Low-dose X-ray-stimulated LaGaO3:Sb,Cr near-infrared persistent luminescence nanoparticles for deep-tissue and renewable in vivo bioimaging

Bo Mei Liu, Rui Zou, Sun Qi Lou, Yi Fan Gao, Li Ma, Ka Leung Wong, Jing Wang

Research output: Contribution to journalArticlepeer-review

67 Scopus citations

Abstract

X-ray-stimulated near-infrared persistent luminescence nanoparticles (NIR-PLNPs) offer attractive capabilities for autofluorescence free deep-seated imaging and depth-independent treatment, but still suffer from adverse effects caused by high-dose X-ray irradiation (>5 Gy). From the viewpoint of two centers of NIR-PLNPs, i.e., X-ray photon absorption center and defects center, we here propose a top-down composition design strategy for the development of low dose X-ray-stimulated NIR-PLNPs with improved X-ray photon absorption efficiency and optimized persistent luminescence (PersL) performance. Successfully, hypersensitive X-ray-stimulated NIR-PLNPs LaGaO3:Sb3+,Cr3+ with a super-long PersL emission (>500 h) at ∼750 nm are prepared. The nature of high Z atomic constituents of the host LaGaO3 endows these NIR-PLNPs with strong X-ray absorption capacity. Simply by codoping with size-mismatched ions Sb3+, the concentration of oxygen vacancies in the host is rationally optimized, leading to the enhanced NIR PersL performance of Cr3+ ions. In vivo bioimaging demonstrates that the designed X-ray-stimulated NIR-PLNPs LaGaO3:Sb3+,Cr3+ can be readily reactivated under X-ray irradiation with even a lower dose to 0.37 Gy, showing the advantages of these nanoparticles on deep-seated imaging and treatment. More importantly, we anticipate that our proposed top-down composition design strategy can be applied to develop much low dose X-ray-stimulated NIR-PLNPs in the future.

Original languageEnglish
Article number127133
JournalChemical Engineering Journal
Volume404
DOIs
StatePublished - Jan 15 2021

Keywords

  • Bioimaging
  • Nanoparticle
  • Near-infrared
  • Persistent luminescence
  • X-ray

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