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Chapter 11 Addendum
Apoptosis—programmed cell death; organized
series of events to recapture biomolecules in an
ordered fashion and utilize metabolites from the
cells that are dying; DNA fragmented, cell
shrinks into blebs that can then be digested by
phagocytic cells
Vs.
Necrosis—decaying tissue from wound,
infection, cell contents leak out of membrane
systems and enzymes can damage surrounding
tissue
Apoptosis pathways in nematodes and
mammals
Discovered in
worms, analogs
in mammals
Pink=major proteases
involved in scavenging
Apoptosis controls
• External signals involved in development e.g.
removing webbing from digits. Works as signal
transduction
• Internal signals such as excessive DNA damage
and increased mis-folded proteins in ER to
avoid necrotic tissue damage
Disruption of normal brain development by
blocking apoptosis
Extra neurons & webbed digits
Chapter 12
The Cell Cycle
Reproduction
100 µm
Tissue renewalGrowth and development
20 µm200 µm
The Key Roles of Cell Division
•Reproduction
•Repair e.g. wound healing
•Growth
•Replacement e.g. skin
Animal mitosis video live
Cell division results in genetically
identical daughter cells
• Cells duplicate their genetic material before they
divide, ensuring that each daughter cell receives an
exact copy of the genetic material, DNA
• A dividing cell duplicates its DNA, allocates the two
copies to opposite ends of the cell, and only then
splits into daughter cells
• A cell’s endowment of DNA (its genetic
information) is called its genome
• DNA molecules in a cell are packaged into
chromosomes
• Every eukaryotic species has a characteristic
number of chromosomes in each cell nucleus
• Somatic (nonreproductive) cells have two sets
of chromosomes = 2n (diploid)
• Germ cells (reproductive cells: sperm and eggs)
have half as many chromosomes as somatic
cells = 1n (haploid)
• Eukaryotic chromosomes consist of chromatin,
a complex of DNA and protein that condenses
during cell division (about 50/50)
Fig. 4.6
Distribution of Chromosomes During
Cell Division
• In preparation for cell division, DNA is replicated
and the chromosomes condense
• Each duplicated chromosome has two sister
chromatids, which separate during cell division
• The centromere is the narrow “waist” of the
duplicated chromosome, where the two
chromatids are most closely attached
Figure 12.5-3
Chromosomes
Centromere
Chromosome
arm
Chromosomal
DNA molecules
1
Chromosome
duplication
Sister
chromatids
2
3
Separation of
sister chromatids
Fig. 4.5
• Eukaryotic cell division consists of:
– Mitosis, the division of the nucleus
– Cytokinesis, the division of the cytoplasm
• Gametes are produced by a variation of cell
division called meiosis
• Meiosis yields nonidentical daughter cells that
have only one set of chromosomes, half as
many as the parent cell
LE 12-5
G1
G2
S
(DNA synthesis)
INTERPHASE
Cytokinesis
MITOTIC(M) PHASE
M
itosis
Phases of the Cell Cycle
• Mitosis is conventionally divided into five phases:
– Prophase
– Prometaphase
– Metaphase
– Anaphase
– Telophase
• Cytokinesis is well underway by late telophase
Fig. 4.8
The Mitotic Spindle: A Closer Look
• The mitotic spindle is an apparatus of
microtubules that controls chromosome
movement during mitosis
• Assembly of spindle microtubules begins in the
centrosome, the microtubule organizing center
• The centrosome replicates in interphase,
forming two centrosomes that migrate to
opposite ends of the cell, as spindle
microtubules grow out from them
• An aster (a radial array of short microtubules)
extends from each centrosome
Figure 12.8
Sister
chromatids
Aster
Centrosome
Metaphase
plate
(imaginary)
Kineto-
chores
Kinetochore
microtubules
Microtubules
Overlapping
nonkinetochore
microtubules
Chromosomes
Centrosome
1 µm 0.5 µm
The spindle includes the
centrosomes, the spindle
microtubules, and the asters
MT: aster, kinetochore, polar
Chromosome
movement
Microtubule Motor
protein
Chromosome
Kinetochore
Tubulin
subunits
•In anaphase, sister chromatids separate and move along
the kinetochore microtubules toward opposite ends of the
cell
•In anaphase the cohesins are cleaved by an enzyme
called separase
•The microtubules shorten by depolymerizing at their
kinetochore ends
• Nonkinetochore (or polar) microtubules from
opposite poles overlap and push against each
other, elongating the cell
• In telophase, genetically identical daughter
nuclei form at opposite ends of the cell
Figure 12.10
(a) Cleavage of an animal cell (SEM) (b) Cell plate formation in a plant cell (TEM)
Cleavage furrow
Contractile ring of
microfilaments
Daughter cells
100 µm
1 µm
Daughter cells
New cell wallCell plate
Wall of parent cellVesicles
forming
cell plate
Cytokinesis: division of cytoplasm;
begins in anaphase or telophase
Figure 12.11
Nucleus
10µm
Nucleolus
Chromosomes
condensing Chromosomes
PrometaphaseProphase
Cell plate
1 2
3 4 5Metaphase Anaphase Telophase
Binary Fission
• Prokaryotes (bacteria and archaea) reproduce
by a type of cell division called binary fission
• In binary fission, the chromosome replicates
(beginning at the origin of replication), and the
two daughter chromosomes actively move
apart
Figure 12.12-4
Chromosome
replication
begins.
