Chapter 16

Question 1

A) What does symbiosis mean?

Answer 1

live together

Question 2

B) What is mutualism? Give an example.

Answer 2

both benefit from relationship. some produse vit k and b which the host needs. host provides safe environment for bacteria to grow

Question 3

C) What is commensalism? Give and example.

.

Answer 3

one is benefited but the other is unharmed: microbes on skin do not hurt it, but the skin provides food

Question 4

D) What is parasitism? Give an example

Answer 4

one damaged the other to benefit itself: all pathogens, protozoa, and hemilinths

Question 5

A) What are the normal microbiota in the body? [Figure 16.1]

Answer 5

ones normally found in the healthy body.

Question 6

1) What is the normal microbiota most significant contribution?

Answer 6

protection against pathogens.

• taking up nutrients
• covering binding sites
• producing toxins

Question 7

2) How does the normal microbiota stimulate adaptive immunity?

Answer 7

they can influence development of mucousa- lymphiod tissues. The andtibodies that are produced against normal flora can bind to pathogens. T cells can also recognize harmless microbiota and therefore keep system from overreacting.

Question 8

3) What is the hygiene hypothesis?

Answer 8

insuficient exposure to microbes can lead to allergies.

Question 9

A) What does the word colonization mean?

Answer 9

microbe establishing and then growing on a surface.

Question 10

B) When can you call a relationship an infection?

Answer 10

it is parasitic

Question 11

C) What is subclinical infection?

Answer 11

mild to no symptoms that are not noticed, but there is and infection

Question 12

D) What is an infectious disease?

Answer 12

results in disease

Question 13

E) What are symptoms as opposed to signs?

Answer 13

are subjective effects of disease by the patient.

signs= objective evidence ie rash etc.

Question 14

F) What is the difference between primary and secondary infection?

Answer 14

initial infection

secondary: a infection that arrises due to the primary

Question 15

H) What is a primary pathogen?

Answer 15

mircobe that causes disease in healthy individuals

Question 16

I) What is an opportunistic pathogen?

Answer 16

takes advantage of a immunocompromised individual.

Question 17

J) What does the work virulence mean?

Answer 17

degree of how pathogenic/ stronf an organism is.

Question 18

K) What are virulence factors?

Answer 18

traits of microo’s that specifically allow it to cause disease.

Question 19

L) What makes a disease communicable?

Answer 19

spread form one host ot another

Question 20

M) What is the infectious dose and how is it expressed?

Answer 20

the number of microbes neccessary to establish an infection

Question 21

N) What is the course of an infectious disease? [Figure 16.2]

Answer 21

includes several stages:

incubation period, illness conalescence, latency, reoccurence

Question 22

1) What are the different phases?

Answer 22

Incubation: time between ehn host was exposed and onset of illness

illness: person will expirience symptoms
- promodal phase of infection: first vague symptoms
convalesence: recovery from disease.

Question 23

O) What are the differences between a localized infection and a systemic infection?

Answer 23

limited to a small area

systemic: spreads through the whole body

Question 24

P) What does bacteremia mean?

Answer 24

bacteria is circulating in the blood stream

Question 25

Q)What does toxemia mean?

Answer 25

toxins are circulating in blood stream

Question 26

R) What does viremia mean?

Answer 26

viral particles are circulating in blood stream

Question 27

A) What are Koch’s postulates? [Figure 16.3]

Answer 27

criteria koch used to determine that Bacillus anthraxis causes anthrax. it provides a foundation for establishing a certain microbe causes a specific infectious disease

Question 28

2) When does Koch’s postulates not work?

Answer 28

• is organisms cannot be grown in a medium in a lab.
• some cases of polio and cholera do not expieirence symptoms
• some are poly microbial meaning that different micro’s together cause a disease
• some diseases do not infect animal, only humans

Question 29

B) What are Molecular Koch’s postulates?

Answer 29

similair to koch’s postulates, but rely on molecular techniques to study a microbes virulance factors

• virulant gene is found in pathogenic strains of org
• mutating virulance gene takes away virulance of pathogen
• reimplementing the virulance causes the disease/ restores virulance

Question 30

C) What are the four patterns that pathogenic mechanisms follow?

Answer 30

• micro o must be present in every case of disease
• org must be grown in pure culture from diseased host
• same disease must be produced when pure cultures is introduced to suseptible host
• organinsm must be recovered from infected host.

