MFD 27 (PD)

Question 1

Describe the process of carrying out a checkerboard-DNA, DNA- hybridisation format

Answer 1

1. extract DNA from samples
2. attach to DNA probes to wells on plate , parallel to each other
3. label DNA from samples
4. Apply multiple clinical samples perpendicular to DNA probes at 90 degree angle
5. Observe signal of probe (thus results are semi-quantitative)

Question 2

Why is checkerboard-DNA, DNA- hybridisation format useful in identifying cause of periodontal diseasw?

2) How many species can you look at at a time
3) What do we use now?

Answer 2

can screen huge numbers of bacteria, thus can loo for association between disease and bacteria as well as grouping bacteria which appear together into complexes.

2) 40
3) sequence everything with next generation sequecning

Question 3

What are the red complex species of periodontal disease?

Answer 3

Porphymonas gingivalis
Tanella forsythia
T .denticola

Question 4

What sort of bacteria bind to fusobacterium nucleatum, the bridging bacteria between early colonisers (streptococcus) and later colonisers?

Answer 4

later colonises are more pathogenic
and include red complex bacteria e.g. p.gingivalis
T.forsythia
Treponomea denticola

Question 5

What do all red complex bacteria have in common?

Answer 5

they are all gram-negative, proteolytic, anaerobes

Question 6

P.gingivalis

1) What shape is it?
2) What sort of pigment does it produce?
3) What can it adhere to?
4) What agar should be used to identify it?

Answer 6

1) rod
2) black and brown porphyrin (haem-containing pigements)
3) I am assuming fusobacterium nucleatum as well as certain forms of streptococci, therefore don’t really need the bridging organism
4) blood agar

Question 7

T.forsythia

1) shape?
2) is it a challenge to grow in the lab?
3) how does one wild type of it hide itself from the immune system?

Answer 7

1) short rods with tapered ends
2) difficult to grow in a monoculture, growth is facilitated by other bacteria
3) has a glycosylated S-layer on the outside

Question 8

T. denticola

1) Which phylum is it apart of?
2) what is the name of the bacterium it is related to ? What disease this bacterium cause
3) How does it adhere?
4) Are they motile?

Answer 8

1) spirochaetes (they have distinctive double membranes)
2) Treponemea pallidum, (causes syphilis)
3) in outer sheath have a major protein
4) have a flagellum, yes

Question 9

TM7 phylum has recently now able to be cultured. How did they do it?

Answer 9

they enriched a plaque sample,
continuously using flourscent insitu hybridisation to see which sample had the phylum then , carryied on enriching till the got a pure culture.

Question 10

What is the significance of TM7 phylum in dentistry?

2) what shape are they?

Answer 10

is present in mild periodontitis compared with health or severe disease
2) variance, rod or cocci depending on partner bacterium species it grows with

Question 11

WHy is it important that we can grow bacteria in pure cultire?

Answer 11

to carry out koch’s postulates

Question 12

How big is the genome of TM7 genome?

2) What is the significance of this?
3) How was the genome identified?

Answer 12

1) less than 1Mbp
2) very small , reflects how bacteria is dependent on other species as could not be grown alone , had o be co-cultured with A. odontolycitus
3) via reconstruction of meta-genomic sequence

Question 13

What animals are used in animal models for perio?

2) which is the most difficult to work with?
3) Which are the most similiar to humans?

Answer 13

1) rodents, dogs, primates
2) primates
3) primates

Question 14

Co-infection in animal models leads to greater damadge than with any of the bacteria alone, the bacteria being: P.ging and F.nucleatum

Answer 14

true

Question 15

Why are animal models not useful the way koch intended in periodontal disease?

Answer 15

as perio is likely due to more than one bacterium and its more to do with level than the infecting bacterium that is important

Question 16

Why can’t we use koch’s postulate to find cause of periodontal disease?
2) to enphasise, what is it not to do with?

Answer 16

1) as perio is likely due to more than one bacterium and its more to do with level than the infecting bacterium that is important
2) a) the fact that we can’t pure culture the bacterium (false e.g TM7 phylum)
b) that fact that there are no animal models availble (there are e.g primates)
c) the fact that no infecting organism can be detected (false, we can detect e.g. Checkerboard DNa, DNA hybridisation)

Question 17

What other way is there than koch’s postulate to find the cause of disease?

