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B-cell restriction - an alternative piece to the puzzle

机译:B细胞限制 - 拼图的替代品

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Effective vaccination is based on three critical aspects of the B-cell response towards infectious agents: (i) that B-cells can generate specific antibodies towards a vast molecular diversity of antigens; proteins, sugars, DNA and lipids. There seems to be no limit to the ability to raise antibodies to everything. (ii) once stimulated, B-cells can perfect their antibodies through affinity maturation to complement every nook and cranny of the epitope and (iii) that the pathogen remains genetically stable and does not change to any great extent. Thus, antibodies produced against the vaccine and subsequent boosts recognize the viral virulent field isolates in future encounters and effectively knock them out. However, some vaccine targets, such as flu virus and HIV, are extremely genetically dynamic. The rapid genetic drift of these viruses renders them moving targets which assist in their ability to evade immune surveillance. Here we postulate that in the case of hyper-variable pathogens the B-cell response actually might be too good. We propose that restricting B-cell activities may prove effective in counteracting the genetic diversity of variant viruses such as flu and HIV. We suggest two levels of B-cell restriction: (i) to focus the B-cell response exclusively towards neutralizing epitopes by creating epitope-based immunogens; (ii) to restrict affinity maturation of B-cells to prevent the production of overly optimized exquisitely specific antibodies. Together, these B-cell restrictions provide a new modality for vaccine design.
机译:有效疫苗是基于朝感染剂的B细胞应答的三个关键方面:(i)该B细胞可以产生朝向抗原的广阔分子多样性的特异性抗体;蛋白质,糖类,DNA和脂质。似乎有没有限制产生抗体的一切的能力。 (ⅱ)一次刺激时,B细胞可以通过亲和力成熟完善其抗体,以补充每个角落和表位的裂隙和(iii)该病原体保持遗传稳定的,并且不改变任何大的程度。因此,针对疫苗和后续加强产生的抗体识别病毒的毒力株领域未来的遭遇和有效地敲出来。然而,一些疫苗的目标,如流感病毒和HIV,是非常动态的基因。这些病毒的快速遗传漂变使他们移动它帮助他们逃避免疫监视能力的目标。在这里,我们推测,在高变的情况下,病原体的B细胞反应实际上可能是太美好了。我们建议,限制B细胞的活动可以证明是有效的对抗变种病毒如流感和艾滋病病毒的遗传多样性。我们建议B细胞限制的两个级别:(i)至完全集中的B细胞应答的中和朝向通过创建基于表位的免疫原的表位; (ⅱ),以限制B细胞的亲和力成熟,以防止生产过于优化精美特异性抗体。总之,这些B细胞限制为疫苗设计的新模式。

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