可制备有效免疫毒素的人抗HIV gp160单克隆抗体的鉴定
Identification of Human Anti-HIV gp160 Monoclonal Antibodies That Make Effective Immunotoxins.
作者信息
Pincus Seth H, Song Kejing, Maresh Grace A, Hamer Dean H, Dimitrov Dimiter S, Chen Weizao, Zhang Mei-Yun, Ghetie Victor F, Chan-Hui Po-Ying, Robinson James E, Vitetta Ellen S
机构信息
Research Institute for Children, Children's Hospital, New Orleans, Louisiana, USA
Department of Pediatrics and Department of Microbiology, Immunology, and Parasitology, Louisiana State University Health Sciences Center, New Orleans, Louisiana, USA.
出版信息
J Virol. 2017 Jan 18;91(3). doi: 10.1128/JVI.01955-16. Print 2017 Feb 1.
UNLABELLED
The envelope (Env) glycoprotein of HIV is the only intact viral protein expressed on the surface of both virions and infected cells. Env is the target of neutralizing antibodies (Abs) and has been the subject of intense study in efforts to produce HIV vaccines. Therapeutic anti-Env Abs can also exert antiviral effects via Fc-mediated effector mechanisms or as cytotoxic immunoconjugates, such as immunotoxins (ITs). In the course of screening monoclonal antibodies (MAbs) for their ability to deliver cytotoxic agents to infected or Env-transfected cells, we noted disparities in their functional activities. Different MAbs showed diverse functions that did not correlate with each other. For example, MAbs against the external loop region of gp41 made the most effective ITs against infected cells but did not neutralize virus and bound only moderately to the same cells that they killed so effectively when they were used in ITs. There were also differences in IT-mediated killing among transfected and infected cell lines that were unrelated to the binding of the MAb to the target cells. Our studies of a well-characterized antigen demonstrate that MAbs against different epitopes have different functional activities and that the binding of one MAb can influence the interaction of other MAbs that bind elsewhere on the antigen. These results have implications for the use of MAbs and ITs to kill HIV-infected cells and eradicate persistent reservoirs of HIV infection.
IMPORTANCE
There is increased interest in using antibodies to treat and cure HIV infection. Antibodies can neutralize free virus and kill cells already carrying the virus. The virus envelope (Env) is the only HIV protein expressed on the surfaces of virions and infected cells. In this study, we examined a panel of human anti-Env antibodies for their ability to deliver cell-killing toxins to HIV-infected cells and to perform other antiviral functions. The ability of an antibody to make an effective immunotoxin could not be predicted from its other functional characteristics, such as its neutralizing activity. Anti-HIV immunotoxins could be used to eliminate virus reservoirs that persist despite effective antiretroviral therapy.
未标记
HIV的包膜(Env)糖蛋白是唯一在病毒粒子和感染细胞表面表达的完整病毒蛋白。Env是中和抗体(Abs)的靶标,并且一直是研发HIV疫苗的深入研究对象。治疗性抗Env抗体也可通过Fc介导的效应机制或作为细胞毒性免疫偶联物发挥抗病毒作用,例如免疫毒素(ITs)。在筛选单克隆抗体(MAbs)向感染或Env转染细胞递送细胞毒性剂的能力的过程中,我们注意到它们的功能活性存在差异。不同的单克隆抗体表现出各不相关的多样功能。例如,针对gp41外环区域的单克隆抗体制成的免疫毒素对感染细胞最有效,但不能中和病毒,并且仅适度结合其在免疫毒素中有效杀死的相同细胞。转染细胞系和感染细胞系之间IT介导的杀伤也存在差异,这与单克隆抗体与靶细胞的结合无关。我们对一种特征明确的抗原的研究表明,针对不同表位的单克隆抗体具有不同的功能活性,并且一种单克隆抗体的结合可影响在抗原其他部位结合的其他单克隆抗体的相互作用。这些结果对使用单克隆抗体和免疫毒素杀死HIV感染细胞及根除HIV感染的持续储存库具有启示意义。
重要性
使用抗体治疗和治愈HIV感染的兴趣日益增加。抗体可中和游离病毒并杀死已携带病毒的细胞。病毒包膜(Env)是在病毒粒子和感染细胞表面表达的唯一HIV蛋白。在本研究中,我们检测了一组人抗Env抗体向HIV感染细胞递送细胞杀伤毒素及执行其他抗病毒功能的能力。无法根据抗体的其他功能特性(如中和活性)预测其制成有效免疫毒素的能力。抗HIV免疫毒素可用于消除尽管进行了有效的抗逆转录病毒治疗仍持续存在的病毒储存库。
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