1. 9
The Cell Cycle

2. Overview: The Key Roles of Cell Division
The ability of organisms to produce more of their own kind best distinguishes living things from nonliving matter
The continuity of life is based on the reproduction of cells, or cell division
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3. Figure 9.1
Figure 9.1 How do a cell’s chromosomes change during cell division? 3

4. In unicellular organisms, division of one cell reproduces the entire organism
Cell division enables multicellular eukaryotes to develop from a single cell and, once fully grown, to renew, repair, or replace cells as needed
Cell division is an integral part of the cell cycle, the life of a cell from formation to its own division
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5. (a) Reproduction (b) Growth and development (c) Tissue renewal 100 m
Figure 9.2
100 m
200 m
(a) Reproduction
(b) Growth and
development
Figure 9.2 The functions of cell division
20 m
(c) Tissue renewal 5

6. (a) Reproduction 100 m Figure 9.2a
Figure 9.2a The functions of cell division (part 1: reproduction)
(a) Reproduction 6

7. (b) Growth and development
Figure 9.2b
200 m
Figure 9.2b The functions of cell division (part 2: growth and development)
(b) Growth and development 7

8. (c) Tissue renewal 20 m Figure 9.2c
Figure 9.2c The functions of cell division (part 3: tissue renewal)
(c) Tissue renewal 8

9. Concept 9.1: Most cell division results in genetically identical daughter cells
Most cell division results in the distribution of identical genetic material—DNA—to two daughter cells
DNA is passed from one generation of cells to the next with remarkable fidelity
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10. Cellular Organization of the Genetic Material
All the DNA in a cell constitutes the cell’s genome
A genome can consist of a single DNA molecule (common in prokaryotic cells) or a number of DNA molecules (common in eukaryotic cells)
DNA molecules in a cell are packaged into chromosomes
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11. Eukaryotic chromosomes
Figure 9.3
Figure 9.3 Eukaryotic chromosomes
20 m
Eukaryotic chromosomes 11

12. Somatic cells (nonreproductive cells) have two sets of chromosomes
Eukaryotic chromosomes consist of chromatin, a complex of DNA and protein
Every eukaryotic species has a characteristic number of chromosomes in each cell nucleus
Somatic cells (nonreproductive cells) have two sets of chromosomes
Gametes (reproductive cells: sperm and eggs) have one set of chromosomes
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13. Distribution of Chromosomes During Eukaryotic Cell Division
In preparation for cell division, DNA is replicated and the chromosomes condense
Each duplicated chromosome has two sister chromatids, joined identical copies of the original chromosome
The centromere is where the two chromatids are most closely attached
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14. Sister chromatids Centromere 0.5 m Figure 9.4
Figure 9.4 A highly condensed, duplicated human chromosome (SEM)
0.5 m 14

15. Once separate, the chromatids are called chromosomes
During cell division, the two sister chromatids of each duplicated chromosome separate and move into two nuclei
Once separate, the chromatids are called chromosomes
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16. Chromosomal DNA molecules
Figure 9.5-1
Chromosomal
DNA molecules
Chromosomes 1
Centromere
Chromosome
arm
Figure Chromosome duplication and distribution during cell division (step 1) 16

17. Chromosomal DNA molecules
Figure 9.5-2
Chromosomal
DNA molecules
Chromosomes 1
Centromere
Chromosome
arm
Chromosome duplication 2
Sister
chromatids
Figure Chromosome duplication and distribution during cell division (step 2) 17

18. Chromosomal DNA molecules
Figure 9.5-3
Chromosomal
DNA molecules
Chromosomes 1
Centromere
Chromosome
arm
Chromosome duplication 2
Sister
chromatids
Figure Chromosome duplication and distribution during cell division (step 3)
Separation of sister
chromatids 3 18

19. Eukaryotic cell division consists of
Mitosis, the division of the genetic material in 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
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20. Concept 9.2: The mitotic phase alternates with interphase in the cell cycle
In 1882, the German anatomist Walther Flemming developed dyes to observe chromosomes during mitosis and cytokinesis
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21. Phases of the Cell Cycle
The cell cycle consists of
Mitotic (M) phase, including mitosis and cytokinesis
Interphase, including cell growth and copying of chromosomes in preparation for cell division
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22. Interphase (about 90% of the cell cycle) can be divided into subphases
G1 phase (“first gap”)
S phase (“synthesis”)
G2 phase (“second gap”)
The cell grows during all three phases, but chromosomes are duplicated only during the S phase
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23. S G1 (DNA synthesis) G2 Cytokinesis Mitosis Figure 9.6
Figure 9.6 The cell cycle 23

