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猪圆环病毒2型ORF3蛋白特异性抗原表位及核输出信号的鉴定

Characterization of specific antigenic epitopes and the nuclear export signal of the Porcine circovirus 2 ORF3 protein.

作者信息

Gu Jinyan, Wang Lun, Jin Yulan, Lin Cui, Wang Huijuan, Zhou Niu, Xing Gang, Liao Min, Zhou Jiyong

机构信息

Institute of Immunity and College of Veterinary Medicine, Nanjing Agricultural University, Nanjing 210095, PR China.

Key Laboratory of Animal Virology, Ministry of Agriculture, Zhejiang University, Hangzhou 310058, PR China.

出版信息

Vet Microbiol. 2016 Feb 29;184:40-50. doi: 10.1016/j.vetmic.2016.01.006. Epub 2016 Jan 7.

DOI:10.1016/j.vetmic.2016.01.006
PMID:26854343
Abstract

Porcine circovirus 2 (PCV2) is the etiological agent of postweaning multisystemic wasting syndrome. PCV2 ORF3 protein is a nonstructural protein known to induce apoptosis, but little is known about the biological function of ORF3 protein. Therefore, we undertook this study to map ORF3 protein epitopes recognized by a panel of monoclonal antibodies (mAbs) and to characterize putative nuclear localization (NLS) and nuclear export (NES) sequences in ORF3. The linear epitopes targeted by two previously published mAbs 3B1 and 1H3 and a novel mouse mAb 3C3 were defined using overlapping pools of peptides. Here, we find that ORF3 in PCV2 infected cells contains a conformational epitope targeted by the antibody 3C3, which is distinct from linear epitopes recognized by the antibodies 3B1 and 1H3 in recombinant ORF3 protein. These results suggest that the linear epitope recognized by 3B1 and 1H3 is masked in PCV2 infected cells, and that the conformational epitope is unique to PCV2 infection. Furthermore, we find that ORF3 protein expressed in cytoplasm in early stages of PCV2 infection and then accumulated in nucleus over time. Moreover, we localize a NES at the N-terminus (residues 1-35aa) of ORF3 which plays critical role in nuclear export activity. These findings provide a novel insight that deepens our understanding of the biological function of PCV2 ORF3.

摘要

猪圆环病毒2型(PCV2)是断奶后多系统消耗综合征的病原体。PCV2的ORF3蛋白是一种已知可诱导细胞凋亡的非结构蛋白,但对ORF3蛋白的生物学功能了解甚少。因此,我们开展了这项研究,以绘制一组单克隆抗体(mAb)识别的ORF3蛋白表位,并鉴定ORF3中假定的核定位(NLS)和核输出(NES)序列。使用重叠肽库确定了两种先前发表的单克隆抗体3B1和1H3以及一种新型小鼠单克隆抗体3C3靶向的线性表位。在此,我们发现PCV2感染细胞中的ORF3包含一个由抗体3C3靶向的构象表位,这与重组ORF3蛋白中抗体3B1和1H3识别的线性表位不同。这些结果表明,3B1和1H3识别的线性表位在PCV2感染细胞中被掩盖,并且该构象表位是PCV2感染所特有的。此外,我们发现PCV2感染早期在细胞质中表达的ORF3蛋白,随后随时间推移在细胞核中积累。此外,我们在ORF3的N端(第1 - 35个氨基酸残基)定位了一个NES,它在核输出活性中起关键作用。这些发现提供了一个新的见解,加深了我们对PCV2 ORF3生物学功能的理解。

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