Robbins - Ch. 2 - Cell Response to Stress and Insult

Question 1

what are the four aspects of a disease process that make up the core of pathology?

Answer 1

etiology (cause)

pathogenesis (mechanism/ development)

morphogenesis (structural alterations)

clinical manifestations

Question 2

what does adaptation mean?

Answer 2

that the functional and structural responses to change in physio state or pathologic stimuli are reversible

Question 3

what are the 4 adaptation responses?

Answer 3

1) hypertrophy
2) hyperplasia
3) atrophy
4) metaplasia

Question 4

what does hypertrophy refer to?

Answer 4

an increase in the size of cells that result in an increase in the size of the affected organ

Question 5

how do cells get bigger?

Answer 5

incr protein synthesis

Question 6

what is physiologic hypertrophy caused by?

Answer 6

incr in functional demand, or by stimulation by hormones or growth factors

Question 7

what is the most common stimulus for hypertrophy of muscle?

Answer 7

increased workload

Question 8

what is the stimulus for hypertrophy in the heart?

Answer 8

chronic hemodynamic overload

Question 9

what is a good example of massive physiologic growth due to hormone-induced enlargement?

Answer 9

the uterus during pregnancy

• uterine hypertrophy is stimulated by estrogenic hormones acting on smooth m. resulting in incr. synthesis of smooth m. proteins - increasing its size

Question 10

what is hypertrophy a result of?

Answer 10

increased production of cellular proteins!

Question 11

what are the 3 basic steps in molecular pathogenesis of cardiac hypertrophy?

Answer 11

1) the integrated actinos of mechanical sensors (which are triggered by Incr. workload), growth factors, and vasoactive agents.
2) two biochem pathways: PI3K/AKT pathway (physiologic), and signaling downstream of G-protein coupled receptors (pathologic)
3) these singnals activate tf’s: GATA4, NFAT, and MEF2

***THESE TFs INCR. SYNTHESIS OF PROTEINS = HYPERTROPHY***

Question 12

what is hyperplasia?

Answer 12

an incr in the number of cells in an organ or tissue in response to a stimulus

Question 13

where can hyperplasia not occur?

Answer 13

skeletal muscle

cardiac cells

neurons

Question 14

what is physiologic hyperplasia due to? when does it occur?

Answer 14

the action of hormones or growth factors

• when there is a need to increase functional capacity of the hormone sensitive organ; or when there is a need for compensatory increase after damage or resection

Question 15

whats an example of hormonal hyperplasia?

Answer 15

• the proliferation of the glandular epithelium of the female breast at puberty and during pregnancy, which is accompanied by enlargement of the glandular epithelial cells

Question 16

what is a good example of compensatory hyperplasia?

Answer 16

liver regeneration after hepatectomy

Question 17

what is the 3rd example of physiologic hyperplasia?

Answer 17

bone marrow: undergoes rapid hyperplasia in response to a deficiency of terminally differentiated blood cells; like in the event of acute bleeding or hemolysis

growth factor: erythropoeitin

Question 18

what is pathologic hyperplasia caused by?

Answer 18

excessive or inapproapriate actions of hormones or growth factors acting on target cells

Question 19

what are examples of a hormone-induced hyperplasia?

Answer 19

endometrial hyperplasia

benign prostatic hyperplasia

Question 20

what is important to note about pathologic hyperplasia?

Answer 20

although they are abnormal, the process remains controlled and the hyperplasia regresses If stimulus is removed

- while hyperplasia Is distinct from cancer, pathologic hyperplasia consittutes a fertile soil in which cancerous prolferations may eventually arise

Question 21

hyperplasia is a characteristic response to which viral infection?

Answer 21

papillomavirus; skin warts and several mucosal lesions composed of masses of hyperplastic epithelium

Question 22

what drive hyperplasia?

Answer 22

its a result of growth factor-driven proliferation of mature cells

(in some cases, theres an increased output of new cells from stem cells, too)

Question 23

what is atrophy?