24. Mitosis is conventionally divided into five phases
Prophase
Prometaphase
Metaphase
Anaphase
Telophase
Cytokinesis overlaps the latter stages of mitosis
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25. Video: Microtubules Mitosis
Video: Animal Mitosis
Video: Microtubules Mitosis
Animation: Mitosis
Video: Microtubules Anaphase
Video: Nuclear Envelope
© 2014 Pearson Education, Inc. 25

26. Two sister chromatids of
Figure 9.7a
10 m
G2 of Interphase
Prophase
Prometaphase
Chromosomes
(duplicated,
uncondensed)
Early mitotic
spindle
Centromere
Fragments
of nuclear
envelope
Centrosomes
(with centriole
pairs)
Nonkinetochore
microtubules
Aster
Figure 9.7a Exploring mitosis in an animal cell (part 1: G2 of interphase through prometaphase)
Plasma
membrane
Nucleolus
Kinetochore
Kinetochore
microtubule
Nuclear
envelope
Two sister chromatids of
one chromosome 26

27. Telophase and Cytokinesis
Figure 9.7b
10 m
Metaphase
Anaphase
Telophase and
Cytokinesis
Metaphase
plate
Cleavage
furrow
Nucleolus
forming
Figure 9.7b Exploring mitosis in an animal cell (part 2: metaphase through cytokinesis)
Nuclear
envelope
forming
Spindle
Centrosome at
one spindle pole
Daughter
chromosomes 27

28. Two sister chromatids of
Figure 9.7c
G2 of Interphase
Prophase
Centrosomes
(with centriole
pairs)
Chromosomes
(duplicated,
uncondensed)
Early mitotic
spindle
Centromere
Aster
Figure 9.7c Exploring mitosis in an animal cell (part 3: G2 of interphase and prophase)
Plasma
membrane
Nucleolus
Nuclear
envelope
Two sister chromatids of
one chromosome 28

29. Prometaphase Metaphase Fragments of nuclear envelope Nonkinetochore
Figure 9.7d
Prometaphase
Metaphase
Fragments
of nuclear
envelope
Nonkinetochore
microtubules
Metaphase
plate
Figure 9.7d Exploring mitosis in an animal cell (part 4: prometaphase and metaphase)
Kinetochore
Kinetochore
microtubule
Spindle
Centrosome at
one spindle pole 29

30. Telophase and Cytokinesis
Figure 9.7e
Anaphase
Telophase and
Cytokinesis
Cleavage
furrow
Nucleolus
forming
Figure 9.7e Exploring mitosis in an animal cell (part 5: anaphase, telophase and cytokinesis)
Nuclear
envelope
forming
Daughter
chromosomes 30

31. G2 of Interphase 10 m Figure 9.7f
Figure 9.7f Exploring mitosis in an animal cell (part 6: G2 of interphase micrograph)
G2 of Interphase 31

32. Figure 9.7g
10 m
Figure 9.7g Exploring mitosis in an animal cell (part 7: prophase micrograph)
Prophase 32

33. Prometaphase 10 m Figure 9.7h
Figure 9.7h Exploring mitosis in an animal cell (part 8: prometaphase micrograph)
Prometaphase 33

34. Figure 9.7i
10 m
Figure 9.7i Exploring mitosis in an animal cell (part 9: metaphase micrograph)
Metaphase 34

35. Figure 9.7j
10 m
Figure 9.7j Exploring mitosis in an animal cell (part 10: anaphase micrograph)
Anaphase 35

36. Telophase and Cytokinesis
Figure 9.7k
10 m
Figure 9.7k Exploring mitosis in an animal cell (part 11: telophase and cytokinesis micrograph)
Telophase and
Cytokinesis 36

