共 48 条
Analysis of Intraviral Protein-Protein Interactions of the SARS Coronavirus ORFeome
被引:167
作者:

von Brunn, Albrecht
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机构:
Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany

Teepe, Carola
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Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany

Simpson, Jeremy C.
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机构:
European Mol Biol Lab, Heidelberg, Germany Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany

Pepperkok, Rainer
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机构:
European Mol Biol Lab, Heidelberg, Germany Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany

Friedel, Caroline C.
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机构:
Univ Munich, Inst Informat, D-8000 Munich, Germany Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany

Zimmer, Ralf
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Univ Munich, Inst Informat, D-8000 Munich, Germany Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany

Roberts, Rhonda
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机构:
Univ N Carolina, Chapel Hill, NC USA Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany

Baric, Ralph
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h-index: 0
机构:
Univ N Carolina, Chapel Hill, NC USA Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany

Haas, Juergen
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h-index: 0
机构:
Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany
机构:
[1] Univ Munich, Genzentrum, Max Von Pettenkofer Inst, Lehrstuhl Virol, Munich, Germany
[2] Univ Munich, Inst Informat, D-8000 Munich, Germany
[3] European Mol Biol Lab, Heidelberg, Germany
[4] Univ N Carolina, Chapel Hill, NC USA
来源:
PLOS ONE
|
2007年
/
2卷
/
05期
基金:
英国医学研究理事会;
关键词:
D O I:
10.1371/journal.pone.0000459
中图分类号:
O [数理科学和化学];
P [天文学、地球科学];
Q [生物科学];
N [自然科学总论];
学科分类号:
07 ;
0710 ;
09 ;
摘要:
The severe acute respiratory syndrome coronavirus (SARS-CoV) genome is predicted to encode 14 functional open reading frames, leading to the expression of up to 30 structural and non-structural protein products. The functions of a large number of viral ORFs are poorly understood or unknown. In order to gain more insight into functions and modes of action and interaction of the different proteins, we cloned the viral ORFeome and performed a genome-wide analysis for intraviral protein interactions and for intracellular localization. 900 pairwise interactions were tested by yeast-two-hybrid matrix analysis, and more than 65 positive non-redundant interactions, including six self interactions, were identified. About 38% of interactions were subsequently confirmed by CoIP in mammalian cells. Nsp2, nsp8 and ORF9b showed a wide range of interactions with other viral proteins. Nsp8 interacts with replicase proteins nsp2, nsp5, nsp6, nsp7, nsp8, nsp9, nsp12, nsp13 and nsp14, indicating a crucial role as a major player within the replication complex machinery. It was shown by others that nsp8 is essential for viral replication in vitro, whereas nsp2 is not. We show that also accessory protein ORF9b does not play a pivotal role for viral replication, as it can be deleted from the virus displaying normal plaque sizes and growth characteristics in Vero cells. However, it can be expected to be important for the virus-host interplay and for pathogenicity, due to its large number of interactions, by enhancing the global stability of the SARS proteome network, or play some unrealized role in regulating protein-protein interactions. The interactions identified provide valuable material for future studies.
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