Abstract
Implanted biomaterials play a key role in current success of orthopedic and trauma surgery. However, implant-related infections remain among the leading reasons for failure with high economical and social associated costs. According to the current knowledge, probably the most critical pathogenic event in the development of implant-related infection is biofilm formation, which starts immediately after bacterial adhesion on an implant and effectively protects the microorganisms from the immune system and systemic antibiotics. A rationale, modern prevention of biomaterial-associated infections should then specifically focus on inhibition of both bacterial adhesion and biofilm formation. Nonetheless, currently available prophylactic measures, although partially effective in reducing surgical site infections, are not based on the pathogenesis of biofilm-related infections and unacceptable high rates of septic complications, especially in high-risk patients and procedures, are still reported.
In the last decade, several studies have investigated the ability of implant surface modifications to minimize bacterial adhesion, inhibit biofilm formation, and provide effective bacterial killing to protect implanted biomaterials, even if there still is a great discrepancy between proposed and clinically implemented strategies and a lack of a common language to evaluate them.
To move a step forward towards a more systematic approach in this promising but complicated field, here we provide a detailed overview and an original classification of the various technologies under study or already in the market. We may distinguish the following: 1. Passive surface finishing/modification (PSM): passive coatings that do not release bactericidal agents to the surrounding tissues, but are aimed at preventing or reducing bacterial adhesion through surface chemistry and/or structure modifications; 2. Active surface finishing/modification (ASM): active coatings that feature pharmacologically active pre-incorporated bactericidal agents; and 3. Local carriers or coatings (LCC): local antibacterial carriers or coatings, biodegradable or not, applied at the time of the surgical procedure, immediately prior or at the same time of the implant and around it. Classifying different technologies may be useful in order to better compare different solutions, to improve the design of validation tests and, hopefully, to improve and speed up the regulatory process in this rapidly evolving field.
Keywords: Orthopaedics, Trauma, Implant, Joint, Prosthesis, Biofilm, Infection, Coating, Antibacterial, Classification
Introduction
Even if current peri-operative infection prevention methods, like antibiotic prophylaxis, have significantly reduced the incidence of surgical site infections (SSI), up to 2.5 % of primary hip and knee arthroplasties and to 10 % of revision arthroplasties can still be complicated by periprosthetic joint infection (PJI) [1]. Moreover, according to recent analysis, these figures could even be underestimated and are on the rise [2], while multi-resistant pathogens are often retrieved [3]. The occurrence of PJI is a devastating complication, often requiring implant removal, with high morbidity and possible mortality raise [4] and elevated economical and social costs [5].
Implant-related infections are the results of a complex interaction of various factors, including bacterial load, microorganism’s and host’s type, surgical procedure and technique, and type of implant and of antibacterial prophylaxis.
In fact, even elective surgery may not be performed in a completely sterile environment, and operating rooms have been shown to become contaminated within the first few hours of service [6, 7]. While in the majority of cases the rather low bacterial load eventually present at surgery may be generally overcome by the host’s immunological defense and the systemic antibiotic prophylaxis [8], in some patients a SSI may eventually develop, especially in high-risk patients, in which relevant co-morbidities may increase the relative risk for infection up to 20 times compared to normal population [9–11]. Similarly, the most complex surgical procedures and techniques have been shown to be more prone to septic complications [12]. In this context, implant features, including size, shape, material, and intended use, also play an important role [13], while, for example, local antibacterial prophylaxis, like the use of antibiotic-loaded bone cement or bone grafts has been shown to reduce the incidence of implant-related infections [14, 15]. In line with these considerations, a strong recommendation was delivered, in a recent international consensus meeting on PJI, concerning the need for developing effective antibacterial surfaces that prevent bacterial adhesion and colonization of implants and proliferation into the surrounding tissues [16].
In the present review, we provide a detailed description and an original classification of the technologies already available or under investigation, aimed at minimizing implant-related infections in orthopedics and trauma surgery.
Rationale of antibacterial coating of implants
Prophylactic systemic antibiotics are administered routinely to patients who receive an orthopedic device to prevent peri-operative infection [8]. However, systemic administration of antibiotics has many potential disadvantages including the need for a correct timing of administration, the relatively low drug concentration at the target site, and the limited ability to kill bacteria eventually present on the implant surface or embedded in biofilms.
When Anthony Gristina first proposed the concept of a “race for the surface”, more than three decades ago, he described a simplified model of implant-related infection, whereby host and bacterial cells compete in determining the ultimate fate of the implant [17]. According to this model, when the host cells colonize the implant surface first, the probability of attachment of bacterial cells is very low and vice versa. Further studies have now made it clear that the process is much more complex and only partially understood.
Bacteria have a highly successful and diversified strategy to adhere and survive on virtually all natural and synthetic surfaces [18, 19]. Surface characteristics of a biomaterial such as roughness, hydrophobicity, and electrostatic charge play only conditional roles [20], while a number of potential receptors for bacterial adhesive ligands are offered by the protein film that covers an implant immediately after its placement into the host body [21–23]. Complement, albumin, and several other host proteins and lipids are the main components of this conditional protein film [24–26]. The process of bacterial adhesion can be divided into a reversible phase, based on nonspecific interactions between implant surface and bacterial adhesions, and an irreversible phase, mediated by molecular and cellular interactions and closely associated with expression of biofilm-specific gene clusters in reversibly attached bacteria. All the process from bacterial adhesion to the production of a mature biofilm is extremely efficient and is normally completed within 12 to 18 h [27–30].
On the host side, the detailed process of implant osteo and tissue integration is also incompletely unveiled [31, 32]. According to Gristina’s model, host cells, once attached to implant surfaces, should lead to periprosthetic bone regeneration and remodeling, protecting the biomaterial against bacterial colonization [33]. However, bacteria may survive to osteointegration or to fibrous tissue encapsulation of an implant, while peri-implant fibrous tissue may even prevent direct contact between host immunity cells and bacterial molecules, while the presence of the implant has been shown to impair innate local host response [34–36].
As a result, there is a strong need for intrinsic implant surface antibacterial functionality to overcome the implant-induced defects in the local immune response and to prevent the striking ability of bacteria to quickly adhere on a substrate and immediately produce a protective biofilm barrier, providing a competitive advantage to the host’s cells over the contaminating microorganisms. This is of utmost importance especially in patients with underlying compromised immunity [37] and in those undergoing revision surgery [38] in which the relative risk of infection is multiplied.
At the same time, any coating technology should prove to be safe in the short and long term, should not interfere with osteointegration or induce bacterial resistance in the long run, and should be easy to implement in the clinical practice and at an affordable cost. Also, since bacterial colonization, from microbial adhesion to an established mature biofilm layer only takes few hours [39], any antibacterial protection should act at the exact time of surgery and for at least some hours or days thereafter.
Classification of antibacterial coating technologies
Local antibacterial implant protection can be achieved in different ways. Currently, there is not a single, universally accepted classification of coating technologies, standardized validation methods are lacking and regulatory aspects appear somewhat inadequate in view of the clinical needs and expectations. Table 1 summarizes the basic requirements that an “ideal” coating technology should fulfill to meet the needs of a widespread clinical use.
Table 1.
Requirements | Fulfillments | |||
---|---|---|---|---|
Safety | No systemic toxicity | No local toxicity | No detrimental effects on bone healing | No unwanted long-term side effects |
In vitro activity | No cytotoxicity or genotoxicity | Proven bactericidal and antibiofilm activity on different surfaces | Large spectrum | No induction of resistance |
Efficacy | Proven in vivo | Case series | Multicenter trials | Randomized trials |
Ease-of-use | Easy handling | Versatility | Resistance to press-fit insertion | Storage |
Market | Acceptable cost | Large availability | Easy to manufacture | Overcomes regulatory issues |
According to their strategy of action, antibacterial coatings can be classified in at least three groups (Table 2):
Passive surface finishing/modification (PSM). Here all surface chemistry and/or structure modifications aimed at preventing or reducing bacterial adhesion, without releasing bactericidal agents to the surrounding tissues, are included.
