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REGULATION OF CELL CYCLE

SALMAN UL ISLAM, (MS),
CELLULAR BIOCHEMISTRY LAB.
2013298039
CONTENTS
Introduction
 Overview of the cell cycle
 Cell-cycle control system
 Summary

INTRODUCTION
“Where a cell arises, there must be a previous cell,
just as animals can only arise from animals and
plants from plants.
 A cell reproduces by carrying out an orderly
sequence of events in which it duplicates its
contents and then divides in two.
 This cycle of duplication and division, known as the
cell cycle, is the essential mechanism by which all
living things reproduce.

How is cell division and
growth regulated?
Growth factors
-- stimulate cell growth

Mitogens
-- trigger cell division

Survival signals
-- disable apoptotic mechanisms

Cell Cycle Regulation
OVERVIEW OF THE CELL CYCLE










The eucaryotic cell cycle is traditionally divided into
four phases:
M phase: constituted by mitosis (nucleus division)
and cytokinesis (cell splits in two). The period
between one M phase and the next is called
interphase. The interphase encompasses the
remaining three phases of the cell cycle.
S phase ( S=synthesis): the cell replicates its
nuclear DNA. S phase is flanked by two phases in
which the cell continues to grow.
G 1 phase (G= gap): it is the interval between the
completion of M phase and the beginning of S
phase (DNA synthesis).
G2 phase: interval between the end of S phase and
the beginning of M phase.
Essential Cell Biology (© Garland Science 2010)
CHECKPOINTS IN CELL-CYCLE REGULATION
Two important checkpoints occur in G1 and G2.
 The G1 checkpoint allows the cell to confirm that
the environment is favorable for cell proliferation
and its DNA is intact before committing to S phase.
 G2 checkpoint ensures that cells do not enter
mitosis until damaged DNA is repaired and DNA
replication is complete.

Essential Cell Biology (© Garland Science 2010)
CELL-CYCLE CONTROL SYSTEM
DEPENDS ON CYCLICALLY ACTIVATED
PROTEIN KINASES
Key proteins are activated and then inactivated that
regulate DNA replication, mitosis, and cytokinesis.
Phosphorylation followed by dephosphorylation is
one of the most common ways to switch the activity
of proteins on and then off.
 Protein kinases are activated at appropriate times
in the cycle, after which they quickly become
deactivated again.
 Switching these kinases on and off is done by
cyclins, so kinases are therefore known as cyclindependent protein kinases or Cdks.

Essential Cell Biology (© Garland Science 2010)
CDKS ACTIVITY IS ALSO REGULATED BY
PHOSPHORYLATION AND DEPHOSPHORYLATION

For M-Cdk to be maximally active, it has to
phosphorylated at one or more sites by a specific
protein kinase, and dephophorylated at other sites
by specific protein phosphatase.
 The removal of the inhibitory phosphate groups by
the phosphatase is the final step that activates the
M-Cdk at the end of interphase.
 Then M-Cdk complex can activate more of the
same complexes. This positive feedback produces
the sudden, explosive increase in M-Cdk activity
that drives the cell abruptly into M phase.

Essential Cell Biology (© Garland Science 2010)
Essential Cell Biology (© Garland Science 2010)
CDKS ARE REGULATED BY ACCUMULATION AND
DESTRUCTION OF CYCLINS

Cyclin concentration plays an important part in
timing the events of cell cycle.
 M cyclin= cyclin that helps drive cells into M phase.
 M-cyclin synthesis starts immediately after cell
division and continues steadily throughout
interphase. The cyclin concentrates, so that its
concentration rises gradually and helps time the
onset of mitosis; its rapid elimination then helps
initiate the exit from mitosis.

Essential Cell Biology (© Garland Science 2010)
Essential Cell Biology (© Garland Science 2010)
CDKS ARE REGULATED BY ACCUMULATION
AND DESTRUCTION OF CYCLINS (CONT…)
As mitosis nears completion, multiple molecules of
the protein ubiquitin are covalently attached to the
M-cyclin by anaphase promoting complex (APC).
 This ubiquitination marks the cyclin for degradation
in proteosomes, large proteolytic machines found in
all eucaryotic cells. Destruction of the cyclin
inactivates the Cdk.

