Dynamic analyses of a soft tissue–implant interface: Biological responses to immediate versus delayed dental implants

Author:

Aellos Fabiana1ORCID,Grauer Joseph A.12,Harder Kasidy G.13,Dworan Julia S.14,Fabbri Giacomo5,Cuevas Pedro L.1,Yuan Xue6ORCID,Liu Bo1,Brunski John B.1,Helms Jill A.1ORCID

Affiliation:

1. Department of Surgery Stanford University School of Medicine Stanford California USA

2. Dr. Gerald Niznick College of Dentistry University of Manitoba Winnipeg Manitoba Canada

3. Max Rady College of Medicine University of Manitoba Winnipeg Manitoba Canada

4. Department of Anatomy Center for Anatomy and Cell Biology, Medical University of Vienna Vienna Austria

5. Private Practice Ban Mancini Fabbri Dental Clinic Cattolica Italy

6. Department of Otolaryngology‐Head and Neck Surgery School of Medicine, Indiana University Indianapolis Indiana USA

Abstract

AbstractAimTo qualitatively and quantitatively evaluate the formation and maturation of peri‐implant soft tissues around ‘immediate’ and ‘delayed’ implants.Materials and MethodsMiniaturized titanium implants were placed in either maxillary first molar (mxM1) fresh extraction sockets or healed mxM1 sites in mice. Peri‐implant soft tissues were evaluated at multiple timepoints to assess the molecular mechanisms of attachment and the efficacy of the soft tissue as a barrier. A healthy junctional epithelium (JE) served as positive control.ResultsNo differences were observed in the rate of soft‐tissue integration of immediate versus delayed implants; however, overall, mucosal integration took at least twice as long as osseointegration in this model. Qualitative assessment of Vimentin expression over the time course of soft‐tissue integration indicated an initially disorganized peri‐implant connective tissue envelope that gradually matured with time. Quantitative analyses showed significantly less total collagen in peri‐implant connective tissues compared to connective tissue around teeth around implants. Quantitative analyses also showed a gradual increase in expression of hemidesmosomal attachment proteins in the peri‐implant epithelium (PIE), which was accompanied by a significant inflammatory marker reduction.ConclusionsWithin the timeframe examined, quantitative analyses showed that connective tissue maturation never reached that observed around teeth. Hemidesmosomal attachment protein expression levels were also significantly reduced compared to those in an intact JE, although quantitative analyses indicated that macrophage density in the peri‐implant environment was reduced over time, suggesting an improvement in PIE barrier functions. Perhaps most unexpectedly, maturation of the peri‐implant soft tissues was a significantly slower process than osseointegration.

Funder

Osteology Foundation

Publisher

Wiley

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