Two copies
of origin
E. coli cell
Origin of
replication
Cell wall
Plasma
membrane
Bacterial
chromosome1
2 Origin OriginOne copy of the
origin is now at
each end of the
cell.
3
Two daughter
cells result.
4
Replication
finishes.
The Evolution of Mitosis
• Since prokaryotes evolved before eukaryotes,
mitosis probably evolved from binary fission
• Certain protists exhibit types of cell division that
seem intermediate between binary fission and
mitosis
Figure 12.13
Bacterial
chromosome
(a) Bacteria
Chromosomes
Microtubules
Intact nuclear
envelope
(b) Dinoflagellates (d) Most eukaryotes
Fragments
of nuclear
envelope
Kinetochore
microtubule
Kinetochore
microtubule
(c) Diatoms and some yeasts
Intact
nuclear
envelope
1. Which of the following best
describes the kinetochore?
a. a structure composed of several proteins that
associate with the centromere region of a
chromosome and that can bind to spindle
microtubules
b. the centromere region of a metaphase chromosome
at which the DNA can bind with spindle proteins
c. the array of vesicles that will form between two
dividing nuclei and give rise to the metaphase plate
d. the ring of actin microfilaments that will cause the
appearance of the cleavage furrow
e. the core of proteins that forms the cell plate in a
dividing plant cell
1. Which of the following best
describes the kinetochore?
a. a structure composed of several proteins that
associate with the centromere region of a
chromosome and that can bind to spindle
microtubules
b. the centromere region of a metaphase chromosome
at which the DNA can bind with spindle proteins
c. the array of vesicles that will form between two
dividing nuclei and give rise to the metaphase plate
d. the ring of actin microfilaments that will cause the
appearance of the cleavage furrow
e. the core of proteins that forms the cell plate in a
dividing plant cell
The eukaryotic cell cycle is regulated by
a molecular control system
• The frequency of cell division varies with the
type of cell
• These cell cycle differences result from
regulation at the molecular level
• The cell cycle appears to be driven by specific
chemical signals present in the cytoplasm
• Some evidence for this hypothesis comes from
experiments in which cultured mammalian cells
at different phases of the cell cycle were fused
to form a single cell with two nuclei
Figure 12.14
Experiment 1 Experiment 2Experiment
Results
Conclusion
S
S S
G1
G1M
M M
G1 nucleus
immediately entered
S phase and DNA
was synthesized.
G1 nucleus began
mitosis without
chromosome
duplication.
Molecules present in the cytoplasm control
the progression to S and M phases.
LE 12-14
G1 checkpoint
G1
S
M
M checkpoint
G2 checkpoint
G2
Control
system
The clock has specific
checkpoints where the cell
cycle stops until a go-ahead
signal is received
LE 12-15
G1
G1 checkpoint
G1
G0
If a cell receives a go-ahead
signal at the G1 checkpoint,
the cell continues on in the
cell cycle.
If a cell does not receive a
go-ahead signal at the G1
checkpoint, the cell exits the
cell cycle and goes into G0, a
nondividing state.
