Moss - Control of Cell Numbers and Cell Size

Question 1

what is apoptosis?

Answer 1

programmed “cell death”

Question 2

what are the morphological characteristics of apoptotic cell death:

Answer 2

• cells shrink, condense, and round-up
• nuclear envelope disassembles
• chromatin condenses and breaks into fragments
• cytoskeleton collapses
• plasma membrane blebs and bulges, but remains intact
• cell corpse may break into fragments
• surface of corpse changes to be recognized by neighboring cells for phagocytosis
• they are engulfed by neighboring cells before the contents spill out
• apoptotic cell vanishes without a trace

Question 3

TRUE or FALSE: the plasma membrane remains intact when it blebs and bulges during apoptotic cell death

Answer 3

TRUE

Question 4

what are apoptotic bodies?

Answer 4

the fragments that a cell corpse may break into during apoptotic cell death

Question 5

why does the surface of the cell corpse change to be recognized for neighboring cells?

Answer 5

for phagocytosis

Question 6

what is the following cell?

Answer 6

a normal white blood cell has microvilli, which are membrane covered microfilaments, extensions of the cytoskeleton

Question 7

what is the following cell?

Answer 7

an apoptotic white blood cell with blebs

Question 8

what are blebs?

Answer 8

regions of the membrane that are detached from the cytoskeleton

seen during apoptosis

Question 9

what do the arrows in the following picture indicate?

Answer 9

apoptotic cells that are shrunken with condensed cytoplasm. The nuclei are condensed and fragmented. Note the lack of inflammation

micrograph of mouse pancreas

Question 10

what is the difference between an apoptotic cell and a necrotic cell?

Answer 10

apoptosis

• an active ATP-dependent process
• mutations prevent
• completely enclosed

necrosis

• mainly passive
• no mutation can prevent
• leaks
• inflammation

Question 11

what is the intrinsic pathway?

Answer 11

cell decides to self-kill; death stimulus; radiation, hypoxia, etc.

Question 12

what is the extrinsic pathway?

Answer 12

a cell (killing cell), decides to initiate the death cycle in another cell (dying cell)

Question 13

what is common to both the intrinsic and extrinsic pathways?

Answer 13

caspase cascade

Question 14

what is the caspase cascade?

Answer 14

the initiator caspase (caspase-8, made of dimers) is inactive and must be cleaved

once cleaved the pro-caspase is active

a second initiator caspase (caspase-9) can be cleaved

both pro-caspases interact with the executioner caspase (caspase-3) and are cleaved of nuclear components, cytoskeletal components etc.

this final cleavage causes morphological changes in the nucleus and plasma membrane

the cell is engulfed and phagocytosed by another cell

Question 15

what is the amplification step of the caspase cascade?

Answer 15

interaction of the two pro-caspases with the executioner caspase

Question 16

what is a caspase made of? How is it assembled/activated?

Answer 16

two inactive procaspase molecules are cleaved of their pro-domains and assembled into one active caspase molecule

Question 17

what are caspases?

Answer 17

they are proteinases that have a cysteine at their active site and cleave their target proteins at specific aspartic acid residues

Question 18

what does proteolytic cleavage do to procaspases?

Answer 18

proteolytic cleavage of a pro-caspase rearranges the protein to form the active site

Question 19

what activates initiator and executioner caspases?

Answer 19

proteolytic cleavage

Question 20

when are initiator caspases active?

Answer 20

when they dimerize

Question 21

when are executioner caspases activated?

Answer 21

when they are cleaved by their initiator caspases

Question 22

what kind of proteolytic cleavage leads to apoptosis?

Answer 22

one involving initiator and executioner caspases

Question 23

what leads to the amplification of the initial apoptotic signal?

Answer 23

one initiator caspase activating many executioner caspases

Question 24

TRUE or FALSE: One initiator caspase can activate many executioner caspases, leading to the amplification of the initial apoptotic signal

Answer 24

TRUE

Question 25

what are BH3-only proteins? what do they do?

Answer 25

they are pro-apoptotic proteins

they act as sensors of a variety of apoptotic signals

they inhibit the anti-apoptotic Bcl2 proteins, allowing the pro-apoptotic effector proteins to cluster, which causes the release of cytochrome c

some may bind the effector proteins directly to stimulate aggregation

Question 26

what do pro-apoptotic BH3-only proteins inhibit? what does this allow?

