Periodontal disease

Question 1

What is the difference between gram positive and gram negative bacterium?

Answer 1

Gram negative - 2 cell membranes with thin cell wall between creating a space called the perioplasm - more transport proteins, outer capsule is LPS
-don’t retain stain so appear pink

Gram positive - thick cell wall (peptidoglycan) retains stain (purple) and one cell membrane

Question 2

What are polymicrobial infecfions?

Answer 2

Interactions between two or more organisms leading to disease,

• sum of parts and their virulence factors cause disease and not one in isolation, -
• interaction with host defences are key

Question 3

Describe the arrangement of subgingival plaque

Answer 3

Microorganisms firmly attached at the bottom of the JE, more loosely attached towards the top, lots of polymicrobial attachments in the gingival crevicular fluid

• Contains a predominantly Gram-positive layer attached to hard tissue
• Overlying layers contain Gram-negative anaerobes and motile bacteria
• All exist in close, mixed communities

Question 4

Treatment for periodontal disease?

Answer 4

RSD, removing plaque, antimicrobial therapy

Question 5

What changes a quiescent site into an active site?

Answer 5

Change in the host e.g. smoking, immune status, age, environmental factors
Change in microbial challenge - type, number, virulence factors

Question 6

What bacteria dominates in ANUG?

Answer 6

Fuso-spirochaetal complex

Question 7

What is amelogensisis imperfecta?

Answer 7

Enamel hasn’t formed properly - very sensitive teeth with rough enamel

Question 8

Which teeth are probed in children?

Answer 8

6 teeth - UR6, UR1, UL6, LL6,LL1, LR1

Question 9

Challenges to toothbrushing?

Answer 9

Retroclined teeth in cleft lip and palate, abnormalities of tooth, Orthodontic appliances, sensitive teeth, physical or learning disabilities

Question 10

How do periodontal pockets develop?

Answer 10

When the junctional epithelium detaches from the enamel

Question 11

Why is the JE thin?

Answer 11

This allows the transport of nutrients from the connective tissue to the tooth and outside of it as well (sulcus).

Question 12

What is the depth of normal sulcus?

Answer 12

0.5-2.0mm

Question 13

When do the inital changes of early gingivitis occur?

Answer 13

Occurs in the first week

Question 14

When does the early lesion occur?

Answer 14

Occurs in second week

Question 15

When does chronic marginal gingivitis occur: established lesion?

Answer 15

within 2-3 weeks

Question 16

When does destructive periodontitis occur?

Answer 16

Timescale unknown

Question 17

What is the initial response to plaque?

Answer 17

Increased blood flow (looks red)

oedema
development - plasma leaking out of blood, increased blood vessels

Migration of neutrophils

Loss of perivascular collagen of blood vessels - leaky

Question 18

What changes occur in the early lesion?

Answer 18

Increase in neutrophils and crevicular fluid (macrophages and lyphocytes)

• junctional epithelium starts to proliferate (hyperplastic - rete pegs) but still attached to tooth and ends at the ACJ

fibroblasts show signs of damage and get collagen loss but fibres inserting into cementum still attached

Question 19

What happens in chronic marginal gingivitis: the established lesion?

Answer 19

Increased in vascularity and formation of GCF

Increase in lymphocytes and plasma cells (chronic cells now not acute cells)

JE becomes detached from tooth but still attached at ACJ

JE may be ulcerated

Marked loss of collagen but fibres into cementum still intact

sulcus may appear deepened but no true pocket formation

Question 20

What happens in destructive periodontitis?

Answer 20

Loss of the collagen fibres inserting into cementum

Junctional epithelium migrates downwards onto cementum

Destruction of alveolar bone (due to inflammation damaging the bone)

True pocket formation

Quite a lot of PDL fibres lost

destruction is not continuous but occurs in bursts?

Question 21

How do we manage destructive periodontitis?

Answer 21

RSD

Removal of plaque, calculus, debris

Inflammation subsides

Junctional epithelium proliferates

Attaches to tooth- long epithelial attachment

Little or no regeneration of bone or
collagen fibres inserting into cementum (fibroblasts)

Question 22

What type of studies are the Loe studies?

Answer 22

Longitudinal studies

Question 23

What do germ free animals show?

