The protein known as p97 or VCP in mammals and Cdc48 in yeast is a versatile ATPase complex involved in several biological functions including membrane fusion, protein folding, and activation of membrane-bound transcription factors. In addition, p97 plays a central role in degradation of misfolded secretory proteins via the ER-associated degradation pathway. This functional diversity of p97 depends on its association with various cofactors, and to further our understanding of p97 function it is important that these cofactors are identified and analyzed. Here, we isolate and characterize the human protein named Rep8 or Ubxd6 as a new cofactor of p97. Mouse Rep8 is highly tissue-specific and abundant in gonads. In testes, Rep8 is expressed in post-meiotic round spermatids, whereas in ovaries Rep8 is expressed in granulosa cells. Rep8 associates directly with p97 via its UBX domain. We show that Rep8 is a transmembrane protein that localizes to the ER membrane with its UBX domain facing the cytoplasm. Knock-down of Rep8 expression in human cells leads to a decreased association of p97 with the ER membrane and concomitantly a retarded degradation of misfolded ER-derived proteasome substrates. Thus, Rep8 tethers p97 to the ER membrane for efficient ER-associated degradation.
The tissue-specific Rep8/UBXD6 tethers p97 to the endoplasmic reticulum membrane for degradation of misfolded proteins.
组织特异性的 Rep8/UBXD6 将 p97 锚定到内质网膜上,以降解错误折叠的蛋白质
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作者:Madsen Louise, Kriegenburg Franziska, Vala Andrea, Best Diana, Prag Søren, Hofmann Kay, Seeger Michael, Adams Ian R, Hartmann-Petersen Rasmus
| 期刊: | PLoS One | 影响因子: | 2.600 |
| 时间: | 2011 | 起止号: | 2011;6(9):e25061 |
| doi: | 10.1371/journal.pone.0025061 | 研究方向: | 免疫/内分泌 |
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