37. The Mitotic Spindle: A Closer Look
The mitotic spindle is a structure made of microtubules and associated proteins
It controls chromosome movement during mitosis
In animal cells, assembly of spindle microtubules begins in the centrosome, the microtubule organizing center
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38. The centrosome replicates during interphase, forming two centrosomes that migrate to opposite ends of the cell during prophase and prometaphase
An aster (radial array of short microtubules) extends from each centrosome
The spindle includes the centrosomes, the spindle microtubules, and the asters
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39. During prometaphase, some spindle microtubules attach to the kinetochores of chromosomes and begin to move the chromosomes
Kinetochores are protein complexes that assemble on sections of DNA at centromeres
At metaphase, the centromeres of all the chromosomes are at the metaphase plate, an imaginary structure at the midway point between the spindle’s two poles
Video: Mitosis Spindle
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40. Aster Centrosome Sister chromatids Metaphase plate (imaginary) Kineto-
Figure 9.8
Aster
Centrosome
Sister
chromatids
Metaphase plate
(imaginary)
Kineto-
chores
Microtubules
Chromosomes
Overlapping
nonkinetochore
microtubules
Figure 9.8 The mitotic spindle at metaphase
Kinetochore
microtubules
1 m
0.5 m
Centrosome 40

41. Microtubules Chromosomes 1 m Centrosome Figure 9.8a
Figure 9.8a The mitotic spindle at metaphase (part 1: TEM)
1 m
Centrosome 41

42. Kinetochores Kinetochore microtubules 0.5 m Figure 9.8b
Figure 9.8b The mitotic spindle at metaphase (part 2: kinetochore TEM)
0.5 m 42

43. The microtubules shorten by depolymerizing at their kinetochore ends
In anaphase, sister chromatids separate and move along the kinetochore microtubules toward opposite ends of the cell
The microtubules shorten by depolymerizing at their kinetochore ends
Chromosomes are also “reeled in” by motor proteins at spindle poles, and microtubules depolymerize after they pass by the motor proteins
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44. Experiment Results Conclusion Kinetochore Spindle pole Chromosome
Figure 9.9
Experiment
Results
Kinetochore
Spindle
pole
Conclusion
Chromosome
movement
Mark
Kinetochore
Figure 9.9 Inquiry: At which end do kinetochore microtubules shorten during anaphase?
Motor
protein
Tubulin
subunits
Microtubule
Chromosome 44

45. Experiment Kinetochore Spindle pole Mark Figure 9.9a
Figure 9.9a Inquiry: At which end do kinetochore microtubules shorten during anaphase? (part 1: experiment) 45

46. Results Conclusion Chromosome movement Kinetochore Motor Tubulin
Figure 9.9b
Results
Conclusion
Chromosome
movement
Figure 9.9b Inquiry: At which end do kinetochore microtubules shorten during anaphase? (part 2: results and conclusion)
Kinetochore
Motor
protein
Tubulin
subunits
Microtubule
Chromosome 46

47. Nonkinetochore microtubules from opposite poles overlap and push against each other, elongating the cell
At the end of anaphase, duplicate groups of chromosomes have arrived at opposite ends of the elongated parent cell
Cytokinesis begins during anaphase or telophase and the spindle eventually disassembles
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48. Cytokinesis: A Closer Look
In animal cells, cytokinesis occurs by a process known as cleavage, forming a cleavage furrow
In plant cells, a cell plate forms during cytokinesis
Animation: Cytokinesis
Video: Cytokinesis and Myosin
© 2014 Pearson Education, Inc. 48

49. (a) Cleavage of an animal cell (SEM)
Figure 9.10
(a) Cleavage of an animal cell (SEM)
(b) Cell plate formation in a plant cell (TEM)
100 m
Cleavage furrow
Vesicles
forming
cell plate
Wall of parent
cell
1 m
Cell plate
New cell wall
Figure 9.10 Cytokinesis in animal and plant cells
Contractile ring of
microfilaments
Daughter cells
Daughter cells 49

50. (a) Cleavage of an animal cell (SEM)
Figure 9.10a
(a) Cleavage of an animal cell (SEM)
100 m
Cleavage furrow
Figure 9.10a Cytokinesis in animal and plant cells (part 1: cleavage of animal cell)
Contractile ring of
microfilaments
Daughter cells 50

51. Cleavage furrow 100 m Figure 9.10aa
Figure 9.10aa Cytokinesis in animal and plant cells (part 1a: cleavage of animal cell, SEM)
Cleavage furrow
100 m 51