For many cells, the G1
checkpoint seems to be
the most important one
Copyright © 2005 Pearson Education, Inc. publishing as Benjamin Cummings
The Cell Cycle Clock: Cyclins and
Cyclin-Dependent Kinases
• Two types of regulatory proteins are involved in
cell cycle control: cyclins and cyclin-dependent
kinases (Cdks)
• The activity of cyclins and Cdks fluctuates
during the cell cycle
• MPF (maturation-promoting factor) is a cyclin-
Cdk complex that triggers a cell’s passage past
the G2 checkpoint into the M phase
Figure 12.16
MPF
activity
(a) Fluctuation of MPF activity and cyclin
concentration during the cell cycle (b) Molecular mechanisms that help regulate
the cell cycle
Time
Degraded
cyclin
Cdk
Cyclin is
degraded
MPF Cyclin
Cdk
G2
checkpoint
Cyclin
concentration
M M M G1G2G2G1 G1S S
G
1
S
G 2
M
Copyright © 2005 Pearson Education, Inc. publishing as Benjamin Cummings
Stop and Go Signs: Internal and External Signals at
the Checkpoints
• An example of an internal signal is that
kinetochores not attached to spindle
microtubules send a molecular signal that
delays anaphase
• Some external signals are growth factors,
proteins released by certain cells that stimulate
other cells to divide
• For example, platelet-derived growth factor
(PDGF) stimulates the division of human
fibroblast cells in culture
Copyright © 2005 Pearson Education, Inc. publishing as Benjamin Cummings
PowerPoint Lectures for
Biology, Seventh Edition
Neil Campbell and Jane Reece
Lectures by Chris Romero
Figure 12.18-4
Scalpels
1
Petri
dish
A sample of
human connective
tissue is cut
up into small
pieces.
2
Enzymes digest
the extracellular
matrix, resulting
in a suspension of
free fibroblasts.
3
Cells are transferred
to culture vessels.
4 PDGF is added
to half the
vessels.
Without PDGF With PDGF Cultured fibroblasts (SEM)
10µm
• Another example of external signals is density-
dependent inhibition, in which crowded cells
stop dividing
• Most animal cells also exhibit anchorage
dependence, in which they must be attached to
a substratum in order to divide
• Cancer cells do NOT have either
Figure 12.19
Anchorage dependence: cells
require a surface for division
Density-dependent inhibition:
cells form a single layer
Density-dependent inhibition:
cells divide to fill a gap and
then stop
(a) Normal mammalian cells (b) Cancer cells
20 µm 20 µm
Loss of Cell Cycle Controls in Cancer Cells
• Cancer cells do not respond normally to the
body’s control mechanisms
• Cancer cells form tumors, masses of abnormal
cells within otherwise normal tissue
• If abnormal cells remain at the original site, the
lump is called a benign tumor
• Malignant tumors invade surrounding tissues
and can metastasize, exporting cancer cells to
other parts of the body, where they may form
secondary tumors
• Cancer cells may not need growth factors to
grow and divide
– They may make their own growth factor
– They may convey a growth factor’s signal without
the presence of the growth factor
– They may have an abnormal cell cycle control
system
Figure 12.20
Tumor
Glandular
tissue
A tumor grows
from a single
cancer cell.
1 2 3
Cancer cells invade
neighboring tissue. Cancer cells spread
through lymph and
blood vessels to other
parts of the body.
4
A small percentage
of cancer cells may
metastasize to
another part of the
body.
Cancer
cell
Blood
vessel
Lymph
vessel
Breast cancer cell
(colorized SEM)
Metastatic
tumor
5µm
2. Of the events of a typical cell division listed below,
which is most likely to occur THIRD in an animal cell
that is going through mitosis?
a. Kinetochore proteins associated with the
centromeres bind with associated microtubules.
b. Segregation of complete genomic sets of
chromosomes occurs.
c. The nuclear envelope membranes are converted
from flat bilayers into many spherical vesicles.
d. The number of chromosomes in the cell doubles as
double-chromatid chromosomes are split into pairs
of single-chromatid chromosomes.
e. Vesicles fuse to one another to form new nuclear
envelope membranes.
2. Of the events of a typical cell division listed below,
which is most likely to occur THIRD in an animal cell
that is going through mitosis?
a. Kinetochore proteins associated with the centromeres bind
with associated microtubules. prometaphase
b. Segregation of complete genomic sets of chromosomes
occurs. Anaphase—simultaneous with d
c. The nuclear envelope membranes are converted from flat
bilayers into many spherical vesicles.
