2024 Cell Cycle - Mitosis PDF

Summary

This is a presentation about the Cell Cycle and Mitosis. It includes lesson objectives, and information on cell division, mitosis, meiosis, and disease prevention. The presentation is aimed at secondary school biology students.

Full Transcript

THE CELL CYCLE AND CELL DIVISION

Presented by:

APRIL JOY A. TALAS
 LESSON OBJECTIVES
By the end of this session, the learners will be able to:

1. Characterized the phases of the cell cycle and their
control points (STEM_BIO11/12-Id-f-6)
2. Described the stages of mitosis/meiosis given 2n=6
(STEM_BIO11/12-Id-f-7)
3. Compared mitosis and meiosis, and their role in the
cell-division (STEM_BIO11/12-Id-f-7)
Have you ever
wondered how a
tiny fertilized egg
grows into a fully
developed
human being?
Cell division is key to life: from the moment we are first
conceived, we are continually changing and growing.
 Are the terms "cell cycle" and
"cell division" interchangeable,
or do they refer to different
processes in the life of a cell?
The Cell Cycle
The cell cycle is an ordered series of events involving cell growth
and cell division.
Cells on the path to cell division proceed through a series of
precisely timed and carefully regulated stages of growth,
DNA replication, and division.
The cell cycle has two major phases: interphase and the mitotic
phase.
During interphase, the cell grows, and DNA is replicated.
During the mitotic phase, the replicated DNA and cytoplasmic
contents are separated, and the cell divides.
 CELL DIVISION
Cell division is a fundamental process found in both
prokaryotes (bacteria) and eukaryotes, leading to
the creation of two new cells.
In organisms, there are three primary types of cell
division:

Prokaryotes (bacteria)
— Binary fission
Divides forming two new identical cells
 PROKARYOTIC CELL DIVISION
1. Binary Fission

Three (3) major steps;
DNA Replication
DNA is copied resulting into two identical chromosomes

Chromosome Segregation
Chromosomes separate and move towards ends (poles) of cell

Cytokinesis (Separation)
Cytoplasm divides forming two (2) cells

Each new daughter cell is Genetically Identical to parent cell
Prokaryotic Cell
Division
▪ Eukaryotes

— Mitosis
essential for growth, development, and
repair in multicellular organisms, as well
as reproduction in single-celled
organism.

— Meiosis
formation of sex cells, or gametes
 EUKARYOTIC CELL DIVISION
Cell division that results in two daughter cells each having the same
number and kind of chromosomes as the parent cell.

1. MITOSIS:
Two (2) main steps:
1. Mitosis
Fours steps; [Prophase, Metaphase, Anaphase, Telophase]

2. Cytokinesis
Cytoplasm divides forming two new daughter cells

Mitosis yields two daughter cells, each with the same number and
type of chromosomes as the parent cell.
 Eukaryotic Cell Division
Cell division that results in four daughter cells
1. MEIOSIS:
Consists of two consecutive cell divisions
1. Meiosis I
Mitosis: Fours steps; [Prophase I, Metaphase I, Anaphase I, Telophase I]
Cytokinesis: Results in two haploid daughter cells, each with half the original
chromosome number
2. Meiosis II – without DNA replication
Mitosis: Fours steps; [Prophase II, Metaphase II, Anaphase II, Telophase II]
Cytokinesis: takes place in both haploid daughter cells, yielding a total of
four haploid daughter cells, each with a unique genetic makeup. These cells
are considered gametes.
Resulting in four non-identical daughter cells, each containing half the number of
chromosomes as the parent cell.
WHY DO CELLS DIVIDE?
Cell division is a fundamental process with
various vital roles in the functioning of our
bodies and the continuation of life. It plays a
crucial role in our growth, development, repair
of worn-out tissues, and even in reproduction.
 1. Growth and Development:
Growth and development require continuous cell division to
produce new cells. This process enables us to increase our
size, add height, build muscle, and develop various organs
and tissues throughout our lifespan.

