Aggressive Periodontitis Clinical Trial
Official title:
Clinical Evaluation of Systemic Moxifloxacin Compared to Amoxicillin Plus Metronidazole Adjunct to Non-surgical Treatment in Generalized Aggressive Periodontitis: A Randomized Clinical Trial
The objective of this randomized clinical study was to evaluate the effect of systemic
administration of moxifloxacin compared to amoxicillin plus metronidazole combined with
non-surgical treatment in patients with generalized aggressive periodontitis (GAgP) in
6-month follow-up.
A total of 40 systemically healthy patients with GAgP will evaluate in this randomized
clinical trial. Periodontal parameters (plaque index, gingival index, probing depth, bleeding
on probing, clinical attachment level) will be recorded at baseline, 1st, 3rd and 6th month.
Patients will receive either 400 mg moxifloxacin per os once daily or 500 mg metronidazole
and 500 mg amoxicillin per os three times daily for 7 days consecutively.
The American Academy of Periodontology and the European Federation of Periodontology were
reported that patients with GAgP may have benefit from adjunctive administration of
antibiotics. Antibiotics are used as an adjunct to nonsurgical treatment either locally or
systemically. Systemic antimicrobial agents as adjunct to nonsurgical treatment provide
additional benefits over mechanical therapy alone in terms of probing depth reduction and
periodontal attachment gain.
Amoxicillin is a moderate spectrum, bacteriolytic β-lactam antibiotic, and metronidazole
which is active against anaerobic bacteria is a nitroimidazole. scaling and root planing
combination with metronidazole plus amoxicillin therapy was found to be more effective in
suppressing P. gingivalis and eradication of A. actinomycetemcomitans and preventing
re-colonization of A. actinomycetemcomitans because of the synergistic effect of this
combination and their wide spectrum of activity. It was found to be superior to azithromycin,
doxycycline, and metronidazole in the treatment of GAgP.
Quinolones were introduced for use in urinary tract infections in the 1970s. Moxiflocaxin is
a fourth generation fluoroquinolone antibiotic exhibits good tissue penetration and high oral
bioavailability and has improved activity against Gram- positive, aerobic and anaerobes.
Moxifloxacin is used in the systemic treatment of respiratory infections, acute sinusitis,
odontogenic abscesses, osteomyelitis of the mandible and locally in the treatment of
ophthalmic infections.
Moxiflocaxin has good activity against putative periodontal pathogens, including
Porphyromonas gingivalis, Tanneralla forsythia, Prevotella spp, Fusobacterium nucleatum,
Actinomyces spp, Campylobacter rectus, Peptostreptococcus spp. and Aggregatibacter
actinomycetemcomitans, located within biofilm or intracellulary. It was shown that A.a.
strains were highly susceptible to fluoro-quinolones ciprofloxacin and moxifloxacin. Some of
the adjunctive antibiotics are secreted in saliva in insufficient concentrations to inhibit
A.a. Moxifloxacin seems to be secreted in saliva at higher levels than in plasma and may also
concentrate at the site of infection since it penetrates polymorphonuclear granulocytes and
epithelial cells. Moxifloxacin was found to be superior to clindamycin, metronidazole or
doxycycline.
Systemic administration of moxifloxacin as an adjunct to scaling and root planing was found
to be more effective compared to scaling and root planing alone or scaling and root planing
in conjunction with doxycycline in the treatment of severe chronic periodontitis. To best our
knowledge, there is no study that evaluates the effect of moxifloxacin adjunct to scaling and
root planing in the treatment of GAgP.
The aim of this single center, randomized clinical study was to evaluate the impact of
adjunctive systemic moxifloxacin compared to the use of adjunctive systemic amoxicillin and
metronidazole during full-mouth scaling and root planing on the success of the treatment of
patients with GAgP with 6-month follow-up. The hypothesis was the use of adjunctive systemic
moxifloxacin would provide the similar clinical results as adjunct systemic amoxicillin and
metronidazole during scaling and root planing.
This study was a single-center, randomized, parallel-design clinical trial with 6 month
follow-up. It was conducted at Kocaeli University, Faculty of Dentistry, Department of
Periodontology between 2011-2013. The study protocol was approved by the Ethics Committee of
the Medical Faculty of Kocaeli University (KOU KAEK 5/9) and was conducted in accordance with
the Helsinki declaration of 1975, as revised in 2000.
The GAgP patients were recruited from patients seeking periodontal treatment at Kocaeli
University, Faculty of Dentistry, Department of Periodontology, Kocaeli, Turkey.
Approximately, 12.000 patients were screened the dates between June 2011 and September 2012.
A complete medical, dental, periodontal and radiographic examination was performed. The study
protocol explained to the patients. From patients who willing to participate to the study,
written informed consent was obtained and included the study.
