EFFECT OF RESTORATIIVE MATERIIALS ON THE DENTAL
PULP
By:dr.heidary
The pulp undergoes histopathological changes in response to irritation or destruction of dentin Pulp injury may result from anoxious stimuli due to several factors: Biological → dental cariesPhysical → restorative procedureChemical → restorative material
CYTOTOXICITY AND BIOCOMPATIBILITY OF DIRECTAND INDIRECT PULP CAPPING MATERIALSCalcium hydroxide products are the best choice for conservative treatment of the pulp due to their therapeutic and biological potential and the property of stimulating the formation of sclerotic and reparative dentin as well as protecting the pulp against thermal stimuli.
CYTOTOXICITY AND BIOCOMPATIBILITY OF DIRECTAND INDIRECT PULP CAPPING MATERIALSMonomers present in resin composites and adhesive systems ( BISGMA, UDMA, TEGDMA, HEMA) have been shown to have cytotoxic effects in direct contact with fibroblasts and may be leached during the polymerization when the conversion degree is not fully reached.
CYTOTOXICITY AND BIOCOMPATIBILITY OF DIRECTAND INDIRECT PULP CAPPING MATERIALSdirect pulp capping with adhesive systems produces different degrees of pulp inflammation, even without bacterial presence . Some studies support the idea that when hermetic seal of cavity is obtained, the dentin pulp complex protection materials are unnecessary and they not influence the pulp repair, but hermetic seal of the restoration is difficult to be obtained
CYTOTOXICITY AND BIOCOMPATIBILITY OF DIRECTAND INDIRECT PULP CAPPING MATERIALS RMGICs are more cytotoxic to the pulp cells than conventional GICs due to the presence of unpolymerized monomers, and should not be applied directly to the pulp tissue
RELEASE OF SUBSTANCE Bis-GMA Bis-EMA UDMA TEGDMA EGDMA Methylmethacrylate (MMA) Filler particles (silicon, boron, sodium and barium) Formaldehyde : released into water under certain
circumstances; It is very likely generated by an oxidation of unsatured methacrylate groups
Bisphenol A (BPA): was found in the extract of one pit and fissure sealant and in saliva in contact with resin-based composite. Minute amounts of BPA were detected after placement of UDMA-based and Bis-GMA based composite fillings.
Fluoride
SISTEMIC TOXICITY Estrogenicity Administered intragastrically daily to female mouse display 54.5% reduction in the number of pregnancies vs 100% in control mice
LOCAL TOXICITY AND TISSUE COMPATIBILITY
CytotoxicityInfluence on cell metabolismAntimicrobial propertiesPulp reactionsReactions of gingival and oral mucosa
MECHANISMS OF CYTOTOXICITYUnbound free monomers released by dental resins during polymerization.
Approximately 15–50% of the methacrylic groups remain unreacted.
CYTOTOXICITY
Citotoxicity depends also on: Degree of polymerization
Basic chemistry of the resin matrix (methacrylate-based materials are more toxic)
Filler content
INFLUENCE ON CELL METABOLISM Composite resin /monomers may interfere with
cell metabolism at nonlethal concentrations
INFLUENCE ON CELL METABOLISM
The intracellular level of reactive oxygen species ROS ( H2O2 , superoxide anion , OH radical ) increased after exposure to HEMA, TEGDMA, or composites resin.
Camphorquinone , after irradiation with blue light, directly increased intracellular and extracellular ROS concentration → DNA damage via oxidation of DNA bases
INFLUENCE ON CELL METABOLISM
Methacrylates may interfere with cellular cholesterol and phospholipids and thus alter membrane-related functions.
ANTIMICROBIAL PROPERTIESResin-based composite hasn’t real antimicrobial activity, many studies show in fact these types behaviour:
Resin-based composites and luting composites increase the growth of Streptococcus Mutans
TEGDMA and EGDMA promote bacterial proliferation of two cariogenic species: Streptococcus Sobrinus . Lactobacillus Acidophilus Then composite’s matrix helps adhesion of bacterial microorganisms
PULP REACTIONS Comparatively few studies have addressed
the effect of resin-based composites or adhesives on the pulp in deep cavities.
Small resin particles derived from dentin adhesives were documented in dentin tubules and in pulp, this particles were surrounded by macrophages, a situation indicative of a foreign body or inflammatory reaction.
PULP REACTIONS Thermal effects on the pulp: an increase of 5,5° C of
the temperature in the pulp will cause irreversible pulpar demage in 15% of all cases
Postoperative sensitivity → the possible causes can be:
trauma caused by preparation microleakage with bacterial penetration polymerization shrinkage deformation of the restoration under stress
Sixty days after the capping procedure the tooth was extracted and processed for histological evaluation of the pulp tissue. Note the presence of bonding agent (BA) on the pulp exposure site and inside of the connective tissue (BA – arrow). Intense chronic inflammatoty reaction mediated by macrophages and a number of dilatedand congested blood vessles (BV) is observed
Pulp exposure capped with an adhesive system.Note that no hard tissue barrier was formed 60 days afterthe pulp therapy
The change in the chemical structure of the composite and the variation in the ratio of filler and monomer have a significant effect on the element release and cytotoxicity level of the materials. the flowable materials of the traditional composites were more cytotoxic than their standards.
NEEDLE ASPIRATIONNeedle(18-gauge) aspiration may be described as
the use of suction to remove fluids from a cavity or space
Aspirated samples may be used for microbial isolation
Clinical advantages of needle aspiration over I&D include:
.1reduced scarring
.2evaluation of volume and character of the aspirate
.3use of the aspirate for culture and sensitivity testing .4 the lack of postoperative drain removal
THANKS JAMEI