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Literature DB >> 27535055

Functional and Structural Characterization of P[19] Rotavirus VP8* Interaction with Histo-blood Group Antigens.

Xiaoman Sun¹, Dandi Li¹, Ruchao Peng², Nijun Guo¹, Miao Jin¹, Yongkang Zhou¹, Guangcheng Xie¹, Lili Pang¹, Qing Zhang¹, Jianxun Qi², Zhao-Jun Duan³.

Abstract

Rotaviruses (RVs) of species A (RVA) are a major causative agent of acute gastroenteritis. Recently, histo-blood group antigens (HBGAs) have been reported to interact with human RVA VP8* proteins. Human P[19] is a rare P genotype of porcine origin that infects humans sporadically. The functional and structural characteristics of P[19] VP8* interaction with HBGAs are unknown. In this study, we expressed and purified the VP8* proteins of human and porcine P[19] RVs. In oligosaccharide and saliva binding assays, P[19] VP8* proteins showed obvious binding to A-, B-, and O-type saliva samples irrespective of the secretor status, implying broad binding patterns. However, they did not display specific binding to any of the oligosaccharides tested. In addition, we solved the structure of human P[19] VP8* at 2.4 Å, which revealed a typical galectin-like fold. The structural alignment demonstrated that P[19] VP8* was most similar to that of P[8], which was consistent with the phylogenetic analysis. Structure superimposition revealed the basis for the lack of binding to the oligosaccharides. Our study indicates that P[19] RVs may bind to other oligosaccharides or ligands and may have the potential to spread widely among humans. Thus, it is necessary to place the prevalence and evolution of P[19] RVs under surveillance. IMPORTANCE: Human P[19] is a rare P genotype of porcine origin. Based on phylogenetic analysis of VP8* sequences, P[19] was classified in the P[II] genogroup, together with P[4], P[6], and P[8], which have been reported to interact with HBGAs in a genotype-dependent manner. In this study, we explored the functional and structural characteristics of P[19] VP8* interaction with HBGAs. P[19] VP8* showed binding to A-, B-, and O-type saliva samples, as well as saliva of nonsecretors. This implies that P[19] has the potential to spread among humans with a broad binding range. Careful attention should be paid to the evolution and prevalence of P[19] RVs. Furthermore, we solved the structure of P[19] VP8*. Structure superimposition indicated that P[19] may bind to other oligosaccharides or ligands using potential binding sites, suggesting that further investigation of the specific cell attachment factors is warranted.

Entities: Chemical Disease Species

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Year: 2016 PMID： 27535055 PMCID： PMC5068527 DOI： 10.1128/JVI.01566-16

Source DB: PubMed Journal: J Virol ISSN： 0022-538X Impact factor: 5.103

40 in total

1. VP6-sequence-based cutoff values as a criterion for rotavirus species demarcation.

Authors: Jelle Matthijnssens; Peter H Otto; Max Ciarlet; Ulrich Desselberger; Marc Van Ranst; Reimar Johne
Journal: Arch Virol Date: 2012-03-20 Impact factor: 2.574

2. Rotavirus VP8*: phylogeny, host range, and interaction with histo-blood group antigens.

Authors: Yang Liu; Pengwei Huang; Ming Tan; Yiliu Liu; Jacek Biesiada; Jarek Meller; Alejandro A Castello; Baoming Jiang; Xi Jiang
Journal: J Virol Date: 2012-07-03 Impact factor: 5.103

3. Specificity and affinity of sialic acid binding by the rhesus rotavirus VP8* core.

Authors: Philip R Dormitzer; Zhen-Yu J Sun; Ola Blixt; James C Paulson; Gerhard Wagner; Stephen C Harrison
Journal: J Virol Date: 2002-10 Impact factor: 5.103

4. Molecular characterization of a human rotavirus reveals porcine characteristics in most of the genes including VP6 and NSP4.

Authors: V Varghese; S Das; Ng B Singh; K Kojima; S K Bhattacharya; T Krishnan; N Kobayashi; T N Naik
Journal: Arch Virol Date: 2003-09-22 Impact factor: 2.574

5. Association between norovirus and rotavirus infection and histo-blood group antigen types in Vietnamese children.

Authors: Nguyen Van Trang; Hau ThiBich Vu; Nhung ThiHong Le; Pengwei Huang; Xi Jiang; Dang Duc Anh
Journal: J Clin Microbiol Date: 2014-02-12 Impact factor: 5.948

6. Sialic acid dependence in rotavirus host cell invasion.

Authors: Thomas Haselhorst; Fiona E Fleming; Jeffrey C Dyason; Regan D Hartnell; Xing Yu; Gavan Holloway; Kim Santegoets; Milton J Kiefel; Helen Blanchard; Barbara S Coulson; Mark von Itzstein
Journal: Nat Chem Biol Date: 2008-12-21 Impact factor: 15.040

7. Identification of two independent neutralization domains on the VP4 trypsin cleavage products VP5* and VP8* of human rotavirus ST3.

