Bright X-ray and up-conversion nanophosphors annealed using encapsulated sintering agents for bioimaging applications

Hongyu Chen; Fenglin Wang; Thomas L. Moore; Bin Qi; Dino Sulejmanovic; Shiou Jyh Hwu; O. Thompson Mefford; Frank Alexis; Jeffrey N. Anker

doi:10.1039/c7tb01289f

Bright X-ray and up-conversion nanophosphors annealed using encapsulated sintering agents for bioimaging applications

Hongyu Chen
, Fenglin Wang
, Thomas L. Moore
, Bin Qi
, Dino Sulejmanovic
, Shiou Jyh Hwu
, O. Thompson Mefford
, Frank Alexis
, Jeffrey N. Anker^*

^*Corresponding author for this work

Clemson University College of Engineering, Computing and Applied Sciences
Clemson University

Research output: Contribution to journal › Article › peer-review

23 Scopus citations

Abstract

Nanophosphors are promising contrast agents for deep tissue optical imaging applications because they can be excited by X-ray or near infrared light through tissue without background interference. For these bioimaging applications, the nanophosphors should ideally be small, monodispersed and brightly luminescent. However, most methods used to improve luminescence yield by annealing the particles to reduce crystal and surface defects (e.g. using flux or sintering agents) also cause particle fusion or require multiple component core-shell structures. Here, we report a novel method to prepare bright, uniformly sized X-ray nanophosphors (Gd₂O₂S:Eu or Tb) and upconversion nanophosphors (Y₂O₂S:Yb/Er, or Yb/Tm) with large crystal domain size without causing aggregation. A core-shell nanoparticle is formed, with NaF only in the core. We observe that increasing the NaF sintering agent concentration up to 7.6 mol% increases both crystal domain size and luminescence intensity (up to 40% of commercial microphosphors) without affecting the physical particle diameter. Above 7.6 mol%, particle fusion is observed. The annealing is insensitive to the cation (Na⁺ or K⁺) but varies strongly with anion, with F^- > Cl^- > CO₃^2- > Br^- > I^-. The luminescence depends strongly on crystal domain size. The data agree reasonably well with a simple domain surface quenching model, although the size-dependence suggests additional quenching mechanisms within small domains. The prepared bright nanophosphors were subsequently functionalized with PEG-folic acid to target MCF-7 breast cancer cells which overexpress folic acid receptors. Both X-ray and upconversion nanophosphors provided low background and bright luminescence which was imaged through 1 cm chicken breast tissue at a low dose of nanophosphors 200 μL (0.1 mg mL^-1). We anticipate these highly monodispersed and bright X-ray and upconversion nanophosphors will have significant potential for tumor targeted imaging.

Original language	English
Pages (from-to)	5412-5424
Number of pages	13
Journal	Journal of Materials Chemistry B
Volume	5
Issue number	27
DOIs	https://doi.org/10.1039/c7tb01289f
State	Published - 2017
Externally published	Yes

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10.1039/c7tb01289f

Cite this

@article{01d0928a15594ea1837644284fe80af6,

title = "Bright X-ray and up-conversion nanophosphors annealed using encapsulated sintering agents for bioimaging applications",

abstract = "Nanophosphors are promising contrast agents for deep tissue optical imaging applications because they can be excited by X-ray or near infrared light through tissue without background interference. For these bioimaging applications, the nanophosphors should ideally be small, monodispersed and brightly luminescent. However, most methods used to improve luminescence yield by annealing the particles to reduce crystal and surface defects (e.g. using flux or sintering agents) also cause particle fusion or require multiple component core-shell structures. Here, we report a novel method to prepare bright, uniformly sized X-ray nanophosphors (Gd2O2S:Eu or Tb) and upconversion nanophosphors (Y2O2S:Yb/Er, or Yb/Tm) with large crystal domain size without causing aggregation. A core-shell nanoparticle is formed, with NaF only in the core. We observe that increasing the NaF sintering agent concentration up to 7.6 mol\% increases both crystal domain size and luminescence intensity (up to 40\% of commercial microphosphors) without affecting the physical particle diameter. Above 7.6 mol\%, particle fusion is observed. The annealing is insensitive to the cation (Na+ or K+) but varies strongly with anion, with F- > Cl- > CO32- > Br- > I-. The luminescence depends strongly on crystal domain size. The data agree reasonably well with a simple domain surface quenching model, although the size-dependence suggests additional quenching mechanisms within small domains. The prepared bright nanophosphors were subsequently functionalized with PEG-folic acid to target MCF-7 breast cancer cells which overexpress folic acid receptors. Both X-ray and upconversion nanophosphors provided low background and bright luminescence which was imaged through 1 cm chicken breast tissue at a low dose of nanophosphors 200 μL (0.1 mg mL-1). We anticipate these highly monodispersed and bright X-ray and upconversion nanophosphors will have significant potential for tumor targeted imaging.",

author = "Hongyu Chen and Fenglin Wang and Moore, \{Thomas L.\} and Bin Qi and Dino Sulejmanovic and Hwu, \{Shiou Jyh\} and Mefford, \{O. Thompson\} and Frank Alexis and Anker, \{Jeffrey N.\}",

note = "Publisher Copyright: {\textcopyright} 2017 The Royal Society of Chemistry.",

year = "2017",

doi = "10.1039/c7tb01289f",

language = "Ingl{\'e}s",

volume = "5",

pages = "5412--5424",

journal = "Journal of Materials Chemistry B",

issn = "2050-7518",

publisher = "Royal Society of Chemistry",

number = "27",

}

TY - JOUR

T1 - Bright X-ray and up-conversion nanophosphors annealed using encapsulated sintering agents for bioimaging applications

