. 2025 Jul 1.

doi: 10.1007/s00259-025-07432-7. Online ahead of print.

Lysosome-escaping and nucleus-targeting nanomedicine for enhanced cancer catalytic internal radiotherapy

Weiwei Su^{1

2

3}, Han Wang⁴, Shuai Zhao², Xiuru Ji⁴, Hongjing Jiang⁴, Kexian Li⁵, Changjing Zuo⁶, Jianming Zheng⁷, Dalong Ni^{8

9}, Jiajia Hu¹⁰

Affiliations

¹ Department of Radiology, Naval Medical Center, Shanghai, China.
² Department of Nuclear Medicine, Changhai Hospital, Naval Medical University (Second Military Medical University), Shanghai, China.
³ Department of Pathology, Changhai Hospital, Naval Medical University (Second Military Medical University), Shanghai, China.
⁴ Department of Orthopaedics, Shanghai Key Laboratory for Prevention and Treatment of Bone and Joint Diseases, Shanghai Institute of Traumatology and Orthopaedics, Ruijin Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai, China.
⁵ Research Department, Naval Medical Center, Shanghai, China.
⁶ Department of Nuclear Medicine, Changhai Hospital, Naval Medical University (Second Military Medical University), Shanghai, China. cjzuo@smmu.edu.cn.
⁷ Department of Pathology, Changhai Hospital, Naval Medical University (Second Military Medical University), Shanghai, China. jmzheng1962@163.com.
⁸ Department of Orthopaedics, Shanghai Key Laboratory for Prevention and Treatment of Bone and Joint Diseases, Shanghai Institute of Traumatology and Orthopaedics, Ruijin Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai, China. ndl12353@rjh.com.cn.
⁹ Department of Biomaterials and Stem Cells, Suzhou Institute of Biomedical Engineering and Technology, Chinese Academy of Science, 88 Keling Road, Gao Xin District, Suzhou, 215613, China. ndl12353@rjh.com.cn.
¹⁰ Department of Nuclear Medicine, Ruijin Hospital, Shanghai Jiao Tong University School of Medicine, 197 Ruijin Er Road, Huang Pu District, Shanghai, 200025, China. jiajiahu@shsmu.edu.cn.

PMID: 40590905
DOI: 10.1007/s00259-025-07432-7

Lysosome-escaping and nucleus-targeting nanomedicine for enhanced cancer catalytic internal radiotherapy

Weiwei Su et al. Eur J Nucl Med Mol Imaging. 2025.

. 2025 Jul 1.

doi: 10.1007/s00259-025-07432-7. Online ahead of print.

Authors

Weiwei Su^{1

2

3}, Han Wang⁴, Shuai Zhao², Xiuru Ji⁴, Hongjing Jiang⁴, Kexian Li⁵, Changjing Zuo⁶, Jianming Zheng⁷, Dalong Ni^{8

9}, Jiajia Hu¹⁰

Affiliations

¹ Department of Radiology, Naval Medical Center, Shanghai, China.
² Department of Nuclear Medicine, Changhai Hospital, Naval Medical University (Second Military Medical University), Shanghai, China.
³ Department of Pathology, Changhai Hospital, Naval Medical University (Second Military Medical University), Shanghai, China.
⁴ Department of Orthopaedics, Shanghai Key Laboratory for Prevention and Treatment of Bone and Joint Diseases, Shanghai Institute of Traumatology and Orthopaedics, Ruijin Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai, China.
⁵ Research Department, Naval Medical Center, Shanghai, China.
⁶ Department of Nuclear Medicine, Changhai Hospital, Naval Medical University (Second Military Medical University), Shanghai, China. cjzuo@smmu.edu.cn.
⁷ Department of Pathology, Changhai Hospital, Naval Medical University (Second Military Medical University), Shanghai, China. jmzheng1962@163.com.
⁸ Department of Orthopaedics, Shanghai Key Laboratory for Prevention and Treatment of Bone and Joint Diseases, Shanghai Institute of Traumatology and Orthopaedics, Ruijin Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai, China. ndl12353@rjh.com.cn.
⁹ Department of Biomaterials and Stem Cells, Suzhou Institute of Biomedical Engineering and Technology, Chinese Academy of Science, 88 Keling Road, Gao Xin District, Suzhou, 215613, China. ndl12353@rjh.com.cn.
¹⁰ Department of Nuclear Medicine, Ruijin Hospital, Shanghai Jiao Tong University School of Medicine, 197 Ruijin Er Road, Huang Pu District, Shanghai, 200025, China. jiajiahu@shsmu.edu.cn.