Answer 23

No bacteria, no disease

germ free animals + bacteria = disease but not all animals equally

periodontitis causing bacteria is transmissable but not for all animals - disease may or may not arise

Question 24

How would you sample subgingival plaque?

Answer 24

Curette/paper point - perio probe (difficult)

Question 25

Why can 16s rRNA be sequenced easily?

Answer 25

16s rDNA gene is very well conserved due to essential function -acts as molecular clock and species signature as evolves slowly in time.

16s = bacteria
18s = human/animal

Question 26

What type of bacteria are raised in perio disease?

Answer 26

Anaerobic gram negative bacteria

Question 27

What evidence for specific microbial aetiology?

Answer 27

High numbers of certain bacteria cultured from diseased sites and sequences identified in molecular studies

Can cause disease in certain animal models

Have demonstrable virulence factors

Question 28

What is the evidence against specific microbial aetiology?

Answer 28

Potential pathogens present in health and in non-diseased sites

Do these indicate a pathogenic environment or are we missing a key organism?

Question 29

Which 3 bacteria are always associated with increased probing depth, BOP in high numbers?

Answer 29

P.gingivalis
Ta.forsythia
T.denticola

Question 30

What is the key nutritional source for tannerella and how do they get this?

Answer 30

Sialic acid - acquisition of this requires cleavage from host proteins

Inhibition with Tamiflu STOPS growth

Question 31

What shape is T.denticola?

Answer 31

Small, thin spiral shaped bacrerium

Question 32

Why are groups of organisms more important than single pathogens?

Answer 32

Different bacteria have different virulence factors

A combination of these factors is more likely to cause disease

The qualitative mixture of pathogens determines disease progression

Question 33

What has p.gingivalis shown in mouse models?

Answer 33

Has been shown to shift the whole population from non- pathogenic to pathogenic even though itself only being present in low numbers

New idea of one pathogen causing a dysbiosis of a community is new and important theory also being noticed in other conditions e.g. obesity

Question 34

What are some mechanisms of tissue damage by bacterium?

Answer 34

• evasion of host defences
• infuction of inflammation
• soft tissue damage
• bone resoprtion

Question 35

Why does ANUG differ clinically and in aetiology?

Answer 35

Tissue invasion

selection of specific bacteria by host-derived nutrients - fuso-spirochaetal complex (treponema vincentii, other treponemes, fusobacteria, p.intermedia

Question 36

Why would visible plaque be present in more 8 year olds than 5 year olds?

Answer 36

Parents stop helping with brushing at 8 years old but still helping at 5 years old

Question 37

What percentage of 15 year olds had bleeding on probing in 2013 survey of childrens’ dental health in the UK?

Answer 37

40%

Question 38

Why is gingivitis less prevalent on the left hand side of the mouth than the right hand side?

Answer 38

More right handed people better at brushing left side of mouth than right side

Question 39

Which gender has lower plaque and calculus scores?

Answer 39

Females

Question 40

Which BPE codes are used for 7-11 year olds?

Answer 40

0-2

Question 41

Which BPE codes are used for 12-17 year olds?

Answer 41

0-4

Question 42

What are the common gingival disorders in children?

Answer 42

Chronic gingivitis (plaque-induced)
Gingival hyperplasia
Traumatic lesions
Acute gingivitis (infective)

Question 43

What can chronic gingivitis be exacerbated by?

Answer 43

exfoliating teeth, malocclusion or presence of orthodontic appliances

Question 44

What is localised gingival recession in children ususally associated with?

Answer 44

Malaligned teeth, self inflicted injury, toothbrushing habits

Question 45

What drugs can cause gingival hyperplasia?

Answer 45

Phenytoin (anti epileptic)
Cyclosporin (immunosuppresent)
Nifedepine (calcium channel blocker)

Question 46

What does cyclosporin do?

Answer 46

Selective immunosuppressent - inhibits t lymphocyte proliferation

used mainly to prevent graft rejection

gingival hyperplasia in 30% of cases and made worse by poor OH

affects fibroblasts promoting protein synthesis and collagen formation

Question 47

What systemic diseases can gingival hyperplasia indicate?

