• Metformin and phenformin target energy production in cancer cells by
inhibiting Complex I of the mitochondrial respiratory chain, activating 5’-
adenosine monophosphate-activated protein kinase (AMPK) and
lowering body insulin levels by altering insulin/insulin-like growth factor�I (I/IGF) pathway.
• Northwestern inventors designed a new series of AuIII complexes,
featuring both energy-disrupting metformin or phenformin ligands
and multitarget AuIII species.
• In vitro evidence demonstrated that metabolic changes caused by
3met initiated attempts of cancer cells to protect themselves by
metabolic reprogramming, UPR and mitophagy. These defense
processes were successfully prevented by shutdown of mitochondrial
respiration and impairment of autophagic flux, leading to the
inhibition of protein degradation and apoptotic cell death.
• High degree of selectivity of the novel complexes to cancer cells over
healthy cells were observed. Lead drug candidate 3met halted the
growth of aggressive breast tumors in a mammary fat pad breast
cancer model and activated the immune response, indicating the
potential benefits of this drug candidate for TNBC patients with high
risk of metastasis and relapse.