PMID: 40590905
DOI: 10.1007/s00259-025-07432-7

Abstract

Purpose: Radio-nanomedicine, such as ¹²⁵I-labelled TiO₂ nanoparticles (¹²⁵I-TiO₂ NPs), presents a promising tumour treatment approach. By leveraging ¹²⁵I as an electron donor to activate TiO₂ NPs and promote γ-ray-induced H₂O radiolysis, ¹²⁵I-TiO₂ generates reactive oxygen species (ROS) and induces DNA damage, thus enabling catalytic internal radiotherapy (CIR). Since DNA is a key target of radiation and ROS-induced damage, enhancing nuclear delivery is critical. However, lysosomal entrapment of ¹²⁵I-TiO₂ NPs greatly restricts the efficacy of CIR. To overcome this limitation, we conjugated ¹²⁵I-TiO₂ with transactivator of transcription/hemagglutinin-2 (¹²⁵I-TiO₂-TAT/HA2), hypothesising that TAT/HA2-mediated lysosomal escape and nuclear accumulation could improve the anti-tumour effects of ¹²⁵I-TiO₂.

Methods: TiO₂ NPs and TiO₂-TAT/HA2 were synthesised and labelled with ¹²⁵I. Subcellular localisation was observed by confocal microscopy and biological transmission electron microscopy (bio-TEM). The effects of ¹²⁵I-TiO₂-TAT/HA2 on PANC-1 cells were assessed by the CCK-8 assay (cell viability), flow cytometry (apoptosis and ROS generation), proliferating cell nuclear antigen (PCNA) staining (proliferation), γ-H2AX immunofluorescence (DNA damage), and western blotting (DNA repair protein expression). In a subcutaneous pancreatic cancer mouse model, the intratumoural intra-tumoural retention of cyanine 5-labelled NPs (Cy5-NPs) was tracked via fluorescence imaging, whereas ¹²⁵I-TiO₂-TAT/HA2 was monitored by single-photon emission computed tomography (SPECT). Mice received intra-tumoural injections of DMEM, ¹²⁵I, ¹²⁵I-TiO₂, or ¹²⁵I-TiO₂-TAT/HA2, and tumour volume and mouse weight and survival were recorded. Tumour glycometabolism was evaluated using ¹⁸F-fluorodeoxyglucose positron emission tomography/computed tomography (¹⁸F-FDG PET/CT) before and after treatment. Haematoxylin and eosin (H&E), TdT-mediated dUTP nick end labelling (TUNEL), and immunohistochemical staining (Ki-67, DNA repair proteins) were performed.

Results: The labelling rates of ¹²⁵I-TiO₂ and ¹²⁵I-TiO₂-TAT/HA2 averaged 89.0% and 90.1%, respectively. Confocal microscopy and bio-TEM confirmed the nucleus-targeting ability of TiO₂-TAT/HA2. In vitro, ¹²⁵I-TiO₂-TAT/HA2 significantly increased apoptosis and DNA damage and reduced DNA repair protein expression (RAD51and 53BP1) versus ¹²⁵I-TiO₂ (all p < 0.05). ¹²⁵I-TiO₂-TAT/HA2 additionally reduced PCNA expression and increased ROS production (both p > 0.05). In vivo, Cy5-NPs, ¹²⁵I-TiO₂, and ¹²⁵I-TiO₂-TAT/HA2 exhibited prolonged intra-tumoural retention. Tumours treated with ¹²⁵I-TiO₂-TAT/HA2 displayed a significantly smaller volume, enhanced necrosis and apoptosis (H&E, TUNEL), and downregulated DNA repair protein expression (all p < 0.05) and reduced Ki-67 expression (p > 0.05) compared with the effects of ¹²⁵I-TiO₂.

Conclusion: ¹²⁵I-TiO₂-TAT/HA2 exhibited markedly enhanced efficacy, likely through the precise nuclear delivery of ROS rather than increased ROS production. This strategy presents a promising method to improve tumour therapy, and it could be adapted for other macromolecular therapeutics.

Keywords: Lysosome escaping; Nucleus targeting; Radio-nanomedicine; TAT/HA2; Tumour treatment.

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Conflict of interest statement

Declarations. Ethics approval: Approval was granted by the Experimental Animal Ethics Committee of the Second Military Medical University (Approval Number, 20181101087). Consent to publish: Informed consent was obtained from the authors for the publication of this article. Competing interests: The authors declare no competing interests.

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Lysosome-escaping and nucleus-targeting nanomedicine for enhanced cancer catalytic internal radiotherapy

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Lysosome-escaping and nucleus-targeting nanomedicine for enhanced cancer catalytic internal radiotherapy

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