Your search keyword '"Hantaan virus glycoprotein"' showing total 2 results

1. Integrative Analysis of HTNV Glycoprotein Derived MHC II Epitopes by In Silico Prediction and Experimental Validation

Author

Hao Sun, Zhenhua Lu, Guoyun Xuan, Ning Liu, Tianhu Wang, Yang Liu, Mingfu Lan, Jiahao Xu, Yuancai Feng, Shuang Xu, Yuchen Lu, Baozeng Sun, Jinpeng Zhang, Xiyang Zhang, Yuanjie Sun, Shuya Yang, Yun Zhang, Yusi Zhang, Linfeng Cheng, Dongbo Jiang, and Kun Yang

Subjects

Hantaan virus glycoprotein, major histocompatibility complex II epitope, in silico prediction, enzyme-linked immunospot assay, pan-major histocompatibility complex reaction, Microbiology, QR1-502

Abstract

Hantaan virus (HTNV), the causative pathogen of hemorrhagic fever with renal syndrome (HFRS), is a negative RNA virus belonging to the Orthohantaviridae family. HTNV envelope glycoprotein (GP), encoded by the genomic medium segment, is immunogenic and is therefore a promising vaccine candidate. Major histocompatibility complex class I (MHC-I) epitopes derived from HTNV has been extensively studied, but little is known of MHC-II epitopes. In silico predictions based on four databases indicated that the full-length HTNV GP has 1121 15-mer epitopes, of which 289 had a high score for binding to the human and murine MHC-II superfamily. It found that epitope ILTVLKFIANIFHTS could potentially bind most MHC-II molecules covering human and murine haplotypes. Dominant epitopes were validated by enzyme-linked immunospot assay of splenocytes from immunized mice; 6 of 10 epitopes supported the predictions including TATYSIVGPANAKVP, TKTLVIGQCIYTITS, FSLLPGVAHSIAVEL, CETYKELKAHGVSCP, CGLYLDRLKPVGSAY, and NLGENPCKIGLQTSS. Conservation analysis of dominant epitopes revealed host–virus interactions without geographic stratification, thus meeting the requirements of candidate vaccines for large-population prophylaxis. These findings provide insight into hantavirus antigenicity and suggest that vaccines targeting MHC-II could provide immune protection in large population to complement symptomatic therapies for the treatment of HFRS.

Published

2021

2. Integrative Analysis of HTNV Glycoprotein Derived MHC II Epitopes by In Silico Prediction and Experimental Validation.

Author

Sun, Hao, Lu, Zhenhua, Xuan, Guoyun, Liu, Ning, Wang, Tianhu, Liu, Yang, Lan, Mingfu, Xu, Jiahao, Feng, Yuancai, Xu, Shuang, Lu, Yuchen, Sun, Baozeng, Zhang, Jinpeng, Zhang, Xiyang, Sun, Yuanjie, Yang, Shuya, Zhang, Yun, Zhang, Yusi, Cheng, Linfeng, and Jiang, Dongbo

Subjects

HEMORRHAGIC fever with renal syndrome, GLYCOPROTEIN analysis, EPITOPES, MAJOR histocompatibility complex, HISTOCOMPATIBILITY class I antigens

Abstract

Hantaan virus (HTNV), the causative pathogen of hemorrhagic fever with renal syndrome (HFRS), is a negative RNA virus belonging to the Orthohantaviridae family. HTNV envelope glycoprotein (GP), encoded by the genomic medium segment, is immunogenic and is therefore a promising vaccine candidate. Major histocompatibility complex class I (MHC-I) epitopes derived from HTNV has been extensively studied, but little is known of MHC-II epitopes. In silico predictions based on four databases indicated that the full-length HTNV GP has 1121 15-mer epitopes, of which 289 had a high score for binding to the human and murine MHC-II superfamily. It found that epitope ILTVLKFIANIFHTS could potentially bind most MHC-II molecules covering human and murine haplotypes. Dominant epitopes were validated by enzyme-linked immunospot assay of splenocytes from immunized mice; 6 of 10 epitopes supported the predictions including TATYSIVGPANAKVP, TKTLVIGQCIYTITS, FSLLPGVAHSIAVEL, CETYKELKAHGVSCP, CGLYLDRLKPVGSAY, and NLGENPCKIGLQTSS. Conservation analysis of dominant epitopes revealed host–virus interactions without geographic stratification, thus meeting the requirements of candidate vaccines for large-population prophylaxis. These findings provide insight into hantavirus antigenicity and suggest that vaccines targeting MHC-II could provide immune protection in large population to complement symptomatic therapies for the treatment of HFRS. [ABSTRACT FROM AUTHOR]

Published

2021