Question 31

D) What is balanced pathogenicity?

Answer 31

pathogens and host evolve. the pathogen becomes less virulent while the host becomes less suceptible.

Question 32

A) Where are adhesins located and how are they used? [Figure 16.4]

Answer 32

bacteria use them. usually located on tips of pili.

can also be on curface structures

Question 33

1) Where do the adhesins attach?

Answer 33

the receptor.

Question 34

2) How specific is adhesin-receptor binding?

Answer 34

highly specific

Question 35

B) How do microorganisms colonize a mucosal surface?

Answer 35

they must produce their own iron binding molecules so they can survive on it ( cause lactoferrin and transferrin use up all fe )

Question 36

1) What are siderophores used for?

Answer 36

produce, or bind to hosts fe molecules

Question 37

2) How do these microorganisms avoid secretory IgA?

Answer 37

they have rapid turn over pilli and IgA prtoease which cleases IgA antibodies

Question 38

C) How does the type III secretion system work and what does it do? [Figure 16.5]

Answer 38

these are when pathogens “gives a shot” of protiens into eukaryotic cells to induce changes in it. some cause it to engulf the bacteria

Question 39

A) Which bacteria rely on skin damaging injuries to penetrate.

Answer 39

staphylococcus aureus, and yersina pestis

Question 40

B) How do pathogens enter the mucous membrane?

Answer 40

2 ways

• direct uptake by cells
• exploiting antigen sampling processes

Question 41

1) What is membrane ruffling and when does it occur? [Figure 16.6]

Answer 41

this is when gram neg bacteria inject effector protiens into host. These protiens changes the cytosplams and causes the membrane to ruffle. These ruffles enclose bacteria and bring then into the cell.

Question 42

2) How can a pathogen exploit the antigen-sampling process? [Figure 16.7]

Answer 42

this is when bacteria take advantage of the MALT system which brings in the bacteria to the macrophages, but some can kill the macrophages before they destroy them

Question 43

A) How do pathogens hide in host cells? [Figure 16.8]

Answer 43

they stay within the cell and cause ti to make an actin tail which propels it around and rams into other cells to transfer bacteria

Question 44

B) What are serum resistant bacteria? How do they avoid be killed?

Answer 44

these are bacteria that avoid being killed by compliment systems. They hijack hosts cells mechanisms that they use to trigger compliment system.

Question 45

C) How do pathogens prevent encounters with phagocytes?

Answer 45

They so this by avoiding macrophages and neutrophils altogether.

Question 46

1) What is C5a peptidase?

Answer 46

This degrades compliment systen C5 ( a chemoatractant)

Question 47

2) How do membrane-damaging toxins do what they do?

Answer 47

kill phagocytes by forming pores in phagocytes membranes

Question 48

D) How do pathogens avoid being recognized by phagocytes?

Answer 48

they prevent osponins, or other antibodies from coating it and therefore avoiding recognition by phagocytes.

Question 49

1) What benefit are capsules to pathogens?

Answer 49

They bind the hosts regulatory protiens of C3b mechanism

Question 50

2) How does the m protein benefit Streptococcus pyogenes?

Answer 50

binds to C3b regulatory protiens in hosts cell

Question 51

3) What do Fc receptors do? [Figure 16.10]

Answer 51

bind in the Fc regions of antibodies interfering with their function as osponins (Fc= red flag of antibody)

Question 52

E) How do some pathogens survive within phagocytes?

Answer 52

• they escape from the phagosome before it joins with the lysosomes and then they multiply in the hosts cells cytoplasm
• Prevent fusion of phagosome to lysosome: so this by prod. protien that blocks the fusion
• Survive in the pagolysosome- able to withstand the conditions

Question 53

F) What mechanisms do pathogens have for avoiding antibodies?

Answer 53

• IgA protease- tgus cleaves to IgA ( antibody found in mucous)
• Antigenic Variation: routinely alter the structure of surface antigens
• mimicking host molecules: pathogens cover themselves in molecules normally found in host.

Question 54

A) What are exotoxins? What are some examples? [Table 16.1]

Answer 54

protiens produced which have very specific damaging effects. botulism( can cause paralysis), diptheria( destrys cells, pus and blood all form a membrabe that disloges in back of airway and blocks it),

Question 55

2) What does the immune system do when exotoxins are present?

