Does the Non-surgical Application of Enamel Matrix Derivative Reduce the Need of Periodontal Surgical Intervention in Subjects With Severe (Stage III) Periodontitis?

Periodontal Diseases Clinical Trial

Official title:

Does the Non-surgical Application of Enamel Matrix Derivative Reduce the Need of Periodontal Surgical Intervention in Subjects With Severe (Stage III) Periodontitis? A Randomized, Multicenter, Clinical Trial

Clinical Trial Details — Status: Recruiting

Administrative data

• NCT number: NCT05418621
• Other study ID #: PERIO-EMD 3
• Status: Recruiting
• Phase: Phase 3
• Start date: March 1, 2021
• Est. completion date: June 2025

Study information

• Verified date: November 2022
• Source: University of Pisa
• Contact: n/a
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

Periodontal treatment relies on a sequential series of different phases that are usually incapsulated in three main phases: non-surgical treatment, surgical phase and, finally, supportive phase. Whilst, on the one hand not all patients may undergo surgical interventions, on the other hand non-surgical periodontal and supportive treatment are administered to all subjects affected by periodontitis. Both phases are constituted by closed, non-surgical, root instrumentation which is often carried out with similar techniques. Thus, non-surgical periodontal treatment (NSPT) is the one key stone of the treatment of periodontitis.

NSPT is very efficacious. A significant majority of the diseased sites are usually managed non-surgically (Graziani et al., 2017)). Moreover, bleeding on probing and symptoms are significantly decreased by NSPT. Importantly, NSPT is also capable to reduce systemic inflammation (Teeuw et al., 2014), improve glycaemic control (Sanz et al., 2018) and overall ameliorate oral health related quality of life (Graziani, Music, et al., 2019). Lastly, NSPT is cost effective as its costs are moderate and it may be performed by both dentists and hygienists.

Nevertheless, NSPT is often uncapable to solve an entire clinical case and surgical treatment is advocated as in fact the complete closure of the pockets ranges from 57 to 75% according to a follow-up of 3⁄4 months or 6/8 respectively (Solini et al., 2019). Periodontal surgery is also effective, but it is nonetheless a surgical intervention which cannot be defined as deprived of side effects (Graziani et al., 2018).

Thus, in order to improve the outcome of NSPT numerous adjunctive treatment modalities have been advocated (Braun et al., 2008; Graziani et al., 2017; Haffajee et al., 2003). Yet the objective of reducing the need for surgery has been rarely evaluated.

Recently, our group ran a trial in which enamel matrix derivatives (EMD) has been applied as non-surgical adjunct. The findings highlighted that EMD application lowers systemic inflammation, increases blood clot stability and, locally, reduces of the need for surgery by 32% compared to the control group without EMD.

Thus, a multicentre responding to the following questions:

• Flapless application of EMD reduce the need for periodontal surgery?

• Are the results stable over time?

• Can the results be generalized among different clinicians? EMD is a resorbable, implantable material and supports periodontal regeneration, which takes place over more than a year. It consists of hydrophobic enamel matrix proteins extracted from developing embryonal enamel of porcine origin in a propylene glycol alginate carrier.

The gel has a suitable viscosity to facilitate application directly onto root surfaces exposed during periodontal surgery. Once applied onto an exposed root surface the protein self assembles into an insoluble three-dimensional matrix and creates a suitable environment for selective periodontal cell migration and attachment, which re-establishes lost tooth supporting tissues. Subsequent to formation of new attachment, alveolar bone can also be regenerated due to the osteogenic capacity of the restored periodontal ligament. EMD is degraded by enzymatic processes of normal wound healing.

Recruitment information / eligibility

• Status: Recruiting
• Enrollment: 140
• Est. completion date: June 2025
• Est. primary completion date: September 2024
• Accepts healthy volunteers: No
• Gender: All
• Age group: 18 Years and older

Eligibility

Inclusion Criteria

• Accept the form of the study and signs a declaration of informed consent; understand and are willing, able and likely to comply with all study procedures and restrictions.

