1. Chapter 11- Cell Communication

2. Evolution of Cell Signaling
A signal transduction pathway is a series of steps by which a signal on a cell’s surface is converted into a specific cellular response
Signal transduction pathways convert signals on a cell’s surface into cellular responses
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3. The Three Stages of Cell Signaling: A Preview
Earl W. Sutherland discovered how the hormone epinephrine acts on cells
Sutherland suggested that cells receiving signals went through three processes:
Reception
Transduction
Response
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4. Plasma membrane 1 Reception Receptor Signaling molecule 1
Fig
EXTRACELLULAR
FLUID
CYTOPLASM
Plasma membrane 1 1
Reception
Receptor
Figure 11.6 Overview of cell signaling
Signaling
molecule

5. Plasma membrane 1 Reception Transduction Receptor Signaling molecule 1
Fig
EXTRACELLULAR
FLUID
CYTOPLASM
Plasma membrane 1 1
Reception 2
Transduction
Receptor
Relay molecules in a signal transduction pathway
Figure 11.6 Overview of cell signaling
Signaling
molecule

6. Plasma membrane 1 Reception Transduction Response Receptor Activation
Fig
EXTRACELLULAR
FLUID
CYTOPLASM
Plasma membrane 1
Reception 2
Transduction 3
Response
Receptor
Activation
of cellular
response
Relay molecules in a signal transduction pathway
Figure 11.6 Overview of cell signaling
Signaling
molecule

7. Most signal receptors are plasma membrane proteins
Concept 11.2: Reception: A signal molecule binds to a receptor protein, causing it to change shape
The binding between a signal molecule (ligand) and receptor is highly specific
A shape change in a receptor is often the initial transduction of the signal
Most signal receptors are plasma membrane proteins
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8. Receptors in the Plasma Membrane
Most water-soluble signal molecules bind to specific sites on receptor proteins in the plasma membrane
There are three main types of membrane receptors:
G protein-coupled receptors
Receptor tyrosine kinases
Ion channel receptors
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9. A G protein-coupled receptor is a plasma membrane receptor that works with the help of a G protein
The G protein acts as an on/off switch: If GDP is bound to the G protein, the G protein is inactive
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10. Signaling-molecule binding site
Fig. 11-7a
Signaling-molecule binding site
Figure 11.7 Membrane receptors—G protein-coupled receptors, part 1
Segment that
interacts with
G proteins
G protein-coupled receptor

11. Figure 11.7 Membrane receptors—G protein-coupled receptors, part 2
Fig. 11-7b
Plasma
membrane
G protein-coupled
receptor
Inactive
enzyme
Activated
receptor
Signaling molecule
GDP
G protein
(inactive)
Enzyme
GDP
GTP
CYTOPLASM 1 2
Activated
enzyme
Figure 11.7 Membrane receptors—G protein-coupled receptors, part 2
GTP
GDP P i
Cellular response 3 4

12. Receptor tyrosine kinases are membrane receptors that attach phosphates to tyrosines
A receptor tyrosine kinase can trigger multiple signal transduction pathways at once
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13. Fully activated receptor tyrosine kinase
Fig. 11-7c
Signaling
molecule (ligand)
Ligand-binding site
Signaling
molecule
 Helix
Tyr
Tyr
Tyrosines
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Tyr
Receptor tyrosine
kinase proteins
Dimer
CYTOPLASM 1 2
Activated relay
proteins
Figure 11.7 Membrane receptors—receptor tyrosine kinases
Cellular
response 1
Tyr
Tyr P
Tyr
Tyr P
Tyr
Tyr P P
Tyr
Tyr P
Tyr
Tyr P
Tyr
Tyr P P
Cellular
response 2
Tyr
Tyr P
Tyr
Tyr P
Tyr P
Tyr P 6
ATP
6 ADP
Activated tyrosine
kinase regions
Fully activated receptor
tyrosine kinase
Inactive
relay proteins 3 4

