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MOLECULAR BASIS OF 
MUTATIONS 
PRESENTED BY-SHALINI 
SAINI 
3RD SEM
INTRODUCTION 
• Term mutation was given by Devries in 1901 while 
studying evening primerose Oenothera lamarckiana 
• Most of these were chromosomal variations 
• Some were point variations 
• Originally the term mutation was given to both 
chromosomal as well as point mutations. 
• Recently chromosomal mutations are studied 
separately. 
• The term mutation is now given only to point 
mutations.
DEFINITION 
• Any sudden change occurring in 
hereditary material is called as mutation. 
• They may be harmful, beneficial or 
neutral. 
• A mutation is defined as an inherited change 
in genetic information.
TYPES OF GENES MUTATIONS 
• Number of ways to classify gene mutations: 
– On the basis of the molecular nature of the 
defect. 
– On the nature of the phenotypic effect-- amino 
acid sequence of the protein is altered or not. 
– On the basis of the causative agent of the 
mutation.
TYPES OF MUTATIONS 
TWO TYPES OF MUTATION OCCURS IN NATURE 
• SOMATIC MUTATION 
• GERM LINE MUTATION 
Somatic mutations 
• Arise in the somatic cells. 
• Passed on to other cells through the process of mitosis. 
• Effect of these mutations depends on the type of the cell in which 
they occur & the developmental stage of the organism. 
• If occurs early in development, larger the clone of the mutated 
cells.
GERM LINE MUTATION- 
• They occur in the cells that produce gametes 
• Passed on to future generations 
• In multicellular organisms, the term mutation is 
generally used for germ line mutations
MUTAGENS RESPONSIBLE FOR 
MUTATION 
The physical and chemical agent that caused 
mutation is known as mutagen. 
Chemical mutagen 
 Alkylating agent 
 Base analogs 
 Methylating agent 
 DNA intercalating agent 
 DNA crosslink agent 
 Reactive oxygen species (ROS)
Physical mutagen:- 
Uv radiation 
Ionising radiation
CHEMICAL MUTAGEN
On the basis of causative agent types of 
mutations 
Spontaneous mutations: 
• Mutations that result from natural changes in DNA. 
• Spontaneous mutation contain depurination and deamination 
for a particular base are two common chemical event that 
produces spontaneous mutation. 
Induced mutations: 
• Results from changes caused by environmental chemicals & 
radiations. 
• Any environmental agent that increases the rate of mutation 
above the spontaneous is called a mutagen such as chemicals 
& radiations.
Nitrous Acid Causes Oxidative 
Deamination of Bases
DNA level view of the same two events as last slide
• Induced 
Mutation
Base modifying agents 
These are chemicals that act as mutagens 
by modifying the chemical structure and 
properties of bases. 
Three types of mutagens that work in this 
way: 1)deaminating agent 
2)hydroxylating agent 
3)an alkylating agent
Alkylating agent 
 These are naturally occuring and human made 
highly reactive chemicals that alter the structure of 
DNA and cause mutations. 
 e.g. Ethylmethane sulphonate(EMS) and mustard 
gases, MMS. 
 They donate an alkyl group to amino and keto 
groups in nucleotides. 
 EMS alkylates the keto group in no 6 position of 
guanine and in number 4 position of thymine.
 e.g. 6-ethylguanine acts as an analog of adenine 
and pairs with thymine.
Hydroxylating agent 
 Hydroxylamine is a mutagen that reacts 
specifically with cytosine ,modifying it by 
adding a hydroxyl group (OH) so that it 
pair with adenine instead of guanine.
Base analogs 
• Base analogs are bases that are similar to those 
normally found in DNA . 
• The base analogs pair with a different base in 
DNA. 
• One base analog mutagen is 5- bromouracil, 
which has a bromine residue instead of methyl 
group of thymine. 
• In normal states,5BU resembles thymine and 
pairs with adenine in DNA.
• In rare states, it pairs with guanine 
• Not all base analogs are mutagens. 
• For e.g. AZT(azidothymidine) ,an approved drug 
given to patients with AIDS, is an analog of 
thymidine. 
• It is not a mutagen because it does not base pair 
changes.
Mutagenic effects of the base analog 5-bromouracil (5BU)
Intercalating agent 
• Intercalating agent inserts itself between 
adjacent base pairs of the DNA strand that 
is template for new DNA synthesis. 
• An extra base is inserted into the new DNA 
strand opposite the intercalating agent. 