• Systemically healthy (according to exclusion criteria 4) participants of either genders who are attending a periodontal centre for periodontal care.

• Aged 18 or over.

• Presenting at least 20 teeth (excluded wisdom teeth).

• Being affected by generalized Periodontitis (stage III) irrespectively of the grade (Tonetti et al., 2018) i.e. presenting at least 5 mm of clinical atattachment loss at the interdental areas, radiographic bone resorption of more than 30% of the root length extending to at least the middle portion of the root, less than 5 teeth lost for periodontal reason, presenting characteristics for complexity (intrabony defects, furcation defects, moderate ridge defects)

• Bleeding on probing on at least 30% of the sites and a minimum of 4 teeth with at least one site with PPD =6mm

Exclusion Criteria:

• Persons incapable of responding to the questions.

• An employee of the sponsor, employee of the general dental practice, and/or a family relative of the employees mentioned above.

• Women known to be pregnant or lactating (a specific declaration form will be signed by the patient, stating the non-pregnant or lactating status).

• Persons suffering of pathologies known to affect the outcome of periodontal therapy (i.e. diabetes, osteoporosis, immunosuppression).

• Persons undergoing therapy which will may complicate adherence to protocol or showing an impact on periodontal outcome (i.e. chemotherapy and immunosuppressive treatments).

• Persons who require antibiotic coverage (following infectious endocarditis, using prosthetic cardiac valves, other pathologies).

• Persons undergoing pharmacological treatment associated with gingival hypertropia development (phenytoin, phenobarbital, lamotrigine, vigabatrin, ethosuximide, topiramate, primidone, nifedipine, amlodipine, verapamil, cyclosporine).

Persons with implant-supported restorations affected by peri-implantitis (as defined by the 2017 Classification, i.e. presence of bleeding and/or suppuration on gentle probing, probing depths of =6 mm, bone levels =3 mm apical of the most coronal portion of the intraosseous part of the implant).

• Smokers declaring to smoke more than 20 cigarettes per day.

• Persons with Body Mass Index above 29(obese subjects).

• Anyone who in the investigators' opinion is not suitable to take part in the study.

• Allergy/idiosyncrasy to anaesthesia or components of the device object of the study.

• Previous periodontal subgingival instrumentation within the previous 12 months.

• Antibiotics intake in the previous 3 months.

Related Conditions & MeSH terms

• Periodontal Diseases
• Periodontitis

Intervention

Drug:
• Enamel Matrix Derivative application
in the test group, EMD (Emdogain FL®, Institute Straumann AG, Basel, Switzerland) will be applied with a dedicated syringe until overflowing from the pocket border, taking particular care in avoiding trauma to the tissues.

Other:
• Saline application
in the control group, a lavage of sterile saline will be applied with a syringe with a thin blunt tip until overflowing from the pocket border, taking particular care in avoiding trauma to the tissues.

Locations

Country	Name	City	State
Italy	Azienda Ospedaliero Universitaria Pisana	Pisa
Italy	University Hospital of Pisa	Pisa

Sponsors (1)

