Obese Clinical Trial
Official title:
Relationship Between Obesity and Periodontal Disease
Obesity is an epidemic with increasing prevalence in the Asia Pacific region. The first
Malaysian national estimate in 1996 of obesity was 5.8%. A systematic review reported a
marked increase in obesity in 2003, 2004 and 2006 with 12.2%, 12.3% and 14.0% respectively.
Periodontal disease is a chronic inflammatory disease which results in gingival
inflammation, irreversible attachment loss, alveolar bone destruction and eventually tooth
loss. Worldwide, the prevalence of periodontitis in the adult population is about 10-15%.
Periodontal disease, through inflammation and destruction of the periodontium produces
clinical signs and symptoms, some of which may have a considerable impact on quality of life
(QoL).
A positive association between obesity and periodontal disease was repeatedly demonstrated
worldwide. Obese individuals have elevated levels of circulating TNF- α and IL-6 compared to
normal weight individuals. These cytokines decrease after weight loss. Adipokines produced
by adipose tissue could be one of the mechanisms mediating the association between obesity
and periodontal disease. This suggests that obesity may have the potential to modify the
host's immunity and inflammatory system.
This project will extend the existing information on the association between obesity and
periodontal disease including QoL aspect to a Malaysia population. It will also improve
knowledge on the cellular and molecular mechanisms that underpin obesity-periodontal disease
relationship. By extension, this study also will cast light on the effects of periodontal
interventions for the subgroup population.
Obesity is an epidemic with increasing prevalence in most countries in the Asia Pacific
region. It is characterized by abnormal or excessive lipid deposition as a result of chronic
disproportion between energy intake and energy outflow. The first Malaysian national
estimate in 1996 of obesity was 5.8%. A systematic review reported a marked increase in
obesity in 1996, 2003, 2004 and 2006 with 5.5%, 12.2%, 12.3% and 14.0%. Obesity is highest
among adults of 40-59 years old, is greater risk in women compared to men and is highest
among Indians followed by Malays, Chinese and Aboriginals.
Periodontitis and obesity are both chronic health problems, and an association between the
two conditions exists. A positive association was repeatedly demonstrated between obesity
and periodontal disease in multiple studies around the world.
Periodontal disease is a chronic oral infection, in which destruction of tooth supporting
structures, periodontal ligament and alveolar bone occurs, leading ultimately to tooth loss.
Worldwide, the prevalence of periodontitis in the adult population is about 10-15%. In
Malaysia, the National Oral Health study reported 90.2% of the adults presented with some
forms of periodontal conditions. About 5.5% of these subjects had deep pockets of 6 mm or
more.
Periodontal disease, through inflammation and destruction of the periodontium produces a
wide range of clinical signs and symptoms, some of which may have a considerable impact on
quality of life (QoL). A study conducted using a community sample found a significant
association between periodontal disease and quality of life (QoL). They also found that
self-reported symptoms of periodontal diseases such as swollen gums, sore gums and receding
gums has an apparent impact on the quality of life of the person. With the mechanism of
obesity, it is expected that the obese patients may have experienced more severe periodontal
diseases and hence they may experience more impact on the quality of life. However, the
evidence is still lacking.
Cytokines play a role in the pathogenesis of periodontitis. They play an active role in
wound repair and in transient inflammation. They also activate defence mechanisms in which
they may give rise to considerable tissue damage in severe inflammation.
Adipose tissue cells namely adipocytes, preadipocytes and macrophages secrete protein
signals collectively known as adipokines or adipocytokines. Adipokines are involved in
inflammation and the acute-phase response. Production of adipokines increased in obesity,
and raised circulating levels of several acute-phase proteins and inflammatory cytokines.
This has led to the concept that obese is a state of chronic low-grade systemic inflammation
causally link to insulin resistance and metabolic syndrome.
Salivary components comprising of several inflammatory and immune mediators have been
identified which are involved in periodontal destruction. Among all the adipokines, resistin
which is an adipocyte-derived cytokine is raised in obese mice. In humans, it is suggested
that resistin is largely expressed from neutrophils, macrophages, and monocytes other than
adipocytes. Resistin is identified as a proinflammatory adipokine that potentially links
obesity to diabetes. It is also believed that human resistin stimulates the production and
secretion of other proinflammatory molecules like tumor necrosis factor (TNF)-α and
interleukin (IL)-12. Studies have shown high levels of resistin in subjects having chronic
periodontitis and this may affect systemic health. In a study by Devanoorkar et al., stated
that the decrease in the resistin levels was not statistically significant following
non-surgical periodontal therapy.
The reason for the interest in GCF/serum levels of resistin in periodontitis lies in the
fact that epidemiological research indicates that periodontitis interplays between obesity
and diabetes mellitus. It is possible that raised levels of resistin in periodontitis can
explain at least in part the link between periodontitis and other chronic inflammatory
diseases. Therefore, the overall aim of this systematic review was to provide evidence of
resistin biomarker in chronic periodontal disease which might underpin the relationship
between periodontal disease, diabetes and obesity. Evidence from case-control studies are
all summarized and evaluated.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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