Answer 23

a reduction in size of an organ or tissue due to a decrease in cell size and number

Question 24

what are physiologic atrophy examples?

Answer 24

embryonic: notochord, thyroglossal duct
- decrease in uterus size after birth

Question 25

what are the 6 common causes of pathologic atrophy?

Answer 25

1) decreased workload (atrophy of disuse)
2) loss of innervation (denervation atrophy)
3) diminished blood supply
4) inadequate nutrition
5) loss of endocrine stimulation
6) pressure

Question 26

what is the initial response in atrophy?

Answer 26

decrease in cell size and organelles, which reduces metabolic needs of the cell (sufficient enough to survive)

Question 27

what is the main mechanism of atrophy?

Answer 27

atrophy results from:

1) decreased protein synthesis

2) Increased protein degradation

in cells

Question 28

what is the mechanism of degradation of cell proteins?

Answer 28

mainly ubiquitin-proteasome pathway

nutrient deficiency and disuse may activate ubiquitin ligases, which tag and target proteins for degradation via proteasomes

Question 29

what may atrophy be accompanied by?

Answer 29

autophagy, marked by the appearance of increased numbers of autophagic vacuoles

autophagy is the process in which starved cells eat its own components in an attempt to reduce nutrient demand to match the supply

• some vacuoles resist digestion: residual bodies

eg; lipofuscin granules

Question 30

what is metaplasia?

Answer 30

the reversible change in which one differentiated cell type (epithelial or mesenchymal) is replaced by another cell type

Question 31

what is the most common epithelial metaplasia?

Answer 31

columnar to squamous; eg: respiratory tract in response to chronic irritation (smokers)

eg: stones in excretory ducts of salivary glands, pancrease, or bile ducts, may do this too

Question 32

why is the change to metaplastic squamous cells in the respiratory tract a double-edge sword?

Answer 32

• important protection against infection (musuc and ciliary action) are lost
• also, the influences that predispose to metaplasia, can initiate malignant transformation in metaplasitc epithelium (thus, common form of cancer in resp. tract is composed of squamous cell)

Question 33

what is Barrett esophagus an example of?

Answer 33

metaplasia from squamous to columnar type

Question 34

what is connective tissue metaplasia?

Answer 34

formation of cartilage, bone, or adipose tissue in tissues not normally containing these elements

eg: myositis ossificans: bone formation in muscle after intramuscular hemorrhage

Question 35

describe the mechanism of metaplasia

Answer 35

important to note that metaplasia does not result from a change in the phenotype of an already differentiated cell type;

its the result of a reprogramming of a stem cell, or of undifferentiated mesenchymal cells present in the connective tissue

Question 36

what is the differentiation of a stem cell to a particular lineage due to?

Answer 36

signals generated by cytokines, growth factors, and EXCmatrix components in the environment

Question 37

what are the 7 causes of cell injury?

Answer 37

1) oxygen deprivation
2) physical agents
3) chemical agents and drugs
4) infectious agents
5) immunologic reactions
6) genetic derangements
7) nutritional imbalances

Question 38

describe oxygen deprivation

Answer 38

• hypoxia is a deficiency of oxygen, which reduces aerobix oxidative respiration causing injury

= causes of hypoxia:

• ischemia
• hypoxemia
• decr. oxygen-carrying capacity (Hb related [CO-poinsoning] or blood loss)

Question 39

what do physical agents include?

Answer 39

mechanical trauma, temp change, sudden changes in atmospheric pressure, radiation, electric shock

Question 40

in regards to cell injury or death, what is there a time lag between?

Answer 40

the stress and the morphologic changes;

Question 41

when can you expect to see light microscopic changes of myocadium cell death?

Answer 41

4-12 hours

Question 42

what is reversible injury characterized by?

Answer 42

• swelling of cell and its organelles
• blebbing of plasma membr.
• detacchment of ribosomes from ER
• clumping of nuclear chromatin

*these morphologic changes are associated with decr generation of ATP, loss of cell membr. integrity, defects in protein synthesis, cytoskeletal damage, and DNA damage

Question 43

what two features of reversible cell injury can be recognized under a light microscope?

