Chapter 13

Question 1

A) What is the comparative size of a virus? [Figure 13.1]

Answer 1

100 to 1000 fold smaller than cells they infect

Question 2

B) What is a virion? [Figure 13.2]

Answer 2

nucliec acid surrounded by a protein coat and enzymes

Question 3

1) What is a capsid and how does it protect the virion?

Answer 3

protien coat that protect from enzymes and toxic chemicals

Question 4

2) What is a nucleocapsid?

Answer 4

nucleic acid and capsid

Question 5

C) What makes and enveloped virus unique? [Figure 13.2b]

Answer 5

they have lipid bilayer around capsid and between them a speciall matrix protien- makes them more susceptable to disinfectants

Question 6

1) Why are naked viruses considered “naked”?

Answer 6

ones without an envelope

Question 7

D) What type of nucleic acid do viruses have?

Answer 7

either rna or dna, but never both

Question 8

E) How do viruses attach to host cells? [Figure 13.1, 13.2 and Entry of Virus into Host Cell Video]

Answer 8

attatch to receptors on host cell some have protien structures that are called spikes that stick out of their capsid

Question 9

F) What different shapes do viruses have? [Figure 13.3]

Answer 9

icosahederal- like a ball
helical- cyndrical
complex- what is in most pictures

Question 10

G) Know the classifications of human viruses. [Table 13.1]

Answer 10

q?????????

Question 11

H) Know the informal terms for viruses grouped by primary route of transmission. [Table 13.2]

Answer 11

enteric- fecal- oral route(norovirus, roraviruses aka diahrea, enteroviruses)
Respiratory- respiratory or salivary route(influenza measles, rhinoviruses aka colds)
Zoonotic- vector( lice ect) (westnile, dengue)
Sexually- sexual contact (genital herpes

Question 12

I) What are arboviruses and how did they get their name?

Answer 12

spread by anthropods( west nile, elephantitis) ar (anthropod) bo(born)

Question 13

A) What are the major types of relationships between viruses and host cells? [Figure 13.4]

Answer 13

It can be a latent phase
or
Productive infection which multiplication can occur leading to the cell lysing, or virons are release by cell so it doesn’t lyse

Question 14

B) What are lytic or virulent phages?

Answer 14

phages exit via lysing the host.

Question 15

1) What are so called productive infections?

Answer 15

viral infections/ phages new virus particles are released from cell lysing

Question 16

2) What is the infection cycle of the T4 phage? [Figure 13.5 and steps in replication of T4 phage in E.coli video]

Answer 16

t4 is protien cell on the phage and it attaches to the receptor of host cell. Then it degrades a small portion of a bacteria.the tail contracts and then injects phage dna into the host . proteins replicate and are made in a sequential order.
1at protiens produced- nuclease degraders, and a protien that modifies the host cell’s rna polymerase - so no host cells genes are expressed.
then phages are formed.
lysozyme is produced which digests the cell’s wall causing it to lyse releaseing phage particles which go and infect other cells.

Question 17

C) What are temperate phages? [Figure 13.6]

Answer 17

can either become lytic or store their dna into the host cell’s genome

Question 18

1)What is a lysogenic infection?

Answer 18

is when they store their dna in the host cells gnome.

Question 19

2) What is a lysogen?

Answer 19

infected cell of lysogenic carriers

Question 20

D) What do we know about the lambda phage? [Lambda phage replication cycle video]

Answer 20

it is a temperat phage with a linear chromosome, but with ends that connect to eachother forming a circle.
in lysogeny it uses integrase ( enzyme) to insert phage dna into host’s. It can be taken out by another enzyme and then it becomes lytic

Question 21

1) What is a prophage?

Answer 21

replicates along with host chromosome prior to division

Question 22

2) What happens during phage induction?

Answer 22

phage escapes damaged host. due to host cells sos system cutting out the respressor protien responsible for the integration of the prophage

Question 23

E) What is superinfection conversion?

Answer 23

infection by the same phage

Question 24

F) How are lysogens protected from infections by the same phage?

Answer 24

called immunity to superinfection. This is because the repressor that maintians the prophage will also bind to operators on oncoming dna. the oeratoe is a regualtory region that controls infection , thus it will prevent expression of the dna that joins to ir.

Question 25

G) What is lysogenic conversion? [Table 13.3]

Answer 25

is a change in the lysogens phenotype du to specific prophage.