52. (b) Cell plate formation in a plant cell (TEM)
Figure 9.10b
(b) Cell plate formation in a plant cell (TEM)
Vesicles
forming
cell plate
Wall of parent
cell
1 m
Cell plate
New cell wall
Figure 9.10b Cytokinesis in animal and plant cells (part 2: cell plate formation in plant cell)
Daughter cells 52

53. Vesicles Wall of parent 1 m forming cell cell plate Figure 9.10ba
Figure 9.10ba Cytokinesis in animal and plant cells (part 2a: cell plate formation in plant cell, TEM)
Vesicles
forming
cell plate
Wall of parent
cell
1 m 53

54. Chromosomes condensing Nucleus Nucleolus Chromosomes 10 m Prophase
Figure 9.11
Chromosomes
condensing
Nucleus
Nucleolus
Chromosomes
10 m 1
Prophase 2
Prometaphase
Cell plate
Figure 9.11 Mitosis in a plant cell 3
Metaphase 4
Anaphase 5
Telophase 54

55. Nucleus Chromosomes condensing Nucleolus 10 m Prophase 1 Figure 9.11a
Figure 9.11a Mitosis in a plant cell (part 1: prophase)
10 m 1
Prophase 55

56. Chromosomes 10 m Prometaphase 2 Figure 9.11b
Figure 9.11b Mitosis in a plant cell (part 2: prometaphase)
10 m 2
Prometaphase 56

57. Figure 9.11c
Figure 9.11c Mitosis in a plant cell (part 3: metaphase)
10 m 3
Metaphase 57

58. Figure 9.11d
Figure 9.11d Mitosis in a plant cell (part 4: anaphase)
10 m 4
Anaphase 58

59. Cell plate 10 m Telophase 5 Figure 9.11e
Figure 9.11e Mitosis in a plant cell (part 5: telophase)
10 m 5
Telophase 59

60. Binary Fission in Bacteria
Prokaryotes (bacteria and archaea) reproduce by a type of cell division called binary fission
In E. coli, the single chromosome replicates, beginning at the origin of replication
The two daughter chromosomes actively move apart while the cell elongates
The plasma membrane pinches inward, dividing the cell into two
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61. Origin of Cell wall replication Plasma membrane E. coli cell Bacterial
Figure
Origin of
replication
Cell wall
Plasma
membrane
E. coli cell
Bacterial
chromosome 1
Chromosome
replication
begins.
Two copies
of origin
Figure Bacterial cell division by binary fission (step 1) 61

62. Origin of replication Cell wall Plasma membrane E. coli cell Bacterial
Figure
Origin of
replication
Cell wall
Plasma
membrane
E. coli cell
Bacterial
chromosome 1
Chromosome
replication
begins.
Two copies
of origin 2
One copy of the
origin is now at
each end of the
cell.
Origin
Origin
Figure Bacterial cell division by binary fission (step 2) 62

63. Origin of replication Cell wall Plasma membrane E. coli cell Bacterial
Figure
Origin of
replication
Cell wall
Plasma
membrane
E. coli cell
Bacterial
chromosome 1
Chromosome
replication
begins.
Two copies
of origin 2
One copy of the
origin is now at
each end of the
cell.
Origin
Origin 3
Replication
finishes.
Figure Bacterial cell division by binary fission (step 3) 63

64. Origin of replication Cell wall Plasma membrane E. coli cell Bacterial
Figure
Origin of
replication
Cell wall
Plasma
membrane
E. coli cell
Bacterial
chromosome 1
Chromosome
replication
begins.
Two copies
of origin 2
One copy of the
origin is now at
each end of the
cell.
Origin
Origin 3
Replication
finishes.
Figure Bacterial cell division by binary fission (step 4) 4
Two daughter
cells result. 64

65. The Evolution of Mitosis
Since prokaryotes evolved before eukaryotes, mitosis probably evolved from binary fission
Certain protists (dinoflagellates, diatoms, and some yeasts) exhibit types of cell division that seem intermediate between binary fission and mitosis
© 2014 Pearson Education, Inc. 65

66. (b) Diatoms and some yeasts
Figure 9.13
Chromosomes
Microtubules
Intact nuclear
envelope
(a) Dinoflagellates
Kinetochore
microtubule
Figure 9.13 Mechanisms of cell division
Intact nuclear
envelope
(b) Diatoms and some yeasts 66

