loss
rise to mild retinoblastoma or incomplete
penetrance
BMD patients
Some times in-frame deletions/duplications
DMD deletions
mostly disrupt the reading frame

17
Deletions/insertions/duplications

In untranslated regions
these might affect transcription/expression
and/or stability of the message
Fragile X
MD expansions

Large-scale mutations in chromosomal structure

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Amplifications (gene duplications)

leading to multiple copies of all chromosomal
regions
double-minute chromosomes
Sometimes, so many copies of the amplified region
are produced
they can actually form their own small
pseudo-chromosomes
increasing the dosage of the genes

21
Amplifications
22
Chromosomal translocations

Fusion genes
Mutations to juxtapose previously separate
pieces of DNA
potentially bringing together separate genes to
form functionally distinct (e.g. bcr-abl)
Chromosomal translocation
interchange of genetic parts from nonhomologous
chromosomes

23
Interstitial deletions

an intra-chromosomal deletion
removes a segment of DNA from a single chromosome
For example, cells isolated from a human
astrocytoma, a type of brain tumor
have a chromosomal deletion removing sequences
between the "fused in glioblastoma" (fig) gene
and the receptor tyrosine kinase "ros", producing
a fusion protein (FIG-ROS)
The abnormal FIG-ROS fusion protein has
constitutively active kinase activity
causes oncogenic transformation (a transformation
from normal cells to cancer cells)

24
Astrocytoma Astrocyte
25
Astrocytoma

a primary tumor of the central nervous system
develops from the large, star-shaped glial cells
known as astrocytes
Most frequently astrocytomas occur in the brain
but occasionally they appear along the spinal
cord
occur most often in middle-aged men
Symptoms of an astrocytoma, similar to other
brain tumors
depend on the precise location of the growth
For instance, if the frontal lobe is affected
mood swings and changes in personality may occur
a temporal lobe tumor is more typically
associated with speech and coordination
difficulties

Chromosomal inversions
Reversing the orientation of a chromosomal
segment
Loss of heterozygosity
loss of one allele
either by a deletion
recombination event

27
By effect on function

Loss-of-function mutations
Gain-of-function mutations
Dominant negative mutations
Lethal mutations

28
Loss-of-function mutations

Wild type alleles typically encode a product
necessary for a specific biological function
If a mutation occurs in that allele, the function
for which it encodes is also lost
The degree to which the function is lost can vary

29
Loss-of-function mutations

gene product having less or no function
Phenotypes associated with such mutations are
most often recessive
to produce the wild type phenotype!
Exceptions are when the organism is haploid
or when the reduced dosage of a normal gene
product is not enough for a normal phenotype
(haploinsufficiency)

30
Loss-of-function mutations

mutant allele will act as a dominant
the wild type allele may not compensate for the
loss-of-function allele
the phenotype of the heterozygote will be equal
to that of the loss-of-function mutant (as
homozygot)
to produce the mutant phenotype !

31
Loss-of-function mutations

Null allele
When the allele has a complete loss of function
it is often called an amorphic mutation
Leaky mutations
If some function may remain, but not at the level
of the wild type allele
The degree to which the function is lost can vary

32
Gain-of-function mutations

change the gene product such that it gains a new
and abnormal function
These mutations usually have dominant phenotypes
Often called a neomorphic mutation
A mutation in which dominance is caused by
changing the specificity or expression pattern of
a gene or gene product, rather than simply by
reducing or eliminating the normal activity of
that gene or gene product

33
Gain-of-function mutations

Although it would be expected that most mutations
would lead to a loss of function
it is possible that a new and important function
could result from the mutation
the mutation creates a new allele
associated with a new function
Any heterozygote containing the new allele along
with the original wild type allele will express
the new allele
Genetically this will define the mutation as a
dominant

34
Dominant negative mutations

Dominant negative mutations
antimorphic mutations
an altered gene product that acts
antagonistically to the wild-type allele
These mutations usually result in an altered
molecular function (often inactive)
Dominant
or semi-dominant phenotype

35
Dominant negative mutations

In humans
Marfan syndrome is an example of a dominant
negative mutation
occurring in an autosomal dominant disease
the defective glycoprotein product of the
fibrillin gene (FBN1)
antagonizes the product of the normal allele

36
Fibrillin gene
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39
Lethal mutations

lead to a phenotype
incapable of effective reproduction

40
By aspect of phenotype affectedMorphological
mutations

usually affect the outward appearance of an
individual
Mutations can change the height of a plant or
change it from smooth to rough seeds.
Biochemical mutations result in lesions stopping
the enzymatic pathway
Often, morphological mutants are the direct
result of a mutation due to the enzymatic pathway

41
Special classesConditional mutation

wild-type (or less severe) phenotype under
certain "permissive" environmental conditions
a mutant phenotype under certain "restrictive"
conditions
For example a temperature-sensitive mutation can
cause cell death at high temperature (restrictive
condition), but might have no deletirious
consequences at a lower temperature (permissive
condition).