2. Tissue Repair:
Tissue repair relies on cell division to replace damaged cells.
When accidents occur, such as skin abrasions or nail
breakage, cell division is essential for the production of new
cells to heal and regenerate the injured tissue.
 3. Maintaining Tissue Integrity:
As cells age and wear out, they need to be replaced to
maintain tissue integrity and functionality.
Cell division ensures that our organs and tissues remain in
optimal working condition.

4. Disease Prevention:
Proper regulation of cell division is crucial for preventing
diseases, as uncontrolled cell division can lead to conditions like
psoriasis or, more dangerously, cancer. Strict checkpoints and
stages in the cell division cycle help prevent these aberrations
by ensuring that cell division proceeds accurately and safely.
Examples:
Skin Regeneration Blood Cell Renewal Intestinal Lining Liver Regeneration
The outer layer of Our blood is composed The cells lining our The liver has a
our skin, the of various types of intestines have a high remarkable ability to
epidermis, constantly cells, including red turnover rate due to the regenerate. When a
undergoes cell blood cells, white constant exposure to portion of the liver is
division to replace blood cells, and food and digestive damaged or
dead skin cells. This platelets. Cell division processes. Cell division removed, the
ensures that the skin in the bone marrow in the intestinal lining remaining cells
remains intact, continuously produces replenishes these cells, undergo rapid cell
protective, and these blood cells, allowing for efficient division to replace
capable of healing ensuring a steady absorption of nutrients the lost tissue,
wounds and supply to support and maintaining a ensuring the organ's
abrasions. bodily functions like healthy gut barrier. continued
oxygen transport and functionality.
immune response.
 5. Reproduction:
Reproduction relies on cell division to create new organisms.
Without cell division, there would be no generation of
offspring, leading to the eventual extinction of a species and
the end of life as we know it.

6. Controlling DNA Overloading:
Cell division controls DNA overloading by ensuring that each
daughter cell receives an identical and manageable portion of
the genetic material, preventing genetic instability and
potential harm.
CELL CYCLE
Introduction
The cell cycle is a precisely regulated series of
events encompassing phases of growth, rest, and
cell division.
It spans from the moment a cell emerges
following division to the point when it divides
itself.
This cycle comprises distinct stages, each serving
a specific purpose.
Phases of the Cell Cycle
Growth and Development: The cell grows and develops
its functionality.
DNA Replication: The cell duplicates its genetic material
to prepare for division.
Preparation for Division: This stage readies the cell for
division, ensuring that all components are in order.
Cell Division: The cell divides into two daughter cells,
each with an identical genetic makeup.
Following division, a new cell cycle commences
 CONTROL OF THE CELL CYCLE
It is essential that daughter cells be
exact duplicates of the parent cell.
Mistakes in the duplication or
distribution of the chromosomes lead
to mutations that may be passed
forward to every new cell produced
from the abnormal cell.
To prevent a compromised cell from
continuing to divide, there are
internal control mechanisms that
operate at three main cell cycle
checkpoints at which the cell cycle
can be stopped until conditions are
favorable.
 CONTROL OF THE CELL CYCLE
Regulatory proteins called cyclins control the cell cycle at checkpoints:

Cyclins are a family of regulatory
proteins that control the progression
of the cell cycle.
Cyclins activate cyclin dependent
kinases (CDKs), which control cell
cycle processes.
A critical control point in the Cell
Cycle where ‘stop’/halt the cycle
(negative regulation) and ‘go-ahead’/
next phase (positive regulation)
signals can regulate the cell cycle is
called the checkpoint.
The concentrations of cyclin proteins change
throughout the cell cycle.
Regulation of the Cell
Cycle by External Events