The periodontal diagnosis of subjects with GAgP was established on the basis of clinical and
radiographic criteria defined by the 1999 International World Workshop for a Classification
of Periodontal Diseases and Conditions. Patients were included if they were between 18 and 35
years of age and otherwise healthy. The bone loss estimation was radiographically performed
in each patient for the assessment of the extent and severity of alveolar bone loss. Medical
and dental histories were questioned. Subjects were excluded if they had any known systemic
diseases or conditions that can/could influence the periodontal status (cancer,
cardiovascular and respiratory diseases), history of hepatitis or HIV infection,
immunosuppressive chemotherapy, current pregnancy, planning a pregnancy or lactation,
requirement for antibiotic prophylaxis, oral diseases other than GAgP, ongoing orthodontic
therapy, a history of antibiotic therapy or periodontal treatment within the preceding six
months. Subjects were excluded if they had known allergies to quinolones or penicillin or
metronidazole.
Periodontal Examination The full-mouth clinical periodontal measurements were recorded at 6
sites per tooth (mesio-buccal, mid-buccal, disto-buccal, disto-lingual, mid-lingual, and
mesio-lingual) including plaque index (PI), gingival index (GI), probing depth (PD), bleeding
on probing (BOP) and clinical attachment level (CAL). CAL was calculated from the
cement-enamel junction to the base of the periodontal pocket. Williams periodontal probe was
used for periodontal measurements. All measurements and scaling and root planing were
performed by the same single calibrated and trained periodontist in a standardized manner.
Allocation concealment The patients were randomly assigned to one of the study groups. To
ensure complete masking of allocation, before the recruitment of the patients, forty
identical, opaque-colored, impermeable plastic bags which include toothbrush, interproximal
brush, toothpaste and either moxifloxacin or amoxicillin and metronidazole were prepared and
coded. A code number was given to each subject. Randomization codes were kept separately from
the clinical evaluation forms by one of the authors until the treatment and follow-up visits
were completed. The examiner who performed the treatment was unaware of the allocation.
Prior to treatment, all subjects were gone through motivation sessions for oral hygiene.
Following to periodontal measurements, full-mouth supragingival scaling using ultrasonic
scaler and polishing were performed, and a toothbrush, toothpaste and an interproximal
toothbrush were provided to all subjects. One week later, the patients were examined for
plaque accumulation and oral hygiene. The patients who cannot maintain proper oral hygiene
were excluded from the study. Only 39 patients fulfilled the qualification criteria for
enrollment for the present study.
Subjects were randomly assigned to receive one of the two treatment groups. Moxifloxacin
group received scaling and root planing and an adjunctive systemic antibiotic, 400 mg
moxifloxacin, once in a day for 7 days and amoxicillin and metronidazole group received a
combination of 500 mg of amoxicillin and 500 mg metronidazole three times per day for 7 days.
The subjects were instructed to take first dose of the antibiotics in the morning of the
first session since the microorganisms are organized on the root surface and protected from
antimicrobial agents. Scaling and root planing were performed on 2 consecutive days in 24
hours under the local anesthesia. On each day, scaling and root planing were performed in 2
quadrants using ultrasonic scalers and manual instruments . The endpoint of scaling and root
planing was a tactile smooth root surface.
The subjects were insistently informed about the intake of the antibiotics properly, and they
asked to inform the researches if they needed to take another antibiotics or
anti-inflammatory agents for another reason during and following the study for 6 months.
Patients used a 0.2% chlorhexidine digluconate rinse twice a day for a month and brushed
their teeth by tooth brushes and interproximal tooth brushes twice a day. Patients asked to
report any adverse events and side effects of the antimicrobial agents as soon as possible.
Subjects were monitored one week after the second scaling and root planing session. At this
session, antibiotic intake, adverse events and side effects were questioned; oral hygiene and
plaque accumulation were controlled. Subjects were screened at 1, 3 and 6 months after
completion of nonsurgical treatment. During these sessions, clinical periodontal parameters,
any medical history change, especially, whether antibiotic therapy had been prescribed for
any reason was recorded. At the end of these sessions, supragingival scaling was performed,
if needed.
The present study was conducted within in the same clinic, and the patients were taken to the
same dental chair and treated with a same experienced periodontist for to discard
discrepancies and to provide standardized and controlled environment.
Sample size calculation
The primary outcome variable was probing depth changes. The sample size was calculated based
on previous information from a study conducted in our department, using data relative to the
mean difference and standard deviation (SD) between the experimental periods for the probing
depth parameters.57 Considering a mean probing depth difference of 1.3 mm between evaluation
periods, it was estimated that 13 patients for each group would be necessary to provide 95%
power (0.54 SD, α error of 0.05, and β error of 0.2).58 However, we aimed to recruit 20
patients to each group if we lose to follow the patients during the study.
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