67. Concept 9.3: The eukaryotic cell cycle is regulated by a molecular control system
The frequency of cell division varies with the type of cell
These differences result from regulation at the molecular level
Cancer cells manage to escape the usual controls on the cell cycle
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68. Evidence for Cytoplasmic Signals
The cell cycle is driven by specific signaling molecules present in the cytoplasm
Some evidence for this hypothesis comes from experiments with cultured mammalian cells
Cells at different phases of the cell cycle were fused to form a single cell with two nuclei at different stages
Cytoplasmic signals from one of the cells could cause the nucleus from the second cell to enter the “wrong” stage of the cell cycle
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69. Conclusion Molecules present in the cytoplasm
Figure 9.14
Experiment
Experiment 1
Experiment 2 S G1 M G1
Results S S M M
Figure 9.14 Inquiry: Do molecular signals in the cytoplasm regulate the cell cycle?
G1 nucleus
immediately entered
S phase and DNA
was synthesized.
G1 nucleus began
mitosis without
chromosome
duplication.
Conclusion Molecules present in the cytoplasm
control the progression to S and M phases. 69

70. Checkpoints of the Cell Cycle Control System
The sequential events of the cell cycle are directed by a distinct cell cycle control system, which is similar to a timing device of a washing machine
The cell cycle control system is regulated by both internal and external controls
The clock has specific checkpoints where the cell cycle stops until a go-ahead signal is received
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71. G1 checkpoint Control system S G1 G2 M M checkpoint G2 checkpoint
Figure 9.15
G1 checkpoint
Control
system S G1 G2 M
Figure 9.15 Mechanical analogy for the cell cycle control system
M checkpoint
G2 checkpoint 71

72. For many cells, the G1 checkpoint seems to be the most important
If a cell receives a go-ahead signal at the G1 checkpoint, it will usually complete the S, G2, and M phases and divide
If the cell does not receive the go-ahead signal, it will exit the cycle, switching into a nondividing state called the G0 phase
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73. Without go-ahead signal, cell enters G0. With go-ahead signal,
Figure 9.16
G1 checkpoint G0 G1 G1
Without go-ahead signal,
cell enters G0.
With go-ahead signal,
cell continues cell cycle. G1 S
(a) G1 checkpoint M G2 G1 G1 M G2 M G2
Figure 9.16 Two important checkpoints
M checkpoint G2
checkpoint
Anaphase
Prometaphase
Metaphase
Without full chromosome
attachment, stop signal is
received.
With full chromosome
attachment, go-ahead signal
is received.
(b) M checkpoint 73

74. Without go-ahead signal, cell enters G0. With go-ahead signal,
Figure 9.16a
G1 checkpoint G0 G1 G1
Without go-ahead signal,
cell enters G0.
With go-ahead signal,
cell continues cell cycle.
Figure 9.16a Two important checkpoints (part 1: G1 checkpoint)
(a) G1 checkpoint 74

75. Without full chromosome attachment, stop signal is received.
Figure 9.16b G1 G1 M G2 M G2
M checkpoint G2
checkpoint
Anaphase
Prometaphase
Metaphase
Without full chromosome
attachment, stop signal is
received.
Figure 9.16b Two important checkpoints (part 2: M checkpoint)
With full chromosome
attachment, go-ahead signal
is received.
(b) M checkpoint 75

76. The cell cycle is regulated by a set of regulatory proteins and protein complexes including kinases and proteins called cyclins
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77. An example of an internal signal occurs at the M phase checkpoint
In this case, anaphase does not begin if any kinetochores remain unattached to spindle microtubules
Attachment of all of the kinetochores activates a regulatory complex, which then activates the enzyme separase
Separase allows sister chromatids to separate, triggering the onset of anaphase
© 2014 Pearson Education, Inc. 77

78. 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
© 2014 Pearson Education, Inc. 78

79. Scalpels A sample of human connective tissue is cut up into small
Figure
Scalpels 1
A sample of
human connective
tissue is cut
up into small
pieces.
Petri
dish
Figure The effect of platelet-derived growth factor (PDGF) on cell division (step 1) 79

80. Scalpels A sample of human connective tissue is cut up into small
Figure
Scalpels 1
A sample of
human connective
tissue is cut
up into small
pieces.
Petri
dish 2
Enzymes digest
the extracellular
matrix, resulting
in a suspension of
free fibroblasts.
Figure The effect of platelet-derived growth factor (PDGF) on cell division (step 2) 80

