Available online 14 March 2025

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Clinical chemotherapy for prostate cancer is still compromised by high treatment thresholds and severe off-target toxicity of drugs. Given the limited progress in improving therapeutic outcomes and reducing toxicity with the existing toolbox, efforts to broaden the chemotherapeutic window are highly desired. Here, we discover that gossypol (GSP, a natural compound) dramatically enhances the chemosensitivity of cabazitaxel (CTX), even at previously ineffective concentrations. Based on this interesting finding, we exploit a carrier-free chemotherapeutic nano-booster for prostate cancer treatment, which is molecularly co-assembled by GSP and cabazitaxel (CTX). GSP not only readily forms nanoassembly with CTX, but also functions as a chemotherapeutic enhancer that unlocks an ultra-low-dose chemotherapeutic window. Not only that, precise dual-drug nanoassembly confers CTX a significantly larger maximum tolerable dose. As expected, the nano-booster exerts striking therapeutic benefits in mouse prostate tumor xenograft models. This study advances chemotherapeutic window expansion and self-sensitized chemotherapy toward clinical applicability.

Graphical abstractA natural compound, gossypol (GSP), was discovered to dramatically enhance the chemosensitivity of cabazitaxel (CTX). Furthermore, a molecularly self-assembled chemotherapeutic nano-booster (sp-GC NAs) was successfully developed, unlocking an ultra-low-dose chemotherapeutic window.Download: Download high-res image (162KB)Download: Download full-size imageKeywords

Prostate cancer treatment

Gossypol

Cabazitaxel

Chemotherapeutic enhancer

Precise dual-drug nanoassembly

Therapeutic window broadening

Carrier-free nanoassembly

Cancer chemotherapy

© 2025 The Authors. Published by Elsevier B.V. on behalf of Chinese Pharmaceutical Association and Institute of Materia Medica, Chinese Academy of Medical Sciences.