Authors: L Padilla-Noriega; S J Dunn; S López; H B Greenberg; C F Arias
Journal: Virology Date: 1995-01-10 Impact factor: 3.616

8. Uniformity of rotavirus strain nomenclature proposed by the Rotavirus Classification Working Group (RCWG).

Authors: Jelle Matthijnssens; Max Ciarlet; Sarah M McDonald; Houssam Attoui; Krisztián Bányai; J Rodney Brister; Javier Buesa; Mathew D Esona; Mary K Estes; Jon R Gentsch; Miren Iturriza-Gómara; Reimar Johne; Carl D Kirkwood; Vito Martella; Peter P C Mertens; Osamu Nakagomi; Viviana Parreño; Mustafizur Rahman; Franco M Ruggeri; Linda J Saif; Norma Santos; Andrej Steyer; Koki Taniguchi; John T Patton; Ulrich Desselberger; Marc Van Ranst
Journal: Arch Virol Date: 2011-05-20 Impact factor: 2.574

9. Rapid emergence and predominance of a broadly recognizing and fast-evolving norovirus GII.17 variant in late 2014.

Authors: Martin C W Chan; Nelson Lee; Tin-Nok Hung; Kirsty Kwok; Kelton Cheung; Edith K Y Tin; Raymond W M Lai; E Anthony S Nelson; Ting F Leung; Paul K S Chan
Journal: Nat Commun Date: 2015-12-02 Impact factor: 14.919

10. Poly-LacNAc as an age-specific ligand for rotavirus P[11] in neonates and infants.

Authors: Yang Liu; Pengwei Huang; Baoming Jiang; Ming Tan; Ardythe L Morrow; Xi Jiang
Journal: PLoS One Date: 2013-11-11 Impact factor: 3.240

11 in total

Review 1. Glycan structures and their recognition roles in the human blood group ABH/Ii, Le^{a, b, x, y} and Sialyl Le^a,x active cyst glycoproteins.

Authors: Albert M Wu
Journal: Glycoconj J Date: 2019-11-26 Impact factor: 2.916

2. Human Group C Rotavirus VP8*s Recognize Type A Histo-Blood Group Antigens as Ligands.

Authors: Xiaoman Sun; Lihong Wang; Jianxun Qi; Dandi Li; Mengxuan Wang; Xin Cong; Ruchao Peng; Wengang Chai; Qing Zhang; Hong Wang; Hongling Wen; George F Gao; Ming Tan; Zhaojun Duan
Journal: J Virol Date: 2018-05-14 Impact factor: 5.103

3. Genetic susceptibility to rotavirus infection in Chinese children: a population-based case-control study.

Authors: Jin-Xia Wang; Li-Na Chen; Can-Jing Zhang; Hong-Lu Zhou; Yan-Hong Zhang; Xin-Jiang Zhang; Zhi-Yong Hao; Chao Qiu; Jing-Chen Ma; Yu-Liang Zhao; Weiming Zhong; Ming Tan; Xi Jiang; Song-Mei Wang; Xuan-Yi Wang
Journal: Hum Vaccin Immunother Date: 2020-12-09 Impact factor: 3.452

Functional and Structural Characterization of P[19] Rotavirus VP8* Interaction with Histo-blood Group Antigens.

1. VP6-sequence-based cutoff values as a criterion for rotavirus species demarcation.

2. Rotavirus VP8*: phylogeny, host range, and interaction with histo-blood group antigens.

3. Specificity and affinity of sialic acid binding by the rhesus rotavirus VP8* core.

4. Molecular characterization of a human rotavirus reveals porcine characteristics in most of the genes including VP6 and NSP4.

5. Association between norovirus and rotavirus infection and histo-blood group antigen types in Vietnamese children.

6. Sialic acid dependence in rotavirus host cell invasion.

7. Identification of two independent neutralization domains on the VP4 trypsin cleavage products VP5* and VP8* of human rotavirus ST3.

8. Uniformity of rotavirus strain nomenclature proposed by the Rotavirus Classification Working Group (RCWG).

9. Rapid emergence and predominance of a broadly recognizing and fast-evolving norovirus GII.17 variant in late 2014.

10. Poly-LacNAc as an age-specific ligand for rotavirus P[11] in neonates and infants.

Review 1. Glycan structures and their recognition roles in the human blood group ABH/Ii, Le^{a, b, x, y} and Sialyl Le^a,x active cyst glycoproteins.

2. Human Group C Rotavirus VP8*s Recognize Type A Histo-Blood Group Antigens as Ligands.

3. Genetic susceptibility to rotavirus infection in Chinese children: a population-based case-control study.

4. Glycan Binding Specificity and Mechanism of Human and Porcine P[6]/P[19] Rotavirus VP8*s.

5. Structural Basis of Glycan Recognition in Globally Predominant Human P[8] Rotavirus.

6. Structural basis of glycan specificity of P[19] VP8*: Implications for rotavirus zoonosis and evolution.

Review 7. Pregnancy Galectinology: Insights Into a Complex Network of Glycan Binding Proteins.

8. GII.13/21 Noroviruses Recognize Glycans with a Terminal β-Galactose via an Unconventional Glycan Binding Site.

Review 9. Structural Basis of Glycan Recognition of Rotavirus.

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

Review 1. Glycan structures and their recognition roles in the human blood group ABH/Ii, Lea, b, x, y and Sialyl Lea,x active cyst glycoproteins.

Review 7. Pregnancy Galectinology: Insights Into a Complex Network of Glycan Binding Proteins.

Review 9. Structural Basis of Glycan Recognition of Rotavirus.

Review 1. Glycan structures and their recognition roles in the human blood group ABH/Ii, Le^{a, b, x, y} and Sialyl Le^a,x active cyst glycoproteins.