81. Scalpels A sample of human connective tissue is cut up into small
Figure
Scalpels 1
A sample of
human connective
tissue is cut
up into small
pieces.
Petri
dish 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.
Figure The effect of platelet-derived growth factor (PDGF) on cell division (step 3) 81

82. Scalpels A sample of human connective tissue is cut up into small
Figure
Scalpels 1
A sample of
human connective
tissue is cut
up into small
pieces.
Petri
dish 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.
Figure The effect of platelet-derived growth factor (PDGF) on cell division (step 4)
Cultured fibroblasts
(SEM)
Without PDGF
With PDGF
10 m 82

83. Cultured fibroblasts (SEM) 10 m Figure 9.17a
Figure 9.17a The effect of platelet-derived growth factor (PDGF) on cell division (SEM)
10 m 83

84. 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 exhibit neither density-dependent inhibition nor anchorage dependence
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85. Anchorage dependence: cells require a surface for division
Figure 9.18
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
Figure 9.18 Density-dependent inhibition and anchorage dependence of cell division
20 m
20 m
(a) Normal mammalian cells
(b) Cancer cells 85

86. (a) Normal mammalian cells
Figure 9.18a
20 m
(a) Normal mammalian cells
Figure 9.18a Density-dependent inhibition and anchorage dependence of cell division (part 1: normal cells) 86

87. 20 m (b) Cancer cells Figure 9.18b
Figure 9.18b Density-dependent inhibition and anchorage dependence of cell division (part 2: cancer cells) 87

88. Loss of Cell Cycle Controls in Cancer Cells
Cancer cells do not respond to signals that normally regulate the cell cycle
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
© 2014 Pearson Education, Inc. 88

89. A normal cell is converted to a cancerous cell by a process called transformation
Cancer cells that are not eliminated by the immune system form tumors, masses of abnormal cells within otherwise normal tissue
If abnormal cells remain only 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 additional tumors
© 2014 Pearson Education, Inc. 89

90. 5 m Breast cancer cell (colorized SEM) Metastatic tumor Lymph vessel
Figure 9.19
5 m
Breast cancer cell
(colorized SEM)
Metastatic
tumor
Lymph
vessel
Tumor
Blood
vessel
Figure 9.19 The growth and metastasis of a malignant breast tumor
Glandular
tissue
Cancer
cell 1
A tumor grows
from a single
cancer cell. 2
Cancer cells
invade
neighboring
tissue. 3
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. 90

91. Tumor Glandular tissue A tumor grows from a single cancer cell.
Figure 9.19a
Tumor
Glandular
tissue 1
A tumor grows
from a single
cancer cell. 2
Cancer cells
invade
neighboring
tissue. 3
Cancer cells spread
through lymph and
blood vessels to
other parts of the
body.
Figure 9.19a The growth and metastasis of a malignant breast tumor (part 1) 91

92. Metastatic tumor Lymph vessel Blood vessel Cancer cell
Figure 9.19b
Metastatic
tumor
Lymph
vessel
Blood
vessel
Cancer
cell
Figure 9.19b The growth and metastasis of a malignant breast tumor (part 2) 3
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. 92

93. 5 m Breast cancer cell (colorized SEM) Figure 9.19c
Figure 9.19c The growth and metastasis of a malignant breast tumor (SEM) 93

94. One of the big lessons in cancer research is how complex cancer is
Recent advances in understanding the cell cycle and cell cycle signaling have led to advances in cancer treatment
Medical treatments for cancer are becoming more “personalized” to an individual patient’s tumor
One of the big lessons in cancer research is how complex cancer is
© 2014 Pearson Education, Inc. 94

95. Amount of fluorescence per cell (fluorescence units)
Figure 9.UN01
Control
Treated
200
A B C
A B C
160
120
Number of cells 80 40
Figure 9.UN01 Skills exercise: interpreting histograms
200
400
600
200
400
600
Amount of fluorescence per cell (fluorescence units) 95

96. Telophase and Cytokinesis
Figure 9.UN02 G1 S
Cytokinesis
Mitosis G2
MITOTIC (M) PHASE
Prophase
Figure 9.UN02 Summary of key concepts: mitotic phase and interphase
Telophase and
Cytokinesis
Prometaphase
Anaphase
Metaphase 96

97. Figure 9.UN03
Figure 9.UN03 Test your understanding, question 6 97