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光敏色素A的N端和C端结构域中的序列对于PFR泛素化和降解是必需的。

Sequences within both the N- and C-terminal domains of phytochrome A are required for PFR ubiquitination and degradation.

作者信息

Clough R C, Jordan-Beebe E T, Lohman K N, Marita J M, Walker J M, Gatz C, Vierstra R D

机构信息

Cellular and Molecular Biology Program, University of Wisconsin-Madison 53706, USA.

出版信息

Plant J. 1999 Jan;17(2):155-67. doi: 10.1046/j.1365-313x.1999.00360.x.

DOI:10.1046/j.1365-313x.1999.00360.x
PMID:10074713
Abstract

Photoconversion of the plant photoreceptor phytochrome A (phyA) from its inactive Pr form to its biologically active Pfr from initiates its rapid proteolysis. Previous kinetic and biochemical studies implicated a role for the ubiquitin/26S proteasome pathway in this breakdown and suggested that multiple domains within the chromoprotein are involved. To further resolve the essential residues, we constructed a series of mutant PHY genes in vitro and analyzed the Pfr-specific degradation of the resulting photoreceptors expressed in transgenic tobacco. One important site is within the C-terminal half of the polypeptide as its removal stabilizes oat phyA as Pfr. Within this half is a set of conserved lysines that are potentially required for ubiquitin attachment. Substitution of these lysines did not prevent ubiquitination or breakdown of Pfr, suggesting either that they are not the attachment sites or that other lysines can be used in their absence. A small domain just proximal to the C-terminus is essential for the form-dependent breakdown of the holoprotein. Removal of just six amino acids in this domain generated a chromoprotein that was not rapidly degraded as Pfr. Using chimeric photoreceptors generated from potato PHYA and PHYB, we found that the N-terminal half of phyA is also required for Pfr-specific breakdown. Only those chimeras containing the N-terminal sequences from phyA were ubiquitinated and rapidly degraded as Pfr. Taken together, our data demonstrate that, whereas an intact C-terminal domain is essential for phyA degradation, the N-terminal domain is responsible for the selective recognition and ubiquitination of Pfr.

摘要

植物光受体光敏色素A(phyA)从无活性的Pr形式光转化为生物活性的Pfr形式会引发其快速的蛋白质水解。先前的动力学和生化研究表明泛素/26S蛋白酶体途径在这种降解过程中起作用,并暗示色素蛋白内的多个结构域参与其中。为了进一步确定关键残基,我们在体外构建了一系列突变体PHY基因,并分析了转基因烟草中表达的所得光受体的Pfr特异性降解。一个重要位点位于多肽的C端后半部分,因为去除该部分可使燕麦phyA以Pfr形式稳定存在。在这后半部分中有一组保守的赖氨酸,它们可能是泛素附着所必需的。这些赖氨酸的替换并没有阻止Pfr的泛素化或降解,这表明它们要么不是附着位点,要么在没有它们的情况下其他赖氨酸可以被利用。紧接C末端的一个小结构域对于全蛋白的形式依赖性降解至关重要。在该结构域中仅去除六个氨基酸就产生了一种色素蛋白,该色素蛋白不会作为Pfr快速降解。使用由马铃薯PHYA和PHYB产生的嵌合光受体,我们发现phyA的N端后半部分对于Pfr特异性降解也是必需的。只有那些包含phyA N端序列的嵌合体才会被泛素化并作为Pfr快速降解。综上所述,我们的数据表明,完整的C末端结构域对于phyA降解至关重要,而N末端结构域负责Pfr的选择性识别和泛素化。

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