Prophase/Prometaphase
d. The number of chromosomes in the cell doubles as double-
chromatid chromosomes are split into pairs
of single-chromatid chromosomes. Anaphase
e. Vesicles fuse to one another to form new nuclear envelope
membranes. telophase

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Chapter12cellcycle 151125145605-lva1-app6891

  • 1. Chapter 11 Addendum Apoptosis—programmed cell death; organized series of events to recapture biomolecules in an ordered fashion and utilize metabolites from the cells that are dying; DNA fragmented, cell shrinks into blebs that can then be digested by phagocytic cells Vs. Necrosis—decaying tissue from wound, infection, cell contents leak out of membrane systems and enzymes can damage surrounding tissue
  • 2. Apoptosis pathways in nematodes and mammals Discovered in worms, analogs in mammals Pink=major proteases involved in scavenging
  • 3. Apoptosis controls • External signals involved in development e.g. removing webbing from digits. Works as signal transduction • Internal signals such as excessive DNA damage and increased mis-folded proteins in ER to avoid necrotic tissue damage
  • 4. Disruption of normal brain development by blocking apoptosis Extra neurons & webbed digits
  • 6. Reproduction 100 µm Tissue renewalGrowth and development 20 µm200 µm The Key Roles of Cell Division •Reproduction •Repair e.g. wound healing •Growth •Replacement e.g. skin
  • 8. Cell division results in genetically identical daughter cells • Cells duplicate their genetic material before they divide, ensuring that each daughter cell receives an exact copy of the genetic material, DNA • A dividing cell duplicates its DNA, allocates the two copies to opposite ends of the cell, and only then splits into daughter cells • A cell’s endowment of DNA (its genetic information) is called its genome • DNA molecules in a cell are packaged into chromosomes
  • 9. • Every eukaryotic species has a characteristic number of chromosomes in each cell nucleus • Somatic (nonreproductive) cells have two sets of chromosomes = 2n (diploid) • Germ cells (reproductive cells: sperm and eggs) have half as many chromosomes as somatic cells = 1n (haploid) • Eukaryotic chromosomes consist of chromatin, a complex of DNA and protein that condenses during cell division (about 50/50)
  • 11. Distribution of Chromosomes During Cell Division • In preparation for cell division, DNA is replicated and the chromosomes condense • Each duplicated chromosome has two sister chromatids, which separate during cell division • The centromere is the narrow “waist” of the duplicated chromosome, where the two chromatids are most closely attached
  • 14. • Eukaryotic cell division consists of: – Mitosis, the division of the nucleus – Cytokinesis, the division of the cytoplasm • Gametes are produced by a variation of cell division called meiosis • Meiosis yields nonidentical daughter cells that have only one set of chromosomes, half as many as the parent cell
  • 15. LE 12-5 G1 G2 S (DNA synthesis) INTERPHASE Cytokinesis MITOTIC(M) PHASE M itosis Phases of the Cell Cycle
  • 16. • Mitosis is conventionally divided into five phases: – Prophase – Prometaphase – Metaphase – Anaphase – Telophase • Cytokinesis is well underway by late telophase
  • 18. The Mitotic Spindle: A Closer Look • The mitotic spindle is an apparatus of microtubules that controls chromosome movement during mitosis • Assembly of spindle microtubules begins in the centrosome, the microtubule organizing center • The centrosome replicates in interphase, forming two centrosomes that migrate to opposite ends of the cell, as spindle microtubules grow out from them • An aster (a radial array of short microtubules) extends from each centrosome
  • 20. Chromosome movement Microtubule Motor protein Chromosome Kinetochore Tubulin subunits •In anaphase, sister chromatids separate and move along the kinetochore microtubules toward opposite ends of the cell •In anaphase the cohesins are cleaved by an enzyme called separase •The microtubules shorten by depolymerizing at their kinetochore ends
  • 21. • Nonkinetochore (or polar) microtubules from opposite poles overlap and push against each other, elongating the cell • In telophase, genetically identical daughter nuclei form at opposite ends of the cell
  • 22. Figure 12.10 (a) Cleavage of an animal cell (SEM) (b) Cell plate formation in a plant cell (TEM) Cleavage furrow Contractile ring of microfilaments Daughter cells 100 µm 1 µm Daughter cells New cell wallCell plate Wall of parent cellVesicles forming cell plate Cytokinesis: division of cytoplasm; begins in anaphase or telophase
  • 24. Binary Fission • Prokaryotes (bacteria and archaea) reproduce by a type of cell division called binary fission • In binary fission, the chromosome replicates (beginning at the origin of replication), and the two daughter chromosomes actively move apart
  • 25. Figure 12.12-4 Chromosome replication begins. Two copies of origin E. coli cell Origin of replication Cell wall Plasma membrane Bacterial chromosome1 2 Origin OriginOne copy of the origin is now at each end of the cell. 3 Two daughter cells result. 4 Replication finishes.