Active surface finishing/modification (ASM). Active coatings, included in this class, feature pharmacologically active pre-incorporated antibacterial agents, like antibiotics, antiseptics, metal ions, or other organic and inorganic compounds.
Peri-operative antibacterial local carriers or coatings (LCC). According to this strategy, implant protection is achieved through a biodegradable or not-biodegradable antibacterial carrier or coating, applied during surgery on the implant or around it; the coating may simply act by delivering high local concentrations of one or more pre-loaded antibacterials, or it may have a direct or synergistic antibacterial activity. Antibiotic-loaded polymethylmethacrylate is probably the very first example of this coating strategy, used since many years to protect joint implants.
Table 2.
Strategy | Features | Examples | Development stage | Limits |
---|---|---|---|---|
Passive surface finishing/modifications (PSM) | Prevention of bacterial adhesion | Hydrophilic surface | Preclinical | Limited antibacterial and antibiofilm activity |
Super-hydrophobic surface | ||||
Anti-adhesive polymers | Possible interference with osteointegration | |||
Nano-patterned surface | ||||
Albumin | Unknown long-term effects | |||
Hydrogels | Regulatory issues | |||
Biosurfactants | ||||
Active surface finishing/modifications (ASM) | Inorganic | Silver ions and nanoparticles | Market | Incomplete implant coating |
Questionable long-term toxicity | ||||
Limited versatility and applicability | ||||
Limited large-scale applications | ||||
Possible bacterial resistance induction | ||||
Costs | ||||
Other metals (copper, zinc, titanium dioxide etc.) | Preclinical | Questionable long-term toxicity | ||
Regulatory issues | ||||
Non-metals: Iodine | Clinical | Incomplete implant coating | ||
Questionable long-term toxicity | ||||
Challenging large-scale application | ||||
Regulatory issues | ||||
Other non-metal ions (selenium, grapheme, etc.) | Preclinical | Poorly studied compounds | ||
Coating resistance to press-fit insertion | ||||
Questionable long-term toxicity | ||||
Challenging large-scale application | ||||
Regulatory issues | ||||
Organic | Coated/linked antibiotics | Market | Unique application to nail coating | |
Long-term effects on osteointegration | ||||
Single antibiotic (gentamicin) | ||||
Covalently linked antibiotics | Preclinical | Incomplete implant coating. | ||
Questionable long-term toxicity | ||||
Challenging large-scale application | ||||
Regulatory issues | ||||
Antimicrobial peptides | No data on in vivo or clinical effects | |||
Cytokines | Coating resistance to press-fit insertion | |||
Enzymes and biofilm disrupting agents | Questionable long-term toxicity | |||
Challenging large-scale application | ||||
Chitosan derivatives | ||||
Synthetic | Non-antibiotic antimicrobial compounds | |||
Regulatory issues | ||||
“Smart” coatings | ||||
Combined | Multilayer coating | |||
Peri-operative antibacterial local carriers or coatings (LCC) | Not-biodegradable | Antibiotic-loaded polymethylmetacrylate | Market | Resistance and small-colony variants induction |
No antibiofilm effect | ||||
Incomplete implant coating | ||||
May not be used for cementless implants | ||||
Biodegradable | Antibiotic-loaded bone grafts and substitutes | Market | Limited availability | |
Not proven efficacy as implant coating | ||||
Cost | ||||
Fast-resorbable hydrogel | Market | Early clinical use and results |
Although necessarily schematic, this classification may be helpful to compare different technologies both in the clinical practice and concerning regulatory aspect, that should probably differ for different classes.
Passive surface finishing/modification
Chemical and/or physical modifications of the surface layer of an existing biomaterial may result in a substantial change of its susceptibility to bacterial colonization.
Surface characteristics of implants, like surface roughness and chemistry, hydrophilicity, surface energy or potential and conductivity play in fact crucial roles in bacterial adhesion and subsequent biofilm formation. Surface physio-chemical modification of an implant is also relatively simple and economic to achieve and to industrialize.
Ultraviolet light irradiation, for example, is able to increase “spontaneous” wettability on titanium dioxide, which in turn can inhibit bacterial adhesion without compromising osteogenesis on titanium alloy implants [40, 41]. A bacterial anti-adhesive surface can also be achieved by modifying the crystalline structure of the surface oxide layer [42].
Some polymer coatings, like the hydrophilic polymethacrylic acid, polyethylene oxide, or protein-resistant polyethylene glycol can be applied to the surface of titanium implants and result in significant inhibition of bacterial adhesion [43–45]. Even if some of these coatings may impair local osteoblast function, the use of additional bioactive molecules as sericin and RGD motif could restore and even improve the impaired cell function [46]. Hydrophobic and super-hydrophobic surface treatment technologies have also shown a great repellent antibacterial effect in preclinical studies [47, 48].
Other researchers have focused on controlling the biological response to biomaterials via alterations in surface structure and design [49, 50]. In this regard, changing the implant surface at a nanometric scale, at which bacterial adhesion does not simply follow the roughness of the surface but also is dependent on other variables like the quantity of adsorbed proteins, can in fact suppress bacteria adhesion [51].
Treating more specifically protein surfaces and/or protein–bacteria interactions may also be a successful strategy of inhibiting bacterial adhesion to a specific biomaterial [52, 53]. Friedman et al., using a rabbit model, demonstrated reduced bacterial adherence on pure titanium samples and decreased infection rates of implants coated with cross-linked albumin [54].
More recently, novel strategies include production of self-assembled mono- or multilayers, surface grafting or hydrogels, or the use of biosurfactants and microbial amphyphilic compounds with excellent anti-adhesive properties [55, 56].
In summary, a number of anti-adhesive surface modifications have been proposed for different purposes, but only a few will probably be suitable for clinical use. In particular, a strong anti-adhesive layer cannot be used for coating of fixation surfaces of joint arthroplasty since it could also interfere with implant osteointegration, leading to early mechanical failure [48, 49]. Another challenge of designing anti-adhesive technologies relates to the current inability to find a universal treatment that can be applied to all surfaces and biomaterials, all bacterial species and under all (ingrowth and noningrowth) implants. Moreover, passive coating methods should be preferred as long as their antibacterial ability is strong enough to prevent biofilm formation, but the ability of passive coatings to resist bacterial adhesion is generally limited and varies greatly depending on the bacterial species and loads [57]. In vivo efficacy and long-term effects of these new technologies both on host’s cells and on bacterial resistance are also poorly understood and need to be further investigated before clinical applications and market introduction.
Active surface finishing/modification
Surface modifications may include pharmacologically active pre-incorporated antibacterial agents or compounds, like antibiotics, antiseptics, metal ions, or organic molecules. Such pharmacologically activated coatings may change the implant from a passive, pharmacologically inert medical device, to something more and more similar to a drug agent, with difficult to predict long-term effects and challenging regulatory issues.
Historically, two main strategies have been proposed for effective antibacterial surface treatment either “contact killing” or drug eluting, while in terms of durability, we can distinguish between degradable and non-degradable coatings. Killing of bacteria can be achieved by interfering with cell respiration or division, cell wall formation or bacterial signaling network as well as inhibition of the transition of planktonic phenotype of bacteria into a sessile type [58].
Antibacterial surface technologies can employ metals (silver, zinc, copper, etc.), non-metal elements (e.g., iodine, selenium), organic substances (antibiotics, anti-infective peptides, chitosan, other substances), and their combinations.
