Tumor Redox‐Responsive Minimalist B/Fe Nano‐Chains for Chemodynamically Enhanced Ferroptosis and Synergistic Boron Neutron Capture Therapy

Author:

Wang Mixue1,Hao Haotian1,Bai Peirong2,Wu Jiayan3,Zhang Zizhu4,Liu Tong5,Yang Yongzhen1,Li Liping67,Pu Kanyi38ORCID,Zhang Ruiping7

Affiliation:

1. Key Laboratory of Interface Science and Engineering in Advanced Materials Ministry of Education Taiyuan University of Technology Taiyuan 030024 China

2. Third Hospital of Shanxi Medical University Shanxi Bethune Hospital Shanxi Academy of Medical Sciences Taiyuan 030032 China

3. School of Chemistry Chemical Engineering and Biotechnology Nanyang Technological University Singapore 637457 Singapore

4. Beijing Nuclear Industry Hospital Beijing 102413 China

5. Beijing Capture Tech Co. Ltd Beijing 102413 China

6. School of Basic Medical Sciences Shanxi Medical University Taiyuan 030001 China

7. The Radiology Department of Shanxi Provincial People′s Hospital Affiliated to Shanxi Medical University Taiyuan 030001 China

8. Lee Kong Chian School of Medicine Nanyang Technological University Singapore 636921 Singapore

Abstract

AbstractBoron neutron capture therapy (BNCT) as a binary targeted particle radiotherapy strategy has shown potent anti‐cancer potential. However, biological barriers and restricted blood supply pose challenges in achieving adequate boron concentration within deep‐seated tumor lesions. BNCT with other anti‐cancer therapies, such as X‐ray radiotherapy and photothermal therapy, is devised to address the limitations of BNCT efficiency. However, the potential risk of organ‐accumulating toxicity and treatment complexity of dual exogenous activation hinders its development. To address this problem, newly redox‐responsive boron nano‐chains (RBNC) are reported that combine BNCT and endogenous chemodynamic therapy (CDT)‐enhanced ferroptosis. RBNC specifically activates nanoparticle size conversion (large‐to‐small) in response to GSH/H2O2 in the tumor microenvironment, releasing boron delivery agents boron quantum dots (BQD) and Fe3+. RBNC exhibits negligible systemic toxicity while demonstrating high boron accumulation at tumor. Meanwhile, the introduction of Fe3+ not only produces ·OH through reaction with H2O2, but also depletes GSH and reduces GPX4 activity in tumors, resulting in amplified intracellular oxidative stress and chemodynamically enhanced ferroptosis. Thus, the work provides a strategy to solve the problem of insufficient boron concentration and poor targeting of boron delivery agents and fill the gaps of BNCT combined with CDT and ferroptosis.

Funder

National Natural Science Foundation of China

National Key Research and Development Program of China

Publisher

Wiley

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