  • 26. The Evolution of Mitosis • Since prokaryotes evolved before eukaryotes, mitosis probably evolved from binary fission • Certain protists exhibit types of cell division that seem intermediate between binary fission and mitosis
  • 27. Figure 12.13 Bacterial chromosome (a) Bacteria Chromosomes Microtubules Intact nuclear envelope (b) Dinoflagellates (d) Most eukaryotes Fragments of nuclear envelope Kinetochore microtubule Kinetochore microtubule (c) Diatoms and some yeasts Intact nuclear envelope
  • 28. 1. Which of the following best describes the kinetochore? a. a structure composed of several proteins that associate with the centromere region of a chromosome and that can bind to spindle microtubules b. the centromere region of a metaphase chromosome at which the DNA can bind with spindle proteins c. the array of vesicles that will form between two dividing nuclei and give rise to the metaphase plate d. the ring of actin microfilaments that will cause the appearance of the cleavage furrow e. the core of proteins that forms the cell plate in a dividing plant cell
  • 29. 1. Which of the following best describes the kinetochore? a. a structure composed of several proteins that associate with the centromere region of a chromosome and that can bind to spindle microtubules b. the centromere region of a metaphase chromosome at which the DNA can bind with spindle proteins c. the array of vesicles that will form between two dividing nuclei and give rise to the metaphase plate d. the ring of actin microfilaments that will cause the appearance of the cleavage furrow e. the core of proteins that forms the cell plate in a dividing plant cell
  • 30. The eukaryotic cell cycle is regulated by a molecular control system • The frequency of cell division varies with the type of cell • These cell cycle differences result from regulation at the molecular level • The cell cycle appears to be driven by specific chemical signals present in the cytoplasm • Some evidence for this hypothesis comes from experiments in which cultured mammalian cells at different phases of the cell cycle were fused to form a single cell with two nuclei
  • 31. Figure 12.14 Experiment 1 Experiment 2Experiment Results Conclusion S S S G1 G1M M M G1 nucleus immediately entered S phase and DNA was synthesized. G1 nucleus began mitosis without chromosome duplication. Molecules present in the cytoplasm control the progression to S and M phases.
  • 32. LE 12-14 G1 checkpoint G1 S M M checkpoint G2 checkpoint G2 Control system The clock has specific checkpoints where the cell cycle stops until a go-ahead signal is received
  • 33. LE 12-15 G1 G1 checkpoint G1 G0 If a cell receives a go-ahead signal at the G1 checkpoint, the cell continues on in the cell cycle. If a cell does not receive a go-ahead signal at the G1 checkpoint, the cell exits the cell cycle and goes into G0, a nondividing state. For many cells, the G1 checkpoint seems to be the most important one
  • 34. Copyright © 2005 Pearson Education, Inc. publishing as Benjamin Cummings The Cell Cycle Clock: Cyclins and Cyclin-Dependent Kinases • Two types of regulatory proteins are involved in cell cycle control: cyclins and cyclin-dependent kinases (Cdks) • The activity of cyclins and Cdks fluctuates during the cell cycle • MPF (maturation-promoting factor) is a cyclin- Cdk complex that triggers a cell’s passage past the G2 checkpoint into the M phase
  • 35. Figure 12.16 MPF activity (a) Fluctuation of MPF activity and cyclin concentration during the cell cycle (b) Molecular mechanisms that help regulate the cell cycle Time Degraded cyclin Cdk Cyclin is degraded MPF Cyclin Cdk G2 checkpoint Cyclin concentration M M M G1G2G2G1 G1S S G 1 S G 2 M
  • 36. Copyright © 2005 Pearson Education, Inc. publishing as Benjamin Cummings Stop and Go Signs: Internal and External Signals at the Checkpoints • An example of an internal signal is that kinetochores not attached to spindle microtubules send a molecular signal that delays anaphase • Some external signals are growth factors, proteins released by certain cells that stimulate other cells to divide • For example, platelet-derived growth factor (PDGF) stimulates the division of human fibroblast cells in culture