Cell cycle presentation by Salman Ul Islam.
DIFFERENT CYCLIN-CDK COMPLEXES

Essential Cell Biology (© Garland Science 2010)
Distinct Cdks associate with
different cyclins to trigger the
different events of the cell
cycle.
S-PHASE CYCLIN-CDK COMPLEXES
INITIATE DNA REPLICATION ONCE PER
CELL CYCLE








Initiates DNA replication and helps block Rereplication.
DNA replication begins at origins of replication.
Origin recognition complex (ORC) remains bound to the
origin of replication; serves as a sort of landing for other
regulatory proteins.
Cdc6 binds to ORC in G1, promotes additional proteins
binding to form pre-replicative complex, making the
replication origin ready to “fire”. S-Cdk then pulls the
“trigger” initiating DNA replication.
S-Cdk helps phophorylate Cdc6, causing it and the
other proteins in the pre-replicative complex to
dissociate from the ORC after an origin has fired.
Essential Cell Biology (© Garland Science 2010)
CELL CYCLE ARREST
The cell-cycle control system can arrest the cycle at
specific checkpoints. The molecular mechanisms of
these are poorly understood.
 In some cases, however, Cdk inhibitor proteins
come into play.
 For example DNA damage causes increased
concentration and activity of p53 (gene regulatory
protein) which activates the transcription of a gene
encoding a Cdk inhibitor protein called p21.
 The p21 protein binds to G1/S-Cdk, preventing
them from driving the cell into S phase.

Essential Cell Biology (© Garland Science 2010)
CELLS CAN DISMANTLE THEIR CONTROL SYSTEM
AND WITHDRAW FROM THE CELL CYCLE

This is a different matter from pausing in the middle
of a cycle.
 In human body, e.g, nerve cells and skeletal muscle
cells persist for a lifetime without dividing, they
enter G0.
 G0 is modified G1 state in which the cell-cycle
control system is largely dismantled, in that many of
the Cdks and cyclins disappear.
 The G1 checkpoint is therefore sometimes called
Start, passing it represents a commitment to
complete a full dividion cycle.

Essential Cell Biology (© Garland Science 2010)
Essential Cell Biology (© Garland Science 2010)
Eucaryotic
Cell-Cycle
Times

• Cell type
• Early frog embryo cells
• Yeast cells
• Intestinal epithelial cells
• cultured fibroblasts
• Human liver cells

Cell cycle time
~30 minutes
1.5–3 hours
~12 hours
~20 hours
~1 year
SUMMARY








The control system depends on a set of proteins
kinases, each composed of Cyclin and Cdk.
The control system also depends on protein complexes
such as APC.
The Cdks are cyclically activated by both cyclin binding
and the phosphorylation of some amino acids and the
dephosphorylation of others; when activated, Cdks
phophorylate key proteins in the cell.
The cell cycle control system can halt the cycle at
specific check points to ensure that the next step in the
cycle does not begin before the previous one has
finished, and intracellular and extracellular conditions
are favorable.

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Cell cycle presentation by Salman Ul Islam.