Answer 17

look at virulence factors.

Question 18

What are the 4 virulenc efactors p.gingivalis has?

Answer 18

1. adhesions/invasions
2. capsule
3. haemagglutinins
4. proteases
5. LPS

Question 19

What are the 2 adhesions/invasions p.gingivalis has?

Answer 19

minor fimbriae (mfa1)
major fimbriae (mfa2)

Question 20

What is the role of mfa2 in p.gingivalis ?

Answer 20

adhesion and invasion

Question 21

What is the role of mfa1 in p.gingivalis ?

Answer 21

coaggregation

Question 22

What effect does LPS have on the host?

Answer 22

its pro-inflammatory, triggers immune response

Question 23

What are haemagglutinins?

Answer 23

a substance, such as a viral protein, which causes haemagglutination (specific form of agglutination that involves red blood cells (RBCs). It has two common uses in the laboratory: blood typing and the quantification of virus dilutions in a haemagglutination assay.)

Question 24

Whats special about capulated strain of P.gingivlis?

2) What are the capable of?

Answer 24

they are highly virulent

2) they can resist host immunity (phagocytosis, c-reactive protein)

Question 25

P.gingivalis has several proteases, which is the most important?

2) What is their function:
3) What is their secondary function:

Answer 25

1) extracellular cystein proteases (gingipains)
2) a) role in nutrition and processing bacterial proteins
b) cleave host proteins in connective tissue (laminin, fibronectin, collagen)
c) multiple roles in evasion of immune system
3) haemoglutination, adhesion,

Question 26

what are the major antigens in infecitn with P.gingivalis/ what are the 2 types of gingipains?
B) what does Xaa stand for?

Answer 26

1) Arg-Xaa specific proteases (RGP)
2) Lys-Xaa specific proteases(KGP)
B) unspecified amino acid

Question 27

What does keystone pathogen?

2) What is the proposed keystone pathogen in periodontal disease?

Answer 27

present at low levels in disease state, but without it your not going to get that disease
2) P,gingivalis

Question 28

What bacterium is an exception to the ecological -plaque hypothesis?

2) Which type of periodontal disease is it implicated in ?
3) what other diseases is it involved in?

Answer 28

Actinobacillus actinomycetemcomitans

2) localised aggresive periodontitis
3) can cause systemic disease e.g. endocarditis

Question 29

Actinobacillus actinomycetemcomitans

1) Is it gram + or -
2) Is it capnophobic or capnophilic . What does that mean?
3) What shape is it( use latin term)

Answer 29

1) -
2) capnophilic, thrive in the presence of high concentrations of carbon dioxide
3) coccobacillius, bacterium with a shape intermediate between cocci (spherical bacteria) and bacilli (rod)

Question 30

What virulence factors does Actinobacillus actinomycetemcomitans have?

Answer 30

adhesions/nvasions
LPS
leukotoxins
proteases

Question 31

Actinobacillus actinomycetemcomitans

1) What does it use to adhere to surfaces
2) what doe they adhere to together?

Answer 31

fimbria and assciated gene products (tad locus)

2. uses BOTH: to surfaces

Question 32

What does fimbria only do in Actinobacillus actinomycetemcomitans:

Answer 32

Justs FIMBRIAE:

a) epithelial cells
b) enhance receptor mediated endocytosis

Question 33

What is the leukotoxin of Actinobacillus actinomycetemcomitans:

2) What is it anchored to?
3) what does it target? & how?
4) what causes its enhanced expression in JP2 clone?
5) what properties does the JP2 clone have?

Answer 33

116KDa pore-forming toxin

2) cell wall
3) target immune cells by expressing beta-2 integrins, by forming pores in our cell membranes
4) deletion mutation upstream of an operon encoding the leukotoxin
5) strongly haemolytic, strong leukotoxin activity

Question 34

What is an operon?

Answer 34

operon is a functioning unit of DNA containing a cluster of genes under the control of a single promoter.

Question 35

What systemic diseases are associated with periodontal disease?

Answer 35

1. adverse pregnancy outcomes
2. association with DM
3. association with CVD