Pathogenesis of Periodontal Disease 1 Workbook PDF

Summary

This workbook covers the pathogenesis of periodontal disease, focusing on topics such as the development of oral mucosa, dental plaque biofilm, and host defenses. It outlines the factors contributing to the initiation of periodontitis and provides detailed information on various aspects of the disease.

Full Transcript

This workbook is to be used in conjunction with your session on the
subject of **Pathogenesis of Periodontal Disease.**

- The premise of this session is for you to complete the tasks in a
self-directed way

- There are links to documents/resources which will enable you to gain
knowledge of this subject and to complete the tasks as you proceed

- It is important that you complete and have your notes in preparation
for the next session **Pathogenesis of Periodontal Disease 2** in
order that you have underpinning knowledge of the subject.

- Please complete prior to self-checking your responses and
self-assessing your knowledge of this subject.

**Review lectures of: Development of oral mucosa, junctional epithelium,
immunology, dental plaque biofilm, virulence factor, Periodontal
Disease-Microbiology**

**'Host Defences' pdf**

You will need to complete the workbook to meet the intended learning
outcomes:

- Define periodontitis

- Recall the development and role of plaque biofilm in periodontal
disease

- Review the tissues of the periodontium

- List at least 3 types bacteria thought to be associated in the
pathogenesis of periodontal disease and review the virulence factors
deployed in the process

- Outline the host defence in the oral cavity, with reference to the
innate and acquired immune responses

- Describe the functions of cytokines, prostaglandins and matrix
metalloproteinases (MMPs) in the host response

- Describe the basic factors which may contribute to the initiation of
periodontitis

**Periodontitis**

1. Define the term periodontitis:

**Caused by a microbial infection that causes an inflammatory
response leading to irreversible destruction of the periodontal
tissues and supporting structures.**

**Development and role of plaque biofilm in periodontal disease**

2. Define the term **plaque biofilm**

**One or more communities of micro-organisms embedded within an
extra cellular matrix.**

3. Composition of dental plaque biofilm:

Intra-cellular Matrix

Organic

**Proteins\
Glycoproteins\
Polysaccharides\
Lipids\
Intra-cellular matrix\
**

Inorganic (sources between supra & sub)

**Calcium\
Sodium\
Phosphorous\
Potassium\
**

4. Complete the four stages of dental plaque biofilm formation:

1. Initial attachment of bacteria to pellicle

2. Initial colonisation of the tooth surface -- new bacteria join

3. Secondary colonisation -- production of extracellular slime layer

4. Mature biofilm formation - mushroom shaped colonies

**Tissues of the periodontium**

5\. Name the three distinct parts of the gingival epithelium with a
description of where they are found.

a\) Oral epithelium -- keratinised stratified squamous -- what you can
see in the mouth covering free and attached gingiva -- keratinised for
protection against mechanical stress.

b\) Sulcular epithelium -- non keratinised stratified squamous -- faces
tooth but not in contact -- semi-permeable allows for gingival
crevicular fluid to flow -- lines sulcus.

c\) Junctional epithelium -- non keratinised stratified squamous -- joins
gingiva to tooth -- tightly packed epithelial cells and desmosomes --
base of sulcus.

6\. Label the tissues of the periodontium: (a, b, c, d from top to
bottom)

a\) Gingivae

b\) Periodontal ligament

c\) Cementum

d\) Alveolar bone


**Bacteria associated in the pathogenesis of periodontal disease and
their virulence factors**

7. The subgingival environment supports mainly anaerobic bacteria.

True

False

8. Name at least 3 bacteria species found to be associated with
periodontal disease

P.gingivallis

T.denticola

T.forsythia

A.actinomycemcomitans

9\. Note some of the virulence factors of named bacteria which enable
them to colonise, invade and damage the periodontium

P.gingivallis --\
Produce gingipains to allow use of gingival crevicular fluid for
nutrients.

Carbohydrate capsule to resist host defences.

T.denticola --

Adherence mechanisms to bind to fibroblasts.

