Intratumoral administration of astatine-211-labeled gold nanoparticle for alpha therapy

Kato, Hirohisa; Huang, Xuhao; Kadonaga, Yuichiro; Katayama, Daisuke; Ooe, Kazuhiro; Shimoyama, Atsushi; Kabayama, Kazuya; Toyoshima, Atsushi; Shinohara, Atsushi; Hatazawa, Jun; Fukase, Koichi

doi:10.1186/s12951-021-00963-9

Cited by 34 publications

(34 citation statements)

References 29 publications

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“…In contrast, in vitro cellular uptake and DNA DSB induction of both mPEG-modi ed AuNPs were low. We also report that in vitro uptake of 211 At-labeled AuNPs does not correlate with their in vivo anticancer effects in our previous intratumoral administration study [13]. The 120 nm 211 At-AuNPs@mPEG showed evident cytotoxicity in an in vitro cellular assay, while 211 At-labeled AuNPs of smaller sizes did not show cytotoxicity.…”

Section: Discussionmentioning

confidence: 56%

“…We recently reported that 211 At-AuNPs@mPEG exhibited cytotoxicity when they were absorbed by the tumor cells and the intratumoral administration of 211 At-AuNPs@mPEG strongly suppressed the cancer growth in a particle size-dependent manner. Smaller particles showed a more rapid distribution in tumor regions, and 5 nm 211 At-AuNPs@mPEG showed the highest suppression of cancer growth among various sizes of AuNPs tested [13]. A similar nanoseed brachytherapy using 211 At-labeled gold nanostars has also reported signi cant inhibition of the growth of human gliomas in a murine model [25].…”

Section: Discussionmentioning

confidence: 92%

“…Various surface-modi ed 211 At-labeled AuNPs were also readily obtained at RCY. In addition, the At-Au bond was reported to be stable both in theory and experimentally [13,18,34]. Another major problem was that 211 At or 211 At-labeled compounds readily stick to the reaction vessel and reduce the yields of labeled products.…”

Section: Discussionmentioning

confidence: 99%

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Astatine-211-Labeled Gold Nanoparticles for Targeted Alpha-particle Therapy via Intravenous Injection

Huang

Kaneda-Nakashima

Kadonaga

et al. 2022

Preprint

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Background: Alpha-particle radiotherapy has gained considerable attention owing to its potent anti-cancer effect. 211At, with a relatively short half-life of 7.2 h, emits an alpha particle within a few cell diameters with high kinetic energy, which damages cancer cells with high biological effectiveness. In this study, we investigated the intravenous injection of 211At-labeled gold nanoparticles (AuNPs) for targeted alpha-particle therapy (TAT). Results: Different kinds of surface-modified gold nanoparticles can be labeled with 211At in high radiochemical yield in 5 min, and no purification is necessary. In vivo biodistribution results showed the accumulation of 5 nm 211At-AuNPs@mPEG at 2.25 % injection dose per gram in tumors within 3 h via the enhanced permeability and retention effect. Additionally, we observed a long retention time in tumor tissues within 24 h. This is the first study to demonstrate the anti-tumor efficacy of 5 nm 211At-AuNPs@mPEG that can significantly suppress tumor growth in a pancreatic cancer model via intravenous administration. Conclusions: AuNPs are satisfactory carriers for 211At delivery, due to simple and efficient synthesis processes and high stability. Intravenous administration of 5 nm 211At-AuNPs@mPEG has a significant anti-tumor effect. This study provides a new framework for designing nanoparticles suitable for targeted alpha-particle therapy via intravenous injection.