Antibacterial activity of the majority of metal coatings is closely linked to the ionic or nano form rather than to the bulk material [59]. Silver is the most prevalent metal used in biomedical applications. Dissolved silver cations are biochemically active agents that interfere with bacterial cell membrane permeability and cellular metabolism. Silver also contributes to formation of reactive oxygen species and other mechanisms that potentially influence prokaryotic cells [60]. There has been concern, however, about the toxicity of silver ions [61]. Research efforts have focused on the development of silver coating technologies that reduce or even eliminate toxicity while maintaining antibacterial effects [62, 63]. Despite demonstrated clinical efficacy and safety in recent comparative studies [64, 65], routine use of silver-coated implants remains rather limited. The main obstacle to a broader usage of such technology is cytotoxicity on bone cells, that prevented until now coating of the intra-medullary part of the prosthesis. In addition, cost issues and the inability to apply the technology to a variety of prosthetic implants and devices further reduces its application outside oncological or highly selected cases.
Copper and zinc also have potent antibacterial effects on a wide spectrum of bacterial species [66, 67]; however, potential toxic side effects of these metals remain a strong concern [68]. Proposed solutions include copper- and zinc-based nanomaterials or, alternatively, controlled release [69]. The risk of bacterial resistance to metallic coatings remains a potential limitation for their widespread use [70]. Concern also exists about the mechanical properties of implant nanocoatings since damage may occur during surgical implantation especially in cementless implants inserted via press-fit methods [71].
Another interesting technology is related to modification of commonly used alloys, like titanium. The anti-infective potential of titanium dioxide layers has been widely investigated and proven effective in vitro both alone [72] or in combination with other substances [73].
Non-metal elements like hydrogen, chlorine, iodine, or oxygen are commonly used in biomedicine for their anti-infective properties. Selenium bound covalently onto the surface of titanium or titanium alloy implant discs has been shown to prevent Staphylococcus aureus and Staphylococcus epidermidis attachment without affecting osteoblast viability [74]. Selenium catalyzes the formation of superoxide radicals and subsequently inhibits bacterial adhesion and viability. In addition, selenium nanoparticles can inhibit bacterial growth and biofilm formation [75].
Ongoing research is also directed to determine the clinical applicability of carbon substances like graphene or carbon nanotubes, that can be synthesized in multifunctional layers [76]; however, the most interesting technology today under study, related to non-metal elements, is probably iodine coating of titanium alloys, that has recently demonstrated clinical efficacy in a continuous series of 222 patients with excellent results [77].
Several organic compounds with antibacterial properties have the potential to be linked to the surface of implants conferring them anti-infective properties. A large number of studies have investigated the efficacy of surfaces coated with covalently linked antibiotics [78–82]. Clinical effectiveness of such implants is most likely limited to infections caused by bacteria that are sensitive to the specific antibiotic that has been coupled. In addition, strong forces such as covalent binding are insufficiently sensitive to react to weak external stimuli [83]. In fact, despite the theoretical advantages for non-eluting systems, this concept is limited by the fragility of the coatings and killing activity potential of bacteria which might not be directly adjacent to the implant. To overcome these issues, combinations of antibiotics with other compounds have been proposed either alone or in association with a particular mechanism of controlled release [84]. Antibiotics such as gentamicin, vancomycin, and others have been loaded into porous hydroxyapatite (HA) coatings on titanium implants. The antibiotic-HA coatings exhibit significant improvement in preventing infection compared with standard HA coatings in vivo, but there are still many unresolved issues regarding the methodology of antibiotic incorporation into the HA coating and the optimal release kinetics and possible detachment of the coating at the time of press-fit insertion.
Biodegradable polymers and sol–gel coatings are also utilized to form controlled release antibiotic-laden coatings on titanium implants [85, 86]. Clinical applications of antibiotic-loaded D-poly-lactate acid/gentamycin intra-medullary coated nail have been recently reported with early positive results [87].
Some antiseptic agent such as chlorhexidine, chloroxylenol, or poly-hexamethylenebiguanide have demonstrated efficacy and might be an alternative to avoid the risk of drug resistance. Chlorhexidine can be adsorbed to the TiO2 layer on titanium surfaces and is released gradually over several days [88]. Its release pattern is similar to that of antibiotic-laden coatings with an initial rapid release rate followed by slower but sustained release [89].
Another promising approach involves coating implants with antimicrobial peptides, cytokines, or other molecules critical for host response to bacteria invasion. This heterogeneous group of substances has proven experimentally their efficacy against a wide range of pathogens [90]. Antimicrobial peptides, like antibiotics, function via damage of the cell wall and inhibition of key bacterial protein synthesis. In addition, they exert influence upon inflammation, tissue healing, and apoptotic events [91]; resistance to antimicrobial peptides has been reported less frequently than to antibiotics [92]. Initial experiments demonstrated that a thin layer of antimicrobial peptides affixed onto the surfaces of metal alloys exhibit excellent antibacterial effects against typical pathogens related to PJI [93].
Chitosan (CS) is a polycationic polymer derived from chitin that exhibits antibacterial and antifungal activity. The exact mechanism of action remains poorly understood. There is some evidence that CS derivatives can be firmly anchored to titanium alloys and that they have a protective effect against some bacterial species either alone or in combination with other antimicrobial substances like antibiotics or antimicrobial peptides [94, 95]. CS derivatives secured to external fixator pins have been studied as a method of preventing pin tract infections [96]. However, we are not aware of a study to date reporting data from clinical setting.
Long-term impact of permanently coated implants with antibiotics and other organic compounds, never used before either for local or general administration, does raise concerns regarding possible induction of bacterial resistance, local, and general toxicity and possible detrimental effects on implant osteointegration, ultimately preventing clinical applications until now.
Still more complex approaches involve the development of multifunctional surface layers, like functional polymer brush coating, that combine anti-adhesive and antimicrobial substances and other compounds able to enhance tissue integration [97], while “smart coatings”, sensitive and responsive to a variety of stimuli, including the presence of bacteria [98], are another fascinating but futuristic research pathway that poses a number of open questions, like feasible coating manufacturing process, non-adverse reactions in vivo, mechanical resistance, or preservation of intended functionalities throughout the life of the device.
Peri-operative antibacterial carriers or coatings
Instead of pre-manufactured surface modifications, either with or without pharmacologically active agents, a different approach to implant protection may be to provide a traditional implant with an antibacterial carrier or coating at the time of surgery. The separation of the protective solution from the implant until surgery may reduce the regulatory requirements and increase the applicability of a universal antibacterial coating to many different already existing implants and biomaterials.
Local administration of antibiotics historically attracted much attention in orthopaedics. Buchholz et at. first popularized the incorporation of antibiotics into polymethylmethacrylate (PMMA) bone cement for local antibiotic prophylaxis in cemented total joint arthroplasty [99]. Clinical studies have shown that antibiotic-loaded bone cement can decrease deep infection rates of cemented total hip arthroplasties and revision rates due to supposed “aseptic” loosening when combined with systemic antibiotic administration [100] and this solution has been found both effective and economically sound, especially in high-risk patients [101, 102]. However, PMMA was not designed as a local delivery carrier of antibiotics and may have some limits. Antibiotic-loaded PMMA may not overcome biofilm formation and may be associated with the development of antibiotic-resistant “small-colony variants” [103, 104], while the increasing use of cementless implants worldwide, especially at the hip site, make this a possible option only for a restricted number of patients.
Other porous materials for local antibiotic delivery like collagen sponges [105], cancellous bone [106], and calcium phosphate cements [107, 108] were not specifically designed to protect implanted biomaterials, and their use for routine infection prevention in joint prosthesis is limited by their insufficient in vitro, in vivo, and clinical evidence of efficacy in this specific application, their inability to be applied as a coating to all implants’ surfaces, and their relatively high costs and possible interference with primary implant fixation and long-term osteointegration.