Answer 26

They inhibit the anti-apoptotic Bcl2 proteins, allowing the pro-apoptotic effector proteins to cluster, which causes the release of cytochrome c

Question 27

what are anti-apoptotic Bcl2 family proteins?

Answer 27

they bind to and block the activation (by preventing oligomerization) of the pro-apoptotic Bcl2 family proteins (Bax and Bak)

they act to prevent pores that release cytochrome c from forming

Question 28

where are active anti-apoptotic Bcl2 Family proteins (Bcl2 and BclX_L) found?

Answer 28

they are located on the cytosolic surface of the outer mitochondrial membrane

Question 29

how do active anti-apoptotic Bcl2 Family proteins (Bcl2 and BclX_L) bind and block activation of Bax and Bak?

Answer 29

they prevent oligomerization

Question 30

what does every cell need to survive?

Answer 30

at least one active anti-apoptotic Bcl2 protein

Question 31

how do the Bcl2 family proteins regulate apoptosis?

Answer 31

by controlling mitochondrial membrane permeability and the release of cytochrome c and other intermembrane proteins into the cytosol

Question 32

what do active pro-apoptotic effector Bcl2 proteins (Bax and Bak) do?

Answer 32

they aggregate on the outer mitochondrial membrane and cause intermembrane proteins to be released

Question 33

what happens to a cell without effector Bcl2 proteins?

Answer 33

it cannot respond to an intrinsic apoptotic signal

Question 34

what does the intrinsic pathway of apoptosis involve?

Answer 34

mitochondria, specifically the release of cytochrome c from the intermembrane space into the cytosol

Question 35

how does the intrinsic pathway lead to the release of mitochondrial proteins into the cytosol?

Answer 35

diverse apoptotic stimuli, that are not death receptor-mediated, initiate signaling that activate the Bcl2-family proteins Bax and Bak.

cells change their inner mitochondrial membrane, and opening a pore, loss of the mitochondrial transmembrane potential, and release of the mitochondrial proteins into the cytosol

Question 36

how can apoptotic cells that have released cytochrome c be differentiated from nonapoptotic cells?

Answer 36

by fluorescence microscopy

stain antibody to cytochrome c

stain the antibody to the mitochondrial ATP-synthase

merge

you can see whether the cell contains the cytochrome c or not

Question 37

what happens once cytochrome c leaves the cell?

Answer 37

cytosolic cytochrome c binds an adaptor protein (Apaf1), which heptamerizes into an apoptosome

binding of cytochrome c causes the adaptor protein to unfold partly

unfolding of adaptor protein exposes a domain that interacts with the same domain in other activated protein molecules

Question 38

what happens when cytochrome c binds to the adaptor protein?

Answer 38

the adaptor protein partly unfolds, exposing a domain that interacts with the same domain in other activated adaptor proteins

Question 39

what happens after cytochrome c binds the adaptor proteins and it unfolds?

Answer 39

the adaptor protein binds pro-caspase-9, an initiator caspase, and forms a hexamer

Question 40

what happens after the adaptor protein binds pro-caspase-9?

Answer 40

the multimerization of pro-caspase 9 leads to its proteolytic cleavage and activation

this allows it to cleave executioner caspases

Question 41

what is Fas?

Answer 41

the death receptor on a dying cell

Question 42

what is the Fas ligand?

Answer 42

the killing cell

Question 43

what is the process of the extrinsic pathway?

Answer 43

Trimeric Fas ligand binds trimeric Fas

death domains on the cytosolic tails of Fas bind to the intracellular death domain adaptor protein (FADD)

FADD binds initiator caspases (primarily caspase-8), forming the death-inducing complex (DISC)

DISC allows dimerization and activation of initiator caspases

initiator caspases cleave their partners

caspases are released to activate executioner caspases

apoptosis is induced

Question 44

what is FADD? what does it do?

Answer 44

it is an intracellular death domain adaptor that binds to the initiator caspases to form the death-inducing complex after the tails of Fas bind it

Question 45

what does the DISC do?

Answer 45

it allows dimerization and activation of initiator caspases, which cleave their partners, are released to activate executioner caspases, and induce apoptosis

Question 46

what are death receptors (in general)?

Answer 46

they are transmembrane proteins with an extracellular ligand-binding domain, a single transmembrane domain and an intracellular death domain

they belong to the tumor necrosis factor receptor (TNFR) family

their ligands belong to the TNF family of signaling proteins

Question 47

both the death ligand and the death receptor are…..

