Copper(II)-based metal-organic framework delivery of calcium ascorbate for enhanced chemodynamic therapy via H 2 O 2 self-supply and glutathione depletion.

Chemodynamic therapy (CDT) is a promising cancer treatment strategy. However, mild acidic pH, insufficient H 2 O 2 content, and overexpressed glutathione (GSH) in the tumor microenvironment (TME) severely impair CDT efficiency. In this study, a novel therapeutic nanosystem (Cu/ZIF-8/Vc-Ca/HA) was constructed for H 2 O 2 self-supply and GSH depletion co-enhanced CDT. Typically, calcium ascorbate (Vc-Ca) loaded on the surface of Cu 2+ -doped ZIF-8 (Cu/ZIF-8) was designed as an original source for H 2 O 2 generation, and a hyaluronic acid (HA) shell was subsequently coated to act as a tumor-targeted "guide" and protective layer. Along with the HA shell disintegrated in the TME, exposed Cu/ZIF-8/Vc-Ca dissociated in the tumor acidic microenvironment, thus triggering the release of Vc-Ca and Cu 2+ . Vc-Ca selectively produced H 2 O 2 in tumor cells, which provided abundant H 2 O 2 for boosting Fenton-like reactions. Meanwhile, the released Cu 2+ could get converted into Cu + by consuming excess intracellular GSH, which could reduce the tumor antioxidant capability of the nanosystem. Moreover, byproduct Cu + reacted with abundant H 2 O 2 by a highly efficient Fenton-like reaction to generate toxic ˙OH. Biological assays indicated that the Cu/ZIF-8/HA@Vc-Ca nanosystem showed significant anticancer activity by enhancing the CDT process. This study may provide a new strategy for improving the effectiveness of CDT.