TY - JOUR
T1 - Adjuvant antibiotic-loaded bone cement
T2 - Concerns with current use and research to make it work
AU - Hospital for Special Surgery 2019 Biofilm Symposium Workgroup
AU - Schwarz, Edward M.
AU - McLaren, Alex C.
AU - Sculco, Thomas P.
AU - Brause, Barry
AU - Bostrom, Mathias
AU - Kates, Stephen L.
AU - Parvizi, Javad
AU - Alt, Volker
AU - Arnold, William V.
AU - Carli, Alberto
AU - Chen, Antonia F.
AU - Choe, Hyonmin
AU - Coraça-Huber, Débora C.
AU - Cross, Michael
AU - Ghert, Michelle
AU - Hickok, Noreen
AU - Jennings, Jessica Amber
AU - Joshi, Manjari
AU - Metsemakers, Willem Jan
AU - Ninomiya, Mark
AU - Nishitani, Kohei
AU - Oh, Irvin
AU - Padgett, Douglas
AU - Ricciardi, Benjamin
AU - Saeed, Kordo
AU - Sendi, Parham
AU - Springer, Bryan
AU - Stoodley, Paul
AU - Wenke, Joseph C.
N1 - Publisher Copyright:
© 2020 Orthopaedic Research Society. Published by Wiley Periodicals, Inc.
PY - 2021/2
Y1 - 2021/2
N2 - Antibiotic-loaded bone cement (ALBC) is broadly used to treat orthopaedic infections based on the rationale that high-dose local delivery is essential to eradicate biofilm-associated bacteria. However, ALBC formulations are empirically based on drug susceptibility from routine laboratory testing, which is known to have limited clinical relevance for biofilms. There are also dosing concerns with nonstandardized, surgeon-directed, hand-mixed formulations, which have unknown release kinetics. On the basis of our knowledge of in vivo biofilms, pathogen virulence, safety issues with nonstandardized ALBC formulations, and questions about the cost-effectiveness of ALBC, there is a need to evaluate the evidence for this clinical practice. To this end, thought leaders in the field of musculoskeletal infection (MSKI) met on 1 August 2019 to review and debate published and anecdotal information, which highlighted four major concerns about current ALBC use: (a) substantial lack of level 1 evidence to demonstrate efficacy; (b) ALBC formulations become subtherapeutic following early release, which risks induction of antibiotic resistance, and exacerbated infection from microbial colonization of the carrier; (c) the absence of standardized formulation protocols, and Food and Drug Administration-approved high-dose ALBC products to use following resection in MSKI treatment; and (d) absence of a validated assay to determine the minimum biofilm eradication concentration to predict ALBC efficacy against patient specific micro-organisms. Here, we describe these concerns in detail, and propose areas in need of research.
AB - Antibiotic-loaded bone cement (ALBC) is broadly used to treat orthopaedic infections based on the rationale that high-dose local delivery is essential to eradicate biofilm-associated bacteria. However, ALBC formulations are empirically based on drug susceptibility from routine laboratory testing, which is known to have limited clinical relevance for biofilms. There are also dosing concerns with nonstandardized, surgeon-directed, hand-mixed formulations, which have unknown release kinetics. On the basis of our knowledge of in vivo biofilms, pathogen virulence, safety issues with nonstandardized ALBC formulations, and questions about the cost-effectiveness of ALBC, there is a need to evaluate the evidence for this clinical practice. To this end, thought leaders in the field of musculoskeletal infection (MSKI) met on 1 August 2019 to review and debate published and anecdotal information, which highlighted four major concerns about current ALBC use: (a) substantial lack of level 1 evidence to demonstrate efficacy; (b) ALBC formulations become subtherapeutic following early release, which risks induction of antibiotic resistance, and exacerbated infection from microbial colonization of the carrier; (c) the absence of standardized formulation protocols, and Food and Drug Administration-approved high-dose ALBC products to use following resection in MSKI treatment; and (d) absence of a validated assay to determine the minimum biofilm eradication concentration to predict ALBC efficacy against patient specific micro-organisms. Here, we describe these concerns in detail, and propose areas in need of research.
KW - Biofilm Meeting
KW - antibiotic-loaded bone cement (ALBC)
KW - local antibiotics
KW - musculoskeletal infection (MSKI)
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U2 - 10.1002/jor.24616
DO - 10.1002/jor.24616
M3 - Article
C2 - 31997412
AN - SCOPUS:85081232301
SN - 0736-0266
VL - 39
SP - 227
EP - 239
JO - Journal of Orthopaedic Research
JF - Journal of Orthopaedic Research
IS - 2
ER -