Question 26

H) What are filamentous phages?

Answer 26

single stranded dna tha look like long fibers. They do not kill host cell, but infected cells multiply slower than if uninfected.

Question 27

1) What do we know about the M13 phage? [Figures 13.7 and 13.8]

Answer 27

it attatched to f pillus on ecoli It hen enter the cell and then it uses cells dna polymerase to make copy of other strand so it can form a double helix which then makes mrna. As this is happening the chage coat protiens make the capsids that form around the phage dna that is excreted.

Question 28

A)What is generalized transduction?

Answer 28

This is when there is an error in phage assembly. sometimes phages degrade the hosts chromosomes into pieces which are then accidently packaged. These cannot replicate

Question 29

1)How are generalized transducing particles different from phage particles?

Answer 29

they contain pieces to the dna particles of host instead of phage and cannot replicate.

Question 30

B) What is specialized transduction? [Figure 13.9]

Answer 30

excision mistake made by the temerate phage during transition from lysogenic to lytic cycle. This is when it accidently excises some of the bacterias dna with the phage, and a peice of phage is left with the bacterias dna. This makes the phages defective, but can go to other host cells and incorperate into it.

Question 31

A) How do bacteria like Staphylococcus aureus prevent phage attachment?

Answer 31

they produce protiens to cover their receptors on the cell surface so phage cannot attatch.

Question 32

B) What do restriction-modification systems do? [Figure 13.10]

Answer 32

They have two types of enzymes, restriction and modification.
These are trained to recognize foreign dna and will cut them up.
modification: they protect host from the restiction enzyme by covering it’s dna with methyl groups which makes the dna invisible to the restriction enzymes.

Question 33

C)What does the CRISPR system do? [Figure 13.11]

Answer 33

this is when a cell survives phage infection and saves peices of phage dna in chromosome in the CRISPR region. this is so it can recognize and protect itself from subsequent infections of same phage.

Question 34

1)What does CRISPR stand for?

Answer 34

Clusters of Regularly Iinterspersed Short Palindromic Repeats.

Question 35

A) What are plaque assays used for?

Answer 35

used to know how many phage particles.

Question 36

1) What exactly are plaques? [Figure 13.12]

Answer 36

circular zones which show cell lysis caused by phage dna

Question 37

2) What is the titer?

Answer 37

phage concentration in the original plate suspension

Question 38

A)What do animal viruses have on their surface?

Answer 38

studded with attatchment protiens or spikes which are bound to glycoprotiens in the plasma membrane

Question 39

B) What must HIV do before it can enter a cell?

Answer 39

must bind to two receptors

Question 40

C) What makes some animals resistant to certain diseases?

Answer 40

the diseases cannot connect to the two receptors required.

Question 41

D) How do enveloped viruses enter a cell? [Figure 13.3]

Answer 41

2 different mechanisms:
fusion with host membrane:
endocytosis:

Question 42

E) How do naked viruses enter a cell?

Answer 42

can only enter via endocytosis read 318

Question 43

F) What is the process of uncoating and which type of viruses do it?

Answer 43

in all viruses: The phage nucliec acid must be speparated from capsid. this process is called uncoating. this is done by virus scpecific mechanisms which release viral genome.

Question 44

H) What two things need to happen for production of viral particles in an infected cell to take place?

Answer 44

1. expression of viral genes to produce protiens to make capsid and enzymes required for replication.
2. synthesis of multiple copies of genome.

Question 45

I) How do DNA viruses replicate? [Figure 13.4a]

Answer 45

typically replicate in the nucleus using host cells machinery to perform replication

Question 46

J) How do RNA viruses replicate? [Figure 13.4b]

Answer 46

replicate in cytoplams. requires replicase

Question 47

1) What is replicase?

Answer 47

a virally encoded rna polymerase

Question 48

2) What is antigenic drift?

Answer 48

the rna polymerase has no proof reading and can make mistakes, this forms mutations. This can make a different antigen. ex: influenza changes from year to year.

Question 49

K) How do reverse-transcribing viruses replicate? [Figure 13.4c]

Answer 49

rna is used as template to make dna

Question 50

1) What is a Retrovirus? What are some examples?

?

Answer 50

human imunodeficeincy. HIV. It’s rna in smplanted into the cell and is used as a template to make 1 strand dna. then it’s compliment is made and is integrated into host cells dna. Hep B.