Three major
checkpoints are found
in the G1, G2, and M
phases of the Cell
Cycle.
 The first checkpoint (G1) determines whether all conditions
are favorable for cell division to proceed. This checkpoint is
the point at which the cell irreversibly commits to the cell-
division process. In addition to adequate reserves and cell
size, there is a check for damage to the genomic DNA. A
cell that does not meet all the requirements will not be
released into the S phase.
The second checkpoint (G2) bars the entry to the mitotic
phase if certain conditions are not met. The most important
role of this checkpoint is to ensure that all of the
chromosomes have been replicated and that the replicated
DNA is not damaged.
 The final checkpoint (M) occurs in the middle of
mitosis. This checkpoint determines if all of the
copied chromosomes are arranged appropriately to
be separated to opposite sides of the cell. If this
doesn’t happen correctly, incorrect numbers of
chromosomes can be partitioned into each of the
daughter cells, which would likely cause them to die.
 The Cell Cycle
Consist of two(2) main periods:
G1 phase

I. Interphase (G0, G1, S, G2)

M phase
II. Mitotic Phase (M)
S
phase

G2
phase
Interphase involves regular growth processes, DNA
replication, and preparation for cell division (mitosis).
It is sometimes called the "daily living" or metabolic
phase due to its role in maintaining normal cellular
functions.
Surprisingly, despite its previous designation as the
"resting phase," Interphase is highly active.
Cells spend about 90% of their time in Interphase, making
it the longest phase in the cell cycle.
The name changed from "resting phase" to "Interphase"
because cells actively prepare for cell division during this
stage, rather than simply resting.
Interphase consists of three sub-phases:
Gap 1 (G1): The cell's first phase, dedicated
to growth.
Synthesis (S): The second phase, focused
on DNA replication.
Gap 2 (G2): The third phase, where further
cell growth occurs.
 G0 phase

G0 represents a phase where cells temporarily
exit the active cell cycle and enter a quiescent
(inactive) state.
Cells in G0 are not actively preparing for cell
division, but they continue to perform their
usual functions.
The duration of G0 can vary widely depending
on cell type and environmental conditions.
 G0 phase
Cells in G0 can be prompted to re-enter the
active cell cycle when they receive appropriate
signals or stimuli.
G0 is critical for cells with specialized functions
that do not require continuous division, such
as mature nerve cells, muscle cells, and
certain immune cells.
Chromosome and Centrioles
 A single length of DNA undergoes intricate
packaging to form the structures known as
nucleosomes, with many proteins called
histones involved in this process. Histones
primarily facilitate the compaction of DNA.
These nucleosomes coil tightly together,
creating chromatin loops.
These chromatin loops, in turn, wrap around
each other, culminating in the formation of a
complete chromosome.
 Each chromosome exhibits a distinct
structure, featuring two short arms
referred to as p arms, two longer arms
known as q arms, and a centromere
situated at the center, which plays a
crucial role in holding the chromosome
together.
 Human chromosomes can be
represented in two forms: as a single
component or replicated.

During interphase, chromosomes
duplicate, resulting in two sister
chromatids. A chromatid is one of
the two identical halves of a
chromosome that has been
replicated in preparation for cell
division. The two “sister”
chromatids are joined at a
constricted region of the
chromosome called the
centromere.
1
 Chromatin refers to a mixture of DNA and proteins that form the chromosomes
found in the cells of humans and other higher organisms. This
is the relaxed
form of DNA found in the nucleus of a cell when it is not
dividing. It's like a tangled string of genetic material.
Chromosomes are thread-like structures located inside the nucleus of animal
and plant cells. Each chromosome is made of protein and a single molecule of
deoxyribonucleic acid (DNA). When
a cell is getting ready to divide,
the chromatin coils up tightly to form chromosomes.
These are the X-shaped structures that hold your genetic
information.
A chromatid is one of two identical halves of a replicated
chromosome. Sister chromatids are identical copies of
DNA that remain connected by a central point called the
centromere until they are separated during mitosis.
 Before duplication: A chromosome is composed of a single
chromatid. This is when the cell is not preparing to divide,
and the chromosome consists of just one copy of DNA.

After duplication: The chromosome has two chromatids.
These chromatids are identical copies of each other,
connected at a region called the centromere. During cell
division, these chromatids will separate to ensure that each
new cell gets a complete set of chromosomes.