Biocompatible hydrogels do represent a possible alternative solution, as they have demonstrated to be able to deliver local pharmacological agents and may be designed to meet the desired elution pattern [109]. Recently, a fast-resorbable hydrogel coating, that can be loaded intra-operatively with various antibacterials, has been introduced in the European market [110]. Based on the facts that bacterial colonization occurs within the very first hours after implant and that short-term systemic prophylaxis is equally effective as the long-term one to prevent PJIs [111], this novel coating technology introduced the “short-term local protection” of the implant. A short-term local delivery system may in fact meet the requirements needed to win the “run to the surface”, while limiting possible long-term unwanted side effects [112]. This novel fast-resorbable hydrogel coating, “Defensive Antibacterial Coating”, DAC® (Novagenit Srl, Mezzolombardo, Italy), composed of covalently linked hyaluronan and poly-D,L-lactide, (Fig. 1), is designed to undergo complete hydrolytic degradation in vivo within 48 to 72 h, being able to completely release a variety of different antibacterials, including glycopeptides, amynoglycosides, and fluoquinolones (Table 3), at concentrations ranging from 2 % to 10 %. The hydrogel showed a synergistic antibacterial activity with various antibiotics and antibiofilm agents in vitro [113], while in vivo it has been proven effective a rabbit model of highly contaminated implant both with [114] and without systemic prophylaxis [115]. An ongoing European multicenter clinical trial (Fig. 2) is currently investigating the safety and the efficacy of the device [116].
Table 3.
Antibacterial family | Tested antibiotics |
---|---|
Aminoglycosides | Gentamicin |
Tobramycin | |
Amikacin | |
Carbapenems | Meropenem |
Glicopeptides | Vancomycin |
Teicoplanin | |
Quinolones | Ciprofloxacin |
Cyclic lipopeptides | Daptomycin |
Rifamycins | Rifampicin |
Glycylcyclines (Tetracyclines) | Tigecyclin |
Oxazolidinones | Linezolid |
Antifungals | Amphotericin B |
Fluconazole | |
Ketoconazole |
Conclusions
A tremendous amount of research has been done in the last two decades in order to better protect implanted biomaterials from bacterial colonization, but we are still probably at the beginning of the journey. In fact, in spite of the highly successful advances in preclinical studies, a remarkable discrepancy still exists between the proposed strategies and their clinical applications [117, 118]. While most of the coatings under study will not probably be suitable for orthopedic implants, due to cytotoxicity, immunoreactivity, or genotoxicity problems, clinical application of those successfully tested in vitro and in vivo can still be limited by biotechnological, regulatory, economic, and medico-legal issues.
Improving collaborative efforts amongst governments, regulatory agencies, industry leaders, and health care payers will probably allow more and more our patients to benefit from these very promising technologies.
A comprehensive classification and a common language are needed to standardize appropriate tests and realistic regulatory requirements, in order to favor the transition from preclinical studies to effective patient’s protection.
Consent
Written informed consent was obtained from the patient for the publication of this report and any accompanying images.
Footnotes
Competing interests
CLR is a co-inventor of the DAC hydrogel technology and has received reimbursements, fees, and funding from the following companies, involved in the development of some of the technologies cited in the text: DePuySynthes Inc., Zimmer-Biomet Inc., Link Italia Srl, Heraeus GmbH, Tecres SpA, AdlerOrtho Srl. LD has received reimbursements, fees, and funding from the following companies, involved in the development of some of the technologies cited in the text: Zimmer-Biomet Inc., Heraeus GmbH. DR, EG, and SS have no competing interests.
Authors’ contributions
CLR and LD conceived, drafted, and finalized the paper. EG, DR, and SS collected and analyze relevant bibliography and contributed to writing and finalizing the manuscript. All authors read and approved the final manuscript.
Contributor Information
Carlo Luca Romanò, Phone: 00390266214903, Email: carlo.romano@grupposandonato.it.
Sara Scarponi, Email: scarponi1981@libero.it.
Enrico Gallazzi, Email: enrico.gallazzi@gmail.com.
Delia Romanò, Email: delia-romano@libero.it.
Lorenzo Drago, Email: lorenzo.drago@unimi.it.
References
- 1.Lentino JR. Prosthetic joint infections: Bane of orthopedists, challenge for infectious disease specialists. Clin Infect Dis. 2003;36:1157–61. doi: 10.1086/374554. [DOI] [PubMed] [Google Scholar]
- 2.Dale H, Hallan G, Hallan G, Espehaug B, Havelin LI, Engesaeter LB. Increasing risk of revision due to deep infection after hip arthroplasty. Acta Orthop. 2009;80:639–45. doi: 10.3109/17453670903506658. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 3.Aggarwal VK, Bakhshi H, Ecker NU, Parvizi J, Gehrke T, Kendoff D. Organism profile in periprosthetic joint infection: Pathogens differ at two arthroplasty infection referral centers in Europe and in the United States. J Knee Surg. 2014, 10, doi:10.1055/s-0033-1364102. [DOI] [PubMed]
- 4.Zmistowski B, Karam JA, Durinka JB, Casper DS, Parvizi J. Periprosthetic joint infection increases the risk of one-year mortality. J Bone Joint Surg Am. 2013;95:2177–84. doi: 10.2106/JBJS.L.00789. [DOI] [PubMed] [Google Scholar]
- 5.Kurtz SM, Lau E, Watson H, Schmier JK, Parvizi J. Economic burden of periprosthetic joint infection in the United States. J Arthroplast. 2012;27:61–5. doi: 10.1016/j.arth.2012.02.022. [DOI] [PubMed] [Google Scholar]
- 6.An YH, Friedman RJ. Prevention of sepsis in total joint arthroplasty. J Hosp Infect. 1996;33:93–108. doi: 10.1016/S0195-6701(96)90094-8. [DOI] [PubMed] [Google Scholar]
- 7.Humphreys H. Surgical site infection, ultraclean ventilated operating theatres and prosthetic joint surgery: Where now? J Hosp Infect. 2012;81:71–2. doi: 10.1016/j.jhin.2012.03.007. [DOI] [PubMed] [Google Scholar]
- 8.Bratzler DW, Houck PM. Surgical Infection Prevention Guidelines Writers Workgroup; American Academy of Orthopedic Surgeons. Antimicrobial prophylaxis for surgery: an advisory statement from the National Surgical Infection Prevention Project. Clin Infect Dis. 2004;38:1706–15. doi: 10.1086/421095. [DOI] [PubMed] [Google Scholar]
- 9.Illingworth KD, Mihalko WM, Parvizi J, Sculco T, McArthur B, el Bitar Y, et al. How to minimize infection and thereby maximize patient outcomes in total joint arthroplasty: a multicenter approach: AAOS exhibit selection. J Bone Joint Surg Am. 2013;95:e50. doi: 10.2106/JBJS.L.00596. [DOI] [PubMed] [Google Scholar]