• After one more round of replication ,during 
which the intercalating agent is lost ,the 
overall result is a base pair addition 
mutation.
• If the intercalating agent inserts itself into 
the new DNA strand in place of a base 
,then when that DNA helix replicates after 
the intercalating agent is lost. 
• The result is a base pair deletion mutation. 
• If a base pair addition or base pair deletion 
point mutation occurs in a protein coding 
gene, the result is a frameshift mutation. 
• E.g. proflavin,acridine and ethidium 
bromide
Intercalating mutations
Radiation 
• Radiation occurs in non-ionizing or ionizing 
forms. 
• Ionization occur when energy is sufficient to 
knock an electron out of an atomic shell and 
break covalent bonds. 
• Except for UV light ,non ionizing radiation 
does not induce mutations. 
• But all forms ionizing radiation ,such as X 
rays, cosmic rays and radon can induce 
mutation.
Effect of UV radiation 
• UV radiation promotes the formation of 
covalent bonds between adjacent thymine 
residue in a DNA strand ,creating a 
cyclobutyl ring. 
• They form abnormal chemical bond 
between adjacent pyrimidine molecule 
(mainly thymine) in the same strand of the 
double helix.
• Ionizing radiation penetrates tissue, colliding 
with molecules and knocking electrons out 
of orbits ,creating ions. 
• The ion can result in the breakage of 
covalent bonds, including those in the sugar 
phosphate back bone of DNA. 
• Ionizing radiation is the leading causes of 
gross mutation in humans. 
• High dosages of ionizing radiation kill cells 
so use in treating some form of cancer.
Spontaneous generation of addition and deletion mutants by DNA 
looping-out errors during replication
Tautomeric shift and 
mutation
Tautomeric Shifts: 
--chemical fluctuations, 
--conformation states (stable==========unstable) 
Pyrimidine 
Purine
Tautomeric Shifts Affect Base-Pairing 
C:T 
T:G
Mutation Caused by Tautomeric Shifts
DNA damaged by free radicals 
A free radical is any species capable of 
independent existence that contains one or 
more unpaired electrons. 
They are unstable, very reactive and 
short-lived as they tend to catch an 
electron from other molecules.
DNA Modification 
• Free radicals induce several types of DNA damage 
including 
– strand breaks, 
– DNA-protein cross-links 
– and a large range of base and sugar modifications. 
• Of the free radicals the highly reactive hydroxyl 
radical (.OH) is the most prominent in the 
development of base and sugar modifications. 
• DNA damage also occurs through reactive nitrogen 
species undergoing mainly nitration and deamination 
of purines
Mutations on the basis of the Phenotypic 
effects of mutations: 
Most common phenotype in natural 
populations of the organism is called as 
wild type phenotype. 
The effect of mutation is considered 
with reference to wild type phenotype
Forward mutation: 
 a mutation that alters the wild type 
phenotype 
 Reverse mutation (reversion): 
a mutation that changes a mutant 
phenotype back in to the wild type
Missense mutation: a base is substituted that 
alters a codon in the mRNA resulting in a 
different amino acid in the protein product 
TCA 
AGT 
UCA 
TTA 
AAT 
UUA 
Ser Leu LLeeuu
Silent mutation: alters a codon but due to 
degeneracy of the codon, same amino acid is 
specified. 
TCA 
AGT 
UCA 
TCG 
AGC 
UCG 
Ser Ser
Nonsense mutation: changes a sense codon into 
a nonsense codon. Nonsense mutation early in 
the mRNA sequence produces a greatly 
shortened & usually nonfunctional protein 
TCA 
AGT 
UCA 
TGA 
ACT 
UGA 
Ser 
Stop codon
Neutral mutation: mutation that alters the amino 
acid sequence of the protein but does not change 
its function as replaced amino acid is chemically 
similar or the affected aa has little influence on 
protein function. 
CTT 
GAA 
CUU 
ATT 
TAA 
AUU 
Leu Ile
Loss of function mutations: 
Structure of protein is so altered that it no 
longer works correctly. 
 Mutation can occur in regulatory region 
that affects transcription , translation or 
spilicing of the protein. 
 Frequently recessive. 
 Complete or partial loss of the normal 
function.