So, when duplicated, the chromosome has two
chromatids, and when not duplicated, it has just one.
 In humans, the genetic material is organized into
23 pairs of chromosomes, amounting to a total
of 46 chromosomes.
These chromosomes come in two sets: one set
inherited from the mother and the other from
the father.
Among these 23 pairs, one pair is comprised of
sex chromosome (allosomes), and their
composition varies based on an individual's
gender—XX for females and XY for males.
The remaining 22 pairs are termed autosomes,
representing non-sex chromosomes, and remain
identical in appearance for both males and
females.
 Each of our chromosomes contains a multitude of
genes, the fundamental units of genetic
information that govern various aspects of our
traits and functions.
Moreover, at the ends of each chromosome,
there are specialized sections of DNA known as
telomeres.
Telomeres serve a critical role in safeguarding the
chromosome ends during the process of DNA
replication. They function as protective caps,
much like the plastic tip on the end of a shoelace,
ensuring the stability and integrity of our genetic
material.
Centrosome is the point of origin of the mitotic spindle
Gap 1 (G1)

It is the first part of the cell cycle wherein the cell
carries out its normal metabolic function.
During this phase, cells also increased in size as
their organelles increase in number.
Cells spend most of their life cycle in this phase.
The G1 checkpoint ensures that the cell is large
enough to divide, the nutrients are enough to
support the resulting daughter cells and the DNA
is not damaged.
 If a cell receives a ‘go-ahead’ signal at the G1
checkpoint, it will usually continue with the
Cell Cycle.
If the cell does not receive the ‘go-ahead’
signal, it will exit the Cell Cycle and switch to a
non-dividing state called G0.
In G0, a cell is not actively preparing to divide,
it’s just doing its job, for instance, a neuron
conducting nerve impulses or a liver cell storing
carbohydrates.
Most cells in the human body are in the G0
phase.
Centriole Replication
A centrosome is composed of two,
barrel-shaped centrioles embedded
in an amorphous proteinaceous
matrix, known as the pericentriolar
material (PCM).
Like DNA, centrosome duplication is
a semi-conservative process that
occurs once, and only once, per cell
cycle. G1 phase cells possess a
single centrosome containing two
centrioles.
They take part in cell division for the
formation of spindle fibers
necessary for the movement of
chromosomes towards opposite
poles during the separation of sister
chromatids.
S phase (DNA Replication)

The cell makes a copy of genetic material
in the form of nuclear DNA.
During this stage, the cell spends
considerable amount of time and energy
to make copies of its chromosome.
Each chromosomes contains one DNA
molecule that is copied with enough
accuracy through DNA replication.
Semi-conservative replication because two copies of the original DNA
molecule are produced, each copy conserving (replicating) the information
from one half of the original DNA molecule.
S phase (DNA Replication)

This process ensures that the daughter
cell receives exact copies of the parent’s
genetic material during the cell division.
Aside from the DNA, it also produces
protein complex called microtubules- will
help in organizing the cell.
Centrioles duplicate
during the S phase of
the cell cycle, and it
results in the formation
of four centrioles prior
to cell division. They
help in distributing the
duplicated genetic
material equally. Also,
during S phase, DNA
replication occurs inside
the nucleus.
Gap 2 or G2

The critical checkpoint before
transitioning to the next stage.
It make sure that, it grows in correct size
and duplicating DNA without damage.
For most cells the G2 phase is relatively
short; once complete, the cell is ready to
divide.
During interphase, a cell grows larger. The cell replicates its DNA, forming sister chromatids. Each is joined
by a centromere. A collection of microtubules (structural proteins) called a centrosome also replicates.
There are two gap stages during interphase. During gap 1 (G1), the cell grows, while during gap 2 (G2), the
cell finishes growing and performs a quick check of the replicated DNA to make sure it was copied correctly.
 MITOSIS
The mitotic phase, also known as
M phase, is the stage where the
cell undergoes division, ultimately
leading to the creation of two
genetically identical daughter cells.
This phase is a complex, multi-step
process encompassing the division
of both the nucleus (karyokinesis)
and the cytoplasm (cytokinesis).
Karyokinesis: Division of the Nucleus

