Archives of Pharmacal Research
- Volume 21 Issue 6
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- Pages.629-633
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- 1998
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- 0253-6269(pISSN)
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- 1976-3786(eISSN)
P62 and the Sequestosome, a Novel Mechanism for Protein Metabolism
- Shin, Jae-Kyoon (Division of Tumor Virology, Dana-Farber Cancer Institute and Harvard Medical School)
- Published : 1998.12.01
Abstract
In addition to selecting proteins for degradation by the 26S proteasome, ubiqitination appears to serve other regulatory functions, including for endosomal/lysosomal targeting, protein translocation, and enzyme modification. Currently, little is known how multiubiquitin chains are recognized by these cellular mechanisms. Within the 26S proteasome, one subunit (Mcb1/S5a) has been identified that has affinity for multiubiquitin chains and may function as a ubiquitin receptor. We recently found that a non-proteasomal protein p62 also preferentially binds multiubiquitin chains and forms a novel cytoplasmic structure "sequestosome" which serves as a storage place for ubiquitinated proteins. In the present manuscript, the role and regulation of p62 in relation to the sequestosomal function will be reviewed.