严重急性呼吸综合征冠状病毒刺突蛋白中假定的人氨肽酶N受体结合位点。

Putative hAPN receptor binding sites in SARS_CoV spike protein.

作者信息

Yu Xiao-Jing, Luo Cheng, Lin Jian-Cheng, Hao Pei, He You-Yu, Guo Zong-Ming, Qin Lei, Su Jiong, Liu Bo-Shu, Huang Yin, Nan Peng, Li Chuan-Song, Xiong Bin, Luo Xiao-Min, Zhao Guo-Ping, Pei Gang, Chen Kai-Xian, Shen Xu, Shen Jian-Hua, Zou Jian-Ping, He Wei-Zhong, Shi Tie-Liu, Zhong Yang, Jiang Hua-Liang, Li Yi-Xue

机构信息

Shanghai Institutes for Biological Sciences, Chinese Academy of Sciences, Shanghai 200031, China.

出版信息

Acta Pharmacol Sin. 2003 Jun;24(6):481-8.

PMID:12791172

Abstract

AIM

To obtain the information of ligand-receptor binding between the S protein of SARS-CoV and CD13, identify the possible interacting domains or motifs related to binding sites, and provide clues for studying the functions of SARS proteins and designing anti-SARS drugs and vaccines.

METHODS

On the basis of comparative genomics, the homology search, phylogenetic analyses, and multi-sequence alignment were used to predict CD13 related interacting domains and binding sites in the S protein of SARS-CoV. Molecular modeling and docking simulation methods were employed to address the interaction feature between CD13 and S protein of SARS-CoV in validating the bioinformatics predictions.

RESULTS

Possible binding sites in the SARS-CoV S protein to CD13 have been mapped out by using bioinformatics analysis tools. The binding for one protein-protein interaction pair (D757-R761 motif of the SARS-CoV S protein to P585-A653 domain of CD13) has been simulated by molecular modeling and docking simulation methods.

CONCLUSION

CD13 may be a possible receptor of the SARS-CoV S protein, which may be associated with the SARS infection. This study also provides a possible strategy for mapping the possible binding receptors of the proteins in a genome.

摘要