Journal of Cell Biology 2015-10-26

Quality control of mitochondrial protein synthesis is required for membrane integrity and cell fitness.

Uwe Richter, Taina Lahtinen, Paula Marttinen, Fumi Suomi, Brendan J Battersby

文献索引:J. Cell Biol. 211 , 373-89, (2015)

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摘要

Mitochondrial ribosomes synthesize a subset of hydrophobic proteins required for assembly of the oxidative phosphorylation complexes. This process requires temporal and spatial coordination and regulation, so quality control of mitochondrial protein synthesis is paramount to maintain proteostasis. We show how impaired turnover of de novo mitochondrial proteins leads to aberrant protein accumulation in the mitochondrial inner membrane. This creates a stress in the inner membrane that progressively dissipates the mitochondrial membrane potential, which in turn stalls mitochondrial protein synthesis and fragments the mitochondrial network. The mitochondrial m-AAA protease subunit AFG3L2 is critical to this surveillance mechanism that we propose acts as a sensor to couple the synthesis of mitochondrial proteins with organelle fitness, thus ensuring coordinated assembly of the oxidative phosphorylation complexes from two sets of ribosomes. © 2015 Richter et al.


相关化合物

  • 乙醇
  • 甘油
  • 十二烷基硫酸钠
  • 半胱氨酸
  • 缬氨霉素
  • 苄磺酰氟
  • 巯基乙醇
  • 三乙烯二胺
  • 羰基氰化氯苯腙
  • 氯霉素

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