AU - Chen, Hongyu

AU - Wang, Fenglin

AU - Moore, Thomas L.

AU - Qi, Bin

AU - Sulejmanovic, Dino

AU - Hwu, Shiou Jyh

AU - Mefford, O. Thompson

AU - Alexis, Frank

AU - Anker, Jeffrey N.

PY - 2017

Y1 - 2017

N2 - Nanophosphors are promising contrast agents for deep tissue optical imaging applications because they can be excited by X-ray or near infrared light through tissue without background interference. For these bioimaging applications, the nanophosphors should ideally be small, monodispersed and brightly luminescent. However, most methods used to improve luminescence yield by annealing the particles to reduce crystal and surface defects (e.g. using flux or sintering agents) also cause particle fusion or require multiple component core-shell structures. Here, we report a novel method to prepare bright, uniformly sized X-ray nanophosphors (Gd2O2S:Eu or Tb) and upconversion nanophosphors (Y2O2S:Yb/Er, or Yb/Tm) with large crystal domain size without causing aggregation. A core-shell nanoparticle is formed, with NaF only in the core. We observe that increasing the NaF sintering agent concentration up to 7.6 mol% increases both crystal domain size and luminescence intensity (up to 40% of commercial microphosphors) without affecting the physical particle diameter. Above 7.6 mol%, particle fusion is observed. The annealing is insensitive to the cation (Na+ or K+) but varies strongly with anion, with F- > Cl- > CO32- > Br- > I-. The luminescence depends strongly on crystal domain size. The data agree reasonably well with a simple domain surface quenching model, although the size-dependence suggests additional quenching mechanisms within small domains. The prepared bright nanophosphors were subsequently functionalized with PEG-folic acid to target MCF-7 breast cancer cells which overexpress folic acid receptors. Both X-ray and upconversion nanophosphors provided low background and bright luminescence which was imaged through 1 cm chicken breast tissue at a low dose of nanophosphors 200 μL (0.1 mg mL-1). We anticipate these highly monodispersed and bright X-ray and upconversion nanophosphors will have significant potential for tumor targeted imaging.

AB - Nanophosphors are promising contrast agents for deep tissue optical imaging applications because they can be excited by X-ray or near infrared light through tissue without background interference. For these bioimaging applications, the nanophosphors should ideally be small, monodispersed and brightly luminescent. However, most methods used to improve luminescence yield by annealing the particles to reduce crystal and surface defects (e.g. using flux or sintering agents) also cause particle fusion or require multiple component core-shell structures. Here, we report a novel method to prepare bright, uniformly sized X-ray nanophosphors (Gd2O2S:Eu or Tb) and upconversion nanophosphors (Y2O2S:Yb/Er, or Yb/Tm) with large crystal domain size without causing aggregation. A core-shell nanoparticle is formed, with NaF only in the core. We observe that increasing the NaF sintering agent concentration up to 7.6 mol% increases both crystal domain size and luminescence intensity (up to 40% of commercial microphosphors) without affecting the physical particle diameter. Above 7.6 mol%, particle fusion is observed. The annealing is insensitive to the cation (Na+ or K+) but varies strongly with anion, with F- > Cl- > CO32- > Br- > I-. The luminescence depends strongly on crystal domain size. The data agree reasonably well with a simple domain surface quenching model, although the size-dependence suggests additional quenching mechanisms within small domains. The prepared bright nanophosphors were subsequently functionalized with PEG-folic acid to target MCF-7 breast cancer cells which overexpress folic acid receptors. Both X-ray and upconversion nanophosphors provided low background and bright luminescence which was imaged through 1 cm chicken breast tissue at a low dose of nanophosphors 200 μL (0.1 mg mL-1). We anticipate these highly monodispersed and bright X-ray and upconversion nanophosphors will have significant potential for tumor targeted imaging.

UR - https://www.scopus.com/pages/publications/85023764623

U2 - 10.1039/c7tb01289f

DO - 10.1039/c7tb01289f

M3 - Artículo

C2 - 29497532

AN - SCOPUS:85023764623

SN - 2050-7518

VL - 5

SP - 5412

EP - 5424

JO - Journal of Materials Chemistry B

JF - Journal of Materials Chemistry B

IS - 27

ER -

Bright X-ray and up-conversion nanophosphors annealed using encapsulated sintering agents for bioimaging applications

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