- 10.Pruzansky JS, Bronson MJ, Grelsamer RP, Strauss E, Moucha CS. Prevalence of modifiable surgical site infection risk factors in hip and knee joint arthroplasty patients at an urban academic hospital. J Arthroplast. 2014;29:272–6. doi: 10.1016/j.arth.2013.06.019. [DOI] [PubMed] [Google Scholar]
- 11.Aggarwal VK, Tischler EH, Lautenbach C, Williams GR, Jr, Abboud JA, Altena M, et al. Mitigation and education. J Arthroplast. 2014;29:19–25. doi: 10.1016/j.arth.2013.09.028. [DOI] [PubMed] [Google Scholar]
- 12.Namba RS, Inacio MC, Paxton EW. Risk factors associated with surgical site infection in 30,491 primary total hip replacements. J Bone Joint Surg Br. 2012;94:1330e8. doi: 10.2106/JBJS.K.01363. [DOI] [PubMed] [Google Scholar]
- 13.Moriarty TF, Schlegel U, Perren S, Richards RG. Infection in fracture fixation: can we influence infection rates through implant design? J Mater Sci Mater Med. 2010;21:1031e5. doi: 10.1007/s10856-009-3907-x. [DOI] [PubMed] [Google Scholar]
- 14.Jamsen E, Furnes O, Engesaeter LB, Konttinen YT, Odgaard A, Stefansdottir A, et al. Prevention of deep infection in joint replacement surgery. Acta Orthop. 2010;81:660e6. doi: 10.3109/17453674.2010.537805. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 15.van de Belt H, Neut D, Schenk W, van Horn JR, van der Mei HC, Busscher HJ. Infection of orthopedic implants and the use of antibiotic-loaded bone cements. A review. Acta Orthop Scand. 2001;72:557e71. doi: 10.1080/000164701317268978. [DOI] [PubMed] [Google Scholar]
- 16.Cats-Baril W, Gehrke T, Huff K, Kendoff D, Maltenfort M, Parvizi J. International consensus on periprosthetic joint infection: description of the consensus process. Clin Orthop Relat Res. 2013;471:4065–75. doi: 10.1007/s11999-013-3329-4. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 17.Gristina AG, Naylor P, Myrvik Q. Infections from biomaterials and implants: a race for the surface. Med Prog Technol. 1988;14:205–24. [PubMed] [Google Scholar]
- 18.Costerton W, Veeh R, Shirtliff M, Pasmore M, Post C, Ehrlich G. The application of biofilm science to the study and control of chronic bacterial infections. J Clin Investig. 2003;112:1466–77. doi: 10.1172/JCI200320365. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 19.Busscher HJ, van der Mei HC. How do bacteria know they are on a surface and regulate their response to an adhering state? PLoS Pathog. 2012;8:e1002440. doi: 10.1371/journal.ppat.1002440. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 20.Chen Y, Busscher HJ, van der Mei HC, Norde W. Statistical analysis of long- and short-range forces involved in bacterial adhesion to substratum surfaces as measured using atomic force microscopy. Appl Environ Microbiol. 2011;77:5065–70. doi: 10.1128/AEM.00502-11. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 21.Wagner C, Aytac S, Hansch GM. Biofilm growth on implants: bacteria prefer plasma coats. Int J Artif Organs. 2011;34:811–7. doi: 10.5301/ijao.5000061. [DOI] [PubMed] [Google Scholar]
- 22.Wang Y, Subbiahdoss G, de Vries J, Libera M, van der Mei HC, Busscher HJ. Effect of adsorbed fibronectin on the differential adhesion of osteoblast-like cells and Staphylococcus aureus with and without fibronectin-binding proteins. Biofouling. 2012;28:1011–21. doi: 10.1080/08927014.2012.725471. [DOI] [PubMed] [Google Scholar]
- 23.Ribeiro M, Monteiro FJ, Ferraz MP. Infection of orthopedic implants with emphasis on bacterial adhesion process and techniques used in studying bacterial-material interactions. Biomatter. 2012;2:176–94. doi: 10.4161/biom.22905. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 24.Jenney CR, Anderson JM. Adsorbed serum proteins responsible for surface dependent human macrophage behavior. J Biomed Mater Res. 2000;49:435–47. doi: 10.1002/(SICI)1097-4636(20000315)49:4<435::AID-JBM2>3.0.CO;2-Y. [DOI] [PubMed] [Google Scholar]
- 25.Thevenot P, Hu W, Tang L. Surface chemistry influences implant biocompatibility. Curr Top Med Chem. 2008;8:270–80. doi: 10.2174/156802608783790901. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 26.Roach P, Eglin D, Rohde K, Perry CC. Modern biomaterials: a review—bulk properties and implications of surface modifications. J Mater Sci Mater Med. 2007;18:1263–77. doi: 10.1007/s10856-006-0064-3. [DOI] [PubMed] [Google Scholar]
- 27.Costerton JW, Stewart PS, Greenberg EP. Bacterial biofilms: a common cause of persistent infections. Science. 1999;284:1318–22. doi: 10.1126/science.284.5418.1318. [DOI] [PubMed] [Google Scholar]
- 28.Stoodley P, Ehrlich GD, Sedghizadeh PP, Hall-Stoodley L, Baratz ME, Altman DT, et al. Orthopaedic biofilm infections. Curr Orthop Pract. 2011;22:558–63. doi: 10.1097/BCO.0b013e318230efcf. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 29.Laverty G, Gorman SP, Gilmore BF. Biomolecular mechanisms of staphylococcal biofilm formation. Future Microbiol. 2013;8:509–24. doi: 10.2217/fmb.13.7. [DOI] [PubMed] [Google Scholar]
- 30.Foster TJ, Geoghegan JA, Ganesh VK, Hook M. Adhesion, invasion and evasion: the many functions of the surface proteins of Staphylococcus aureus. Nat Rev Microbiol. 2014;12:49–62. doi: 10.1038/nrmicro3161. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 31.Anderson JM, Rodriguez A, Chang DT. Foreign body reaction to biomaterials. Semin Immunol. 2008;20:86–100. doi: 10.1016/j.smim.2007.11.004. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 32.Gardner AB, Lee SK, Woods EC, Acharya AP. Biomaterials-based modulation of the immune system. Biomed Res Int. 2013, 2013, doi:10.1155/2013/732182. [DOI] [PMC free article] [PubMed]
- 33.Busscher HJ, van der Mei HC, Subbiahdoss G, Jutte PC, van den Dungen JJ, Zaat SA, et al. Biomaterial-associated infection: locating the finish line in the race for the surface. Sci Transl Med. 2012;4:153rv10. doi: 10.1126/scitranslmed.3004528. [DOI] [PubMed] [Google Scholar]
- 34.Zimmerli W, Lew PD, Waldvogel FA. Pathogenesis of foreign body infection. Evidence for a local granulocyte defect. J Clin Investig. 1984;73:1191–200. doi: 10.1172/JCI111305. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 35.Higgins DM, Basaraba RJ, Hohnbaum AC, Lee EJ, Grainger DW, Gonzalez-Juarrero M. Localized immunosuppressive environment in the foreign body response to implanted biomaterials. Am J Pathol. 2009;175:161–70. doi: 10.2353/ajpath.2009.080962. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 36.Zimmerli W, Sendi P. Pathogenesis of implant-associated infection: the role of the host. Semin Immunopathol. 2011;33:295–306. doi: 10.1007/s00281-011-0275-7. [DOI] [PubMed] [Google Scholar]
- 37.Berbari EF, Osmon DR, Lahr B, Eckel-Passow JE, Tsaras G, Hanssen AD, et al. The Mayo prosthetic joint infection risk score: implication for surgical site infection reporting and risk stratification. Infect Control Hosp Epidemiol. 2012;33:774–81. doi: 10.1086/666641. [DOI] [PubMed] [Google Scholar]