14. A ligand-gated ion channel receptor acts as a gate when the receptor changes shape
When a signal molecule binds as a ligand to the receptor, the gate allows specific ions, such as Na+ or Ca2+, through a channel in the receptor
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15. 1 Signaling molecule (ligand) Gate closed Ions Plasma membrane
Fig. 11-7d 1
Signaling
molecule
(ligand)
Gate
closed
Ions
Plasma
membrane
Ligand-gated
ion channel receptor 2
Gate open
Cellular
response
Figure 11.7 Membrane receptors—ion channel receptors 3
Gate closed

16. Intracellular Receptors
Some receptor proteins are intracellular, found in the cytosol or nucleus of target cells
Small or hydrophobic chemical messengers can readily cross the membrane and activate receptors
Examples of hydrophobic messengers are the steroid and thyroid hormones of animals
An activated hormone-receptor complex can act as a transcription factor, turning on specific genes
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17. Hormone (testosterone) Plasma membrane Receptor protein DNA NUCLEUS
Fig
Hormone
(testosterone)
EXTRACELLULAR
FLUID
Plasma
membrane
Receptor
protein
DNA
Figure 11.8 Steroid hormone interacting with an intracellular receptor
NUCLEUS
CYTOPLASM

18. Hormone (testosterone) Plasma membrane Receptor protein Hormone-
Fig
Hormone
(testosterone)
EXTRACELLULAR
FLUID
Plasma
membrane
Receptor
protein
Hormone-
receptor
complex
DNA
Figure 11.8 Steroid hormone interacting with an intracellular receptor
NUCLEUS
CYTOPLASM

19. Hormone (testosterone) Plasma membrane Receptor protein Hormone-
Fig
Hormone
(testosterone)
EXTRACELLULAR
FLUID
Plasma
membrane
Receptor
protein
Hormone-
receptor
complex
DNA
Figure 11.8 Steroid hormone interacting with an intracellular receptor
NUCLEUS
CYTOPLASM

20. Hormone (testosterone) Plasma membrane Receptor protein Hormone-
Fig
Hormone
(testosterone)
EXTRACELLULAR
FLUID
Plasma
membrane
Receptor
protein
Hormone-
receptor
complex
DNA
Figure 11.8 Steroid hormone interacting with an intracellular receptor
mRNA
NUCLEUS
CYTOPLASM

21. Hormone (testosterone) Plasma membrane Receptor protein Hormone-
Fig
Hormone
(testosterone)
EXTRACELLULAR
FLUID
Plasma
membrane
Receptor
protein
Hormone-
receptor
complex
DNA
Figure 11.8 Steroid hormone interacting with an intracellular receptor
mRNA
NUCLEUS
New protein
CYTOPLASM

22. Signal transduction usually involves multiple steps
Concept 11.3: Transduction: Cascades of molecular interactions relay signals from receptors to target molecules in the cell
Signal transduction usually involves multiple steps
Multistep pathways can amplify a signal: A few molecules can produce a large cellular response
Multistep pathways provide more opportunities for coordination and regulation of the cellular response
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23. Signal Transduction Pathways
The molecules that relay a signal from receptor to response are mostly proteins
Like falling dominoes, the receptor activates another protein, which activates another, and so on, until the protein producing the response is activated
At each step, the signal is transduced into a different form, usually a shape change in a protein
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24. Protein Phosphorylation and Dephosphorylation
In many pathways, the signal is transmitted by a cascade of protein phosphorylations
Protein kinases transfer phosphates from ATP to protein, a process called phosphorylation
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25. Protein phosphatases remove the phosphates from proteins, a process called dephosphorylation
This phosphorylation and dephosphorylation system acts as a molecular switch, turning activities on and off
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26. Phosphorylation cascade
Fig. 11-9
Signaling molecule
Receptor
Activated relay
molecule
Inactive
protein kinase 1
Active
protein
kinase 1
Inactive
protein kinase 2
ATP
Phosphorylation cascade
ADP
Active
protein
kinase 2 P PP P i
Figure 11.9 A phosphorylation cascade
Inactive
protein kinase 3
ATP
ADP
Active
protein
kinase 3 P PP P i
Inactive
protein
ATP
ADP P
Active
protein
Cellular
response PP P i

