Peri-implant Mucositis Clinical Trial
Official title:
The Use of Non-Steroidal Anti-Inflammatory Drugs as a Tool of Positive Change in Peri-Implants Mucositis Microbiome
Dental implants are often used to replace missing teeth. In fact, in the US over 700,000
implants are places every year and over 2 million implants are places world wide.
Peri-implant mucositis in an inflammatory condition affecting dental implants and is
recognized as a risk factor for peri-implantitis (a condition affecting the bone around
implants and eventually leading to implant loss). The prevalence of Peri-implant Mucositis
has been reported in the literature to range from 50-90% whereas the prevalence of
Peri-implantitis has been reported as high as 20%. it is commonly believed that a dysbiotic
microbiome is the primary cause for these conditions.
The inflammatory burden around diseased implants creates a high-protein environment which is
necessary for the survival of pathogenic bacteria. It is logical, therefore, that reducing
inflammation by Non Steroidal Anti-Inflammatory Drugs (NSAIDs) may create a shift in the
dysbiotic microbiome to a symbiotic microbiome. The aim of the current study is to test the
effects of oral NSAIDs on the peri-implant microbiome.
Inflammation around dental implants has been defined as Peri-implant mucositis and
Peri-implantitis . Peri-implant mucositis is a localized inflammation limited to the mucosal
tissue surrounding the implant whereas peri-implantitis has advanced to the bone surrounding
the implant as well. The prevalence of Peri-implant Mucositis has been reported in the
literature to range from 50-90% whereas the prevalence of Peri-implantitis has been reported
as high as 20%. Due to the fact that there are many similarities in the clinical
manifestations of infection in the gingiva and peri-implant mucosal tissue, studies
attempted to compare the microbial characteristics around teeth to that found around
implants. Emerging data suggests that the microbiome around infected teeth has some
similarities and dissimilarities to peri-implant infection. Such differences may stem from
different inflammatory characteristics as well as the presence of a non-vital foreign
material (the dental implant) in the area. Some of the known pathogenic strains identified
in the peri-implant sulcus are anaerobic a-saccharolytic bacteria, which feed off the
adjacent tissue inflammatory exudate. Logically, attenuation of the inflammation would
deprive the nearby bacteria of nourishment needed to sustain their growth.
The use of non-steroidal anti-inflammatory drugs (NSAID) to control chronic inflammatory
disease has been used extensively in medicine. Its action of blocking cyclooxygenase
inflammatory pathway and in-effect blocking the production of Prostaglandin-E2 (PGE2) has
led to its use with general pain control as well as its long term use in the treatment of
tissue inflammation and pain caused by rheumatoid arthritis or osteoarthritis, tendinitis
and bursitis.
Offenbacher et al. as early as in 1981 discovered that patients with periodontitis had
significantly higher levels of PGE2 in the sulcular fluid between gingiva and the tooth
(GCF) . In a follow up study over a period of 18-36 months, Offenbacher observed that
patients who had exhibited periodontal attachment loss had significantly higher levels of
PGE2. This led Williams et al. to study the effects of Flurbiprofen, a phenylalkanoic
derivative family of of non-steroidal anti-inflammatory drugs, on naturally occurring
periodontal disease in an animal model over a period of 12 months. The study demonstrated
decreases in alveolar bone loss in flurprofen treated animals at 3, 6 , 9 and 12 months.
William et al then followed with a clinical trial where 44 patients who self administered
peroral flurbiprofen twice daily for a period of 24 months. The study reported severely
depressed bone loss rates over the period of the trial and as early as 6 months after
administration of flurbiprofen that continued over the length of the trial. Other studied
the drugs effect on other more aggressive forms of the disease with similar results . These
results have been duplicated around implants as well. Jeffcoat et al demonstrated that oral
intake flurbiprofen helped reduce bone loss around implants in the first year of service.
Reddy similarly demonstrated with use of digital subtraction radiography, flurbiprofen taken
orally was able to help increase bone density and apposition around implants after just 4
months.
The positive effect of systemic antibiotics and as well topical anti microbials on the
pathogenic bacteria in the gingiva sulcus and peri-implant crevice has been well documented
and is indisputable. The removal of these bacteria has helped promote tissue health. Similar
results have been documented around implants as well. However more recently the reverse
approach to disease control has gained popularity. Instead of trying just to reduce the
bacterial challenge through antimicrobial/antibiotic therapy, modulating the host response
to decrease the inflammatory destruction of the tissue, could be a more efficient and
effective way of controlling the disease In decreasing the inflammatory environment, the
pathogenic bacteria feeding off the inflammatory exudate would be greatly decreased,
effecting a major change in the microbiome. To date nobody has characterized this change.
The purpose of the study is to test the effects of oral NSAIDS on the peri-implant
microbiome. Also, clinical parameters will be tested for correlation with the microbial
findings.
Methods:
The study design is random controlled double blind clinical trial. Patients visiting the
graduate periodontal clinic at the Hadassah Medical Center will be examined for eligibility
for the study. Implants with peri-implant mucositis (clinical signs of inflammation without
radiographically bone loss) will be included. Patients (n=50) will undergo clinical
examination (which will include probing depths, presence or absence of suppuration and
bleeding on probing) and sampling of the subgingival bacterial deposits using a perio-strip.
Patients will be randomly assigned to the experimental flurbiprofen group (100 mg bid) or
placebo group (n=25 for each group). Drug consumption will be set for the duration of 2
weeks. At the end of drug intake period (day 14) and two weeks afterwards (day 28) all
subjects will be re-examined, which will include a new clinical exam and sampling of the
subgingival bacterial deposits. The microbiological samples will be analyzed using 16s
Ribosomal Pyro-sequencing. The microbiome profile of the Flurbiprofen group before and after
treatment and two weeks post-treatment will be compared. as well as the microbiome from the
placebo group compared with the Flurbiprofen group. Statistical differences will be
evaluated using ANOVA with Bonferroni correction. Correlation between the clinical
parameters and microbiological parameters will be tested using Pearson correlation.
Significance:
The study asks the question whether the use of a well-known NSAID that had proven beneficial
effects in maintaining the mucosal tissue integrity around implants and help control and
prevent peri-implant inflammation. Studies have shown that implants placed 5 years
previously will most likely have some form of peri-implant mucositis . Just as gingivitis
can lead to periodontal disease, Peri-implant mucositis can lead to peri-implantitis a more
destructive inflammatory disease that puts implant survival in jeopardy. Therefore, a drug
that can limit the amount of destructive bacteria around the implant can be a very effective
non-invasive method of treatment. Additionally with the use of a more comprehensive
taxonomical identification of the peri-implant micro-genome, there will be a better
understanding of the bacterial role in the destructive process associated with peri-implant
inflammation
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