- 38.Engelsman AF, Saldarriaga-Fernandez IC, Nejadnik MR, van Dam GM, Francis KP, Ploeg RJ, et al. The risk of biomaterial-associated infection after revision surgery due to an experimental primary implant infection. Biofouling. 2010;26:761–7. doi: 10.1080/08927014.2010.515027. [DOI] [PubMed] [Google Scholar]
- 39.Holá V, Růžička F, Votava M. The dynamics of staphylococcus epidermis biofilm formation in relation to nutrition, temperature, and time. Scr Medica. 2006;79:169–74. [Google Scholar]
- 40.Gallardo-Moreno AM, Pacha-Olivenza MA, Saldana L, Perez-Giraldo C, Bruque JM, Vilaboa N, et al. In vitro biocompatibility and bacterial adhesion of physico-chemically modified Ti6Al4V surface by means of UV irradiation. Acta Biomater. 2009;5:181e92. doi: 10.1016/j.actbio.2008.07.028. [DOI] [PubMed] [Google Scholar]
- 41.Yu JC, Ho W, Lin J, Yip H, Wong PK. Photocatalytic activity, antibacterial effect, and photoinduced hydrophilicity of TiO2 films coated on a stainless steel substrate. Environ Sci Technol. 2003;37:2296e301. doi: 10.1021/es0259483. [DOI] [PubMed] [Google Scholar]
- 42.Del Curto B, Brunella MF, Giordano C, Pedeferri MP, Valtulina V, Visai L, et al. Decreased bacterial adhesion to surface-treated titanium. Int J Artif Organs. 2005;28:718e30. doi: 10.1177/039139880502800711. [DOI] [PubMed] [Google Scholar]
- 43.Zhang F, Zhang Z, Zhu X, Kang ET, Neoh KG. Silk-functionalized titanium surfaces for enhancing osteoblast functions and reducing bacterial adhesion. Biomaterials. 2008;29:4751–9. doi: 10.1016/j.biomaterials.2008.08.043. [DOI] [PubMed] [Google Scholar]
- 44.Harris LG, Tosatti S, Wieland M, Textor M, Richards RG. Staphylococcus aureus adhesion to titanium oxide surfaces coated with non-functionalized and peptide-functionalized poly(L-lysine)-grafted-poly(ethylene glycol) copolymers. Biomaterials. 2004;25:4135–48. doi: 10.1016/j.biomaterials.2003.11.033. [DOI] [PubMed] [Google Scholar]
- 45.Kaper HJ, Busscher HJ, Norde W. Characterization of poly(ethylene oxide) brushes on glass surfaces and adhesion of Staphylococcus epidermidis. J Biomat Sci Polym Ed. 2003;14:313–24. doi: 10.1163/156856203321478847. [DOI] [PubMed] [Google Scholar]
- 46.Oh S, Moon KS, Lee SH. Effect of RGD peptide-coated TiO2 nanotubes on the attachment, proliferation, and functionality of bone-related cells. J Nanomaterials. 2013;2013:1–11. [Google Scholar]
- 47.Zhu H, Guo Z, Liu W. Adhesion behaviors on superhydrophobic surfaces. Chem Commun (Camb) 2014;18:3900–13. doi: 10.1039/c3cc47818a. [DOI] [PubMed] [Google Scholar]
- 48.Braem A, van Mellaert L, Mattheys T, Hofmans D, de Waelheyns E, Geris L, et al. Staphylococcal biofilm growth on smooth and porous titanium coatings for biomedical applications. J Biomed Mater Res A. 2013, doi:10.1002/jbm.a.34688. [DOI] [PubMed]
- 49.Bacakova L, Filova E, Parizek M, Ruml T, Svorcik V. Modulation of cell adhesion, proliferation and differentiation on materials designed for body implants. Biotechnol Adv. 2011;29:739–67. doi: 10.1016/j.biotechadv.2011.06.004. [DOI] [PubMed] [Google Scholar]
- 50.Lu T, Qiao Y, Liu X. Surface modification of biomaterials using plasma immersion ion implantation and deposition. Interface Focus. 2012;2:325–36. doi: 10.1098/rsfs.2012.0003. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 51.Singh AV, Vyas V, Patil R, Sharma V, Scopelliti PE, Bongiorno G, et al. Quantitative characterization of the influence of the nanoscale morphology of nanostructured surfaces on bacterial adhesion and biofilm formation. PLoS One. 2011;6:e25029. doi: 10.1371/journal.pone.0025029. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 52.Campoccia D, Montanaro L, Arciola CR. A review of the biomaterials technologies for infection-resistant surfaces. Biomaterials. 2013;34:8533–54. doi: 10.1016/j.biomaterials.2013.07.089. [DOI] [PubMed] [Google Scholar]
- 53.Yeo IS, Kim HY, Lim KS, Han JS. Implant surface factors and bacterial adhesion: a review of the literature. Int J Artif Organs. 2012;35:762–72. doi: 10.5301/ijao.5000154. [DOI] [PubMed] [Google Scholar]
- 54.An YH, Bradley J, Powers DL, Friedman RJ. The prevention of prosthetic infection using a cross-linked albumin coating in a rabbit model. J Bone Joint Surg Br. 1997;79:816–9. doi: 10.1302/0301-620X.79B5.7228. [DOI] [PubMed] [Google Scholar]
- 55.Rivardo F, Turner RJ, Allegrone G, Ceri H, Martinotti MG. Anti-adhesion activity of two biosurfactants produced by Bacillus spp. prevents biofilm formation of human bacterial pathogens. Appl Microbiol Biotechnol. 2009;83:541–53. doi: 10.1007/s00253-009-1987-7. [DOI] [PubMed] [Google Scholar]
- 56.Rodrigues L, Banat IM, Teixeira J, Oliveira R. Biosurfactants: potential applications in medicine. J Antimicrob Chemother. 2006;57:609–18. doi: 10.1093/jac/dkl024. [DOI] [PubMed] [Google Scholar]
- 57.Hetrick EM, Schoenfisch MH. Reducing implant-related infections: active release strategies. Chem Soc Rev. 2006;35:780–9. doi: 10.1039/b515219b. [DOI] [PubMed] [Google Scholar]
- 58.Stoodley P, Hall-Stoodley L, Costerton B, DeMeo P, Shirtliff M, Gawalt E, et al. Biofilms, biomaterials, and device-related infections. In: Ratner BD, Hoffman AS, Schoen FJ, Lemons JE, et al., editors. Biomaterials science: an introduction to materials in medicine. Waltham, MA, USA: Academic Press (Elsevier); 2013. pp. 565–83. [Google Scholar]
- 59.Lemire JA, Harrison JJ, Turner RJ. Antimicrobial activity of metals: mechanisms, molecular targets and applications. Nat Rev Microbiol. 2013;11:371–84. doi: 10.1038/nrmicro3028. [DOI] [PubMed] [Google Scholar]
- 60.Chernousova S, Epple M. Silver as antibacterial agent: ion, nanoparticle, and metal. Angew Chem Int Ed Engl. 2013;52:1636–53. doi: 10.1002/anie.201205923. [DOI] [PubMed] [Google Scholar]
- 61.Mijnendonckx K, Leys N, Mahillon J, Silver S, van Houdt R. Antimicrobial silver: uses, toxicity and potential for resistance. Biometals. 2013;26:609–21. doi: 10.1007/s10534-013-9645-z. [DOI] [PubMed] [Google Scholar]
- 62.Noda I, Miyaji F, Ando Y, Miyamoto H, Shimazaki T, Yonekura Y, et al. Development of novel thermal sprayed antibacterial coating and evaluation of release properties of silver ions. J Biomed Mater Res B Appl Biomater. 2009;89:456–65. doi: 10.1002/jbm.b.31235. [DOI] [PubMed] [Google Scholar]
- 63.Panacek A, Kolar M, Vecerova R, Prucek R, Soukupova J, Krystof V, et al. Antifungal activity of silver nanoparticles against Candida spp. Biomaterials. 2009;30:6333–40. doi: 10.1016/j.biomaterials.2009.07.065. [DOI] [PubMed] [Google Scholar]
- 64.Wafa H, Grimer RJ, Reddy K, Jeys L, Abudu A, Carter SR, et al. Retrospective evaluation of the incidence of early periprosthetic infection with silver-treated endoprostheses in high-risk patients: case–control study. Bone Joint J. 2015;97-B(2):252–7. doi: 10.1302/0301-620X.97B2.34554. [DOI] [PubMed] [Google Scholar]
