Session VIII - Basic Science


Fri., 10/6/06 Basic Science, Paper #49, 4:54 pm

The Effect on Infection Resistance of a Local Antiseptic and Antibiotic Coating on Osteosynthesis Implants: An In Vitro and In Vivo Study

Thomas Kälicke, MD (*); Thomas Manfred Frangen, MD (*);
Jörg Schierholz, MD (*); Gert Muhr, MD (*); Manfred Köller, MD (*);
Dominik Seybold, MD (*); Stephan Arens, MD (*);
Berufsgenossenschaftliche Kliniken Bergmannsheil, Department of Surgery, Trauma Center, University of Bochum, Bochum, Germany

Purpose: The purpose of this study was to acquire information about the effect of an antibacterial and biodegradable poly-L-lactide (PLLA) coated titanium plate osteosynthesis on local infection resistance.

Methods: For our in vitro and in vivo experiments, we used 6-hole AO DC minifragment titanium plates. The implants were coated with biodegradable, semiamorphous PLLA (coating about 30 µm thick). This acted as a carrier substance to which either antibiotics or antiseptics were added. The antibiotic we applied was a combination of Rifampicin and fusidic acid; the antiseptic was a combination of Octenidin and Irgasan.

This produced the following groups:

Group I: 6-hole AO DC minifragment titanium plate without PLLA

Group II: 6-hole AO DC minifragment titanium plate with PLLA without antibiotics/antiseptics

Group III: 6-hole AO DC minifragment titanium plate with PLLA + 3% Rifampicin and 7% fusidic acid,

Group IV: 6-hole AO DC minifragment titanium plate with PLLA + 2% Octenidin and 8% Irgasan.

In vitro, we investigated the degradation and the release of the PLLA coating over a period of 6 weeks, the bactericidal efficacy of antibiotics/antiseptics after their release from the coating, and the bacterial adhesion of Staphylococcus aureus to the implants. In vivo, we compared the infection rates in white New Zealand rabbits after titanium plate osteosynthesis of the tibia with or without antibacterial coating after local percutaneous bacterial inoculations at different concentrations (2 ¥ 105 to 2 ¥ 108). The plate, the contaminated soft tissues, and the underlying bone were removed under sterile conditions after 28 days and quantitatively evaluated for bacterial growth. A stepwise experimental design with an "up and down" dosage technique was used to adjust the bacterial challenge in the area of the ID50 (50% infection dose). Statistical evaluation of the differences between the infection rates of both groups was performed using the two-sided Fisher exact test (P <0.05).

Results: Over a period of six weeks, a continuous degradation of the PLLA coating of 13%, on average, was seen in vitro in 0.9% NaCl solution. The elution tests on titanium implants with antibiotic or antiseptic coatings produced average release values of 60% of the incorporated antibiotic or 62% of the incorporated antiseptic within the first 60 minutes. This was followed by a much slower, but nevertheless continuous, release of the incorporated antibiotic and antiseptic over days and weeks. At the end of the test period of 42 days, 20% of the incorporated antibiotic and 15% of the incorporated antiseptic had not yet been released from the coating. The antibacterial effect of the antibiotic/antiseptic is not lost by integrating it into the PLLA coating. The overall infection rate in the in vivo investigation was 50%. For groups I and II, the infection rates were both 83% (10 of 12 animals). In groups III and IV with antibacterial coating, the infection rates were both 17% (2 of 12 animals). The ID50 in the antibacterial-coated groups III and IV was recorded as 1 ¥ 108 CFU, whereas the ID50 values in groups I and II without antibacterial coating were a hundred times lower at 1 ¥ 106 CFU, respectively. The difference between the groups with and without antibacterial coating was statistically significant (P = 0.033).

Conclusions: Using an antibacterial biodegradable PLLA coating on titanium plates, a significant reduction of infection rate in an in vitro and in vivo investigation could be demonstrated. For the first time we were able to show, under standardized and reproducible conditions, that an antiseptic coating leads to the same reduction in infection rate as an antibiotic coating. Taking the problem of antibiotic-induced bacterial resistance into consideration, we thus regard the antiseptic coating, which shows the same level of effectiveness, as advantageous.


If noted, the author indicates something of value received. The codes are identified as a-research or institutional support; b-miscellaneous funding; c-royalties; d-stock options; e-consultant or employee; n-no conflicts disclosed, and *disclosure not available at time of printing.
· The FDA has not cleared this drug and/or medical device for the use described in this presentation (i.e., the drug or medical device is being discussed for an "off label" use). · · FDA information not available at time of printing.