A meta-analysis of bone cement mediated antibiotic release: Overkill, but a viable approach to eradicate osteomyelitis and other infections tied to open procedures.

Mater Sci Eng C Mater Biol Appl

Department of Materials Science and Engineering, The University of Michigan, 2300 Hayward St., Ann Arbor, MI 48109, United States of America; Department of Biomedical Engineering, The University of Michigan, 2300 Hayward St., Ann Arbor, MI 48109, United States of America; Macromolecular Science and Engineering Program, The University of Michigan, 2300 Hayward St., Ann Arbor, MI 48109, United States of America. Electronic address:

Published: April 2021

AI Article Synopsis

  • Research shows that antibiotics (0-6% w/w) in bone cements can successfully combat localized infections, with gentamycin-infused mixtures being commonly produced by manufacturers.
  • Studies suggest that while antibiotic-infused cements may delay infections, over 99% of vancomycin remains trapped and not bioavailable after solidification, despite its potency against staph infections.
  • The mechanical strength of these antibiotic-loaded cements is reduced by simulated fluid exposure, with some samples failing to meet industry standards, highlighting the need for better drug delivery systems and formulations for improved bioavailability.

Article Abstract

A number of clinical studies have highlighted the success of antibiotics formulated at concentrations between 0 and 6% w/w into bone cements to address localized infections. Separately, some commercial manufacturers have produced gentamycin-infused bone cement mixtures as a countermeasure to infection. The anecdotal evidence suggests that antibiotic infused cements can help eradicate or delay the onset of infections. Quantifying the functionality of that response is more challenging. We have surveyed the literature to identify studies in which controlled drug release or mechanical behavioral assessments have been conducted on drug-infused cements. The focus here is on vancomycin (VAN) in part due to its higher potency relative to gentamycin and its more common usage for staph infections. Takeaways from the limited pool of research studies indicate that large fractions (>99%) of the infused vancomycin remain sequestered in the cement and aren't bioavailable after solidification. Antibiotic fluence ranged from 1 to 283 μg/cmhr. The initial strength of the various antibiotic loaded samples as produced were 52-96 MPa. Simulated exposures in a fluid environment by submersion reduced the antibiotic loaded strengths between 3 and 29%. Some strength measurements were noted below the ASTM F451 standard for acrylic bone cement although drug releasing spacers likely have different requirements. The glassy behavior of the cured cement led to both vancomycin and gentamicin having low permeability and a burst response. Smaller drug molecules and more gel-like immobilization matrices with lower glass transition temperatures offer higher potential for larger and more comprehensive drug bioavailability.

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Source
http://dx.doi.org/10.1016/j.msec.2021.111999DOI Listing

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