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Section: Discussionmentioning

confidence: 56%

Section: Discussionmentioning

confidence: 92%

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Astatine-211-Labeled Gold Nanoparticles for Targeted Alpha-particle Therapy via Intravenous Injection

Huang

Kaneda-Nakashima

Kadonaga

et al. 2022

Preprint

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“…This approach has been utilized in several reports and has already shown effective results when labeling antibodies with 211 At 42 , 43 . An additional possible use for NPs labeled with 211 At could be brachytherapy as shown in a recent report, where tumor growth was inhibited for 38 days 44 . When administering the 211 At-PMs directly at the tumor site, accumulation in the liver can be avoided and, therefore, the degradation of the micelles and consequent deastatination may be limited.…”

Section: Resultsmentioning

confidence: 99%

Covalent core-radiolabeling of polymeric micelles with ¹²⁵I/²¹¹At for theranostic radiotherapy

Sporer¹,

Poulie²,

Bäck³

et al. 2022

Nanotheranostics

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Astatine-211 ( 211 At) is one of the most promising α-emitters for targeted alpha therapy, especially of cancer metastases. However, the lack of a stable isotope, frequent in vivo deastatination, and limited radiochemical knowledge makes it challenging to apply. Here, we report a new strategy for radiolabeling the lipophilic core of polymeric micelles (PMs) with covalently bound 211 At. The PMs were radiolabeled via either an indirect synthon-based method or directly on the amphipathic block copolymer. The radiochemistry was optimized with iodine-125 ( 125 I) and then adapted for 211 At, enabling the use of both elements as a potential theranostic pair. PMs that were core-radiolabeled with both 125 I or 211 At were prepared and characterized, based on a PEG(5k)-PLGA(10k) co-polymer. The stability of the radiolabeled PMs was evaluated in mouse serum for 21 h, showing radiochemical stability above 85%. After in vivo evaluation of the 211 At- labeled PMs, 4-5 % ID/g of the 211 At could still be detected in the blood, showing a promising in vivo stability of the PMs. Further, 211 At-labeled PMs accumulated in the spleen (20-30 %ID/g) and the liver (2.5- 5.5 %ID/g), along with some detection of 211 At in the thyroid (3.5-9 %ID/g). This led to the hypothesis that deastatination takes place in the liver, whereas good stability of the 211 At core-radiolabel was observed in the blood.

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“… 31 In the immunotherapy of PDAC, nanomedicines can be developed to facilitate antitumour immune responses through a series of immuno-potentiating functions after being directly injected into tumours. 32 , 33 Immunotherapy drug through intratumoural injection in PDAC exerted prominent antitumour effects and resulted in tumour decrease in several clinical trials (NCT02045589; NCT03198546). 34 , 35 Moreover, intra-tumoural delivery of agents has also been reported in the application of other tumour types.…”

Section: Discussionmentioning

confidence: 99%

Optical magnetic multimodality imaging of plectin-1-targeted imaging agent for the precise detection of orthotopic pancreatic ductal adenocarcinoma in mice

et al. 2022

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Intratumoral administration of astatine-211-labeled gold nanoparticle for alpha therapy

Cited by 34 publications

References 29 publications

Astatine-211-Labeled Gold Nanoparticles for Targeted Alpha-particle Therapy via Intravenous Injection

Astatine-211-Labeled Gold Nanoparticles for Targeted Alpha-particle Therapy via Intravenous Injection

Covalent core-radiolabeling of polymeric micelles with ¹²⁵I/²¹¹At for theranostic radiotherapy

Optical magnetic multimodality imaging of plectin-1-targeted imaging agent for the precise detection of orthotopic pancreatic ductal adenocarcinoma in mice

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Intratumoral administration of astatine-211-labeled gold nanoparticle for alpha therapy

Cited by 34 publications

References 29 publications

Astatine-211-Labeled Gold Nanoparticles for Targeted Alpha-particle Therapy via Intravenous Injection

Astatine-211-Labeled Gold Nanoparticles for Targeted Alpha-particle Therapy via Intravenous Injection

Covalent core-radiolabeling of polymeric micelles with 125I/211At for theranostic radiotherapy

Optical magnetic multimodality imaging of plectin-1-targeted imaging agent for the precise detection of orthotopic pancreatic ductal adenocarcinoma in mice

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Covalent core-radiolabeling of polymeric micelles with ¹²⁵I/²¹¹At for theranostic radiotherapy