Immunogenicity by Aggregation of Therapeutic Proteins from Ultraviolet Radiation Produced in the Human Body by Nanoparticles of the Aggregates Themselves

T. Prevenslik
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Abstract

Protein therapeutics is used in the treatment of diabetes and various forms of cancer. A major concern is that repeated administration to patients often leads to undesirable antidrug antibodies with a wide range of life threatening consequences that induce immunogenicity or an adverse response of the immune system. The antibodies are generally thought triggered by the tendency of monomer protein molecules to aggregate, although why aggregation occurs is not known. In protein deposition diseases such as Alzheimer and Parkinson, protein aggregates have stronger immunogenicity. Typically, the aggregates known to elicit immunogenicity are globular proteins having molecular weights from 6-100 kDa and diameters from 3-10 nm that are comparable to inanimate natural or manmade nanoparticles that have been linked to damage of deoxyribonucleic acid by the natural emission of low-level ultraviolet radiation induced by quantum electrodynamics. Similarity suggests the protein aggregates form as monomers cross-link under ultraviolet radiation produced by nanoparticles of the aggregates themselves. How immunogenicity may be reduced is discussed.
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人体紫外线辐射中治疗性蛋白质聚集的免疫原性是由聚集物本身的纳米粒子产生的
蛋白质疗法用于治疗糖尿病和各种形式的癌症。一个主要的问题是,反复给药往往导致患者产生不良的抗药物抗体,这些抗体具有广泛的危及生命的后果,诱发免疫原性或免疫系统的不良反应。一般认为抗体是由单体蛋白分子聚集的倾向引发的,尽管聚集发生的原因尚不清楚。在蛋白质沉积性疾病如阿尔茨海默病和帕金森病中,蛋白质聚集体具有更强的免疫原性。通常,已知引起免疫原性的聚集体是分子量为6-100 kDa,直径为3-10 nm的球状蛋白质,与无生命的天然或人造纳米颗粒相当,这些纳米颗粒与量子电动力学诱导的低水平紫外线辐射自然发射引起的脱氧核糖核酸损伤有关。相似性表明蛋白质聚集体在聚集体本身的纳米粒子产生的紫外线辐射下形成单体交联。讨论了如何降低免疫原性。
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