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Identification of probable genomic packaging signal sequence from SARS-CoV genome by bioinformatics analysis.

  
@article{APS9142,
	author = {Lei Qin and Bin Xiong and Cheng Luo and Zong-Ming Guo and Pei Hao and Jiong Su and Peng Nan and Ying Feng and Yi-Xiang Shi and Xiao-Jing Yu and Xiao-Min Luo and Kai-Xian Chen and Xu Shen and Jian-Hua Shen and Jian-Ping Zou and Guo-Ping Zhao and Tei-Liu Shi and Wei-Zhong He and Yang Zhong and Hua-Liang Jiang and Yi-Xue Li},
	title = {Identification of probable genomic packaging signal sequence from SARS-CoV genome by bioinformatics analysis.},
	journal = {Acta Pharmacologica Sinica},
	volume = {24},
	number = {6},
	year = {2016},
	keywords = {},
	abstract = {AIM: To predict the probable genomic packaging signal of SARS-CoV by bioinformatics analysis. The derived packaging signal may be used to design antisense RNA and RNA interfere (RNAi) drugs treating SARS. METHODS: Based on the studies about the genomic packaging signals of MHV and BCoV, especially the information about primary and secondary structures, the putative genomic packaging signal of SARS-CoV were analyzed by using bioinformatic tools. Multi-alignment for the genomic sequences was performed among SARS-CoV, MHV, BCoV, PEDV and HCoV 229E. Secondary structures of RNA sequences were also predicted for the identification of the possible genomic packaging signals. Meanwhile, the N and M proteins of all five viruses were analyzed to study the evolutionary relationship with genomic packaging signals. RESULTS: The putative genomic packaging signal of SARS-CoV locates at the 3' end of ORF1b near that of MHV and BCoV, where is the most variable region of this gene. The RNA secondary structure of SARS-CoV genomic packaging signal is very similar to that of MHV and BCoV. The same result was also obtained in studying the genomic packaging signals of PEDV and HCoV 229E. Further more, the genomic sequence multi-alignment indicated that the locations of packaging signals of SARS-CoV, PEDV, and HCoV overlaped each other. It seems that the mutation rate of packaging signal sequences is much higher than the N protein, while only subtle variations for the M protein. CONCLUSIONS: The probable genomic packaging signal of SARS-CoV is analogous to that of MHV and BCoV, with the corresponding secondary RNA structure locating at the similar region of ORF1b. The positions where genomic packaging signals exist have suffered rounds of mutations, which may influence the primary structures of the N and M proteins consequently.},
	issn = {1745-7254},	url = {http://www.chinaphar.com/article/view/9142}
}