HIV疫苗研究的范式

M. V. van Regenmortel
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摘要

虽然在过去30年中进行了大量预防性人体免疫缺陷病毒(艾滋病毒)疫苗试验,但值得注意的是,迄今尚未研制出有效的艾滋病毒疫苗。研究范式对应于科学家在试图解决特定问题时使用的理论假设和特定策略。疫苗学中成功使用的许多范例对艾滋病毒无效。例如:1)基于结构的反向疫苗学方法失败了,因为研究人员试图从hiv包膜(Env)表位的抗原结构开始产生疫苗,这些抗原结构与来自hiv感染者的中和单克隆抗体(mab)结合。他们假设这种抗原结构也具有免疫原性,在疫苗中诱导多克隆抗体(Ab)反应,具有与单抗相同的中和能力。2)表位-旁位晶体学复合物中观察到的结构是由两个伙伴之间相互诱导的配合引起的,与它们相互作用之前自由分子中存在的结构不一致。3)从慢性感染个体获得的亲和成熟的中和单克隆抗体不能识别这些抗体存在于接种者体内的种系前体。4)排列在病毒膜内表面的HIV p17基质蛋白是我们这个星球上发现的最混乱的蛋白之一,这阻止了诱导的抗体与糖基化的HIV gp120蛋白结合。5)疫苗学家需要解决所谓的逆问题,例如,猜测是什么多重原因产生了早期想要的有益效果,例如精英控制者中没有有害的艾滋病毒感染。由于免疫系统由许多尚未被阐明的子系统组成,因此不可能解决每个子系统所带来的逆问题。6)疫苗学是一门经验科学,因为我们不了解导致保护性免疫反应的复杂机制,所以它有时会成功。
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Paradigms in HIV vaccine research
Although a large number of preventative human immunodeficiency virus (HIV) vaccine trials have been carried out during the last 30 years, it is remarkable that an effective HIV vaccine has not yet been developed. Research paradigms correspond to theoretical assumptions and particular strategies that scientists use when they try to solve a particular problem. Many paradigms used successfully in vaccinology were ineffective with HIV. For instance: 1) The structure-based reverse vaccinology approach failed because investigators tried to generate a vaccine starting with the antigenic structure of HIV-envelope (Env) epitopes bound to neutralizing monoclonal antibodies (mAbs) derived from HIV-infected individuals. They assumed that this antigenic structure would also possess the immunogenic capacity of inducing in vaccinees a polyclonal antibody (Ab) response with the same neutralizing capacity as the mAb. 2) The structures observed in epitope-paratope crystallographic complexes result from mutually induced fit between the two partners and do not correspond to the structures present in the free molecules before they had interacted. 3) The affinity-matured neutralizing mAbs obtained from chronically infected individuals did not recognize the germline predecessors of these Abs present in vaccinees. 4) The HIV p17 matrix protein that lines the inner surface of the viral membrane is one of the most disordered proteins identified on our planet and this prevents the induced Abs from binding to the glycosylated HIV gp120 protein. 5) Vaccinologists need to solve so-called inverse problems, for instance, guessing what are the multiple causes that produced an earlier wanted beneficial effect such as the absence of deleterious HIV infection in elite controllers. Since the immune system consists of numerous subsystems that have not yet been elucidated, it is impossible to solve the inverse problems posed by each subsystem. 6) Vaccinology is an empirical science that only sometimes succeeds because we do not understand the complex mechanisms that lead to protective immune responses.
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