Issue 11, 2024

Molecular engineering of AIE-active boron clustoluminogens for enhanced boron neutron capture therapy

Abstract

The development of boron delivery agents bearing an imaging capability is crucial for boron neutron capture therapy (BNCT), yet it has been rarely explored. Here we present a new type of boron delivery agent that integrates aggregation-induced emission (AIE)-active imaging and a carborane cluster for the first time. In doing so, the new boron delivery agents have been rationally designed by incorporating a high boron content unit of a carborane cluster, an erlotinib targeting unit towards lung cancer cells, and a donor–acceptor type AIE unit bearing naphthalimide. The new boron delivery agents demonstrate both excellent AIE properties for imaging purposes and highly selective accumulation in tumors. For example, at a boron delivery agent dose of 15 mg kg−1, the boron amount reaches over 20 μg g−1, and both tumor/blood (T/B) and tumor/normal cell (T/N) ratios reach 20–30 times higher than those required by BNCT. The neutron irradiation experiments demonstrate highly efficient tumor growth suppression without any observable physical tissue damage and abnormal behavior in vivo. This study not only expands the application scopes of both AIE-active molecules and boron clusters, but also provides a new molecular engineering strategy for a deep-penetrating cancer therapeutic protocol based on BNCT.

Graphical abstract: Molecular engineering of AIE-active boron clustoluminogens for enhanced boron neutron capture therapy

Supplementary files

Article information

Article type
Edge Article
Submitted
21 Nov 2023
Accepted
01 Feb 2024
First published
01 Feb 2024
This article is Open Access

All publication charges for this article have been paid for by the Royal Society of Chemistry
Creative Commons BY-NC license

Chem. Sci., 2024,15, 4019-4030

Molecular engineering of AIE-active boron clustoluminogens for enhanced boron neutron capture therapy

W. Ma, Y. Wang, Y. Xue, M. Wang, C. Lu, W. Guo, Y. Liu, D. Shu, G. Shao, Q. Xu, D. Tu and H. Yan, Chem. Sci., 2024, 15, 4019 DOI: 10.1039/D3SC06222H

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