99mTc-Functionalized Single-Walled Carbon Nanotubes for Bone Targeting

Tailoring carbon nanotube surface chemistry is essential for biomedical applications. Bisphosphonate–carbon nanotube conjugates were prepared to target regions of active bone metabolism. The conjugates were synthesized using covalent functionalization (G1) or latently reactive polymer–nanotube compl...

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Veröffentlicht in:ACS applied nano materials 2020-12, Vol.3 (12), p.11819-11824
Hauptverfasser: Genady, Afaf R, Fong, Darryl, Slikboer, Samantha R, El-Zaria, Mohamed E, Swann, Rowan, Janzen, Nancy, Faraday, Amber, McNelles, Stuart A, Rezvani, Mojgan, Sadeghi, Saman, Adronov, Alex, Valliant, John F
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Sprache:eng ; jpn
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Zusammenfassung:Tailoring carbon nanotube surface chemistry is essential for biomedical applications. Bisphosphonate–carbon nanotube conjugates were prepared to target regions of active bone metabolism. The conjugates were synthesized using covalent functionalization (G1) or latently reactive polymer–nanotube complexes (G2), and it was found that the noncovalent G2 method afforded higher quality colloidal dispersions. The in vitro cytotoxicity tests against C2C12 cells were carried out and the results revealed low cytotoxicity and good biocompatibility profile for both bisphosphonate–carbon nanotube conjugates. The conjugates were radiolabeled with 99mTc in high radiochemical yield (80–92%). In vitro binding studies to hydroxyapatite showed binding of 77 and 36% for G1 and G2, respectively, after 1 h incubation at room temperature. A biodistribution study of G1 and G2 in vivo in a Balb/c mouse model demonstrated rapid blood clearance after 1 h and superior bone localization of G2 conjugates as compared to G1 conjugates. Photoacoustic imaging of nanotube conjugates confirmed superior in vivo bone localization of G2 as compared to G1. Together, biodistribution studies of radiolabeled complexes and photoacoustic imaging demonstrated that latently reactive polymer–nanotube complexes are a promising platform to modulate carbon nanotube surface chemistry for targeted diagnostic and drug delivery.
ISSN:2574-0970
2574-0970
DOI:10.1021/acsanm.0c02339