Answer 47

trimeric

Question 48

what happens when the death ligand binds the death receptor?

Answer 48

binding of the ligand alters the conformation of the receptor so that it binds a death domain adaptor protein (FADD), which then recruits and activates an initiator caspase to trigger the caspase cascade and cell death

Question 49

what is ALPS (autoimmune lymphoproliferative syndrome)?

Answer 49

it is a disease associated with dominant mutations in the death receptor Fas that include point mutations and C-terminal truncations

in individuals that are heterozygous for these mutations, lymphocytes do not die at their normal rate and accumulate

Question 50

what do the intrinsic and extrinsic pathway have in common?

Answer 50

they are different up until the caspase cascade.

Question 51

what diseases have either too much or too little apoptosis as a major factor?

Answer 51

heart attacks and strokes

autoimmune disease

neurodegenerative diseases

cancer

Question 52

how is apoptosis a factor in heart attacks and strokes?

Answer 52

many cells die by necrosis due to ischemia (lack of blood supply), but some also die by apoptosis

Question 53

how is apoptosis a factor in autoimmune diseases?

Answer 53

caused by mutations in Fas death receptor or Fas ligand, which leads to overproduction of lymphocytes and a breakdown of self-tolerance

Question 54

how is apoptosis a factor in neurodegenerative diseases?

Answer 54

Alzheimer’s, Parkinson’s, Huntington’s diseases, and ALS

cells die due to oxidative stress, perturbed calcium homeostasis, mitochondrial dysfunction

Question 55

how is apoptosis a factor in cancer?

Answer 55

mutations in Bcl2 lead to B-cell lymphoma; p53 is mutated or inhibited in more than half of cancers, thus blocking the signal from DNA damage to the apoptotic pathway

Question 56

what is ABT-737?

Answer 56

a drug that binds anti-apoptotic Bcl2 family proteins, like BclX_L, preventing them from blocking apoptosis

The drug binds within a long hydrophobic pocket of BclX_L which is where the prop-apoptotic BH3-only proteins bind

Question 57

what do survival factors do?

Answer 57

block apoptosis

Question 58

what do mitogens do?

Answer 58

promote cell entry into S phase typically by overcoming intrinsic inhibition of cell cycle

Question 59

what do growth factors do?

Answer 59

stimulate growth in cell size and mass by promoting biosynthesis and inhibiting degradation

Question 60

how do cells prevent their apoptosis?

Answer 60

Cells may compete for limited amounts of survival factors produced by other cells to prevent apoptosis

Question 61

why do cells compete for survival factors to prevent apoptosis?

Answer 61

to control tissue development and maintenance

Question 62

what happens when there is a normal overproduction of nerve cells?

Answer 62

nerves must compete for a limited supply of survival factors that are secreted by the target cells that they connect to

Question 63

what happens to cells if they don’t receive survival factors?

Answer 63

they die

the nerve cells that die must have an active default death pathway that must be inhibited by the survival signal for them to survive

Question 64

how do survival factors stop apoptosis?

Answer 64

they inhibit the default death pathway

Question 65

what can extracellular survival factors do to Bcl2?

Answer 65

they may stimulate transcription of anti-apoptotic Bcl2 proteins

Question 66

what is the difference between a mitogen and a growth factor?

Answer 66

mitogens control cell division

growth factors control cell growth

their pathways are the same

Question 67

what are myoblasts/satellite cells in adult muscle?

Answer 67

muscle stem cells

Question 68

why are satellite cells in muscle activated when you are at the gym?

Answer 68

to add new muscle fibers to the muscle as it is damaged during exercise

Question 69

what is myostatin?

Answer 69

a TGF Beta family member

an extracellular signaling molecule that does the opposite of mitogen

it prevents the cell from dividing and becoming muscle (prevents over proliferation)

Question 70

why do muscle fibers secrete myostatin?

Answer 70

to inhibit proliferation and differentiation of myoblasts

Question 71

what occurs in mice lacking myostatin?

Answer 71

they have muscles 2-3 x normal size

Question 72

what occurs in “double muscled” cattle?

Answer 72

they have mutations in the myostatin gene

Question 73

what is the executioner caspase?

Answer 73

caspase 3

Question 74

what are the initiator caspases?

Answer 74

caspase - 8 (extrinsic)

caspase - 9 (intrinsic)