Answer 47

Sarcoid

cyclic neutopenia

Question 48

What are the 3 types of traumtic gingival injury - self inflicted>

Answer 48

TYPE A - injuries are superimposed upon a pre- existing source of irritation

TYPE B - injuries are secondary to another established habit

TYPE C - injuries are of complex aetiology and are a physical manifestation of an underlying emotional disturbance - resistant to
conventional treatment

Question 49

What acute gingival conditions are common in children?

Answer 49

Acute herpetic gingivostomatitis
Necrotising ulcerative gingivitis
Hand, foot & mouth
Herpengina

Question 50

What are the signs and symptoms of acute herpetic gingivostomatitis?

Answer 50

Pyrexia, >39o C
lymphadenopathy
malaise & irritability
profuse salivation
refusal to eat
sore throat & mouth
symptoms for 7-10 days

clinical features:
multiple small irregular ulcers on gingiva, tongue and palate
erythematous gingiva
occasional extra-oral lesions
salivation
lymphadenopathy
recurrence as herpes labialis in 30%

Question 51

What is the management of AHGS?

Answer 51

fluids and soft diet
analgesics and antipyrexics
isolation of eating/drinking utensils
OHI - chlorhexidine and sponges, soft toothbrush
rest
reassurance and review
Not acyclovir (unless immunocompromised)

Question 52

What systemic conditions may present with gingival changes?

Answer 52

HIV
Chrons’ disease
leukaemia
Langerhans’ cell histiocytosis
scurvy

Question 53

What are the clinical features of aggressive periodontal disease in children?

Answer 53

Around 0.1% of white Caucasians and 2.6% of black Africans may suffer from localized aggressive forms of periodontitis
Onset around puberty
may present with tooth mobility, drifting or periodontal abscess
rapid periodontal attachment loss, usually incisors and first permanent molars
Often a positive family history
Healthy apart from periodontitis

Amounts of microbial deposits are inconsistent with the severity of destruction
Elevated proportions of A. actinomycetemcomitans and in some populations, P.gingivalis
Phagocyte abnormalities (host defence defects) Hyper-responsive macrophage phenotype, including elevated levels of PGE2 and IL-1β
Progression of attachment loss and bone loss may be self arresting

Question 54

What is NOMA characterised by?

Answer 54

Necrosis and ulceration - usually interdental papillae, gingivae bleed profusely, distinctive halitosis

Broad anaerobic infection

can spread rapidly to facial tissues

Question 55

How do you treat NOMA?

Answer 55

OH, hydrogen peroxide mouthwash, metronidazole 3 days

Question 56

How would you manage aggressive periodontal disease in children?

Answer 56

• early diagnosis and interventions critical
• standard mechanical perio therapy - RSD
• systemic or local drug therapy (metronidazole AND amoxycillin tds 1 week)
• maintenance therapy
• periodontal surgery
• chlorhexidine rinses

Question 57

What systemic or genetic conditions may exacerbate periodontal disease or in which perio is worse?

Answer 57

Insulin-dependant diabetes
Down syndrome
Papillion-lefevre syndrome
Enlers-Danlos syndrome
Langerhans’ cell histocytosis
Neutropenias
Hypophosphatasia

Question 58

What are some of the symptoms of Papillon-Lefevre syndrome?

Answer 58

Itchy feet
Loose teeth - bone destruction and resorption of roots
generalised gingival recession
hyperkeratosis of palms and soles

Question 59

What antibacterial substances are in the saliva?

Answer 59

Lactoferrin
Thiocynate
Hydrogen peroxide

Question 60

What is the role of the epithelium

Answer 60

1. Surface epithelium shed
together with any attached
bacteria.
2. Permeability barrier
3. Junctional epithelium may be
more permeable than oral
epithelium.
4. Epithelium can stimulate the
inflammatory and immune
response by releasing cytokines
e.g. IL-1

Question 61

What happens to igA as it gets secreted?

Answer 61

Turns from monomeric to dimeric form

Question 62

What is IL1?

Answer 62

pro- inflammatory cytokine

Question 63

What does GCF contain?

Answer 63

• Complements C1-C9
• Antibodies - opsonins
• Contains clotting cascade- fibrin forms a barrier to
  spread of infection;
  thrombin & Hageman factor promote the
  inflammatory response.
  • Kininogens-converted to kinins by proteases.
  Bradykinin- similar to histamine, promotes
  inflammatory response

Question 64

What does c3a and c5a do?