Gain of function mutations: 
Produces an entirely new trait 
Causes a trait to appear in inappropriate 
tissues or at inappropriate times in development 
Frequently dominant 
Conditional mutations: 
Expressed only under certain conditions 
Lethal mutations: 
Cause the death of the organism
Suppressor mutation: 
Suppresses the effect of other mutation 
 Occurs at a site different from the site of 
original mutation 
 Organism with a suppressor mutation is a 
double mutant but exhibits the phenotype 
of un mutated wild type 
 Different from reverse mutation in which 
mutated site is reverted back into the wild 
type sequence
Molecular basis of mutations
Molecular basis of mutations
Molecular basis of mutations

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Molecular basis of mutations

  • 1. MOLECULAR BASIS OF MUTATIONS PRESENTED BY-SHALINI SAINI 3RD SEM
  • 2. INTRODUCTION • Term mutation was given by Devries in 1901 while studying evening primerose Oenothera lamarckiana • Most of these were chromosomal variations • Some were point variations • Originally the term mutation was given to both chromosomal as well as point mutations. • Recently chromosomal mutations are studied separately. • The term mutation is now given only to point mutations.
  • 3. DEFINITION • Any sudden change occurring in hereditary material is called as mutation. • They may be harmful, beneficial or neutral. • A mutation is defined as an inherited change in genetic information.
  • 4. TYPES OF GENES MUTATIONS • Number of ways to classify gene mutations: – On the basis of the molecular nature of the defect. – On the nature of the phenotypic effect-- amino acid sequence of the protein is altered or not. – On the basis of the causative agent of the mutation.
  • 5. TYPES OF MUTATIONS TWO TYPES OF MUTATION OCCURS IN NATURE • SOMATIC MUTATION • GERM LINE MUTATION Somatic mutations • Arise in the somatic cells. • Passed on to other cells through the process of mitosis. • Effect of these mutations depends on the type of the cell in which they occur & the developmental stage of the organism. • If occurs early in development, larger the clone of the mutated cells.
  • 6. GERM LINE MUTATION- • They occur in the cells that produce gametes • Passed on to future generations • In multicellular organisms, the term mutation is generally used for germ line mutations
  • 7. MUTAGENS RESPONSIBLE FOR MUTATION The physical and chemical agent that caused mutation is known as mutagen. Chemical mutagen  Alkylating agent  Base analogs  Methylating agent  DNA intercalating agent  DNA crosslink agent  Reactive oxygen species (ROS)
  • 8. Physical mutagen:- Uv radiation Ionising radiation
  • 10. On the basis of causative agent types of mutations Spontaneous mutations: • Mutations that result from natural changes in DNA. • Spontaneous mutation contain depurination and deamination for a particular base are two common chemical event that produces spontaneous mutation. Induced mutations: • Results from changes caused by environmental chemicals & radiations. • Any environmental agent that increases the rate of mutation above the spontaneous is called a mutagen such as chemicals & radiations.
  • 11.
  • 12. Nitrous Acid Causes Oxidative Deamination of Bases
  • 13. DNA level view of the same two events as last slide
  • 15. Base modifying agents These are chemicals that act as mutagens by modifying the chemical structure and properties of bases. Three types of mutagens that work in this way: 1)deaminating agent 2)hydroxylating agent 3)an alkylating agent
  • 16. Alkylating agent  These are naturally occuring and human made highly reactive chemicals that alter the structure of DNA and cause mutations.  e.g. Ethylmethane sulphonate(EMS) and mustard gases, MMS.  They donate an alkyl group to amino and keto groups in nucleotides.  EMS alkylates the keto group in no 6 position of guanine and in number 4 position of thymine.
  • 17.  e.g. 6-ethylguanine acts as an analog of adenine and pairs with thymine.
  • 18. Hydroxylating agent  Hydroxylamine is a mutagen that reacts specifically with cytosine ,modifying it by adding a hydroxyl group (OH) so that it pair with adenine instead of guanine.
  • 19.
  • 20. Base analogs • Base analogs are bases that are similar to those normally found in DNA . • The base analogs pair with a different base in DNA. • One base analog mutagen is 5- bromouracil, which has a bromine residue instead of methyl group of thymine. • In normal states,5BU resembles thymine and pairs with adenine in DNA.
  • 21. • In rare states, it pairs with guanine • Not all base analogs are mutagens. • For e.g. AZT(azidothymidine) ,an approved drug given to patients with AIDS, is an analog of thymidine. • It is not a mutagen because it does not base pair changes.