  • 1. REGULATION OF CELL CYCLE SALMAN UL ISLAM, (MS), CELLULAR BIOCHEMISTRY LAB. 2013298039
  • 2. CONTENTS Introduction  Overview of the cell cycle  Cell-cycle control system  Summary 
  • 3. INTRODUCTION “Where a cell arises, there must be a previous cell, just as animals can only arise from animals and plants from plants.  A cell reproduces by carrying out an orderly sequence of events in which it duplicates its contents and then divides in two.  This cycle of duplication and division, known as the cell cycle, is the essential mechanism by which all living things reproduce. 
  • 4. How is cell division and growth regulated? Growth factors -- stimulate cell growth Mitogens -- trigger cell division Survival signals -- disable apoptotic mechanisms Cell Cycle Regulation
  • 5. OVERVIEW OF THE CELL CYCLE      The eucaryotic cell cycle is traditionally divided into four phases: M phase: constituted by mitosis (nucleus division) and cytokinesis (cell splits in two). The period between one M phase and the next is called interphase. The interphase encompasses the remaining three phases of the cell cycle. S phase ( S=synthesis): the cell replicates its nuclear DNA. S phase is flanked by two phases in which the cell continues to grow. G 1 phase (G= gap): it is the interval between the completion of M phase and the beginning of S phase (DNA synthesis). G2 phase: interval between the end of S phase and the beginning of M phase.
  • 6. Essential Cell Biology (© Garland Science 2010)
  • 7. CHECKPOINTS IN CELL-CYCLE REGULATION Two important checkpoints occur in G1 and G2.  The G1 checkpoint allows the cell to confirm that the environment is favorable for cell proliferation and its DNA is intact before committing to S phase.  G2 checkpoint ensures that cells do not enter mitosis until damaged DNA is repaired and DNA replication is complete. 
  • 8. Essential Cell Biology (© Garland Science 2010)
  • 9. CELL-CYCLE CONTROL SYSTEM DEPENDS ON CYCLICALLY ACTIVATED PROTEIN KINASES Key proteins are activated and then inactivated that regulate DNA replication, mitosis, and cytokinesis. Phosphorylation followed by dephosphorylation is one of the most common ways to switch the activity of proteins on and then off.  Protein kinases are activated at appropriate times in the cycle, after which they quickly become deactivated again.  Switching these kinases on and off is done by cyclins, so kinases are therefore known as cyclindependent protein kinases or Cdks. 
  • 10. Essential Cell Biology (© Garland Science 2010)
  • 11. CDKS ACTIVITY IS ALSO REGULATED BY PHOSPHORYLATION AND DEPHOSPHORYLATION For M-Cdk to be maximally active, it has to phosphorylated at one or more sites by a specific protein kinase, and dephophorylated at other sites by specific protein phosphatase.  The removal of the inhibitory phosphate groups by the phosphatase is the final step that activates the M-Cdk at the end of interphase.  Then M-Cdk complex can activate more of the same complexes. This positive feedback produces the sudden, explosive increase in M-Cdk activity that drives the cell abruptly into M phase. 
  • 12. Essential Cell Biology (© Garland Science 2010)
  • 13. Essential Cell Biology (© Garland Science 2010)
  • 14. CDKS ARE REGULATED BY ACCUMULATION AND DESTRUCTION OF CYCLINS Cyclin concentration plays an important part in timing the events of cell cycle.  M cyclin= cyclin that helps drive cells into M phase.  M-cyclin synthesis starts immediately after cell division and continues steadily throughout interphase. The cyclin concentrates, so that its concentration rises gradually and helps time the onset of mitosis; its rapid elimination then helps initiate the exit from mitosis. 
  • 15. Essential Cell Biology (© Garland Science 2010)
  • 16. Essential Cell Biology (© Garland Science 2010)
  • 17. CDKS ARE REGULATED BY ACCUMULATION AND DESTRUCTION OF CYCLINS (CONT…) As mitosis nears completion, multiple molecules of the protein ubiquitin are covalently attached to the M-cyclin by anaphase promoting complex (APC).  This ubiquitination marks the cyclin for degradation in proteosomes, large proteolytic machines found in all eucaryotic cells. Destruction of the cyclin inactivates the Cdk. 
  • 19. DIFFERENT CYCLIN-CDK COMPLEXES Essential Cell Biology (© Garland Science 2010)
  • 20. Distinct Cdks associate with different cyclins to trigger the different events of the cell cycle.
  • 21. S-PHASE CYCLIN-CDK COMPLEXES INITIATE DNA REPLICATION ONCE PER CELL CYCLE      Initiates DNA replication and helps block Rereplication. DNA replication begins at origins of replication. Origin recognition complex (ORC) remains bound to the origin of replication; serves as a sort of landing for other regulatory proteins. Cdc6 binds to ORC in G1, promotes additional proteins binding to form pre-replicative complex, making the replication origin ready to “fire”. S-Cdk then pulls the “trigger” initiating DNA replication. S-Cdk helps phophorylate Cdc6, causing it and the other proteins in the pre-replicative complex to dissociate from the ORC after an origin has fired.
  • 22. Essential Cell Biology (© Garland Science 2010)
  • 23. CELL CYCLE ARREST The cell-cycle control system can arrest the cycle at specific checkpoints. The molecular mechanisms of these are poorly understood.  In some cases, however, Cdk inhibitor proteins come into play.  For example DNA damage causes increased concentration and activity of p53 (gene regulatory protein) which activates the transcription of a gene encoding a Cdk inhibitor protein called p21.  The p21 protein binds to G1/S-Cdk, preventing them from driving the cell into S phase. 
  • 24. Essential Cell Biology (© Garland Science 2010)
  • 25. CELLS CAN DISMANTLE THEIR CONTROL SYSTEM AND WITHDRAW FROM THE CELL CYCLE This is a different matter from pausing in the middle of a cycle.  In human body, e.g, nerve cells and skeletal muscle cells persist for a lifetime without dividing, they enter G0.  G0 is modified G1 state in which the cell-cycle control system is largely dismantled, in that many of the Cdks and cyclins disappear.  The G1 checkpoint is therefore sometimes called Start, passing it represents a commitment to complete a full dividion cycle. 
  • 26. Essential Cell Biology (© Garland Science 2010)
  • 27. Essential Cell Biology (© Garland Science 2010)
  • 28. Eucaryotic Cell-Cycle Times • Cell type • Early frog embryo cells • Yeast cells • Intestinal epithelial cells • cultured fibroblasts • Human liver cells Cell cycle time ~30 minutes 1.5–3 hours ~12 hours ~20 hours ~1 year
  • 29. SUMMARY     The control system depends on a set of proteins kinases, each composed of Cyclin and Cdk. The control system also depends on protein complexes such as APC. The Cdks are cyclically activated by both cyclin binding and the phosphorylation of some amino acids and the dephosphorylation of others; when activated, Cdks phophorylate key proteins in the cell. The cell cycle control system can halt the cycle at specific check points to ensure that the next step in the cycle does not begin before the previous one has finished, and intracellular and extracellular conditions are favorable.