Answer 64

vascular changes, stimulate histamine
release, promote formation of leukotrienes &
prostaglandins; attract phagocytes and aid
phagocytosis

Question 65

What does c9 do?

Answer 65

membrane attack complex, destroys microorganisms

Question 66

What can bacteria metabolise in the GCF?

Answer 66

complement, immunoglobins and other components partly consumed and degraded in the crevice

Question 67

What carbohydrate do neutrophils and macrophages bind to on the bacterium?

Answer 67

Manose sugars

Question 68

What is the function of neturophils?

Answer 68

Production of NETS- neutrophil extracellular traps. (sheds DNA and throws out like net)
• Kill microbes by antimicrobial peptides and is a signal for other neutrophils
• Neutrophils themselves die in the process

Question 69

What happens to patients with reduced number of neutrophils?

Answer 69

Increased priodontal destruction e.g. cyclic neutropenia

defeciency in cathepsin C - papillon lefevre syndrom

• contribute to perio in diabetes and downs syndrome

Question 70

What can an activatd macrophage do?

Answer 70

Phoagocytosis
antigen presentation - stimulate immune response
growth factors - stimulation of fibroblasts + endocthelial cells to promote healing
- secrete cytokines and chemokines to attract inflammatory cells and regulate inflammatory response - secrete Il-1 and TNF

Question 71

What do macrophages do?

Answer 71

Stimulate the immune
response
•Release cytokines
•Phagocytose
•Stimulate healing

Question 72

What can antibodies do for defence?

Answer 72

•Acts as an opsonin
•Activates neutrophil enzyme secretion
•Prevents bacterial attachment
•Activates complement
•Directly inhibits bacterial metabolism
BIND TO SOLUBLE FACTORS
•Neutralises toxins
•Inhibits enzymes

Question 73

What is the cause of tissue damage and bone loss in periodontal disease?

Answer 73

Bacterial products:
- endotoxins - may damage epithelium, fibroblasts
- bacterial enzymes e.g. collagenase, hyaluronidase break
down the connective
tissue
• Lipopolysaccharide,
capsular material,
Peptidoglycans,
muramyl dipeptide,
proteases may cause
bone resorption 

Host products:
• Release of enzymes
from neutrophils
• Complement
• Production on IL-1, IL-6
by macrophages stimulates
bone
resorption & epithelial
proliferation
• Inflammatory mediators, prostaglandins,
other
cytokines, leukotrienes
also stimulate bone
resorption

Question 74

What is the periodontal ligament protected by?

Answer 74

Saliva
Epithelium
Inflammatory response
Immune response

Question 75

When does periodontal disease occur?

Answer 75

when the balance between destruction and repair in the host response to bacteria is disturbed.
This may be due to alterations in bacterial pathogenicity or the host response.

Question 76

What is the old classification of periodontal diseases called?

Answer 76

Armitage 1999

Question 77

What is the Armitage 1999 classification?

Answer 77

I. Gingival diseases (non-plaque induced and plaque
induced)
II. Chronic periodontitis
III. Aggressive periodontitis
IV. Periodontitis as a manifestation of systemic diseases
V. Necrotising periodontal diseases
VI. Abscesses of the periodontium
VII. Periodontitis associated with endodontic lesions
VIII.Developmental or acquired deformities and condition.

Question 78

What is the classification of gingival diseases?

Answer 78

- Developmental - Acquired or hereditary
• Infective
• Non-plaque induced or Plaque induced
• Allergic
• Modified by or attributable to systemic factors
• Inflammatory or non-inflammatory
• Traumatic
• Overgrowth (Hypertrophy, hyperplasia, oedema)

Question 79

What are the characteristics of chronic periodontitis?

Answer 79

Can be localised or generalised (30% of sites affected)
destruction is consistent with local factors
subgingival calculus is a frequent finding
variable microbial pattern
progression is low but rapid bursts can occur
breakdown of periodontal fibres at cervical margin,
alveolar bone resorption
apical proliferation of junctional epithelium beyond ACJ
Associated with local predisposing factors - overhangs, grooves, crowding
risk factors - genetics, age, gender, smoking, plaque levels, systemic disease (diabetes), stress

Question 80

What are the characteristics of aggressive periodontitis ?

