DNA Replication
Semi-conservative: both strands will serve as a template for new strand synthesis
Starts at an origin
Synthesis always in the 5🡪3’ direction b/c the DNA polymerase needs a 3’ hydroxyl end
Can be unidirectional but as a rule it’s bidirectional
Semi-discontinuous: one DNA strand is replicated in fragments
RNA primers required
Origin of replication: provides an opening called a replication bubble that forms two replication forks.
DNA replication proceeds outward from forks
DNA polymerase: covalently links nucleotides together
Deoxynucleoside triphosphates: free nucleotides with three phosphate groups
Breaks covalent bonds to release pyrophosphate (two phosphates) and provides energy to connect nucleotides
DNA polymerase cannot begin synthesis on a bare template strand
Requires a primer to get started
DNA primase makes the primer from RNA
The RNA primer is removed and replaced with DNA later
DNA polymerase only works 5’ to 3’
Leading strand
DNA synthesized in as one long molecule (continuous)
DNA primase makes a single RNA primer
DNA polymerase adds nucleotides in a 5’ to 3’ direction as it slides forward
Lagging strand
DNA synthesized 5’ to 3’ but as Okazaki fragments (discontinuous)
Okazaki fragments consist of RNA primers plus DNA
In both strands
RNA primers are removed by DNA polymerase and replaced with DNA
DNA ligase joins adjacent DNA fragments
Topoisomerases: prevents torsion by DNA breaks
Helicases: separates 2 strands
Primase: RNA primer synthesis
Single-strand binding proteins: prevent reannealing of single strands
DNA Polymerase: synthesis of new strand
Clamp: stabilizes polymerase
DNA ligase: seals nick via phosphodiester linkage
Three mechanisms for accuracy
Hydrogen bonding between A and T, and between G and C is more stable than mismatched combinations
Active site of DNA polymerase is unlikely to form bonds if pairs mismatched
DNA polymerase can proofread to remove mismatched pairs
DNA polymerase backs up and digests linkages
Other DNA repair enzymes as well
E. coli has 5 DNA polymerases
DNA Polymerase II: multiple subunits, responsible for majority of replication
DNA Polymerase I: a single subunit, rapidly removes RNA primers and fills in DNA
DNA Polymerase II, IV, and V: DNA repair and can replicate damaged DNA
DNA polymerases I and III stall at DNA damage
DNA polymerases II, IV, and V don’t stall but go slower and make sure replication is complete
Humans have 12 or more DNA polymerases
Designated with Greek letters
DNA polymerase α*:* its own built in primase subunit
DNA polymerase δ and 𝜀: extend DNA at a faster rate
DNA polymerase 𝛾: replicates mitochondrial DNA
When DNA polymerases α, δ, and 𝜀 encounter abnormalities, they may be unable to replicate
Lesion-replicating polymerases may be able to synthesize complementary strands to the damaged area
Series of short nucleotide sequences repeated at the ends of chromosomes in eukaryotes
Specialized form of DNA replication only in eukaryotes in the telomeres
Telomere at 3’ does not have a complementary strand and is called a 3’ overhang
Shortening of telomeres is correlated with cellular senescence
Telomerase function is reduced as an organism ages
99% of all types of human cancers have high levels of telomerase
Semi-conservative: both strands will serve as a template for new strand synthesis
Starts at an origin
Synthesis always in the 5🡪3’ direction b/c the DNA polymerase needs a 3’ hydroxyl end
Can be unidirectional but as a rule it’s bidirectional
Semi-discontinuous: one DNA strand is replicated in fragments
RNA primers required
Origin of replication: provides an opening called a replication bubble that forms two replication forks.
DNA replication proceeds outward from forks
DNA polymerase: covalently links nucleotides together
Deoxynucleoside triphosphates: free nucleotides with three phosphate groups
Breaks covalent bonds to release pyrophosphate (two phosphates) and provides energy to connect nucleotides
DNA polymerase cannot begin synthesis on a bare template strand
Requires a primer to get started
DNA primase makes the primer from RNA
The RNA primer is removed and replaced with DNA later
DNA polymerase only works 5’ to 3’
Leading strand
DNA synthesized in as one long molecule (continuous)
DNA primase makes a single RNA primer
DNA polymerase adds nucleotides in a 5’ to 3’ direction as it slides forward
Lagging strand
DNA synthesized 5’ to 3’ but as Okazaki fragments (discontinuous)
Okazaki fragments consist of RNA primers plus DNA
In both strands
RNA primers are removed by DNA polymerase and replaced with DNA
DNA ligase joins adjacent DNA fragments
Topoisomerases: prevents torsion by DNA breaks
Helicases: separates 2 strands
Primase: RNA primer synthesis
Single-strand binding proteins: prevent reannealing of single strands
DNA Polymerase: synthesis of new strand
Clamp: stabilizes polymerase
DNA ligase: seals nick via phosphodiester linkage
Three mechanisms for accuracy
Hydrogen bonding between A and T, and between G and C is more stable than mismatched combinations
Active site of DNA polymerase is unlikely to form bonds if pairs mismatched
DNA polymerase can proofread to remove mismatched pairs
DNA polymerase backs up and digests linkages
Other DNA repair enzymes as well
E. coli has 5 DNA polymerases
DNA Polymerase II: multiple subunits, responsible for majority of replication
DNA Polymerase I: a single subunit, rapidly removes RNA primers and fills in DNA
DNA Polymerase II, IV, and V: DNA repair and can replicate damaged DNA
DNA polymerases I and III stall at DNA damage
DNA polymerases II, IV, and V don’t stall but go slower and make sure replication is complete
Humans have 12 or more DNA polymerases
Designated with Greek letters
DNA polymerase α*:* its own built in primase subunit
DNA polymerase δ and 𝜀: extend DNA at a faster rate
DNA polymerase 𝛾: replicates mitochondrial DNA
When DNA polymerases α, δ, and 𝜀 encounter abnormalities, they may be unable to replicate
Lesion-replicating polymerases may be able to synthesize complementary strands to the damaged area
Series of short nucleotide sequences repeated at the ends of chromosomes in eukaryotes
Specialized form of DNA replication only in eukaryotes in the telomeres
Telomere at 3’ does not have a complementary strand and is called a 3’ overhang
Shortening of telomeres is correlated with cellular senescence
Telomerase function is reduced as an organism ages
99% of all types of human cancers have high levels of telomerase