Monoclonal Antibodies Directed against Conserved Epitopes on the Nucleocapsid Protein and the Major Envelope Glycoprotein of Equine Arteritis Virus

Emilie Weiland; Sylvia Bolz; Frank Weiland; Werner Herbst; Martin J. B. Raamsman; Peter J. M. Rottier

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Monoclonal Antibodies Directed against Conserved Epitopes on the Nucleocapsid Protein and the Major Envelope Glycoprotein of Equine Arteritis Virus

机译：针对马动脉炎病毒核壳蛋白和主要包膜糖蛋白上的保守表位的单克隆抗体

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We recently developed a highly effective immunization procedure for the generation of monoclonal antibodies (MAbs) directed against the porcine reproductive and respiratory syndrome virus (E. Weiland, M. Wieczorek-Krohmer, D. Kohl, K. K. Conzelmann, and F. Weiland, Vet. Microbiol. 66:171–186, 1999). The same method was used to produce a panel of 16 MAbs specific for the equine arteritis virus (EAV). Ten MAbs were directed against the EAV nucleocapsid (N) protein, and five MAbs recognized the major viral envelope glycoprotein (G_L). Two of the EAV G_L-specific MAbs and one antibody of unknown specificity neutralized virus infectivity. A comparison of the reactivities of the MAbs with 1 U.S. and 22 newly obtained European field isolates of EAV demonstrated that all N-specific MAbs, the three nonneutralizing anti-G_L MAbs, and the weakest neutralizing MAb (MAb E7/d15-c9) recognized conserved epitopes. In contrast, the two MAbs with the highest neutralization titers bound to 17 of 23 (MAb E6/A3) and 10 of 23 (MAb E7/d15-c1) of the field isolates. Ten of the virus isolates reacted with only one of these two MAbs, indicating that they recognized different epitopes. The G_L-specific MAbs and the strongly neutralizing MAb of unknown specificity (MAb E6/A3) were used for the selection of neutralization-resistant (NR) virus variants. The observation that the E6/A3-specific NR virus variants were neutralized by MAb E7/d15-c1 and that MAb E6/A3 blocked the infectivity of the E7/d15-c1-specific NR escape mutant confirmed that these antibodies reacted with distinct antigenic sites. Immunoelectron microscopy revealed for the first time that the antigenic determinants recognized by the anti-G_L MAbs were localized on the virion surface. Surprisingly, although the immunofluorescence signal obtained with the neutralizing antibodies was relatively weak, they mediated binding of about three times as much gold granules to the viral envelope than the nonneutralizing anti-G_L MAbs.

机译：我们最近开发了一种高效的免疫程序，用于产生针对猪繁殖与呼吸综合征病毒的单克隆抗体（MAb）（E。Weiland，M。Wieczorek-Krohmer，D。Kohl，KK Conzelmann和F. Weiland，Vet Microbiol。66：171-186，1999）。使用相同的方法生产一组专门针对马动脉炎病毒（EAV）的16 MAb。 10个单抗针对EAV核衣壳（N）蛋白，而5个单抗则识别主要的病毒包膜糖蛋白（G _{L ）。两种EAV G _{L 特异性MAb和一种未知特异性的抗体可中和病毒的感染性。将MAb与1个美国和22个新获得的欧洲EAV野外分离株的反应性进行比较，结果表明，所有N特异性MAb，三个非中和性抗G _{L MAb和最弱的中和性MAb（ MAb E7 / d15-c9）识别的保守表位。相反，具有最高中和效价的两个MAb分别与该领域的23个中的17个（MAb E6 / A3）和23个中的10个（MAb E7 / d15-c1）结合。十个病毒分离株仅与这两个单克隆抗体之一反应，表明它们识别不同的表位。使用G _{L 特异的单克隆抗体和未知特异性的强中和单克隆抗体（MAb E6 / A3）选择抗中和性（NR）病毒变体。观察到E6 / A3特异性NR病毒变体被MAb E7 / d15-c1中和并且MAb E6 / A3阻断了E7 / d15-c1特异性NR逃逸突变体的传染性，这证实了这些抗体与独特的抗原反应网站。免疫电子显微镜首次揭示抗G _{L MAb识别的抗原决定簇位于病毒体表面。令人惊讶的是，尽管用中和抗体获得的免疫荧光信号相对较弱，但它们介导的金颗粒与病毒包膜的结合是非中和性抗-G _{L MAb的三倍。}}}}}}