Answer 80

Rarer but often severe
rapid attachement loss and bone destruction
possible familial aggregation of disease
patients are systemically healthy, usually non smokers
Onset - earlier age and less than 30 years
amount of plaque out of proportion with severtiy of disease
can be localised (1st molar and incisor involvement)
can be generalised (3 or more teeth involved)
destruction is greater than local factors
suggests elevated levels of aggregatibacter actinomycetemcomitans and prophyromonas gingivalis
- phagocytre abnormalities
attachement and bone loss may be self arresting

Question 81

What are the characteristics of generalised aggressive periodontitis?

Answer 81

Severe, generalised form, young adults , 30 years
interproximal attachment loss affecting at least 3 permanent teeth other than first molars and incisors
episodic nature of destruction of alveolar bone and attachment
1-2% of western pop, increased in afro-carribeans

Question 82

What are the characteristics of localised aggressive periodontitis?

Answer 82

Severe, localised
onset around puberty
localised attachement loss of at least 2 permanent teeth one of which is a first molar and involving no more than 2 teeth other than first molars and incisors

Question 83

What systemic conditions can affect the periodontium?

Answer 83

• Acquired neutropenia
• Leukemias

Down syndrome
• Leukocyte adhesion deficiency syndromes
• Papillon-Lefevre syndrome
• Chediak-Higashi syndrome
• Histiocytosis syndromes
• Glycogen storage disease
• Infantile genetic agranulocytosis
• Cohen syndrome
• Ehlers-Danlos syndrome types IV and VIII
• Hypophosphatasia

Question 84

What are the symptoms of Ehlers-Danlos syndrome types IV and VIII?

Answer 84

Hyperflexibility of joints
• Increased bleeding and bruising
• Hyperextensible skin
• Underlying molecular abnormality of collagen
• Type IV – bleeding commoner
• Type VIII – aggressive periodontitis, early onset
• All types – pulp stones

Question 85

What are the symptoms of papillon-lefevre? (oral)

Answer 85

• Palmoplantar hyperkeratosis and AP
• Affects 10 and 20 dentition
• Normal dental development until hyperkeratosis
of palms and soles appears
Hyperkeratosis of palms and soles of feet appear in first few years of life.
• Mechanism poorly understood

Question 86

What are the symptoms of downs syndrome?

Answer 86

Bradycephaly, mid-face retrusion, small nose, flattened
nasal bridge, upward sloping palpebral fissures
• Macroglossia, delayed eruption of teeth
• Heart defects, atlanto-axial subluxation (C1-C2 disorder
causing impairment in rotation of the neck), anaenia,
increased risk of leukaemia

Question 87

What are the symptoms of Chediak-Higashi syndrome?

Answer 87

a rare autosomal recessive disorder that arises from a mutation of a lysosomal trafficking regulator protein, which leads to a decrease in phagocytosis. The decrease in phagocytosis results in recurrent pyogenic infections, albinism and peripheral neuropathy.

Combination of defective neutrophil function,
abnormal skin pigmentation and increased
susceptibility to infection

Question 88

What are the characteristics of Necrotising periodontal diseases?

Answer 88

• NUG and NUP
  • Related to diminished systemic resistance to bacterial infection
  • Destructive inflammatory condition – rapid, debilitating, acute
  • Only differ in terms of tissue affected, with NUP extending into periodontal attachment
• Painful ulcerated necrotic papillae & gingival margins,
  ‘punched out’ appearance
  • Ulcers with yellow-grey slough
  • Metallic taste, teeth feel wedged, foetor oris
  • Craters – interproximal, loss of crestal bone
  • Loss of attachment can lead to NUP
  • Regional increased LN, fever , malaise can occur
  • Associated with poor OH, stress, smoking
  • Gram –ve anaerobic infection

Question 89

What are the three types of abscesses in the periodontium?

Answer 89

Gingival

periodontal

pericoronal

Question 90

What developmental or acquired deformities and conditions associated with the periodontium exist?