  • 37. Copyright © 2005 Pearson Education, Inc. publishing as Benjamin Cummings PowerPoint Lectures for Biology, Seventh Edition Neil Campbell and Jane Reece Lectures by Chris Romero Figure 12.18-4 Scalpels 1 Petri dish A sample of human connective tissue is cut up into small pieces. 2 Enzymes digest the extracellular matrix, resulting in a suspension of free fibroblasts. 3 Cells are transferred to culture vessels. 4 PDGF is added to half the vessels. Without PDGF With PDGF Cultured fibroblasts (SEM) 10µm
  • 38. • Another example of external signals is density- dependent inhibition, in which crowded cells stop dividing • Most animal cells also exhibit anchorage dependence, in which they must be attached to a substratum in order to divide • Cancer cells do NOT have either
  • 39. Figure 12.19 Anchorage dependence: cells require a surface for division Density-dependent inhibition: cells form a single layer Density-dependent inhibition: cells divide to fill a gap and then stop (a) Normal mammalian cells (b) Cancer cells 20 µm 20 µm
  • 40. Loss of Cell Cycle Controls in Cancer Cells • Cancer cells do not respond normally to the body’s control mechanisms • Cancer cells form tumors, masses of abnormal cells within otherwise normal tissue • If abnormal cells remain at the original site, the lump is called a benign tumor • Malignant tumors invade surrounding tissues and can metastasize, exporting cancer cells to other parts of the body, where they may form secondary tumors
  • 41. • Cancer cells may not need growth factors to grow and divide – They may make their own growth factor – They may convey a growth factor’s signal without the presence of the growth factor – They may have an abnormal cell cycle control system
  • 42. Figure 12.20 Tumor Glandular tissue A tumor grows from a single cancer cell. 1 2 3 Cancer cells invade neighboring tissue. Cancer cells spread through lymph and blood vessels to other parts of the body. 4 A small percentage of cancer cells may metastasize to another part of the body. Cancer cell Blood vessel Lymph vessel Breast cancer cell (colorized SEM) Metastatic tumor 5µm
  • 43. 2. Of the events of a typical cell division listed below, which is most likely to occur THIRD in an animal cell that is going through mitosis? a. Kinetochore proteins associated with the centromeres bind with associated microtubules. b. Segregation of complete genomic sets of chromosomes occurs. c. The nuclear envelope membranes are converted from flat bilayers into many spherical vesicles. d. The number of chromosomes in the cell doubles as double-chromatid chromosomes are split into pairs of single-chromatid chromosomes. e. Vesicles fuse to one another to form new nuclear envelope membranes.
  • 44. 2. Of the events of a typical cell division listed below, which is most likely to occur THIRD in an animal cell that is going through mitosis? a. Kinetochore proteins associated with the centromeres bind with associated microtubules. prometaphase b. Segregation of complete genomic sets of chromosomes occurs. Anaphase—simultaneous with d c. The nuclear envelope membranes are converted from flat bilayers into many spherical vesicles. Prophase/Prometaphase d. The number of chromosomes in the cell doubles as double- chromatid chromosomes are split into pairs of single-chromatid chromosomes. Anaphase e. Vesicles fuse to one another to form new nuclear envelope membranes. telophase

Editor's Notes

  1. DevBio9e-Fig-03-31-0.jpg
  2. DevBio9e-Fig-03-32-0.jpg
  3. Figure 12.5-3 Chromosome duplication and distribution during cell division (step 3)
  4. Figure 12.8 The mitotic spindle at metaphase
  5. Figure 12.10 Cytokinesis in animal and plant cells
  6. Figure 12.11 Mitosis in a plant cell
  7. Figure 12.12-4 Bacterial cell division by binary fission (step 4)
  8. Figure 12.13 Mechanisms of cell division in several groups of organisms
  9. Answer: A Students should be able to differentiate kinetochore from centromere.
  10. Answer: A Students should be able to differentiate kinetochore from centromere.
  11. Figure 12.14 Inquiry: Do molecular signals in the cytoplasm regulate the cell cycle?
  12. Figure 12.16 Molecular control of the cell cycle at the G2 checkpoint
  13. Figure 12.18-4 The effect of platelet-derived growth factor (PDGF) on cell division (step 4)
  14. Figure 12.19 Density-dependent inhibition and anchorage dependence of cell division
  15. Figure 12.20 The growth and metastasis of a malignant breast tumor
  16. Answer: D The order would be 1) c. 2) a. 3) d. 4) b. 5) e.
  17. Answer: D The order would be 1) c. 2) a. 3) d. 4) b. 5) e.