Answer 43

• cellular swelling
• fatty change

Question 44

what is hydropic change?

Answer 44

aka vacuolar degeneration

• small clear vacuoles are seen within the cytoplasm; these represent distended and pinched-off segments of the ER

Question 45

what are the morphologic changes of necrosis due to?

Answer 45

denaturation of intracellular proteins and enzymatic digestion of the lethally injured cell

Question 46

what do necrotic cells show, histologically?

Answer 46

• increased eosinophilia (H&E stain)
• glassy homogenous appearance
• dead cells may be replaced by large, whorled phospholipid masses called myelin figures (they come from damaged membranes)
• these phospholipid precipitates are either phagocytosed by other cells or further degraded to fatty acids; they can also generate calcium soaps, if Ca binds the fatty acids = calcification

Question 47

what are the nuclear changes that appear in one of 3 patterns, in necrosis?

Answer 47

1) karyolysis: basophilia of chromatin may fade
2) pyknosis: nuclear shrinkage and increased basophilia
3) karyorrhexis: the pyknotic nucleus undergoes fragmentation

Question 48

describe coagulative necrosis

Answer 48

form of necrosis in which the architecture of dead tissue is preserved for a span of at least some days

• exhibit a firm texture
• this happens cuz the injury not only denatures the structual proteins, but also the enzymes; so it blocks proteolysis of the dead cells
• eosinophilic, anucleate cells persist for days
• Ischemia caused by obstruction In a vessel may lead to coagulative necrosis of the supplied tissue in all organs except the brain

- a localized area of coagulative necrosis is called an infarct

Question 49

describe liquefactive necrosis

Answer 49

• digestion of dead cells transforms the tissue inot a liquid viscous mass
• seen in focal (localized) bacterial infection or fungal

eg: hypoxic death of cells within the central nervous system

Question 50

how does the necrosis liquify the tissue?

Answer 50

microbes stimulate the accumulation of leukocytes (neutrophils; pus) and the liberation of enzymes from these leukocytes

• the material is often creamy yellow + dead leukocytes = pus

Question 51

describe gangrenous necrosis

Answer 51

• often a limb, lower leg, that has lost its blood supply and has undergone necrosis involving multiple tissue planes.

Question 52

describe caseous necrosis

Answer 52

encountered most often in foci of tuberculous infection

• microscopic exam: structureless collection of fragmented or lysed cells and amorphous granular debris enclosed within a distinctive inflammatory border

*this appearance lets you know theres a granuloma! meaning a “focus of inflammation”*

Question 53

describe fat necrosis

Answer 53

• refers to focal areas of fat destruction

typical finding: pancreas (pancreatitis)

• results from release of activated pancreatic lipases Into the substance of the pancreas and the peritoneal cavity

Question 54

describe what happens in acute pancreatitis

Answer 54

enzymes leak out of acinar cells and liquefy the membranes of fat cells in the peritoneum.

• the released lipases split the triglyceride-esters contained within fat cells
• the fatty acids combine with calcium to produce fat saponification

Question 55

what can you expect in histologic examination of fat necrosis?

Answer 55

• foci of shadowy outlines of necrotic fat cells
• with basophilic calcium deposits

surrounded by an inflammatory reaction

Question 56

describe fibrinoid necrosis

Answer 56

• seen in immune reactions involving the blood vessels

= pattern occurs when complexes of antigens::antibodies are deposited in the walls of the arteries

• deposits of these complexes + fibrin that leaked out of vessels = bright pink and amorphous appearance in HnE stains called FIBRINOID

Question 57

how does dystrophic calcification happen?

Answer 57

when necrotic cells and cell debris is not destroyed and reabsorbed- they provide a nest for the deposition of calcium salts and other minerals

Question 58

what are key concepts of reversible cell injury

Answer 58

= cell swelling

fatty change

plasma membrane blebbing and loss of microvilli

mitochondrial swelling

dilation of ER

eosinophilia

Question 59

what are the key concepts of necrosis in regards to morphologic alterations?