27. Small Molecules and Ions as Second Messengers
The extracellular signal molecule that binds to the receptor is a pathway’s “first messenger”
Second messengers are small, nonprotein, water-soluble molecules or ions that spread throughout a cell by diffusion
Second messengers participate in pathways initiated by G protein-coupled receptors and receptor tyrosine kinases
Cyclic AMP and calcium ions are common second messengers
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28. Cyclic AMP (cAMP) is one of the most widely used second messengers
Adenylyl cyclase, an enzyme in the plasma membrane, converts ATP to cAMP in response to an extracellular signal
Copyright © 2008 Pearson Education, Inc., publishing as Pearson Benjamin Cummings

29. Fig. 11-10 Figure 11.10 Cyclic AMP Adenylyl cyclase Phosphodiesterase
Pyrophosphate P P i
ATP
cAMP
AMP
Figure Cyclic AMP

30. Many signal molecules trigger formation of cAMP
Other components of cAMP pathways are G proteins, G protein-coupled receptors, and protein kinases
cAMP usually activates protein kinase A, which phosphorylates various other proteins
Further regulation of cell metabolism is provided by G-protein systems that inhibit adenylyl cyclase
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31. First messenger Adenylyl cyclase G protein GTP G protein-coupled
Fig
First messenger
Adenylyl
cyclase
G protein
G protein-coupled
receptor
GTP
ATP
Second
messenger
cAMP
Figure cAMP as second messenger in a G-protein-signaling pathway
Protein
kinase A
Cellular responses

32. Calcium Ions and Inositol Triphosphate (IP3)
Calcium ions (Ca2+) act as a second messenger in many pathways
Calcium is an important second messenger because cells can regulate its concentration
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33. EXTRACELLULAR FLUID Plasma membrane Ca2+ pump ATP Mitochondrion
Fig
EXTRACELLULAR
FLUID
Plasma
membrane
Ca2+ pump
ATP
Mitochondrion
Nucleus
CYTOSOL
Ca2+
pump
Endoplasmic
reticulum (ER)
Figure The maintenance of calcium ion concentrations in an animal cell
Ca2+
pump
ATP
Key
High [Ca2+]
Low [Ca2+]

34. Animation: Signal Transduction Pathways
A signal relayed by a signal transduction pathway may trigger an increase in calcium in the cytosol
Pathways leading to the release of calcium involve inositol triphosphate (IP3) and diacylglycerol (DAG) as additional second messengers
Animation: Signal Transduction Pathways
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35. EXTRA- CELLULAR FLUID Signaling molecule (first messenger) G protein
Fig
EXTRA-
CELLULAR
FLUID
Signaling molecule
(first messenger)
G protein
DAG
GTP
G protein-coupled
receptor
PIP2
Phospholipase C
IP3
(second messenger)
IP3-gated
calcium channel
Figure Calcium and IP3 in signaling pathways
Endoplasmic
reticulum (ER)
Ca2+
CYTOSOL

36. EXTRA- CELLULAR FLUID Signaling molecule (first messenger) G protein
Fig
EXTRA-
CELLULAR
FLUID
Signaling molecule
(first messenger)
G protein
DAG
GTP
G protein-coupled
receptor
PIP2
Phospholipase C
IP3
(second messenger)
IP3-gated
calcium channel
Figure Calcium and IP3 in signaling pathways
Endoplasmic
reticulum (ER)
Ca2+
Ca2+
(second
messenger)
CYTOSOL

37. EXTRA- CELLULAR FLUID Signaling molecule (first messenger) G protein
Fig
EXTRA-
CELLULAR
FLUID
Signaling molecule
(first messenger)
G protein
DAG
GTP
G protein-coupled
receptor
PIP2
Phospholipase C
IP3
(second messenger)
IP3-gated
calcium channel
Figure Calcium and IP3 in signaling pathways
Endoplasmic
reticulum (ER)
Various
proteins
activated
Cellular
responses
Ca2+
Ca2+
(second
messenger)
CYTOSOL