  • 22. Mutagenic effects of the base analog 5-bromouracil (5BU)
  • 23. Intercalating agent • Intercalating agent inserts itself between adjacent base pairs of the DNA strand that is template for new DNA synthesis. • An extra base is inserted into the new DNA strand opposite the intercalating agent. • After one more round of replication ,during which the intercalating agent is lost ,the overall result is a base pair addition mutation.
  • 24. • If the intercalating agent inserts itself into the new DNA strand in place of a base ,then when that DNA helix replicates after the intercalating agent is lost. • The result is a base pair deletion mutation. • If a base pair addition or base pair deletion point mutation occurs in a protein coding gene, the result is a frameshift mutation. • E.g. proflavin,acridine and ethidium bromide
  • 26. Radiation • Radiation occurs in non-ionizing or ionizing forms. • Ionization occur when energy is sufficient to knock an electron out of an atomic shell and break covalent bonds. • Except for UV light ,non ionizing radiation does not induce mutations. • But all forms ionizing radiation ,such as X rays, cosmic rays and radon can induce mutation.
  • 27. Effect of UV radiation • UV radiation promotes the formation of covalent bonds between adjacent thymine residue in a DNA strand ,creating a cyclobutyl ring. • They form abnormal chemical bond between adjacent pyrimidine molecule (mainly thymine) in the same strand of the double helix.
  • 28.
  • 29. • Ionizing radiation penetrates tissue, colliding with molecules and knocking electrons out of orbits ,creating ions. • The ion can result in the breakage of covalent bonds, including those in the sugar phosphate back bone of DNA. • Ionizing radiation is the leading causes of gross mutation in humans. • High dosages of ionizing radiation kill cells so use in treating some form of cancer.
  • 30. Spontaneous generation of addition and deletion mutants by DNA looping-out errors during replication
  • 32. Tautomeric Shifts: --chemical fluctuations, --conformation states (stable==========unstable) Pyrimidine Purine
  • 33. Tautomeric Shifts Affect Base-Pairing C:T T:G
  • 34. Mutation Caused by Tautomeric Shifts
  • 35. DNA damaged by free radicals A free radical is any species capable of independent existence that contains one or more unpaired electrons. They are unstable, very reactive and short-lived as they tend to catch an electron from other molecules.
  • 36. DNA Modification • Free radicals induce several types of DNA damage including – strand breaks, – DNA-protein cross-links – and a large range of base and sugar modifications. • Of the free radicals the highly reactive hydroxyl radical (.OH) is the most prominent in the development of base and sugar modifications. • DNA damage also occurs through reactive nitrogen species undergoing mainly nitration and deamination of purines
  • 37.
  • 38.
  • 39. Mutations on the basis of the Phenotypic effects of mutations: Most common phenotype in natural populations of the organism is called as wild type phenotype. The effect of mutation is considered with reference to wild type phenotype
  • 40. Forward mutation:  a mutation that alters the wild type phenotype  Reverse mutation (reversion): a mutation that changes a mutant phenotype back in to the wild type
  • 41. Missense mutation: a base is substituted that alters a codon in the mRNA resulting in a different amino acid in the protein product TCA AGT UCA TTA AAT UUA Ser Leu LLeeuu
  • 42. Silent mutation: alters a codon but due to degeneracy of the codon, same amino acid is specified. TCA AGT UCA TCG AGC UCG Ser Ser
  • 43. Nonsense mutation: changes a sense codon into a nonsense codon. Nonsense mutation early in the mRNA sequence produces a greatly shortened & usually nonfunctional protein TCA AGT UCA TGA ACT UGA Ser Stop codon
  • 44. Neutral mutation: mutation that alters the amino acid sequence of the protein but does not change its function as replaced amino acid is chemically similar or the affected aa has little influence on protein function. CTT GAA CUU ATT TAA AUU Leu Ile
  • 45. Loss of function mutations: Structure of protein is so altered that it no longer works correctly.  Mutation can occur in regulatory region that affects transcription , translation or spilicing of the protein.  Frequently recessive.  Complete or partial loss of the normal function.
  • 46. Gain of function mutations: Produces an entirely new trait Causes a trait to appear in inappropriate tissues or at inappropriate times in development Frequently dominant Conditional mutations: Expressed only under certain conditions Lethal mutations: Cause the death of the organism
  • 47. Suppressor mutation: Suppresses the effect of other mutation  Occurs at a site different from the site of original mutation  Organism with a suppressor mutation is a double mutant but exhibits the phenotype of un mutated wild type  Different from reverse mutation in which mutated site is reverted back into the wild type sequence