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《Journal of Clinical Microbiology》 |2000年第6期|共11页
作者
Emilie Weiland; Sylvia Bolz; Frank Weiland; Werner Herbst; Martin J. B. Raamsman; Peter J. M. Rottier;
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中图分类医学微生物学（病原细菌学、病原微生物学）;
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1. Large envelope glycoprotein and nucleocapsid protein of equine arteritis virus (EAV) induce an immune response in Balb/c mice by DNA vaccination; strategy for developing a DNA-vaccine against EAV-infection. [J] . Tobiasch E, Kehm R, Bahr U, Virus Genes . 2001,第2期

机译：马动脉炎病毒（EAV）的大包膜糖蛋白和核衣壳蛋白可通过DNA疫苗接种在Balb / c小鼠中诱导免疫反应。开发针对EAV感染的DNA疫苗的策略。
2. Diagnostic application of immunoperoxidase monolayer assay using monoclonal antibodies produced against equine arteritis virus 14-kDa nucleocapsid protein. [J] . Hornyak A, Denes B, Szeredi L, Hybridoma and hybridomics . 2004,第6期

机译：使用针对马动脉炎病毒14-kDa核衣壳蛋白产生的单克隆抗体的免疫过氧化物酶单层测定的诊断应用。
3. PHYLOGENETIC ANALYSIS OF OPEN READING FRAME 5 OF FIELD ISOLATES OF EQUINE ARTERITIS VIRUS AND IDENTIFICATION OF CONSERVED AND NONCONSERVED REGIONS IN THE G(L) ENVELOPE GLYCOPROTEIN [J] . Balasuriya UBR, Timoney PJ, Mccollum WH, Virology . 1995,第2期

机译：马动脉炎病毒野外隔离株开放阅读框5的系统发育分析及G（L）包膜糖蛋白中保守和非保守区的鉴定
4. CHARACTERIZATION OF THE EPITOPE FOR ANTI HUMAN RESPIRATORY SYNCYTIAL VIRUS F PROTEIN MONOCLONAL ANTIBODY 101F USING SYNTHETIC PEPTIDES AND RECOMBINANT F PROTEIN MUTANTS [C] . Marian Kruszynski, Sheng Jiun Wu, Albert Schmidt the European Peptide Symposium . 2007

机译：用合成肽和重组F蛋白突变体表征抗人呼吸道合胞病毒F蛋白单克隆抗体101f的表位
5. Antibody responses of horses to five major glycoproteins of equine herpesvirus 1 and specificity of responses to antigenic domains of glycoproteins B and C. [D] . Ostlund, Eileen Noel. 1992

机译：马对马疱疹病毒1的5种主要糖蛋白的抗体应答以及对糖蛋白B和C抗原域的应答的特异性。
6. Monoclonal Antibodies Directed against Conserved Epitopes on the Nucleocapsid Protein and the Major Envelope Glycoprotein of Equine Arteritis Virus [O] . Emilie Weiland, Sylvia Bolz, Frank Weiland, 2000

机译：针对马动脉炎病毒核壳蛋白和主要包膜糖蛋白上的保守表位的单克隆抗体
7. Monoclonal Antibodies Directed against Conserved Epitopes on the Nucleocapsid Protein and the Major Envelope Glycoprotein of Equine Arteritis Virus [O] . Emilie Weiland, Sylvia Bolz, Frank Weiland, 2000

机译：单克隆抗体针对核衣壳蛋白的保守表位和马动脉炎病毒的主要包膜糖蛋白
8. Bank Vole Monoclonal Antibodies against Puumala Virus Envelope Glycoproteins:Identification of Epitopes Involved in Neutralization [R] . Niklasson, B., Lundkvist, A. 1992

机译：针对puumala病毒包膜糖蛋白的Bank Vole单克隆抗体：中和中涉及的表位的鉴定

Monoclonal Antibodies Directed against Conserved Epitopes on the Nucleocapsid Protein and the Major Envelope Glycoprotein of Equine Arteritis Virus

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