38. Concept 11.4: Response: Cell signaling leads to regulation of transcription or cytoplasmic activities
The cell’s response to an extracellular signal is sometimes called the “output response”
Figure Nuclear responses to a signal: the activation of a specific gene by a growth factor
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39. Nuclear and Cytoplasmic Responses
Ultimately, a signal transduction pathway leads to regulation of one or more cellular activities
The response may occur in the cytoplasm or may involve action in the nucleus
Many signaling pathways regulate the synthesis of enzymes or other proteins, usually by turning genes on or off in the nucleus
The final activated molecule may function as a transcription factor
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40. Growth factor Reception Receptor Phosphorylation cascade Transduction
Fig
Growth factor
Reception
Receptor
Phosphorylation
cascade
Transduction
CYTOPLASM
Inactive
transcription
factor
Active
transcription
factor
Figure Nuclear responses to a signal: the activation of a specific gene by a growth factor
Response P
DNA
Gene
NUCLEUS
mRNA

41. Other pathways regulate the activity of enzymes
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42. Glucose-1-phosphate (108 molecules)
Fig
Reception
Binding of epinephrine to G protein-coupled receptor (1 molecule)
Transduction
Inactive G protein
Active G protein (102 molecules)
Inactive adenylyl cyclase
Active adenylyl cyclase (102)
ATP
Cyclic AMP (104)
Inactive protein kinase A
Active protein kinase A (104)
Figure Cytoplasmic response to a signal: the stimulation of glycogen breakdown by epinephrine
Inactive phosphorylase kinase
Active phosphorylase kinase (105)
Inactive glycogen phosphorylase
Active glycogen phosphorylase (106)
Response
Glycogen
Glucose-1-phosphate
(108 molecules)

43. Signaling pathways can also affect the physical characteristics of a cell, for example, cell shape
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44. RESULTS CONCLUSION Fig. 11-16
Wild-type (shmoos)
∆Fus3
∆formin
CONCLUSION
Mating
factor 1
Shmoo projection forming
G protein-coupled
receptor
Formin P
Fus3
Actin
subunit
Figure How do signals induce directional cell growth in yeast?
GTP P
GDP 2
Phosphory-
lation
cascade
Formin
Formin P 4
Microfilament
Fus3
Fus3 P 5 3

45. Wild-type (shmoos) ∆Fus3 ∆formin RESULTS Fig. 11-16a
Figure How do signals induce directional cell growth in yeast?
Wild-type (shmoos)
∆Fus3
∆formin

46. CONCLUSION Mating factor Shmoo projection forming G protein-coupled
Fig b
CONCLUSION
Mating
factor 1
Shmoo projection
forming
G protein-coupled
receptor
Formin P
Fus3
Actin
subunit
GTP P
GDP 2
Phosphory-
lation
cascade
Formin
Formin P 4
Figure How do signals induce directional cell growth in yeast?
Microfilament
Fus3
Fus3 P 5 3

47. Fine-Tuning of the Response
Multistep pathways have two important benefits:
Amplifying the signal (and thus the response)
Contributing to the specificity of the response
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48. Enzyme cascades amplify the cell’s response
Signal Amplification
Enzyme cascades amplify the cell’s response
At each step, the number of activated products is much greater than in the preceding step
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49. The Specificity of Cell Signaling and Coordination of the Response
Different kinds of cells have different collections of proteins
These different proteins allow cells to detect and respond to different signals
Even the same signal can have different effects in cells with different proteins and pathways
Pathway branching and “cross-talk” further help the cell coordinate incoming signals
Copyright © 2008 Pearson Education, Inc., publishing as Pearson Benjamin Cummings

50. Fig. 11-17 Figure 11.17 The specificity of cell signaling Signaling
molecule
Receptor
Relay
molecules
Response 1
Response 2
Response 3
Cell A. Pathway leads
to a single response.
Cell B. Pathway branches,
leading to two responses.
Figure The specificity of cell signaling
Activation
or inhibition
Response 4
Response 5
Cell C. Cross-talk occurs
between two pathways.
Cell D. Different receptor
leads to a different response.

51. Cell B. Pathway branches, leading to two responses.
Fig a
Signaling
molecule
Receptor
Relay
molecules
Figure The specificity of cell signaling
Response 1
Response 2
Response 3
Cell A. Pathway leads
to a single response.
Cell B. Pathway branches,
leading to two responses.

52. Cell C. Cross-talk occurs between two pathways.
Fig b
Activation
or inhibition
Figure The specificity of cell signaling
Response 4
Response 5
Cell C. Cross-talk occurs
between two pathways.
Cell D. Different receptor
leads to a different response.