42
Nomenclature

Nomenclature of mutations specify the type of
mutation
and base or amino acid changes
Amino acid substitution (e.g. D111E)
The first letter is the one letter code of the
wildtype amino acid
the number is the position of the amino acid from
the N terminus
the second letter is the one letter code of the
amino acid present in the mutation
If the second letter is 'X', any amino acid may
replace the wildtype

43
Nomenclature

Amino acid deletion (e.g. ?F508)
The greek symbol ? or 'delta' indicates a
deletion
The letter refers to the amino acid present in
the wildtype
the number is the position from the N terminus of
the amino acid were it to be present as in the
wildtype

44
Harmful mutations

Changes in DNA caused by mutation can cause
errors in protein sequence
creating partially or completely non-functional
proteins
To function correctly, each cell depends on
thousands of proteins to function in the right
places at the right times
a mutation alters a protein that plays a critical
role in the body
A condition caused by mutations in one or more
genes is called a genetic disorder
only a small percentage of mutations cause
genetic disorders
most have no impact on health
For example, some mutations alter a gene's DNA
base sequence but dont change the function of
the protein made by the gene

45
DNA repair system

Often, gene mutations that could cause a genetic
disorder
repaired by the DNA repair system of the cell
Each cell has a number of pathways through which
enzymes recognize and repair mistakes in DNA
Because DNA can be damaged or mutated in many
ways
the process of DNA repair is an important way in
which the body protects itself from disease

46
Beneficial mutations

A very small percentage of all mutations
have a positive effect
lead to new versions of proteins that help an
organism and its future generations better adapt
to changes in their environment
For example, a specfic 32 base pair deletion in
human CCR5 (CCR5-32) confers HIV resistance to
homozygotes
delays AIDS onset in heterozygotes
The CCR5 mutation is more common in those of
European descent
One theory for the etiology of the relatively
high frequency of CCR5-32 in the european
population is that it conferred resistance to the
bubonic plaque in mid-14th century Europe

47
Selection at the CCR5 locus

CCR5?32/CCR5?32 homozygotes are resistant to HIV
and AIDS

The high frequency and wide distribution of the
?32 allele suggest past selection by an unknown
agent

48
The Role of the Chemokine Receptor Gene CCR5 and
Its Allele (del32 CCR5)

Since the late 1970s
8.4 million people worldwide
including 1.7 million children, have died of AIDS
an estimated 22 million people are infected with
human immunodeficiency virus (HIV)

49
CCR5 and Its Allele ( del32 CCR5)
monocyte/macrophage (M),
T-cell line (Tl)
a circulating T-cell (T)
50

Studies of mutagenesis in many organisms indicate
that the majority (over 90) of mutations are
recessive to wild type
If recessiveness represents the 'default' state,
what are the distinguishing features that make a
minority of mutations give rise to dominant or
semidominant characters?

51
molecular and cellular biology to classify the
molecular mechanisms of dominant mutation

reduced gene dosage, expression, or protein
activity (haploinsufficiency)
increased gene dosage
ectopic or temporally altered mRNA expression
increased or constitutive protein activity
dominant negative effects
altered structural proteins
toxic protein alterations
new protein functions

52
The concepts of dominance recessive

Formulated by Mendel (1965)
Why are some disease dominant and other
recessive?
Dominance is not an intrinsic property of a gene
or mutant allele
Relationship between the phenotypes of 3
genotypes (AA, AB, BB)
Dominant
Semi dominant
Recessive (depending both on its partner allele)

53
Semi dominant

Example of homozygous mutants
Thalassemia, Familial hypercholesterolemia,
Achondroplasia
Phenotype of the homozygote
More severity than heterozygote
Huntington
True dominant to wild type

54
Dominant mutations are much rarer than recessive
ones

Insertional inactivation by retroviral DNA in
mouse genom
10-201 (RecDom)
Wright et al.
Physiology of the gene action
Fisher et al.
Accumulation of modifier alleles at other loci

55
Alga Chlamydomonas

Usually haploid
In a diploid background
Nevertheless recessive behavior
Supporting Wright s theory
Indeed, diploidy
Protects against recessive mutations!