Question 51

L) Where does the assembly process take place for animal viruses?

Answer 51

in cytoplasm or nucleus

Question 52

M) What is budding? [Figure 13.5 and Mechanism for releasing enveloped virions video]

Answer 52

when cell goes to release virus. This si when protine spikes of virus insert into host cells membrane nuceloplasmids are excised and are covered in the matrix built up in those areas.

Question 53

N) How do naked viruses leave a host cell?

Answer 53

released when the host cell dies. they initiate apoptosis( cell programed death)

Question 54

A) What are acute infections? [Figure 13.16a]

Answer 54

Infections that can infect a host, but then be eliminated

Question 55

B) What are persistent infections? [Figure 13.16b-c and Table 13.4]

Answer 55

Infections where the infection cannot be eliminated. There are 2 types chronic, and latent

Question 56

1) What are chronic infections? What are some examples?

Answer 56

Chronic infections are those like HPV ect which will stay active and persistent till the host dies

Question 57

2) What are latent infections? What are some examples?

Answer 57

Latent infections are those which will go into a inactive state in which the host doesn’t expirence symptoms, but then it will activate and the symptoms will arise in the host.

Question 58

• What is a provirus? [Figure 13.17

Answer 58

This is an inactive virus. when the virus doen’t integrate into the cell’s chromosomes, but is independent like a plasmid. They can replicate on their own when they want.

Question 59

A) What is a tumor?

Answer 59

where hosts cells are mutated causing the cell to grow and reproduce abnormally.

Question 60

B) What are proto-oncogenes?

Answer 60

They are genes in cells that regulate growth

Question 61

C) What is a oncogene? How can viruses with them lead to tumors? [Table 13.5]

Answer 61

They are genes carried via virus that are similair to proto oncogenes, and mess with the growth causing tumors.

Question 62

D) Review Figure 13.18

Answer 62

q

Question 63

A) What was the only way to study animal viruses back in the day?

Answer 63

they would innoculate animals with the virus, or they would innoculate a fertilized chicken egg

Question 64

B) How can you use cell and tissue culture to study animal viruses?

Answer 64

you provide a medium that they can grow in although it is really slow.

Question 65

1) What is a primary culture? [Figure 13.9]

Answer 65

when you isolate one cell in a meduim and let it replicte

Question 66

2) What is the cytopathic effect? [Figure 13.20]

Answer 66

when you can tell what virus it is by the morphologicall change that occurs to the cell.

Question 67

3) What is an inclusion body?

Answer 67

when infected cells congregate at site of viral replication

Question 68

C) How can a plaque assay be used to find animal virus concentration?

Answer 68

you look at the clear zones

Question 69

D) How can you use an electron microscope to count animal viruses? [Figure 13.21]

Answer 69

if it is high enough concentration.

Question 70

E) What is a quantal assay and how is it used?

Answer 70

this is when they innoculate a number of subject and then you see which were killed and it is given as a percentage

Question 71

1) What is the ID50?

Answer 71

infective dose 50%

Question 72

2) What is the LD50?

Answer 72

Lethal Dose 50%

Question 73

F) What is hemagglutination? [Figure 13.22]

Answer 73

when viruses connect to multiple rbc s this causes ten to agregate.

Question 74

A) How can you recognize of viral infection in a plant? [Figure13.23]

Answer 74

stunted growth, tumours, yellowing, etc

Question 75

B) What is an example of a plant that has been maintained in a virus-infected state? [Figure 13.24]

Answer 75

tulips

Question 76

C) How do viruses infect plants?

Answer 76

they are carirind through bug or humans going from plant to plant

Question 77

A) What are viroids? [Figure 13.25]

Answer 77

onlly carries short sta rna hat in in a circle.

Question 78

B) What are prions? [Table 13.6, Figure 13.26 and Prion diseases video]

Answer 78

Prions are protiens that in brain kill neurons

Question 79

1) What does the term transmissible spongiform encephalopaties mean?

Answer 79

Term for all prions disease .. arose from the spongy like texture of brains infected by prions.

Question 80

2) What are PrPc and PrPsc? [Figure 13.27]

Answer 80

prPc - is normal non infectious prions

Prpsc- prion prtotien scrapies- infectious

Question 81

3) How do prions cause disease?

Answer 81

a

Question 82

4) What are some examples of prion diseases?

Answer 82

mad cows diseasen jacobs disease