Answer 90

Localised factors:
Developmental - groove, enamel pearl - difficult to keep clean, attracts calculus
Acquired - root fracture - infection going through this site

-recession
• abnormal gingival contour (incomplete eruption)
• aberrant fraenum

occlusal trauma

Question 91

What are the issues with the old classification?

Answer 91

Considerable overlap in disease categories
• Absence of a gingival disease component
• Inappropriate emphasis on age of onset of
disease and rates of progression
• Inadequate or unclear classification criteria

Question 92

What are the goals of periodontal therapy?

Answer 92

Restore health/eliminate disease
Improve patient’s quality of life
Clinical goals

Question 93

What is oral health?

Answer 93

such a state of health of the teeth and supporting tissues, and of efficiency, as is reasonable to safeguard general health” (General Dental Services Regulations)

Question 94

What are clinical goals of periodontal therapy?

Answer 94

No progression.
Reduction in probing depths.
No probing depth > 5mm.
No bleeding on probing.
No smoking
Plaque score < 20% surfaces.

Question 95

What are factors that can affect the outcome of periodontal treatment?

Answer 95

Susceptibility to disease / genetic factors
Plaque control
Previous periodontal disease
Smoking 
Stress
Some systemic diseases eg diabetes
Diet

Question 96

What are the 4 stages of the periodontal treatment strategy?

Answer 96

Initial treatment
Cause-related therapy
Non-surgical treatment
Surgical treatment (0ccasionally)

Question 97

What should initial treatment be based on?

Answer 97

Emergency treatment/ relief of pain (where necessary)

Extraction of teeth having a hopeless prognosis

Oral health education / oral hygiene advice

Plaque control including correction of plaque retention factors

Root surface debridement

Initial occlusal adjustment (where necessary)

Reassessment and monitoring

Question 98

What is cause-related therapy?

Answer 98

Oral health education and advice on plaque control - this is what has caused the perio/gingivitis

Question 99

What evidence was found to have a small but positive effect on reduction in gingivitis in adults from 2000 article?

Answer 99

A single oral hygiene instruction + toothbrush demonstration + scaling - a significant albeit small positive effect on the reduction of gingival inflammation in adults with gingivitis.

Question 100

What non-surgical treatment exists?

Answer 100

Removal of plaque retention factors (includes scaling and correction of restoration margins)
Root surface debridement of periodontal pockets ≥4mm) under LA
Review 3 months following the completion of treatment (review oral hygiene at 1 month) - symptoms, risk factors and plaque scores
Further treatment of non-responding sites.

can do it in quadrants or full mouth

Question 101

What are the indications for RSD?

Answer 101

≥ 4mm
removal of sub-gingival plaque & calculus
removal of surface toxins (endotoxin etc)
under LA usually
Predominantly ultrasonic

Question 102

What hand instruments are used for scaling?

Answer 102

periodontal hoes
files if needed
Langer universal curettes

Question 103

What should you review at 3 months?

Answer 103

Plaque scores, probing depths, bleeding indices, mobility scores

Question 104

What are the good and bad outcomes of RSD?

Answer 104

Reduced probing depths
Less bleeding
No suppuration
Improved tissue contour

Recession
Increased sensitivity
Other complications

Question 105

For what depths can periodontal treatment cause clinical attachment loss?

Answer 105

1-3mm

Question 106

When is periodontal treatment complete?

Answer 106

When probing depths are less than or equal to 4/5mm and BoP is less than 30%

Question 107

How would you monitor periodontal disease?

Answer 107

Probing depths
Recession
Plaque control
Inflammation (bleeding)
Mobility
Drifting/migration
Dentine sensitivity

Question 108

What are the limitations of clinical measurements?

Answer 108

Errors in probing depth measurements
Bleeding on probing:
Low sensitivity/specificity
Smoking
Medication
Flow between sites

Absence of bleeding:
Higher sensitivity/specificity

Question 109

What are the limitations of using radiographs to assess perio?

Answer 109

Show hard/calcified tissue only
Inter/intra operator variance, angulation
Patient factors, tolerance

Question 110

When would systemic antibiotics be used to treat perio?

Answer 110

Aggressive forms of disease

“Refractory” disease

Necrotising forms of periodontal
diseases

Severe disease

Abscesses

Question 111

What periodontal surgery may be carried out?

Answer 111

Flap surgery – open flap debridement

Gingivectomy