Degrade cytokines -- disruption of host defences.

T.forsythia --

Produces proteases and apoptopic factors -- causes cell death to immune
cells.

A.actinomycemcomitans --

Leukotoxin -- can destroy white blood cells, inhibits immune response.

Produces proteases and toxins -- destroy and invade host epithelial
cells.

**Host defences in the oral cavity, innate and acquired immune
responses**

10\. Which type of immune response will be initiated by plaque in the
first instance?

Innate/primary immune response

a. What are the key components of this immune response?

Inflammatory response, epithelium and saliva.

b. Complete the table:

+-----------------------------------+-----------------------------------+
| Host defence | Role in defence |
+===================================+===================================+
| Inflammatory response | a. What is the **fluid |
| | component**, when does it |
| | form and what is it's |
| | function at this stage? |
| | |
| | Gingival crevicular fluid.\ |
| | Forms from the inflammatory |
| | response to inflammation. |
| | |
| | Rinse out microorganisms from the |
| | sulcus, the higher the |
| | inflammation, the increase in |
| | gingival crevicular fluid. |
| | Contains inflammatory mediators |
| | and antibacterial agents. |
| | |
| | b. Which cells are mainly |
| | involved in the **cellular |
| | response** at this stage and |
| | what is their role? |
| | |
| | PMNs (neutrophils, mast cells, |
| | basophils) and macrophages -- |
| | both attack and removed invading |
| | microorganisms/pathogens. |
+-----------------------------------+-----------------------------------+
| Epithelium | a. How does the epithelium |
| | defend against plaque |
| | microorganisms? |
| | |
| | Physical barrier against plaque |
| | microorganisms, cells tightly |
| | packed and attached to each other |
| | through desmosomes. |
| | |
| | Some parts semipermeable to allow |
| | for flow of gingival crevicular |
| | fluid. |
| | |
| | b. How and when is the |
| | protective function of |
| | epithelium compromised? |
| | |
| | Tissue destruction at the |
| | junctional epithelium leading to |
| | a periodontal pocket. Creates |
| | inflammatory response and |
| | compromises protection function |
| | due to micro ulcerations. |
| | |
| | c. Which cells of the junctional |
| | epithelium secrete cytokines |
| | and Tumour Necrosis Factor |
| | during the initiation of the |
| | inflammatory response in the |
| | gingival tissues? |
| | |
| | KERATINOCYTES |
| | |
| | d. What is the name of the |
| | tissue macrophages which are |
| | responsible for releasing |
| | host defences? |
| | |
| | Langerhans' cells |
+-----------------------------------+-----------------------------------+
| Saliva | What is the role of saliva? |
| | |
| | Stops drying of oral tissues. |
| | |
| | Antimicrobial effect -- Secretory |
| | and serum IgA -- influence |
| | bacteria attachment so more |
| | likely to be swallowed. |
+-----------------------------------+-----------------------------------+

The adaptive immune response is also known as the [specific]
or [acquired] immune response and it is activated when
innate immunity is ineffective in eliminating [pathogens]
and infection becomes established. It is highly specific to a particular
pathogen by recognising it's [antigen] due to immunological
[memory]. Adaptive immunity uses two main mechanisms, known
as [humoral] immunity ([antigen] response) and
[cell-mediated] immunity.

**~~antigen~~ ~~humoral~~ ~~antibody~~ ~~acquired~~ ~~cell-mediated~~
~~memory~~** **~~specific~~ ~~pathogens~~**

a. Humoral Immune response is when antibodies are produced against
agents existing in the humours (extra-cellularly).

