Publikation:

FAT10, a ubiquitin-independent signal for proteasomal degradation

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2005

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Hipp, Mark Steffen
Kalveram, Birte

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http://nbn-resolving.de/urn:nbn:de:bsz:352-166793
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https://doi.org/10.1128/MCB.25.9.3483-3491.2005
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Molecular and Cellular Biology. 2005, 25(9), pp. 3483-3491. ISSN 0270-7306. Available under: doi: 10.1128/MCB.25.9.3483-3491.2005

Zusammenfassung

FAT10 is a small ubiquitin-like modifier that is encoded in the major histocompatibility complex and is synergistically inducible by tumor necrosis factor alpha and gamma interferon. It is composed of two ubiquitin-like domains and possesses a free C-terminal diglycine motif that is required for the formation of FAT10 conjugates. Here we show that unconjugated FAT10 and a FAT10 conjugate were rapidly degraded by the proteasome at a similar rate. Fusion of FAT10 to the N terminus of very long-lived proteins enhanced their degradation rate as potently as fusion with ubiquitin did. FAT10-green fluorescent protein fusion proteins were not cleaved but entirely degraded, suggesting that FAT10-specific deconjugating enzymes were not present in the analyzed cell lines. Interestingly, the prevention of ubiquitylation of FAT10 by mutation of all lysines or by expression in ubiquitylation-deficient cells did not affect FAT10 degradation. Thus, conjugation with FAT10 is an alternative and ubiquitin-independent targeting mechanism for degradation by the proteasome, which, in contrast to polyubiquitylation, is cytokine inducible and irreversible.

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570 Biowissenschaften, Biologie

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ISO 690HIPP, Mark Steffen, Birte KALVERAM, Shahri RAASI, Marcus GRÖTTRUP, Gunter SCHMIDTKE, 2005. FAT10, a ubiquitin-independent signal for proteasomal degradation. In: Molecular and Cellular Biology. 2005, 25(9), pp. 3483-3491. ISSN 0270-7306. Available under: doi: 10.1128/MCB.25.9.3483-3491.2005
BibTex
@article{Hipp2005-05FAT10-16679,
  year={2005},
  doi={10.1128/MCB.25.9.3483-3491.2005},
  title={FAT10, a ubiquitin-independent signal for proteasomal degradation},
  number={9},
  volume={25},
  issn={0270-7306},
  journal={Molecular and Cellular Biology},
  pages={3483--3491},
  author={Hipp, Mark Steffen and Kalveram, Birte and Raasi, Shahri and Gröttrup, Marcus and Schmidtke, Gunter}
}
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