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裂殖酵母 mtr1p 调控间期微管皮层驻留时间。

Fission yeast mtr1p regulates interphase microtubule cortical dwell-time.

机构信息

Institut Curie, Paris 75005, France CNRS, UMR 144, Paris 75005, France.

Institut Curie, Paris 75005, France.

出版信息

Biol Open. 2014 Jun 13;3(7):591-6. doi: 10.1242/bio.20148607.

Abstract

The microtubule cytoskeleton plays important roles in cell polarity, motility and division. Microtubules inherently undergo dynamic instability, stochastically switching between phases of growth and shrinkage. In cells, some microtubule-associated proteins (MAPs) and molecular motors can further modulate microtubule dynamics. We present here the fission yeast mtr1(+), a new regulator of microtubule dynamics that appears to be not a MAP or a motor. mtr1-deletion (mtr1Δ) primarily results in longer microtubule dwell-time at the cell tip cortex, suggesting that mtr1p acts directly or indirectly as a destabilizer of microtubules. mtr1p is antagonistic to mal3p, the ortholog of mammalian EB1, which stabilizes microtubules. mal3Δ results in short microtubules, but can be partially rescued by mtr1Δ, as the double mutant mal3Δ mtr1Δ exhibits longer microtubules than mal3Δ single mutant. By sequence homology, mtr1p is predicted to be a component of the ribosomal quality control complex. Intriguingly, deletion of a predicted ribosomal gene, rps1801, also resulted in longer microtubule dwell-time similar to mtr1Δ. The double-mutant mal3Δ rps1801Δ also exhibits longer microtubules than mal3Δ single mutant alone. Our study suggests a possible involvement of mtr1p and the ribosome complex in modulating microtubule dynamics.

摘要

微管细胞骨架在细胞极性、运动和分裂中发挥重要作用。微管固有地经历动态不稳定性,随机地在生长和收缩阶段之间切换。在细胞中,一些微管相关蛋白(MAPs)和分子马达可以进一步调节微管动力学。我们在这里介绍裂殖酵母 mtr1(+),这是一种新的微管动力学调节剂,它似乎不是 MAP 或马达。mtr1 缺失(mtr1Δ)主要导致细胞尖端皮层处微管停留时间延长,表明 mtr1p 直接或间接地作为微管的去稳定因子。mtr1p 与哺乳动物 EB1 的同源物 mal3p 拮抗,mal3p 稳定微管。mal3Δ 导致微管变短,但可以部分被 mtr1Δ 挽救,因为双突变体 mal3Δ mtr1Δ 表现出比 mal3Δ 单突变体更长的微管。根据序列同源性,mtr1p 预测是核糖体质量控制复合物的一个组成部分。有趣的是,预测的核糖体基因 rps1801 的缺失也导致微管停留时间延长,类似于 mtr1Δ。双突变体 mal3Δ rps1801Δ 也表现出比 mal3Δ 单突变体更长的微管。我们的研究表明 mtr1p 和核糖体复合物可能参与调节微管动力学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ff79/4154295/f822140b896b/bio-03-07-591-f01.jpg

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