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酵母中从高尔基体到内质网(ER)的逆行运输需要Dsl1p,它是内质网靶位点的一个组成部分,可与I型衣被蛋白亚基相互作用。

Golgi-to-endoplasmic reticulum (ER) retrograde traffic in yeast requires Dsl1p, a component of the ER target site that interacts with a COPI coat subunit.

作者信息

Reilly B A, Kraynack B A, VanRheenen S M, Waters M G

机构信息

Department of Molecular Biology, Princeton University, Princeton, NJ 08544, USA.

出版信息

Mol Biol Cell. 2001 Dec;12(12):3783-96. doi: 10.1091/mbc.12.12.3783.

Abstract

DSL1 was identified through its genetic interaction with SLY1, which encodes a t-SNARE-interacting protein that functions in endoplasmic reticulum (ER)-to-Golgi traffic. Conditional dsl1 mutants exhibit a block in ER-to-Golgi traffic at the restrictive temperature. Here, we show that dsl1 mutants are defective for retrograde Golgi-to-ER traffic, even under conditions where no anterograde transport block is evident. These results suggest that the primary function of Dsl1p may be in retrograde traffic, and that retrograde defects can lead to secondary defects in anterograde traffic. Dsl1p is an ER-localized peripheral membrane protein that can be extracted from the membrane in a multiprotein complex. Immunoisolation of the complex yielded Dsl1p and proteins of approximately 80 and approximately 55 kDa. The approximately 80-kDa protein has been identified as Tip20p, a protein that others have shown to exist in a tight complex with Sec20p, which is approximately 50 kDa. Both Sec20p and Tip20p function in retrograde Golgi-to-ER traffic, are ER-localized, and bind to the ER t-SNARE Ufe1p. These findings suggest that an ER-localized complex of Dsl1p, Sec20p, and Tip20p functions in retrograde traffic, perhaps upstream of a Sly1p/Ufe1p complex. Last, we show that Dsl1p interacts with the delta-subunit of the retrograde COPI coat, Ret2p, and discuss possible roles for this interaction.

摘要

DSL1是通过其与SLY1的遗传相互作用而被鉴定出来的,SLY1编码一种与t-SNARE相互作用的蛋白质,该蛋白质在内质网(ER)到高尔基体的运输过程中发挥作用。条件性dsl1突变体在限制温度下表现出ER到高尔基体运输的阻断。在这里,我们表明,即使在没有明显顺行运输阻断的情况下,dsl1突变体在高尔基体到ER的逆行运输中也存在缺陷。这些结果表明,Dsl1p的主要功能可能在于逆行运输,并且逆行缺陷可能导致顺行运输中的继发性缺陷。Dsl1p是一种定位于ER的外周膜蛋白,可以在多蛋白复合物中从膜上提取出来。对该复合物进行免疫分离得到了Dsl1p以及大约80 kDa和大约55 kDa的蛋白质。大约80 kDa的蛋白质已被鉴定为Tip20p,其他人已表明该蛋白质与大约50 kDa的Sec20p紧密结合存在。Sec20p和Tip20p都在高尔基体到ER的逆行运输中发挥作用,定位于ER,并与ER t-SNARE Ufe1p结合。这些发现表明,由Dsl1p、Sec20p和Tip20p组成的定位于ER的复合物在逆行运输中发挥作用,可能在Sly1p/Ufe1p复合物的上游。最后,我们表明Dsl1p与逆行COPI衣被的δ亚基Ret2p相互作用,并讨论了这种相互作用的可能作用。

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