- 65.Hardes J, von Eiff C, Streitbuerger A, Balke M, Budny T, Henrichs MP, et al. Reduction of periprosthetic infection with silver-coated megaprostheses in patients with bone sarcoma. J Surg Oncol. 2010;101(5):389–95. doi: 10.1002/jso.21498. [DOI] [PubMed] [Google Scholar]
- 66.Grass G, Rensing C, Solioz M. Metallic copper as an antimicrobial surface. Appl Environ Microbiol. 2011;77:1541–7. doi: 10.1128/AEM.02766-10. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 67.Petrini P, Arciola CR, Pezzali I, Bozzini S, Montanaro L, Tanzi MC, et al. Antibacterial activity of zinc modified titanium oxide surface. Int J Artif Organs. 2006;29:434–42. doi: 10.1177/039139880602900414. [DOI] [PubMed] [Google Scholar]
- 68.Hodgkinson V, Petris MJ. Copper homeostasis at the host-pathogen interface. J Biol Chem. 2012;287:13549–55. doi: 10.1074/jbc.R111.316406. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 69.Pelgrift RY, Friedman AJ. Nanotechnology as a therapeutic tool to combat microbial resistance. Adv Drug Deliv Rev. 2013;65:1803–15. doi: 10.1016/j.addr.2013.07.011. [DOI] [PubMed] [Google Scholar]
- 70.Moseke C, Gbureck U, Elter P, Drechsler P, Zoll A, Thull R, et al. Hard implant coatings with antimicrobial properties. J Mater Sci Mater Med. 2011;22:2711–20. doi: 10.1007/s10856-011-4457-6. [DOI] [PubMed] [Google Scholar]
- 71.Shtansky DV, Gloushankova NA, Bashkova IA, Kharitonova MA, Moizhess TG, Sheveiko AN, et al. Multifunctional Ti-(Ca, Zr)-(C, N, O, P) films for load-bearing implants. Biomaterials. 2006;27:3519–31. doi: 10.1016/j.biomaterials.2006.02.012. [DOI] [PubMed] [Google Scholar]
- 72.Arenas MA, Perez-Jorge C, Conde A, Matykina E, Hernandez-Lopez JM, Perez-Tanoira R, et al. Doped TiO2 anodic layers of enhanced antibacterial properties. Colloids Surf B: Biointerfaces. 2013;105:106–12. doi: 10.1016/j.colsurfb.2012.12.051. [DOI] [PubMed] [Google Scholar]
- 73.Hu H, Zhang W, Qiao Y, Jiang X, Liu X, Ding C. Antibacterial activity and increased bone marrow stem cell functions of Zn-incorporated TiO2 coatings on titanium. Acta Biomater. 2012;8:904–15. doi: 10.1016/j.actbio.2011.09.031. [DOI] [PubMed] [Google Scholar]
- 74.Holinka J, Pilz M, Kubista B, Presterl E, Windhager R. Effects of selenium coating of orthopaedic implant surfaces on bacterial adherence and osteoblastic cell growth. Bone Joint J. 2013;95:678–82. doi: 10.1302/0301-620X.95B5.31216. [DOI] [PubMed] [Google Scholar]
- 75.Tran PA, Webster TJ. Selenium nanoparticles inhibit Staphylococcus aureus growth. Int J Nanomed. 2011;6:1553–8. doi: 10.2147/IJN.S21729. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 76.Martynkova GS, Valaskova M. Antimicrobial nanocomposites based on natural modified materials: a review of carbons and clays. J Nanosci Nanotechnol. 2014;14:673–93. doi: 10.1166/jnn.2014.8903. [DOI] [PubMed] [Google Scholar]
- 77.Tsuchiya H, Shirai T, Nishida H, Murakami H, Kabata T, Yamamoto N, et al. Innovative antimicrobial coating of titanium implants with iodine. J Orthop Sci. 2012;17(5):595–604. doi: 10.1007/s00776-012-0247-3. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 78.Antoci V, Jr, King SB, Jose B, Parvizi J, Zeiger AR, Wickstrom E, et al. Vancomycin covalently bonded to titanium alloy prevents bacterial colonization. J Orthop Res. 2007;25:858–66. doi: 10.1002/jor.20348. [DOI] [PubMed] [Google Scholar]
- 79.Alt V, Bitschnau A, Osterling J, Sewing A, Meyer C, Kraus R, et al. The effects of combined gentamicin-hydroxyapatite coating for cementless joint prostheses on the reduction of infection rates in a rabbit infection prophylaxis model. Biomaterials. 2006;27:4627–34. doi: 10.1016/j.biomaterials.2006.04.035. [DOI] [PubMed] [Google Scholar]
- 80.Schmidmaier G, Lucke M, Wildemann B, Haas NP, Raschke M. Prophylaxis and treatment of implant-related infections by antibiotic-coated implants: a review. Injury. 2006;37:S105–12. doi: 10.1016/j.injury.2006.04.016. [DOI] [PubMed] [Google Scholar]
- 81.Fei J, Liu GD, Pan CJ, Chen JY, Zhou YG, Xiao SH, et al. Preparation, release profiles and antibacterial properties of vancomycin-loaded Ca-P coating titanium alloy plate. J Mater Sci Mater Med. 2011;22:989–95. doi: 10.1007/s10856-011-4277-8. [DOI] [PubMed] [Google Scholar]
- 82.Neut D, Dijkstra RJ, Thompson JI, van der Mei HC, Busscher HJ. A gentamicin-releasing coating for cementless hip prostheses-Longitudinal evaluation of efficacy using in vitro bio-optical imaging and its wide-spectrum antibacterial efficacy. J Biomed Mater Res A. 2012;100:3220–6. doi: 10.1002/jbm.a.34258. [DOI] [PubMed] [Google Scholar]
- 83.Shchukin D, Mohwald H. Materials science. A coat of many functions. Science. 2013;341:1458–9. doi: 10.1126/science.1242895. [DOI] [PubMed] [Google Scholar]
- 84.Shi X, Wu H, Li Y, Wei X, Du Y. Electrical signals guided entrapment and controlled release of antibiotics on titanium surface. J Biomed Mater Res A. 2013;101:1373–8. doi: 10.1002/jbm.a.34432. [DOI] [PubMed] [Google Scholar]
- 85.Guillaume O, Garric X, Lavigne JP, Van Den Berghe H, Coudane J. Multilayer, degradable coating as a carrier for the sustained release of antibiotics: preparation and antimicrobial efficacy in vitro. J Control Release. 2012;162:492–501. doi: 10.1016/j.jconrel.2012.08.003. [DOI] [PubMed] [Google Scholar]
- 86.Tang Y, Zhao Y, Wang H, Gao Y, Liu X, Wang X, et al. Layer-by-layer assembly of antibacterial coating on interbonded 3D fibrous scaffolds and its cytocompatibility assessment. J Biomed Mater Res A. 2012;100:2071–8. doi: 10.1002/jbm.a.34116. [DOI] [PubMed] [Google Scholar]
- 87.Fuchs T, Stange R, Shmidmaier S, Raschke MJ. The use of gentamicin-coated nails in the tibia: preliminary results of a prospective study. Arch Orthop Trauma Surg. 2011;131(10):1419–25. doi: 10.1007/s00402-011-1321-6. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 88.Campbell AA, Song L, Li XS, Nelson BJ, Bottoni C, Brooks DE, et al. Development, characterization, and anti-microbial efficacy of hydroxyapatitechlorhexidine coatings produced by surface-induced mineralization. J Biomed Mater Res. 2000;53:400e7. doi: 10.1002/1097-4636(2000)53:4<400::AID-JBM14>3.0.CO;2-Z. [DOI] [PubMed] [Google Scholar]
- 89.Kozlovsky A, Artzi Z, Moses O, Kamin-Belsky N, Greenstein RB. Interaction of chlorhexidine with smooth and rough types of titanium surfaces. J Periodontol. 2006;77:1194e200. doi: 10.1902/jop.2006.050401. [DOI] [PubMed] [Google Scholar]
- 90.Yount NY, Yeaman MR. Emerging themes and therapeutic prospects for anti-infective peptides. Annu Rev Pharmacol Toxicol. 2012;52:337–60. doi: 10.1146/annurev-pharmtox-010611-134535. [DOI] [PubMed] [Google Scholar]