Lead Sponsor	Collaborator
University of Pisa

Country where clinical trial is conducted

Italy, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Primary	Resolved cases	inter-group differences in % of cases, patient-level analysis, with complete absence of sites with Probing Pocket Depth (PPD) >=6mm	3, 6 and 12 months after treatment
Secondary	number of sites with PPD>=6mm	Intra-group and intergroup changes in % and number of sites with PPD>=6mm. The Probing Pocket Depth (PPD) will be measured as the distance between the gingival margin and the deepest part of the gingival pocket measured through a University of North Carolina -15 periodontal probe (UNC-15) (Hu-Friedy, USA). PPD will be evaluated at 6 sites on each tooth: disto-buccal, buccal, mesio-buccal, disto-lingual, lingual, mesio-lingual. Each measure will be rounded to the nearest millimetre probe.	3, 6 and 12 months after treatment
Secondary	changes in Full Mouth Plaque Score (FMPS)	intragroup and intergroup change in Full Mouth Plaque Score. The Full Mouth Plaque Score (FMPS) will be measured as the presence or absence of plaque on each tooth surface will be assessed. The bacterial deposits are stained with a plaque-disclosing solution (erythrosine). Areas adjacent to the gingival margins that exhibit an intense staining that can be easily removed with the edge of the probe will be dotted as having plaque. The presence of plaque will be evaluated as 1, while the absence as 0 on 6 areas per tooth (disto-buccal, buccal, mesio- buccal, disto-lingual, lingual, mesio-lingual). A dedicated diagram (see attached medical records, chapter 16) will allow to draw the overall plaque accumulation and mean plaque score will be indicated in percentage (% of sites found positive for the presence of plaque on the total of 6 sites per tooth (O'Leary et al., 1972).	3, 6 and 12 months after treatment
Secondary	changes in Full Mouth Bleeding Score (FMBS)	intragroup and intergroup change in Full Mouth Bleeding Score. The Full Mouth Bleeding Score (FMBS) will be measured dichotomously after periodontal probing. It will be considered positive when the bleeding occurs after the retraction of the probe (approximate time for evaluation 30 seconds after probe insertion). It will be considered negative when there is no bleeding. The mean bleeding score is indicated in percentage (% of sites detected positive for bleeding on the total 6 sites per tooth )(Ainamo & Bay, 1975).	3, 6 and 12 months after treatment
Secondary	mean values of PPD	Intra-group and intergroup changes in terms of full mouth mean values of PPD. The Probing Pocket Depth (PPD) will be measured as the distance between the gingival margin and the deepest part of the gingival pocket measured through a University of North Carolina -15 periodontal probe (UNC-15) (Hu-Friedy, USA). PPD will be evaluated at 6 sites on each tooth: disto-buccal, buccal, mesio-buccal, disto-lingual, lingual, mesio-lingual. Each measure will be rounded to the nearest millimetre probe.	3, 6 and 12 months after treatment
Secondary	mean values of recession (REC)	Intra-group and intergroup changes in terms of full mouth mean values of REC. The Recession (Rec) will be measured as the distance in mm from the cement-enamel junction (CEJ) to the gingival margin measured through UNC- 15. In the event that CEJ would not be available, one of the following clinical landmarks will be used: crown margin, restored margin, occlusal point.	3, 6 and 12 months after treatment
Secondary	mean values Clinical Attachment Level (CAL)	Intra-group and intergroup changes in terms of full mouth mean values of CAL. CAL will be calculated as the sum of PPD and REC.	3, 6 and 12 months after treatment
Secondary	Furcation involvement	Intragroup and intergroup changes in terms of furcations degree. Furcation (FI): furcation involvements will be classified according to horizontal probing with Naber's probe in degree I when the probe can enter the orifice of the furcation, degree II when the probe can enter the furcation freely without passing it completely. Class III will be scored when the tip of the Nabers probe will see appearing through the opposite cervice, i.e. "through-and.through" furcation in both mandibular and maxillary molar (Hamp et al., 1975).	3, 6 and 12 months after treatment
