Moderate oxygen (O 2 ) supply and uneven distribution of oxygen at the tumor site usually hinder the therapeutic efficacy of hypoxia-activated prodrugs. In this report, we designed a ferrocene-containing supramolecular nanomedicine (PFC/GOD-TPZ) with the PEG corona and disulfide-bond cross-linked core to co-encapsulate 4-di- N -oxide tirapazamine (TPZ) and glucose oxidase (GOD). The PEG corona of PFC/GOD-TPZ could be weakly acidic tumor pH-responsively detached for an enhanced cellular internalization, while the disulfide-bond cross-linked core could be cleavaged by intracellular glutathione (GSH) to present a GSH-triggered drug-release behavior. Subsequently, the cascade reactions, including catalytic reactions among the released GOD, glucose, and O 2 to generate H 2 O 2 and the subsequent Fenton reaction between ferrocene and H 2 O 2 , occurred. With the depletion of O 2 , the non-toxic TPZ was activated and converted into the cytotoxic therapeutic agent benzotriazinyl (BTZ) radical under the exacerbated hypoxic microenvironment. Collectively, the PFC/GOD-TPZ provides a promising strategy for effective combination therapy of GOD-mediated starvation therapy, chemodynamic therapy (CDT), and hypoxia-activated chemotherapy (CT).
Keyphrases
- combination therapy
- drug release
- drug delivery
- cancer therapy
- endothelial cells
- fluorescent probe
- stem cells
- blood glucose
- hydrogen peroxide
- squamous cell carcinoma
- locally advanced
- water soluble
- type diabetes
- nitric oxide
- radiation therapy
- escherichia coli
- adipose tissue
- contrast enhanced
- positron emission tomography
- reactive oxygen species
- pseudomonas aeruginosa