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Molecular features of biguanides required for targeting of mitochondrial respiratory complex I and activation of AMP-kinase.

Hannah R BridgesVille A SirviöAhmed-Noor A AgipJudy Hirst
Published in: BMC biology (2016)
Biguanides inhibit mitochondrial complex I, but specific molecular features control the uptake of substituted biguanides into mitochondria, so only some biguanides inhibit mitochondrial respiration in vivo. Biguanides with restricted intracellular access may be used to determine physiologically relevant targets of biguanide action, and for the rational design of substituted biguanides for diverse clinical applications.
Keyphrases
  • oxidative stress
  • molecular docking
  • reactive oxygen species
  • cell death
  • cancer therapy