Combination therapy has emerged as a promising approach for treating tumors, although there is room for improvement. This study introduced a novel strategy that combined the enhancement of apoptosis, ferroptosis, and DNA damage to improve therapeutic outcomes for prostate cancer. Specifically, we have developed a supramolecular oxidative stress nanoamplifier, which was comprised of β-cyclodextrin, paclitaxel, and ferrocene-poly(ethylene glycol). Paclitaxel within the system disrupted microtubule dynamics, inducing G2/M phase arrest and apoptosis. Concurrently, ferrocene utilized hydrogen peroxide to generate toxic hydroxyl radicals in cells through the Fenton reaction, triggering a cascade of reactive oxygen species expansion, reduction of glutathione levels, lipid peroxidation, and ferroptosis. The increased number of hydroxyl radicals and the inhibitory effect of THZ531 on DNA repair mechanisms exacerbated DNA damage within tumor cells. As expected, the supramolecular nanoparticles demonstrated excellent drug delivery ability to tumor cells or tissues, exhibited favorable biological safety in vivo , and enhanced the killing effect on prostate cancer.
Keyphrases
- dna damage
- oxidative stress
- dna repair
- hydrogen peroxide
- prostate cancer
- cell cycle arrest
- cell death
- induced apoptosis
- combination therapy
- cancer therapy
- drug delivery
- radical prostatectomy
- reactive oxygen species
- endoplasmic reticulum stress
- nitric oxide
- energy transfer
- diabetic rats
- ischemia reperfusion injury
- water soluble
- dna damage response
- cell cycle
- pi k akt
- wastewater treatment
- fatty acid
- signaling pathway
- resting state
- insulin resistance
- skeletal muscle
- quantum dots
- weight loss