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通过中和性和非中和性单克隆抗体的被动转移来预防小鼠巨细胞病毒感染。

Protection against murine cytomegalovirus infection by passive transfer of neutralizing and non-neutralizing monoclonal antibodies.

作者信息

Farrell H E, Shellam G R

机构信息

Department of Microbiology, University of Western Australia, Queen Elizabeth II Medical Centre, Nedlands.

出版信息

J Gen Virol. 1991 Jan;72 ( Pt 1):149-56. doi: 10.1099/0022-1317-72-1-149.

Abstract

The ability of eight neutralizing monoclonal antibodies (MAbs) specific for structural proteins of murine cytomegalovirus (MCMV) to protect mice passively against MCMV infection was examined to determine firstly whether a correlation existed between the neutralization titres of the MAbs in vitro and the protection afforded by the MAbs in vivo and, secondly, the contribution of the host towards neutralization by the MAbs in vivo. The reduction in MCMV titre in the livers of BALB/c and C57BL/10 mice by the MAbs closely correlated with their neutralization titres in vitro. However, in the spleens of BALB/c mice, in which MCMV replicates to high titre, almost all of the MAbs tested were ineffective in reducing MCMV replication. Indeed, a significant increase in splenic MCMV replication was observed in mice treated 24 h prior to MCMV replication with either neutralizing MAbs or polyclonal Ig. Each of six MAbs prophylactically protected between 66 and 100% of mice from an intraperitoneal challenge with 4 LD50 MCMV regardless of their neutralization titre in vitro. The persistence of MCMV replication in the salivary gland was not prevented by either polyclonal Ig or MAbs. Despite the absolute requirement for complement for the neutralization of MCMV in vitro, both polyclonal Ig and MAb 4F9 protected A/J mice, which are deficient in the fifth component of complement, as efficiently as they did complement competent BALB/c mice. These results demonstrate that MAbs specific for single MCMV polypeptides are protective in vivo. In addition, the extent to which the MAbs protected against MCMV could not be predicted from their immunoreactive or neutralizing titres in vitro or by their effect on splenic MCMV replication in vivo. Furthermore, these studies suggest that the mechanism(s) of neutralization of MCMV in vitro are different to those which act in vivo.

摘要

检测了8种针对鼠巨细胞病毒(MCMV)结构蛋白的中和单克隆抗体(MAb)被动保护小鼠抵抗MCMV感染的能力,以首先确定MAb在体外的中和效价与MAb在体内提供的保护之间是否存在相关性,其次确定宿主对MAb在体内中和作用的贡献。MAb对BALB/c和C57BL/10小鼠肝脏中MCMV滴度的降低与其体外中和效价密切相关。然而,在MCMV复制至高效价的BALB/c小鼠脾脏中,几乎所有测试的MAb在降低MCMV复制方面均无效。事实上,在用中和MAb或多克隆Ig在MCMV复制前24小时处理的小鼠中,观察到脾脏MCMV复制显著增加。六种MAb中的每一种都能预防性地保护66%至100%的小鼠免受4个半数致死剂量MCMV的腹腔攻击,无论其体外中和效价如何。多克隆Ig或MAb均不能阻止MCMV在唾液腺中的持续复制。尽管体外中和MCMV绝对需要补体,但多克隆Ig和MAb 4F9对缺乏补体第五成分的A/J小鼠的保护效果与对有补体活性的BALB/c小鼠一样有效。这些结果表明,针对单个MCMV多肽的MAb在体内具有保护作用。此外,无法根据MAb在体外的免疫反应性或中和效价或其对体内脾脏MCMV复制的影响来预测MAb对MCMV的保护程度。此外,这些研究表明,MCMV在体外的中和机制与在体内起作用的机制不同。

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