L4 Flashcards

1
Q

How are large eukaryotic chromosomes duplicated?

A

From multiple DNA replication origins that act in a bi-directional manner

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2
Q

How many replication origins are on yeast chromosomes?

A

400/500

Can only initiate once per cycle

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3
Q

Yeast replication origins

A

Allow plasmids to be stabile maintained in yeast cells - Autonomously Replicating Sequences (ARS)

Contains 4 regions - A, B1, B2, and B3

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4
Q

Structure of replication origins

A

Contains 4 regions - A, B1, B2, and B3

Domain A which is the critical DNA sequence - 11bp

ACS sequence of domain A is the key to allow initiation of replication

Orientation of domain A is crucial

5’ and 3’ flanking domains important for function

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5
Q

What does the AT rich sequences around the ACS indicate?

A

Indicates it may be involved in DNA unwinding

Less H bonds so easier to separate strands

Lowers energy needed for separation

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6
Q

How can B1 be flipped from different origins even though theres no homology?

A

Sequences are interchangeable

B1 can be replaced by other B1s

But you can’t replace B1 with B2

Can swap B1 domains between different ARS elements - not interchangeable within an ARS element

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7
Q

What does the B3 sequence do?

A

Binds the Abf1 protein

Connection between transcription and replication thats not completely understood yet

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8
Q

What does the ORC do?

A

Origin Replication Complex

Binds to the ACS region of domain A which is critical for replication

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9
Q

Roles of the domains

A

Flanking regions unknown but probably involved in unwinding

Domain A specifically binds components of the initiator complex

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10
Q

Proteins that bind the ARS element

A

Abf1 transcription factor

6 protein subunit complex called the ORC binds binds domain A and part of B1 in an ATP dependent manner

Mutations of domain A that affect function in plasmid assays weaken ORC binding

ORC binds domain A throughout the cell cycle hence can’t be sufficient for DNA replication

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11
Q

How many ORCs are there?

A
Orc1 
Orc2
Orc3
Orc4
Orc5
Orc6
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12
Q

Initiation of DNA replication in yeast

A

2 step process

1) At the end of mitosis, formation of the PRC over the origin which involves association of ORC with Cdc6 and coincides with nuclear entry of Mcm proteins
2) Cells must pass through START to initiate DNA replication

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13
Q

What is the licensing factor model?

A

Diffusible DNA replication inducing factor that is inactivated following DNA replication ensuring that DNA replication only occurs once per cell cycle

This inducing factor gains access to the nucleus following mitosis this ensuring that DNA replication can only reinitiate once mitosis is complete

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14
Q

What is a licensing factor?

A

A protein or complex of proteins that allows an origin of replication to begin DNA replication at that site

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15
Q

What did studies of HELA cells show about replication?

A

They took HELA cells in S phase and fused them with another HELA cell in G1 phase and looked to see what happened in the nuclei at replication
– They found that the cell nucleus in S phase wasn’t affected & went on as normal
– Nucleus in G1 went into replication a lot quicker than it normally would’ve done

What if you take a cell in G2 and fuse it to a cell in S phase??
– G2 nucleus - replication didn’t occur
– Only difference between G1 and G2 is that it’s gone through S phase

Something happens at S phase that that prevents it being initiated by the S phase cell

How does the S phase cell initiate replication in the G1 cell??
– Created the term the licensing factor model
– Idea was that whatever the inducing factor in S phase was, maybe it gains access to the nucleus following mitosis (when the cell is in G1)
– DNA replication only occurs when mitosis has finished – proteins disappear and they can’t get access to the nucleus until mitosis is complete

Nuclear membrane breaks down after mitosis – does the nuclear membrane acts as a barrier to the G2 cell stimulating replicating??
– They made the nuclear membrane in a HELA cell permeable in G2 and fused it with the S phase cell
– This time it underwent replication again even through it was in G2 – disaster for the cell

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16
Q

What are HELA cells?

A

Immortal human cells

17
Q

Formation of PRC

A

At the end of mitosis, you get inactivation of the B cyclin complex

This inactivation in yeast leads to the nuclear localisation and binding of these Mcm proteins and the Cdc6

Formation of this complex on a replication origin is a critical starting point - replication cannot occur otherwise

After mitosis the cell is ‘re-priming’ the system so it can go into mitosis again

18
Q

What are Mcm proteins?

A

Mini chromosome maintenance proteins

Mcm2, Mcm3 and Mcm5 - also known as Cdc46

19
Q

What is Cdc6?

A

Function is the assembly of prereplicative complexes at origins of replication during the G1 phase of the cell division cycle

Is unstable and is resynthesised each cell division cycle