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Mlc1p是酿酒酵母中非常规肌球蛋白Myo2p的轻链。

Mlc1p is a light chain for the unconventional myosin Myo2p in Saccharomyces cerevisiae.

作者信息

Stevens R C, Davis T N

机构信息

Department of Biochemistry, University of Washington, Seattle, Washington 98195-7350, USA.

出版信息

J Cell Biol. 1998 Aug 10;142(3):711-22. doi: 10.1083/jcb.142.3.711.

Abstract

In Saccharomyces cerevisiae, the unconventional myosin Myo2p is of fundamental importance in polarized growth. We explore the role of the neck region and its associated light chains in regulating Myo2p function. Surprisingly, we find that precise deletion of the six IQ sites in the neck region results in a myosin, Myo2-Delta6IQp, that can support the growth of a yeast strain at 90% the rate of a wild-type isogenic strain. We exploit this mutant in a characterization of the light chains of Myo2p. First, we demonstrate that the localization of calmodulin to sites of polarized growth largely depends on the IQ sites in the neck of Myo2p. Second, we demonstrate that a previously uncharacterized protein, Mlc1p, is a myosin light chain of Myo2p. MLC1 (YGL106w) is an essential gene that exhibits haploinsufficiency. Reduced levels of MYO2 overcome the haploinsufficiency of MLC1. The mutant MYO2-Delta6IQ is able to suppress haploinsufficiency but not deletion of MLC1. We used a modified gel overlay assay to demonstrate a direct interaction between Mlc1p and the neck of Myo2p. Overexpression of MYO2 is toxic, causing a severe decrease in growth rate. When MYO2 is overexpressed, Myo2p is fourfold less stable than in a wild-type strain. High copies of MLC1 completely overcome the growth defects and increase the stability of Myo2p. Our results suggest that Mlc1p is responsible for stabilizing this myosin by binding to the neck region.

摘要

在酿酒酵母中,非常规肌球蛋白Myo2p在极性生长中至关重要。我们探究了颈部区域及其相关轻链在调节Myo2p功能中的作用。令人惊讶的是,我们发现精确删除颈部区域的六个IQ位点会产生一种肌球蛋白Myo2-Δ6IQp,它能够以野生型同基因菌株90%的速率支持酵母菌株的生长。我们利用这种突变体对Myo2p的轻链进行了表征。首先,我们证明钙调蛋白定位于极性生长位点在很大程度上依赖于Myo2p颈部的IQ位点。其次,我们证明一种先前未被表征的蛋白质Mlc1p是Myo2p的肌球蛋白轻链。MLC1(YGL106w)是一个必需基因,表现出单倍体不足。MYO2水平降低可克服MLC1的单倍体不足。突变体MYO2-Δ6IQ能够抑制单倍体不足,但不能抑制MLC1的缺失。我们使用改良的凝胶覆盖试验证明了Mlc1p与Myo2p颈部之间的直接相互作用。MYO2的过表达是有毒的,导致生长速率严重下降。当MYO2过表达时,Myo2p的稳定性比野生型菌株低四倍。高拷贝的MLC1完全克服了生长缺陷并增加了Myo2p的稳定性。我们的结果表明,Mlc1p通过与颈部区域结合来负责稳定这种肌球蛋白。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/645e/2148162/17e3c70b19ba/JCB14667.f1.jpg

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