EDEM as an acceptor of terminally misfolded glycoproteins released from calnexin
Y Oda, N Hosokawa, I Wada, K Nagata - Science, 2003 - science.org
Y Oda, N Hosokawa, I Wada, K Nagata
Science, 2003•science.orgTerminally misfolded proteins in the endoplasmic reticulum (ER) are retrotranslocated to the
cytoplasm and degraded by proteasomes through a mechanism known as ER-associated
degradation (ERAD). EDEM, a postulated Man8B-binding protein, accelerates the
degradation of misfolded proteins in the ER. Here, EDEM was shown to interact with
calnexin, but not with calreticulin, through its transmembrane region. Both binding of
substrates to calnexin and their release from calnexin were required for ERAD to occur …
cytoplasm and degraded by proteasomes through a mechanism known as ER-associated
degradation (ERAD). EDEM, a postulated Man8B-binding protein, accelerates the
degradation of misfolded proteins in the ER. Here, EDEM was shown to interact with
calnexin, but not with calreticulin, through its transmembrane region. Both binding of
substrates to calnexin and their release from calnexin were required for ERAD to occur …
Terminally misfolded proteins in the endoplasmic reticulum (ER) are retrotranslocated to the cytoplasm and degraded by proteasomes through a mechanism known as ER-associated degradation (ERAD). EDEM, a postulated Man8B-binding protein, accelerates the degradation of misfolded proteins in the ER. Here, EDEM was shown to interact with calnexin, but not with calreticulin, through its transmembrane region. Both binding of substrates to calnexin and their release from calnexin were required for ERAD to occur. Overexpression of EDEM accelerated ERAD by promoting the release of terminally misfolded proteins from calnexin. Thus, EDEM appeared to function in the ERAD pathway by accepting substrates from calnexin.
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