Structural Biology Program, Memorial Sloan Kettering Cancer Center, New York, United States.
Howard Hughes Medical Institute, New York, United States.
Elife. 2017 Jun 8;6:e26624. doi: 10.7554/eLife.26624.
Native cargo proteins exit the endoplasmic reticulum (ER) in COPII-coated vesicles, whereas resident and misfolded proteins are substantially excluded from vesicles by a retention mechanism that remains unresolved. We probed the ER retention process using the proteostasis regulator 4-phenylbutyrate (4-PBA), which we show targets COPII protein to reduce the stringency of retention. 4-PBA competes with p24 proteins to bind COPII. When p24 protein uptake is blocked, COPII vesicles package resident proteins and an ER-trapped mutant LDL receptor. We further show that 4-PBA triggers the secretion of a KDEL-tagged luminal resident, implying that a compromised retention mechanism causes saturation of the KDEL retrieval system. The results indicate that stringent ER retention requires the COPII coat machinery to actively sort biosynthetic cargo from diffusible misfolded and resident ER proteins.
天然货物蛋白通过 COPII 被膜小泡从内质网(ER)输出,而驻留蛋白和错误折叠的蛋白则通过一个仍未解决的保留机制被大量排除在小泡之外。我们使用蛋白质稳态调节剂 4-苯基丁酸(4-PBA)来探测 ER 保留过程,结果表明 4-PBA 可以靶向 COPII 蛋白,从而降低保留的严格性。4-PBA 与 p24 蛋白竞争结合 COPII。当 p24 蛋白摄取被阻断时,COPII 小泡会包裹驻留蛋白和一个 ER 捕获的突变 LDL 受体。我们进一步表明,4-PBA 触发了带有 KDEL 标签的腔驻留蛋白的分泌,这意味着保留机制受损会导致 KDEL 回收系统饱和。这些结果表明,严格的 ER 保留需要 COPII 外套机制来主动从可扩散的错误折叠和驻留 ER 蛋白中分拣生物合成货物。
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