Crystal structure of SEL1L: Insight into the roles of SLR motifs in ERAD pathway

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作者
Hanbin Jeong
Hyo Jung Sim
Eun Kyung Song
Hakbong Lee
Sung Chul Ha
Youngsoo Jun
Tae Joo Park
Changwook Lee
机构
[1] School of Life Sciences,Department of Biological Sciences
[2] Ulsan National Institute of Science and Technology,undefined
[3] Pohang Accelerator Laboratory,undefined
[4] Pohang University of Science and Technology,undefined
[5] Kyungbuk,undefined
[6] School of Life Sciences,undefined
[7] Gwangju Institute of Science and Technology,undefined
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Scientific Reports | / 6卷
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摘要
Terminally misfolded proteins are selectively recognized and cleared by the endoplasmic reticulum-associated degradation (ERAD) pathway. SEL1L, a component of the ERAD machinery, plays an important role in selecting and transporting ERAD substrates for degradation. We have determined the crystal structure of the mouse SEL1L central domain comprising five Sel1-Like Repeats (SLR motifs 5 to 9; hereafter called SEL1Lcent). Strikingly, SEL1Lcent forms a homodimer with two-fold symmetry in a head-to-tail manner. Particularly, the SLR motif 9 plays an important role in dimer formation by adopting a domain-swapped structure and providing an extensive dimeric interface. We identified that the full-length SEL1L forms a self-oligomer through the SEL1Lcent domain in mammalian cells. Furthermore, we discovered that the SLR-C, comprising SLR motifs 10 and 11, of SEL1L directly interacts with the N-terminus luminal loops of HRD1. Therefore, we propose that certain SLR motifs of SEL1L play a unique role in membrane bound ERAD machinery.
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