- 91.Haney EF, Hancock RE. Peptide design for antimicrobial and immunomodulatory applications. Biopolymers. 2013;100:572–83. doi: 10.1002/bip.22250. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 92.Dobson AJ, Purves J, Kamysz W, Rolff J. Comparing selection on S. aureus between antimicrobial peptides and common antibiotics. PLoS One. 2013;8:e76521. doi: 10.1371/journal.pone.0076521. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 93.Holmberg KV, Abdolhosseini M, Li Y, Chen X, Gorr SU, Aparicio C. Bio-inspired stable antimicrobial peptide coatings for dental applications. Acta Biomater. 2013;9:8224–31. doi: 10.1016/j.actbio.2013.06.017. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 94.Costa F, Maia S, Gomes P, Martins MC. Characterization of hLF1-11 immobilization onto chitosan ultrathin films, and its effects on antimicrobial activity. Acta Biomater. 2014, doi:10.1016/j.actbio.2014.02.028. [DOI] [PubMed]
- 95.Yang CC, Lin CC, Liao JW, Yen SK. Vancomycin-chitosan composite deposited on post porous hydroxyapatite coated Ti6Al4V implant for drug controlled release. Mater Sci Eng C. 2013;33:2203–12. doi: 10.1016/j.msec.2013.01.038. [DOI] [PubMed] [Google Scholar]
- 96.Jennison T, McNally M, Pandit H. Prevention of infection in external fixator pin sites. Acta Biomater. 2014;10:595–603. doi: 10.1016/j.actbio.2013.09.019. [DOI] [PubMed] [Google Scholar]
- 97.Muszanska AK, Rochford ET, Gruszka A, Bastian AA, Busscher HJ, Norde W, et al. Antiadhesive polymer brush coating functionalized with antimicrobial and rgd peptides to reduce biofilm formation and enhance tissue integration. Biomacromolecules. 2014;15:2019–2026. doi: 10.1021/bm500168s. [DOI] [PubMed] [Google Scholar]
- 98.Yu Q, Cho J, Shivapooja P, Ista LK, Lopez GP. Nanopatterned smart polymer surfaces for controlled attachment, killing, and release of bacteria. ACS Appl Mater Interfaces. 2013;5:9295–304. doi: 10.1021/am4022279. [DOI] [PubMed] [Google Scholar]
- 99.Buchholz HW, Engelbrecht H. Depot effects of various antibiotics mixed with Palacos resins. Chirurg. 1970;41:511e5. [PubMed] [Google Scholar]
- 100.Engesaeter LB, Lie SA, Espehaug B, Furnes O, Vollset SE, Havelin LI. Antibiotic prophylaxis in total hip arthroplasty: effects of antibiotic prophylaxis systemically and in bone cement on the revision rate of 22,170 primary hip replacements followed 0–14 years in the Norwegian Arthroplasty Register. Acta Orthop Scand. 2003;74:644e51. doi: 10.1080/00016470310018135. [DOI] [PubMed] [Google Scholar]
- 101.Gutowski CJ, Zmistowski BM, Clyde CT, Parvizi J. The economics of using prophylactic antibiotic-loaded bone cement in total knee replacement. Bone Joint J. 2014;96-B(1):65–9. doi: 10.1302/0301-620X.96B1.31428. [DOI] [PubMed] [Google Scholar]
- 102.Dunbar MJ. Antibiotic bone cements: their use in routine primary total joint arthroplasty is justified. Orthopedics. 2009;32:9. doi: 10.3928/01477447-20090728-20. [DOI] [PubMed] [Google Scholar]
- 103.van de Belt H, Neut D, Schenk W, van Horn JR, van Der Mei HC, Busscher HJ. Staphylococcus aureus biofilm formation on different gentamicin-loaded polymethylmethacrylate bone cements. Biomaterials. 2001;22(12):1607–11. doi: 10.1016/S0142-9612(00)00313-6. [DOI] [PubMed] [Google Scholar]
- 104.Neut D, Hendriks JG, van Horn JR, van der Mei HC, Busscher HJ. Pseudomonas aeruginosa biofilm formation and slime excretion on antibiotic-loaded bone cement. Acta Orthop. 2005;76(1):109–14. doi: 10.1080/00016470510030427. [DOI] [PubMed] [Google Scholar]
- 105.De Grood MP. Pathology, diagnosis and treatment of subdural empyema. Arch Chir Neerl. 1951;3:128e38. [PubMed] [Google Scholar]
- 106.Buttaro MA, Pusso R, Piccaluga F. Vancomycin-supplemented impacted bone allografts in infected hip arthroplasty. Two-stage revision results. J Bone Jt Surg Br. 2005;87:314e9. doi: 10.1302/0301-620x.87b3.14788. [DOI] [PubMed] [Google Scholar]
- 107.Gautier H, Merle C, Auget JL, Daculsi G. Isostatic compression, a new process for incorporating vancomycin into biphasic calcium phosphate: comparison with a classical method. Biomaterials. 2000;21:243e9. doi: 10.1016/S0142-9612(99)00139-8. [DOI] [PubMed] [Google Scholar]
- 108.Yamamura K, Iwata H, Yotsuyanagi T. Synthesis of antibiotic-loaded hydroxyapatite beads and in vitro drug release testing. J Biomed Mater Res. 1992;26:1053e64. doi: 10.1002/jbm.820260807. [DOI] [PubMed] [Google Scholar]
- 109.Overstreet D, McLaren A, Calara F, Vernon B, McLemore R. Local gentamicin delivery from resorbable viscous hydrogels is therapeutically effective. Clin Orthop Relat Res. 2015;473(1):337–47. doi: 10.1007/s11999-014-3935-9. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 110.Pitarresi G, Palumbo FS, Calascibetta F, Fiorica C, Di Stefano M, Giammona G. Medicated hydrogels of hyaluronic acid derivatives for use in orthopedic field. Int J Pharm. 2013;449(1–2):84–94. doi: 10.1016/j.ijpharm.2013.03.059. [DOI] [PubMed] [Google Scholar]
- 111.Heydemann JS, Nelson CL. Short-term preventive antibiotics. Clin Orthop Relat Res. 1986;205:184–7. [PubMed] [Google Scholar]
- 112.Antoci V, Jr, Adams CS, Hickok NJ, Shapiro IM, Parvizi J. Antibiotics for local delivery systems cause skeletal cell toxicity in vitro. Clin Orthop Relat Res. 2007;462:200–6. doi: 10.1097/BLO.0b013e31811ff866. [DOI] [PubMed] [Google Scholar]
- 113.Drago L, Boot W, Dimas K, Malizos K, Hänsch GM, Stuyck J, et al. Does implant coating with antibacterial-loaded hydrogel reduce bacterial colonization and biofilm formation in vitro ? Clin Orthop Relat Res. 2014;472(11):3311–23. doi: 10.1007/s11999-014-3558-1. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 114.Giavaresi G, Meani E, Sartori M, Ferrari A, Bellini D, Sacchetta AC, et al. Efficacy of antibacterial-loaded coating in an in vivo model of acutely highly contaminated implant. Int Orthop. 2014;38(7):1505–12. doi: 10.1007/s00264-013-2237-2. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 115.Logoluso N, Malizos K, Blauth M, Danita A, Simon K, Romanò C. Anti-bacterial hydrogel coating of osteosynthesis implants: early clinical results from a multi-center prospective trial. European Cells and Materials. 2015;30 Suppl 2:35.
- 116.Boot W, Vogely HCh, Nikkels PGJ, Pouran B, van Rijen M, Dhert WJA, et al. Local prophylaxis of implant-related infections using a hydrogel as carrier. European Cells and Materials. 2015;30 Suppl 2:19. [DOI] [PubMed]
- 117.Romanò CL, Logoluso N, Drago L. Antibiofilm strategies in orthopedics: where are we? In Peri-Operative Medical Management for Total Joiint Arthroplasty. Switzerland: Springer International Publishing; 2014. p. 269–86. doi:10.1007/978-3-319-07203-6.
- 118.Gallo J, Holinka M, Moucha CS. Antibacterial surface treatment for orthopaedic implants. Int J Mol Sci. 2014;15(8):13849–80. doi: 10.3390/ijms150813849. [DOI] [PMC free article] [PubMed] [Google Scholar]