Secondary	Dentine sensitivity (Schiff test)	Intra-group and intergroup changes of dentine hypersensitivity as measured with the Schiff test. Schiff test: dentine sensitivity will be assessed trough the study timepoints as reported further using a validated a well described test as the Schiff test (Schiff et al., 1994). The Schiff test is a non-invasive and safety test that consist in spraying air on the tooth and collecting the reaction of the patient in a liker type scale as follows: 0 Subject does not respond to air stimulus; 1 Subject responds to air stimulus but does not request discontinuation of stimulus; 2 Subject responds to air stimulus and requests discontinuation of stimulus; 3 Subject responds to air stimulus, considers stimulus to be painful and requests discontinuation of stimulus.	3, 6 and 12 months after treatment
Secondary	Oral Health Impact profile 14	Oral Health Index Profile-14 (OHIP-14): a validated questionnaire of 14 question aiming at assessing statements grouped in 7 conceptual subscales: functional limitation, physical pain, psychological discomfort, physical disability, psychological disability, social disability and handicap. It allows an evaluation of the OHRQoL (Slade, 1997). The higher the score, the higher the impact of periodontitis on the patients quality of life	3, 6 and 12 months after treatment
Secondary	Attention Network Task	Attention Network Task (ANT; Fan et al., 2002): a task designed to test three attentional networks: alerting, orienting, and executive control.The higher the score, the higher the cognitive abilities.	3, 6 and 12 months after treatment
Secondary	Corsi block-tapping test	Corsi block-tapping test (CBTT; Orsini et al., 1987): a task to assess visuo-spatial short-term memory. The higher the score the better the cognitive ability	3, 6 and 12 months after treatment
Secondary	Tower of London	Tower of London (ToL; Shallice, 1982): a task designed to evaluate problem-solving and planning capabilities.The higher the score the better the cognitive abilities	3, 6 and 12 months after treatment
Secondary	Sickness Questionnaire	Sickness Questionnaire ( SicknessQ ; Andreasson et al., 2018): a brief instrument, composed of 10 items, aimed to assess perceived sickness behaviour. The higher the score the higher the perceived thickness	3, 6 and 12 months after treatment
Secondary	Depression Anxiety Stress Scale	Depression Anxiety Stress Scale - 21 (DASS-21; Lovibond & Lovibond, 1995): self - report questionnaire designed to assess the symptoms of depression, anxiety and stress. The higher the score the higher the symptoms of depression, anxiety and stress.	3, 6 and 12 months after treatment
Secondary	State-Trait Anxiety Inventory_ Form	State-Trait Anxiety Inventory_ Form Y2 ( STAI_Y2; Spielberger, 1983): self - report questionnaire aimed to investigate trait anxiety that refers to relatively stable individual differences in anxiety proneness, that is, to differences between people in the tendency to perceive stressful situation as dangerous or threatening. The higher the score the higher the tendency os being prone to anxiety.	3, 6 and 12 months after treatment
Secondary	State-Trait Anxiety Inventory_ Form Y1	State-Trait Anxiety Inventory_ Form Y1 ( STAI_Y1; Spielberger, 1983): self - report questionnaire aimed to investigate trait anxiety that refers to a palpable reaction or process taking place at a given time and level of intensity. The higher the score the higher the trait of anxiety assessed.	3, 6 and 12 months after treatment
Secondary	Profile Mood State	Profile of Mood State (POMS; Grove, Robert & Prapavessis, 2016): self - report questionnaire aimed to investigate different mood states like.: tension, depression, anger, fatigue, confusion and vigour.	3, 6 and 12 months after treatment
Secondary	Sleep quality	Pittsburgh Sleep Quality Index (PSQI; Buysse et al., 1989): self-assessment scale that provides a reliable, valid and standardized measure of sleep quality. The higher the score the better the sleep quality	3, 6 and 12 months after treatment
Secondary	The Insomnia Severity Index	The Insomnia Severity Index (ISI; Morin, 1993): is a self-report questionnaire designed to assess the nature, severity and daytime impact of insomnia. The higher the score the higher the severity of insomnia.	3, 6 and 12 months after treatment
Secondary	Epworth Sleepiness Scale	Epworth Sleepiness Scale (ESS; Johns, 1991): is a self-assessment tool consisting of 8 items that investigate the general level of daytime sleepiness or the propensity to sleep during different situations of daily life. The higher the score the higher the daily sleepiness.	3, 6 and 12 months after treatment