Complete the table which relates to the humoral immune response:

+-----------------------------------+-----------------------------------+
| **Mode** | **Function** |
+===================================+===================================+
| Epithelial Langerhans' cells | Present antigenic parts from |
| | pathogens and present to |
| | circulating lymphocytes which |
| | stimulates clonal expansion after |
| | recognising the specific antigen. |
+-----------------------------------+-----------------------------------+
| B-cell lymphocytes | Differentiate into plasma cells |
| | which then release antibody |
| | against the specific antigen |
+-----------------------------------+-----------------------------------+
| Antibody IgG and IgA | Protective function. |
+-----------------------------------+-----------------------------------+
| Locally or systemically produced | Prevent adherence of |
| antibody | microorganisms |
| | |
| | Recognise and neutralise |
| | pathogens to mark for |
| | phagocytosis. |
| | |
| | Work with complement system to |
| | lyse bacteria. |
+-----------------------------------+-----------------------------------+

b. Cell-mediated response does not require the use of antibodies- uses
it's own T-Cell receptor.

+-----------------------------------+-----------------------------------+
| Antigen presentation via | TH cells: |
| Langerhans'/dendritic cells to | |
| T-Cell | - produce cytokines |
| | |
| | - assist B cell differentiation |
| | into plasma cells. |
| | |
| | - activate macrophages and |
| | neutrophils. |

+===================================+===================================+
| Progression from gingivitis to | T-cells have immunoregulatory |
| periodontitis elicits a shift | role |
| from T-cell to B-cell lesions | |
+-----------------------------------+-----------------------------------+

**Cytokines, prostaglandins and matrix metalloproteinases (MMPs) in the
host response**

12\. There are several types of chemical mediators involved in
periodontal disease. They are chemical messengers which link and
regulate the inflammatory response, the immune response and tissue
damage. Research where they are released from and complete the following
table:

+-----------------------------------+-----------------------------------+
| **Mediator type** | **Action/function in |
| | periodontitis** |
+===================================+===================================+
| Cytokines e.g. Pro-inflammatory | What are cytokines? Small |
| IL-1, IL-6 and TNF-α | proteins important for |
| | controlling immune cell growth |
| Anti-inflammatory IL-4 and IL-10 | and activity. |
| | |
| | Action of cytokines in |
| | periodontitis: Pathogens release |
| | pro-inflammatory cytokine that |
| | promote further tissue |
| | destruction. |
+-----------------------------------+-----------------------------------+
| Prostaglandins e.g. PGE\_2 | Bone resorption, chemotaxis, |
| | vascular permeability, dilation. |
+-----------------------------------+-----------------------------------+
| Matrix metalloproteinases (MMPs) | Pro-inflammatory- degrade |
| | connective tissue. |
+-----------------------------------+-----------------------------------+

**Factors contributing to the initiation of periodontitis**

13\. In health and in stable gingivitis, there is a dynamic equilibrium
between dental plaque and the host defences. This equilibrium is
disturbed in periodontitis which tips in favour of tissue damage.
Describe what these factors are (refer to Periodontal disease-
Microbiology session):

\> Microbial -- increased presence of plaque

\> Increased pathogenicity of microorganisms within the biofilm --
virulence factors

\> Compromised host defence

14\. For each of the following theories on the role of bacteria in
periodontal disease, give an **outline** of the hypothesis, identify any
**issues and/or support** for them.

**a) Non-specific Plaque Hypothesis**

Stagnation of plaque biofilm within gingival sulcus leads to gingival
inflammation, periodontal disease and tissue destruction.

Too simplistic

Some cases of gingivitis don't lead to periodontitis

Some patients can have light plaque biofilm and have periodontitis**\
**

**b) Specific Plaque Hypothesis**

As periodontal disease develops, oral microbiota shifts from gram
positive beneficial microbes to gram negative pathogens.

Since been found that gram negative microbes are also found in healthy
and stable periodontal sites.

Gram positive bacteria also have been found in larger amounts within
periodontal pocket sites.

**c) Keystone Pathogen- Host Response Hypothesis**

Keystone species in biofilm can have large effects on communities
regardless of number. Triggers shift to dysbiotic biofilm community and
uncontrolled host response is initiated -- causes damage to periodontal
tissues.

Current evidence demonstrates that immune response and uncontrolled host
inflammatory response cause tissue destruction found in periodontal
disease.