International Journal of Molecular Sciences (Feb 2023)

Evaluating the Targeting of a <i>Staphylococcus-aureus</i>-Infected Implant with a Radiolabeled Antibody In Vivo

  • Bruce van Dijk,
  • J. Fred F. Hooning van Duyvenbode,
  • Lisanne de Vor,
  • F. Ruben H. A. Nurmohamed,
  • Marnix G. E. H. Lam,
  • Alex J. Poot,
  • Ruud M. Ramakers,
  • Sofia Koustoulidou,
  • Freek J. Beekman,
  • Jos van Strijp,
  • Suzan H. M. Rooijakkers,
  • Ekaterina Dadachova,
  • H. Charles Vogely,
  • Harrie Weinans,
  • Bart C. H. van der Wal

DOI
https://doi.org/10.3390/ijms24054374
Journal volume & issue
Vol. 24, no. 5
p. 4374

Abstract

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Implant infections caused by Staphylococcus aureus are difficult to treat due to biofilm formation, which complicates surgical and antibiotic treatment. We introduce an alternative approach using monoclonal antibodies (mAbs) targeting S. aureus and provide evidence of the specificity and biodistribution of S.-aureus-targeting antibodies in a mouse implant infection model. The monoclonal antibody 4497-IgG1 targeting wall teichoic acid in S. aureus was labeled with indium-111 using CHX-A”-DTPA as a chelator. Single Photon Emission Computed Tomography/computed tomographyscans were performed at 24, 72 and 120 h after administration of the 111In-4497 mAb in Balb/cAnNCrl mice with a subcutaneous implant that was pre-colonized with S. aureus biofilm. The biodistribution of this labelled antibody over various organs was visualized and quantified using SPECT/CT imaging, and was compared to the uptake at the target tissue with the implanted infection. Uptake of the 111In-4497 mAbs at the infected implant gradually increased from 8.34 %ID/cm3 at 24 h to 9.22 %ID/cm3 at 120 h. Uptake at the heart/blood pool decreased over time from 11.60 to 7.58 %ID/cm3, whereas the uptake in the other organs decreased from 7.26 to less than 4.66 %ID/cm3 at 120 h. The effective half-life of 111In-4497 mAbs was determined to be 59 h. In conclusion, 111In-4497 mAbs were found to specifically detect S. aureus and its biofilm with excellent and prolonged accumulation at the site of the colonized implant. Therefore, it has the potential to serve as a drug delivery system for the diagnostic and bactericidal treatment of biofilm.

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