Customized Therapeutic Surface Coatings for Dental Implants
Abstract
:1. Introduction
2. Mode of Action of Drug-Releasing Coatings
3. Controlling the Drug Release from Coatings
4. Desired Properties for Drug-Releasing Dental Implants
5. Methods of Drugs Coating on Dental Implants
Description | Problems/Benefits | Consequences | Examples |
---|---|---|---|
Physisorption or Adsorption [130,133,136,150,151] | |||
Depending on the implant surface features (roughness, chemistry, surface energy, and wettability), which results in spontaneous adsorption of drugs and therapeutic agents on Ti implant surface via weaker van der Waals forces. | Lack of control over the delivery of molecules. Several parameters such as micro movement of the implant, pH, temperature, and solvent conditions | It is achieved by dipping method Uncontrolled adsorption from the surface | A burst release system, (80%–90%) in 1 h of adsorbed molecule Superficially adsorbed BMP-2 released rapidly in higher concentration |
Covalent Binding [134,152,153,154,155] | |||
Cellular adhesion of proteins via covalent bond to prevent systemic effects of drugs | Immobilization of molecules promote mineralization | Proteins bond to the implant surface directly or through a spacer such as hydroxyl (−OH) or amine (−NH) groups | Cell-adhesive proteins (collagen, osteopontin, fibronectin, or vitronectin) |
Carrier Systems or Self-Organized Nanoporous Surfaces on Silicon, Aluminum, and Titanium [132,136,156,157] | |||
Direct integration of drug into the coating material via carrier molecules (polylactide, polyglycolic acid, hydrogels, polypyrrole, and CaP/HA coating) | Growth factors or antibiotics are incorporated into a HA coating; can be delivered in a physiologic-like manner | Antibiotics, proteins, and growth factors are entrapped in crystals formed by precipitation of CaP/HA solution | A slow-release system, protein loaded into the carrier can be 10 times higher than adsorption |
6. Understanding Coating–Implant Adhesion Interface
7. Therapeutic Dental Implant Coatings
7.1. Biomimetic and Bioactive Coatings
7.2. Antibacterial Coatings
- (a)
- As acute infections occur immediately after implant surgery, short-term antimicrobial drug delivery coatings to the host tissues and device interface would help to prevent bacterial colonization, thus preventing the infection.
- (b)
- Similarly, long-term bacteria can colonize the implant surface; therefore, consistent antimicrobial drug delivery coatings are required to inhibit microbial colonization on the surface over time.
- (c)
- It is important that, while maintaining both long and short-term drug elution from implant coatings, there should be no alteration in the surface materials’ properties; otherwise, it may deteriorate the implant’s osseointegration.
7.3. Antimicrobial Metallic/Metalloid Coatings
7.4. Antimicrobial Peptides (AMPs) Coatings
7.5. Bisphosphonates Coatings
7.6. Zirconia Coatings
8. Limitations and Future Challenges for Coated Dental Implants
9. Conclusions and Future Trends
Funding
Conflicts of Interest
References
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Type | Subgroup | Substance/Biomolecule | References |
---|---|---|---|
Inorganic | Elemental | Nano-diamond | [169,170,171] |
Graphene | [172,173] | ||
Carbon nanotube | [174,175,176,177] | ||
Silver | [178,179] | ||
Ca-P | [180,181,182,183] | ||
Titanium | [117,184] | ||
Organic | Protein | Fibronectin | [185] |
Elastin | [186] | ||
Laminin | [187,188] | ||
Collagen | [131,185,189] | ||
Bone sialoprotein | [185,189] | ||
Osteopontin | [190] | ||
Growth factors | Bone morphogenetic proteins | [133,191,192,193] | |
Peptides | Arginylglycylaspartic acid | [131] | |
Parathyroid hormone | [194,195,196] | ||
Antimicrobial GL13K | [197,198] | ||
Polysaccharides | Hyaluronic acid | [193,199] | |
Chondroitin 4-sulfate | [131] | ||
Chitosan | [58,200,201] | ||
Pectin | [179,202,203] | ||
Drugs | Bisphosphonate | [50,57,204,205] | |
Simvastatin | [194,206,207] | ||
Strontium ranelate | [208] | ||
Gentamycin | [191,209] | ||
Tetracycline | [58] | ||
Vancomycin | [210,211,212] | ||
Doxycycline | [213,214] | ||
Norfloxacin | [215]. | ||
Chlorhexidine | [58,216] |
Antimicrobial Peptides | Type | Site of Expression |
---|---|---|
α-Defensins | HNP-1 | Neutrophils (azurophilic granules), gingival crevicular fluid, and bone marrow |
HNP-2 | ||
HNP-3 | ||
HNP-4 | Neutrophils | |
β-Defensins | hBD-1 | Saliva and suprabasal layer of stratified epithelium |
hBD-2 | Gingival epithelium and saliva | |
hBD-3 | Skin and salivary gland | |
Histatin | 1 | Saliva (parotid and submandibular) |
3 | ||
5 | ||
Adrenomedullin | - | Epithelium |
Cathelicidins | LL-37 | Neutrophils, inflamed epithelia, and saliva and submandibular glands |
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Share and Cite
Zafar, M.S.; Fareed, M.A.; Riaz, S.; Latif, M.; Habib, S.R.; Khurshid, Z. Customized Therapeutic Surface Coatings for Dental Implants. Coatings 2020, 10, 568. https://doi.org/10.3390/coatings10060568
Zafar MS, Fareed MA, Riaz S, Latif M, Habib SR, Khurshid Z. Customized Therapeutic Surface Coatings for Dental Implants. Coatings. 2020; 10(6):568. https://doi.org/10.3390/coatings10060568
Chicago/Turabian StyleZafar, Muhammad Sohail, Muhammad Amber Fareed, Samiya Riaz, Muhammad Latif, Syed Rashid Habib, and Zohaib Khurshid. 2020. "Customized Therapeutic Surface Coatings for Dental Implants" Coatings 10, no. 6: 568. https://doi.org/10.3390/coatings10060568