56
Why most inborn errors of metabolism are
recessive?

Metabolic pathway
Not critical rate limiting steps
Not qualitatively altered function
Perhaps dominat mutations
Developmental malformations

57
Recessive to Dominant mutations

Caenorhabditis elegans (C elegans)
Recessive mutations at a series of loci termed
smg
May alter the behavior of mutations from
recessive to dominant
It seems Wt smg encode proteins
Recognize and degrade mutant mRNA species
(surveillance)

58
Types of dominant mutation

Muller (1932) quantitative changes to a
pre-existing WT character
Amorph
Hypomorph
Hypermorph
Antimorph
neomorph

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Classical genetics molecular mechanism

reduced gene dosage, expression, or protein
activity (haploinsufficiency)
increased gene dosage
ectopic or temporally altered mRNA expression
increased or constitutive protein activity
dominant negative effects
altered structural proteins
toxic protein alterations
new protein functions

61
Classical genetics molecular mechanism

A distinction between (loss of function)
reduced gene dosage, expression, or protein
activity (haploinsufficiency)
And (gain of function)
increased gene dosage
new protein functions

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Reduced gene dosage, expression, or protein
activity (haploinsufficiency)

Inactivation of one of a pair of alleles
It is important groups because of
Mutation gt loss of function
Deletion, Ch Translocation, truncation,
Dosage sensitive genes interesting group
Code for tissue specific protein
Type I collagene
globin
LDL-Receptor
Regulatory genes
PAX3

64
Waardenburg Syndrome (PAX3)

Deafness
pigmentary anomalies
white forelock
heterochromia iridis
partial albinism,
Prominent broad nasal root
Hypertrichosis of the medial part of the eyebrows

65
heterochromia iridis
66
Increased Dosage

Increase gene dosage to three copies affect
phenotype less than reduction to one copy (21,
18, 13, XXY, than X0,)
Critical genes are important
PMP-22 duplication gtCharcot-Marie-Tooth disease
Haploinsufficient gt different phenotype of
Increased Dosage!

67
Increased Dosage in Charcot-Marie-Tooth disease
68
Ectopic or Temporally altered mRNA Expression

Point mutation in g, d, b
Alters binding of the transacting factor
Abrogate the normal switch from expression of
g to d and b

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HPFH as a dß-globin Disease

Large deletions at the ß-globin locus
from the region close to the human A? gene to
well downstream of the human ß-globin
gene and including deletion of the structural d-
and ß-globin genes

72
HPFH

Heterozygotes
a normal level of HbA2
even higher levels of HbF (15 to 30 )
Homozygotes
clinically normal
albeit with reduced MCV and MCH
Compound heterozygotes with b thalassemia
clinically very mild

73
Why mutations of structural proteins are
frequently dominant?

Admixture of normal and abnormal structure
components will disrupt the overall structure
Biochemical analysis
Abnormal mRNA
Cellular processing
Secretion
Without mature Fibrills
Type I Collagen, Fibrillin in Marfan

74
Toxic protein alterations

Usually missense mutations
Cause structural alteration in mono- or
oligomeric proteins
Disrupt normal function
Lead to toxic products or precursors
Sickle cell mutations (hem S, b6GlugtVal)
Although recessive
Coinheritance in cis (hem S b23ValgtIle)
Sickling to manifest in the heterozygote!

75
Toxic protein alterations

Various point mutations in rhodopsin
Slow degeneration of rod photoreceptor outer
segment

76
New protein functions

Creation of new , adventageus protein functions
by mutation
The life blood the evolution
Occurs over protracted time scale
Protein with truly new function rare
Usually pathological
Juxtaposition of domains from different proteins.
Generate new function ABL-BCR (922)
Philadelphia translocation

77
A gene affecting brain size

Microcephaly (MCPH)
Small (430 cc v 1,400 cc) but otherwise normal
brain, only mild mental retardation
MCPH5 shows Mendelian autosomal recessive
inheritance
Due to loss of activity of the ASPM gene

ASPM-/ASPM-
control
Bond et al. (2002) Nature Genet. 32, 316-320
78
Other mechanism

Genomic imprinting
If a gene is transcribed only from the ch
originating from one of the two parents
The locus is hemizygous
Mutation of the allele on the active chromosome
Inactive the locus
Mutation of the other chromosome
No phenotypic effect
Beckwith-wiedermann syndrome

79
Beckwith-wiedermann syndrome (BWS)