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酵母Spt7的C末端加工在缺乏功能性SAGA复合物的情况下发生。

C-terminal processing of yeast Spt7 occurs in the absence of functional SAGA complex.

作者信息

Hoke Stephen M T, Liang Gaoyang, Mutiu A Irina, Genereaux Julie, Brandl Christopher J

机构信息

Department of Biochemistry, Schulich School of Medicine & Dentistry, University of Western Ontario, London, N6A5C1, Canada.

出版信息

BMC Biochem. 2007 Aug 8;8:16. doi: 10.1186/1471-2091-8-16.

Abstract

BACKGROUND

Spt7 is an integral component of the multi-subunit SAGA complex that is required for the expression of approximately 10% of yeast genes. Two forms of Spt7 have been identified, the second of which is truncated at its C-terminus and found in the SAGA-like (SLIK) complex.

RESULTS

We have found that C-terminal processing of Spt7 to its SLIK form (Spt7SLIK) and to a distinct third form (Spt7Form3) occurs in the absence of the SAGA complex components Gcn5, Spt8, Ada1 and Spt20, the latter two of which are required for the integrity of the complex. In addition, N-terminally truncated derivatives of Spt7, including a derivative lacking the histone fold, are processed, indicating that the C-terminus of Spt7 is sufficient for processing and that processing does not require functional Spt7. Using galactose inducible Spt7 expression, we show that the three forms of Spt7 appear and disappear at approximately the same rate with full-length Spt7 not being chased into Spt7SLIK or Spt7Form3. Interestingly, reduced levels of Spt7SLIK and Spt7Form3 were observed in a strain lacking the SAGA component Ubp8, suggesting a regulatory role for Ubp8 in the truncation of Spt7.

CONCLUSION

We conclude that truncation of Spt7 occurs early in the biosynthesis of distinct Spt7 containing complexes rather than being a dynamic process linked to the action of the SAGA complex in transcriptional regulation.

摘要

背景

Spt7是多亚基SAGA复合物的一个组成部分,约10%的酵母基因的表达需要该复合物。已鉴定出两种形式的Spt7,其中第二种在其C端被截断,并存在于类SAGA(SLIK)复合物中。

结果

我们发现,在缺乏SAGA复合物组分Gcn5、Spt8、Ada1和Spt20的情况下,Spt7会被加工成其SLIK形式(Spt7SLIK)和一种不同的第三种形式(Spt7Form3),后两者是复合物完整性所必需的。此外,Spt7的N端截短衍生物,包括一种缺乏组蛋白折叠的衍生物,也会被加工,这表明Spt7的C端足以进行加工,且加工不需要功能性的Spt7。利用半乳糖诱导的Spt7表达,我们表明三种形式的Spt7以大致相同的速率出现和消失,全长Spt7不会被转化为Spt7SLIK或Spt7Form3。有趣的是,在缺乏SAGA组分Ubp8的菌株中观察到Spt7SLIK和Spt7Form3的水平降低,这表明Ubp8在Spt7的截短中起调节作用。

结论

我们得出结论,Spt7的截短发生在含有不同Spt7的复合物生物合成的早期,而不是与SAGA复合物在转录调控中的作用相关的动态过程。

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