Mitosis, a critical component of the
mitotic phase, involves the division of
the nucleus.
Duplicated chromosomes are carefully
aligned, separated, and move towards
opposite poles of the cell.
The process can be broken down into
four distinct stages: Prophase,
Metaphase, Anaphase, and Telophase
(PMAT).
 Cytokinesis: Division of the Cytoplasm

The second part of the mitotic phase is cytokinesis, which involves
the physical separation of cytoplasmic components into the two
daughter cells.
Cytokinesis is responsible for creating two distinct and complete
daughter cells from the parent cell.
It marks the final step in the cell cycle, completing the goal of
distributing an identical set of genetic instructions to each daughter
cell.
As a result, each daughter cell receives one copy of each
chromosome, ensuring that they have the same full set of DNA as
the parent cell.
INTERPHASE
 PROPHASE (START OF MITOSIS)

Chromatin refers to a mixture of DNA and proteins
that form the chromosomes found in the cells of
humans and other higher organisms.
Chromosomes are thread-like structures located
inside the nucleus of animal and plant cells. Each
chromosome is made of protein and a single molecule
of deoxyribonucleic acid (DNA).
A chromatid is one of two identical halves of a
replicated chromosome. Sister chromatids are
identical copies of DNA that remain connected until
they are separated during mitosis.
 A centromere, the point on a chromosome that attaches to the
spindle fibers with a kinetochore during cell division, attaches the
sister chromatids. It is the region where the cell's spindle fibers
attach. The centromere is aided in binding sister chromatids
together by several proteins called cohesins and condensins. Once
the DNA has been replicated, the cell moves to the second gap
phase.
 During mitosis, the genetic material that has been replicated during
the synthesis phase is affected by the actions of two types of
proteins called cohesins and condensins.
Prior to mitosis, the DNA is found spread out inside the nucleus.
A cohesin protein helps bind sister chromatids together at the
centromere until they separate during anaphase.
A condensin is a protein that helps condense DNA into
chromosomes during prophase of mitosis. Condensin reorganizes
chromosomes when they get compacted during prophase. This
reduces the amount of space the DNA takes up..
 PROPHASE (START OF MITOSIS)

Prophase is the first phase of mitosis, in which
sister chromatids condense
the mitotic spindle begins to form, and
centrosomes (the structures that coordinate the
formation of microtubules, which allow cell division
to proceed) segregate to opposite poles.
 PROPHASE (START OF MITOSIS)

During prophase, the sister chromatids condense until
they are tightly packed. This makes them appear X-shaped,
which is the representation of chromosomes with which
most people are familiar.
The centrosomes segregate to the ends of the cell, called
the poles. The centrosomes then start to organize the
formation of the mitotic spindle, the bundle of spindle
fibers attached at one end to the centrosome.
 PROPHASE (START OF MITOSIS)

The mitotic spindle is composed of microtubules that
elongate from the centrosome to the centromeres, the
point on a chromosome that attaches to the spindle fibers
and at which the sister chromatids are attached. The
mitotic spindle helps align the sister chromatids correctly
for proper cell division, ensuring each daughter cell gets
one copy.
Prometaphase
As the cell progresses from prophase to
prometaphase, the nuclear envelope
starts to dissolve.
This breakdown of the nuclear envelope
is a critical step that allows the
chromosomes to become free to move
within the cell.
Additionally, during this process, the
nucleolus, a structure inside the
nucleus, disappears.
Formation of Vesicles:
The breakdown of the nuclear membrane results in
the formation of small vesicles, which are remnants of
the nuclear envelope.
These vesicles play an essential role in providing
access to the centromeres of the chromosomes for
the mitotic spindle.

Attachment of Spindle Fibers:
When a spindle fiber finds a centromere, it attaches at
the kinetochore, a group of proteins bound at the centromere.
The spindle fibers tug the chromosomes back and forth as they
position them correctly for the next stage.
The spindle fiber that extends from the centrosome to the
kinetochore on the centromere is known as a kinetochore
microtubule
End Prophase:
The nuclear membrane
has fragmented, centrioles
microtubules have Microtubules
invaded the nuclear area form a complete
spindle
Centrioles have moved to the chromatids
opposite poles
centrioles
The spindle is completely
formed.
METAPHASE: the third phase of mitosis, where the
chromosomes align themselves along the equator of the cell.