53. Signaling Efficiency: Scaffolding Proteins and Signaling Complexes
Scaffolding proteins are large relay proteins to which other relay proteins are attached
Scaffolding proteins can increase the signal transduction efficiency by grouping together different proteins involved in the same pathway
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54. Signaling Plasma molecule membrane Receptor Three different protein
Fig
Signaling
molecule
Plasma
membrane
Receptor
Three
different
protein
kinases
Figure A scaffolding protein
Scaffolding
protein

55. Termination of the Signal
Inactivation mechanisms are an essential aspect of cell signaling
When signal molecules leave the receptor, the receptor reverts to its inactive state
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56. Apoptosis is programmed or controlled cell suicide
Concept 11.5: Apoptosis (programmed cell death) integrates multiple cell-signaling pathways
Apoptosis is programmed or controlled cell suicide
A cell is chopped and packaged into vesicles that are digested by scavenger cells
Apoptosis prevents enzymes from leaking out of a dying cell and damaging neighboring cells
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57. Fig
Figure Apoptosis of human white blood cells
2 µm

58. Apoptosis in the Soil Worm Caenorhabditis elegans
Apoptosis is important in shaping an organism during embryonic development
The role of apoptosis in embryonic development was first studied in Caenorhabditis elegans
In C. elegans, apoptosis results when specific proteins that “accelerate” apoptosis override those that “put the brakes” on apoptosis
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59. Figure 11.20 Molecular basis of apoptosis in C. elegans
Ced-9
protein (active)
inhibits Ced-4
activity
Mitochondrion
Ced-4
Ced-3
Receptor
for death-
signaling
molecule
Inactive proteins
(a) No death signal
Ced-9
(inactive)
Cell
forms
blebs
Death-
signaling
molecule
Figure Molecular basis of apoptosis in C. elegans
Active
Ced-4
Active
Ced-3
Other
proteases
Nucleases
Activation
cascade
(b) Death signal

60. Ced-9 protein (active) inhibits Ced-4 activity Mitochondrion Ced-4
Fig a
Ced-9
protein (active)
inhibits Ced-4
activity
Mitochondrion
Figure Molecular basis of apoptosis in C. elegans
Ced-4
Ced-3
Receptor
for death-
signaling
molecule
Inactive proteins
(a) No death signal

61. Ced-9 (inactive) Cell forms blebs Death- signaling molecule Active
Fig b
Ced-9
(inactive)
Cell
forms
blebs
Death-
signaling
molecule
Active
Ced-4
Active
Ced-3
Other
proteases
Nucleases
Figure Molecular basis of apoptosis in C. elegans
Activation
cascade
(b) Death signal

62. Apoptotic Pathways and the Signals That Trigger Them
Caspases are the main proteases (enzymes that cut up proteins) that carry out apoptosis
Apoptosis can be triggered by:
An extracellular death-signaling ligand
DNA damage in the nucleus
Protein misfolding in the endoplasmic reticulum
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63. Apoptosis evolved early in animal evolution and is essential for the development and maintenance of all animals
Apoptosis may be involved in some diseases (for example, Parkinson’s and Alzheimer’s); interference with apoptosis may contribute to some cancers
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64. Interdigital tissue 1 mm Fig. 11-21
Figure Effect of apoptosis during paw development in the mouse

65. Reception Transduction Response Receptor Activation of cellular
Fig. 11-UN1 1
Reception 2
Transduction 3
Response
Receptor
Activation
of cellular
response
Relay molecules
Signaling
molecule

66. Fig. 11-UN2

67. You should now be able to:
Describe the nature of a ligand-receptor interaction and state how such interactions initiate a signal-transduction system
Compare and contrast G protein-coupled receptors, tyrosine kinase receptors, and ligand-gated ion channels
List two advantages of a multistep pathway in the transduction stage of cell signaling
Explain how an original signal molecule can produce a cellular response when it may not even enter the target cell
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68. Define the term second messenger; briefly describe the role of these molecules in signaling pathways
Explain why different types of cells may respond differently to the same signal molecule
Describe the role of apoptosis in normal development and degenerative disease in vertebrates
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