Virology Journal (Oct 2018)

Glycan binding patterns of human rotavirus P[10] VP8* protein

  • Li-li Pang,
  • Meng-xuan Wang,
  • Xiao-man Sun,
  • Yue Yuan,
  • Yu Qing,
  • Yan Xin,
  • Jia-yan Zhang,
  • Dan-di Li,
  • Zhao-jun Duan

DOI
https://doi.org/10.1186/s12985-018-1065-9
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 6

Abstract

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Abstract Background Rotaviruses (RVs) are a major cause of acute children gastroenteritis. The rotavirus P [10] belongs to P[I] genogroup of group A rotaviruses that mainly infect animals, while the rotavirus P [10] was mainly identified from human infection. The rotavirus P [10] is an unusual genotype and the recognition pattern of cellular receptors remains unclear. Methods We expressed and purified the RV P [10] VP8* protein and investigated the saliva and oligosaccharide binding profiles of the protein. A homology model of the P [10] VP8* core protein was built and the superimposition structural analysis of P [10] VP8* protein on P [19] VP8* in complex with mucin core 2 was performed to explore the possible docking structural basis of P [10] VP8* and mucin cores. Results Our data showed that rotavirus P [10] VP8* protein bound to all ABO secretor and non-secretor saliva. The rotavirus P [10] could bind strongly to mucin core 2 and weakly to mucin core 4. The homology modeling indicated that RV P [10] VP8* binds to mucin core 2 using a potential glycan binding site that is the same to P [19] VP8* belonging to P[II] genogroup. Conclusion Our results suggested an interaction of rotavirus P [10] VP8* protein with mucin core 2 and mucin core 4. These findings offer potential for elucidating the mechanism of RV A host specificity, evolution and epidemiology.

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