Answer 59

incr. eosinophilia

nuclear shrinkage, fragmentation and dissolution

breakdown of plasma membr and organelles

abundant myelin figures

leakage and enzyme digestion of cell contents

Question 60

what does apoptosis serve to do?

Answer 60

eliminate cells that are no longer needed, and to maintain a steady number of various cell populations in tissues

Question 61

what are some examples of physiologic apoptosis?

Answer 61

1) destruction of cells during embryogenesis
2) involution of hormone-dependent tissues upon hormone withdrawal (eg: endometrial cell breakdown, ovarian follicular atresia, regression of lactating breast, prostatic atrophy after castration)
3) cell loss in proliferating cell populations (immature lymphocytes in bone m. and thymus, and B lymphs in germinal centers that fail to express useful antigen receptors; and epithelial cells in intestinal crypts)
4) elimination of potentially harmful self-reactive lymphocytes

Question 62

what are some examples of apoptosis in pathologic conditions?

Answer 62

• DNA damage
• accumulation of misfolded proteins
• cell death in certain infections
• pathologic atrophy in parenchymal organs after duct obstruction (such as the pancreas, parotid gland, and kidney)

Question 63

describe apoptosis in regards to accumulation of misfolded proteins

Answer 63

if there is excessive accum. of improperly folded proteins in the ER, it leads to ER Stress, which ends up in apoptosis

Question 64

whats an example of pathologic apoptosis in regards to cell death in certain infections

Answer 64

ie: when you get infected with a virus and the cells die out to contain the virus. can lead to a lot of tissue damage

Question 65

what are some morphologic features of apoptosis seen under the electron microscope?

Answer 65

• cell shrinkage
• chromatin is condensed; it aggregates peripherally
• formation of cytoplasmic blebs and apoptotic bodies
• phagocytosis of apoptotic cells or cell bodies, usually by macrophages
• does not elicit inflammatory response

Question 66

what does apoptosis result from, in regards to its mechanism?

Answer 66

the activation of caspases

• so called becasue they are cysteine proteases that cleave proteins after aspartic residue

Question 67

what is the major mechanism of apoptosis in all mammalian cells?

Answer 67

the mitochondrial pathway aka intrinsice pathway

Question 68

what does the intrinsice pathway result from?

Answer 68

• results from an incr permeability of the mitochondrial outer membrane
• cytochrome is released (resides in the intermembrane space)
• the release of this protein is tightly controlled by BCL2 proteins (a protein family)

Question 69

what are the anti-apoptotic proteins found on the outer mitochondrial membrane?

Answer 69

BCL2, BCL-XL, and MCL1

(they also reside in the cytosol and ER membranes)

• they keep the outer membrane impermeable and prevent leakage of cytochrome c

Question 70

what are the two pro-apoptotic proteins? what happens when they are activated?

Answer 70

BAX and BAK

• when activated, they oligomerize within the outer mito protein and promote membrane permeability, releasing cytochrome C

Question 71

what are the “sensors” of the intrinsic pathway?

Answer 71

BAD, BIM, BID, Puma and Noxa

theyre all BH3-only proteins

-they act as sensors of cellular stress and damage, and regulate the balance between apoptotic and anti-apoptotic proteins

Question 72

what happens when cytochrome c is released to the cytosol?

Answer 72

cyto-c binds to a protein called APAF-1 (apoptosis-activating factor-1)

• forms the apoptosome
• apoptosome binds caspase-9
• caspace-9 is the initiator of the mirochondrial pathway, and cleaves other adjacent C9’s - thus its autoamplifying

Question 73

what other proteins leave the mitochondria

Answer 73

Smac and Diable

• they enter cytoplasm, bind to and neutralize IAPs (inhibitors of apoptosis proteins)
• IAPs blocks the activation of capsases, esp caspase-3, which Is the executioner caspase.
• thus, they add on to the inititation of caspase cascade