In this stage, the chromosomes line
up along the cell equator (also
called the metaphase plate), an
imaginary line in the center of a cell
during mitosis, along which sister
chromatids align.
 METAPHASE
Each chromosome is composed of a
pair of identical sister chromatids
Centrioles
linked by the centromere.
The sister chromatids are attached
by their centromere to two spindle
Chromosomes
fibers: one leading to each
centrosome at opposite ends—each
pole—of the cell. The chromosomes Spindle
no longer move back and forth but composed of
microtubules
stay aligned along the equator.
In metaphase the third
stage of mitosis, the
sister chromatids of the
replicated chromosomes
line up along the cell
equator or "metaphase
plate" or "equatorial
plate."
The metaphase plate is
significant because it marks a
critical checkpoint in cell
division. The cell checks to
make sure that all the
chromosomes are properly
aligned before proceeding to
anaphase, where the sister
chromatids are pulled apart
to opposite poles of the cell.
Anaphase: where the sister chromatids separate and start to
move towards opposite sides of the cell.

Chromosome Separation: the paired
chromosomes, also known as sister
chromatids, undergo separation.

Chromatid Movement: The separated
chromatids swiftly move toward opposite
poles of the cell. This movement is
orchestrated by the shortening of kinetochore
microtubules.
Initiation of Cytoplasmic Division:
Simultaneously, anaphase initiates a Chromatids are
being pulled to
partial division of the cell's opposite sides of
cytoplasm. This early phase of the cell.
cytokinesis lays the foundation for
the eventual splitting of the cell into Shortening of the
microtubules
two daughter cells.
Telophase: the nuclear membrane reforms and prepares the
cell to divide in half during cytokinesis.

Chromosomal Arrangement:
Chromosomes reach poles within the cell.
Nuclear Envelope Formation: Vesicles
reform a new nuclear envelope around
daughter cell DNA.
Spindle Breakdown: Mitotic spindle begins
to break down, causing spindle fibers to
disappear.
 Telophase Microtubule and Spindle Fiber
Disintegration: Microtubules and spindle
fibers disintegrate.
Nuclear Membrane Reconstruction:
Nuclear
membrane
Fragments and proteins rebuild the
is nuclear membrane, defining two distinct
returning nuclei.
Chromatin Formation: Chromosomes
gradually uncoil into chromatin, making
DNA accessible.
Chromosomal Visibility: Individual
chromosomes are no longer visible,
Telophase marks mitosis completion, leading to two separate
having transitioned into a less compacted
nuclei and preparing for cytokinesis, the final step in cell chromatin state.
division
Cytokinesis: the pinching off of the cytoplasm to form
two new cells

Involves the splitting of the
cytoplasm into two daughter
cells.
It completes the cell cycle.
Cytokinesis: in animal cells…

In animal cells, cleavage furrow is formed
inward by tiny strands of protein actin
called “microfilaments”
Slowly, the cell membrane begins to form.
This final cell division marks the end of M
phase of the cell cycle. At this point, each
cell resumes the G1 phase or exits the cell
cycle completely if the cell will no longer
divide.
Cytokinesis: in plant cells…

In plant cells, the membrane cannot pinch
because of cell wall.
Instead, a cell plate will form between the
two daughter cells.
The cell plate is made by Golgi apparatus
The vesicle supply new cell wall.
Lipids to form plasma membrane
Cytokinesis:
Occurs at the end of mitosis

Animal cells: a cleavage furrow
separates the daughter cells

Plant cell: a cell plate separates the
daughter cells

Daughter cells are genetically
Cells return to interphase
identical
 The duration of these cell cycle phases
varies considerably in different kinds of
cells.
For a typical rapidly proliferating human
cell with a total cycle time of 24 hours,
the G1 phase might last about 11 hours,
S phase about 8 hours, G2 about 4
hours, and M about 1 hour.
Thank You!