Passive Immunity Should and Will Work for COVID-19 for Some Patients.

Clinical Hematology International Pub Date : 2021-04-16 eCollection Date: 2021-06-01 DOI:10.2991/chi.k.210328.001
Nevio Cimolai
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引用次数: 2

Abstract

In the absence of effective antiviral chemotherapy and still in the context of emerging vaccines for severe acute respiratory syndrome-CoV-2 infections, passive immunotherapy remains a key treatment and possible prevention strategy. What might initially be conceived as a simplified donor-recipient process, the intricacies of donor plasma, IV immunoglobulins, and monoclonal antibody modality applications are becoming more apparent. Key targets of such treatment have largely focused on virus neutralization and the specific viral components of the attachment Spike protein and its constituents (e.g., receptor binding domain, N-terminal domain). The cumulative laboratory and clinical experience suggests that beneficial protective and treatment outcomes are possible. Both a dose- and a time-dependency emerge. Lesser understood are the concepts of bioavailability and distribution. Apart from direct antigen binding from protective immunoglobulins, antibody effector functions have potential roles in outcome. In attempting to mimic the natural but variable response to infection or vaccination, a strong functional polyclonal approach attracts the potential benefits of attacking antigen diversity, high antibody avidity, antibody persistence, and protection against escape viral mutation. The availability and ease of administration for any passive immunotherapy product must be considered in the current climate of need. There is never a perfect product, but yet there is considerable room for improving patient outcomes. Given the variability of human genetics, immunity, and disease, and given the nuances of the virus and its potential for change, passive immunotherapy can be developed that will be effective for some but not all patients. An understanding of such patient variability and limitations is just as important as the understanding of the direct interactions between immunotherapy and virus.

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被动免疫应该也将对某些患者的COVID-19起作用。
在缺乏有效的抗病毒化疗的情况下,以及在新出现的严重急性呼吸系统综合征冠状病毒2型感染疫苗的背景下,被动免疫疗法仍然是一种关键的治疗和可能的预防策略。最初可能被认为是一个简化的供体-受体过程,供体血浆、IV免疫球蛋白和单克隆抗体模式应用的复杂性正变得越来越明显。这种治疗的关键靶点主要集中在病毒中和和附着刺突蛋白的特定病毒成分及其成分(例如受体结合结构域、N-末端结构域)上。累积的实验室和临床经验表明,有益的保护和治疗结果是可能的。出现了剂量和时间依赖性。对生物利用度和分布的概念了解较少。除了保护性免疫球蛋白的直接抗原结合外,抗体效应器功能在结果中具有潜在作用。在试图模拟对感染或疫苗接种的自然但可变的反应时,功能强大的多克隆方法吸引了攻击抗原多样性、高抗体亲和力、抗体持久性和防止逃逸病毒突变的潜在好处。在当前的需求环境下,必须考虑任何被动免疫疗法产品的可用性和易用性。从来没有完美的产品,但在改善患者预后方面还有相当大的空间。考虑到人类遗传、免疫和疾病的可变性,以及病毒的细微差别及其变化的潜力,可以开发出对部分但并非所有患者有效的被动免疫疗法。了解这种患者的变异性和局限性与了解免疫疗法和病毒之间的直接相互作用同样重要。
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