Answer 55

they produce nuetralizing antibodies

Question 56

3) What are toxoids and antitoxins?

Answer 56

a suspension of neutralizing bodies that help with syptoms of toxin mediated disease
toxoids: inactivated toxins, used in vaccines ie tetanus and diptheria

Question 57

4) What do neurotoxins damage?

Answer 57

damage the nervous system

Question 58

5) What symptoms are associated with enterotoxins?

Answer 58

intestinal distrubance, vomiting diareah

Question 59

6) What do cytotoxins damage?

Answer 59

interfere with cellular mechanism or cause lycing in a variety of cells

Question 60

7) What are A-B toxins and what do they offer for vaccine development? [Figure 16.11 and A B Exotoxins and Diphtheria Exotoxin video]

Answer 60

Two parts the A which carries the toxin and the B which binds to specific surface molecules of cells. This is neat because we can just administer the b part and get the body innoculated and build a defense for it.
They also hope to program the B to bind to specific types of cells and administer medications that way.

Question 61

8) What are membrane-damaging toxins and how do they work?

Answer 61

cytotoxins: disrupt plasma membranes causing them to burst. they insert themselves into the membrane and create pores that allow fluids to enter the cell

Question 62

9) How do superantigens affect the body and by what mechanism? [Figure 16.12 and Superantigens video]

Answer 62

they are able to overide the specificity of t cells response causing toxic effects due to release of cytokines. it does this by binding to MHC region of cell making the cell think that antigen is present when it probably is not there

Question 63

10) What does the toxin exfoliatin do to skin?

Answer 63

this causes it to crack because it degrades material that binds together to seperate

Question 64

B) What are endotoxins and how are the different from exotoxins? [Table 16.2]

Answer 64

endotoxins is a lipopolysacharide molecule that makes up outer layer of gram neg cell wall. cannot be converted to toxide to make vaccination. it is heat stable

Question 65

1) What is septic shock? What causes it?

Answer 65

when infection is systemic causing drop in bp, and fever.

Question 66

C) What type of damage can me caused by the inflammatory response?

Answer 66

leakage of permiable vessles results in sweeling, fever,drop in bp etc

Question 67

D) How do immune complexes affect the kidneys and joints?

Answer 67

anitbody-antigen complexes settle in the kidneys and joints to activate compliment system and therefore causing inflamation

Question 68

E) How do cross-reactive antibodies promote and autoimmune response? What’s the consequence?

Answer 68

when antibodies formed end up binding to self cells

Question 69

A) How are viruses able to attach to target cells?

?

Answer 69

they attatch at specific receptors

Question 70

B) How do viruses avoid the effect of interferons?

Answer 70

they end up destroying host genes, or preventing the interferons enzymes from activating

Question 71

C) How do viruses stop apoptosis in host cells and how does this relate to tumors?

Answer 71

by controling protien p53 when this is inhibited tuomors will develop

Question 72

D) How can viruses avoid being detected by the cellular immune response? [Figure 16.13]

Answer 72

interfere with antigen presentation on mhc. Some like herpes prevent any from showing ( but nk cells will kill cells if they don’t have any to recognize) So some will place false molecules out on their surface

Question 73

E) How do viruses, like HIV, avoid antibodies

Answer 73

they do this from moving from one cell to it’s neighbors before antibodies can get them. HIV cause cells to fUSE with their neighbors. This forms a syncyum

Question 74

A) What are dermatophytes how do they invade host tissue?

Answer 74

group of fungi that infect the hair, skin and nails, but do not go deep.

Question 75

1) Which fungi cause the most sever infections?

Answer 75

caused by dimorphic fungi. tjese occur as mold in environment which can then infect them

Question 76

2) What are mycotoxins and who produces them?

Answer 76

toxins produced by fungi. Asperfillus flavus is what grows on grains and nuts and can cause damage to the liver

Question 77

B) How do protozoans and helminthes enter the body?

Answer 77

they can either through bites, being ingested, and some can enter through skin themselves

Question 78

1) How do they avoid antibodies?

Answer 78

coat themselves in host protiens, they can hide within cells, or change their outer cell antigens

Question 79

2) What kind of damage do they cause?

Answer 79

some result in malnutrition, block organs, destroy tissues