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裂殖酵母中的生长素诱导蛋白消耗系统。

Auxin-inducible protein depletion system in fission yeast.

作者信息

Kanke Mai, Nishimura Kohei, Kanemaki Masato, Kakimoto Tatsuo, Takahashi Tatsuro S, Nakagawa Takuro, Masukata Hisao

机构信息

Graduate School of Science, Osaka University, 1-1 Machikaneyama-cho, Toyonaka, Osaka 560-0043, Japan.

出版信息

BMC Cell Biol. 2011 Feb 11;12:8. doi: 10.1186/1471-2121-12-8.

Abstract

BACKGROUND

Inducible inactivation of a protein is a powerful approach for analysis of its function within cells. Fission yeast is a useful model for studying the fundamental mechanisms such as chromosome maintenance and cell cycle. However, previously published strategies for protein-depletion are successful only for some proteins in some specific conditions and still do not achieve efficient depletion to cause acute phenotypes such as immediate cell cycle arrest. The aim of this work was to construct a useful and powerful protein-depletion system in Shizosaccaromyces pombe.

RESULTS

We constructed an auxin-inducible degron (AID) system, which utilizes auxin-dependent poly-ubiquitination of Aux/IAA proteins by SCFTIR1 in plants, in fission yeast. Although expression of a plant F-box protein, TIR1, decreased Mcm4-aid, a component of the MCM complex essential for DNA replication tagged with Aux/IAA peptide, depletion did not result in an evident growth defect. We successfully improved degradation efficiency of Mcm4-aid by fusion of TIR1 with fission yeast Skp1, a conserved F-box-interacting component of SCF (improved-AID system; i-AID), and the cells showed severe defect in growth. The i-AID system induced degradation of Mcm4-aid in the chromatin-bound MCM complex as well as those in soluble fractions. The i-AID system in conjunction with transcription repression (off-AID system), we achieved more efficient depletion of other proteins including Pol1 and Cdc45, causing early S phase arrest.

CONCLUSION

Improvement of the AID system allowed us to construct conditional null mutants of S. pombe. We propose that the off-AID system is the powerful method for in vivo protein-depletion in fission yeast.

摘要

背景

蛋白质的诱导失活是分析其在细胞内功能的有力方法。裂殖酵母是研究染色体维持和细胞周期等基本机制的有用模型。然而,先前发表的蛋白质去除策略仅在某些特定条件下对某些蛋白质有效,并且仍未实现有效去除以导致急性表型,如立即细胞周期停滞。这项工作的目的是在粟酒裂殖酵母中构建一个有用且强大的蛋白质去除系统。

结果

我们在裂殖酵母中构建了一种生长素诱导降解子(AID)系统,该系统利用植物中SCFTIR1对Aux/IAA蛋白进行生长素依赖性多聚泛素化。尽管植物F-box蛋白TIR1的表达降低了Mcm4-aid(一种用Aux/IAA肽标记的DNA复制所必需的MCM复合物的成分),但去除并未导致明显的生长缺陷。我们通过将TIR1与裂殖酵母Skp1(SCF的保守F-box相互作用成分)融合成功提高了Mcm4-aid的降解效率(改进的AID系统;i-AID),细胞表现出严重的生长缺陷。i-AID系统诱导染色质结合的MCM复合物以及可溶性部分中的Mcm4-aid降解。结合转录抑制的i-AID系统(关闭AID系统),我们实现了对包括Pol1和Cdc45在内的其他蛋白质更有效的去除,导致早期S期停滞。

结论

AID系统的改进使我们能够构建粟酒裂殖酵母的条件性敲除突变体。我们提出关闭AID系统是在裂殖酵母中进行体内蛋白质去除的有力方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9c41/3048574/07c8e51d33ec/1471-2121-12-8-1.jpg

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