Extracorporeal Immunopharmacotherapy of Autoimmune Diseases

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Abstract

The article aims to analyze pathogenetic mechanisms of autoimmune diseases development including disorders of both cellular and humoral immunity. The standard drug therapy with corticosteroids and cytostatic leads to a number of side effects such as lipid metabolism disorders (Kushing-syndrome), arterial hypertension, diabetes, and osteoporosis each of which is to be additionally treated. Chimeric monoclonal antibodies (rituximab, natalizumab, etc.) can also cause complications. Therefore apheresis therapy with removal of autoantibodies, circulating immune complexes and other pathological metabolites is pathogenetically justified. However, the greatest effect is reached by means of extracorporeal immunopharmacotherapy when, besides antibodies removal by means of plasmapheresis one performs selection of lymphocytes and their temporary incubation with corticosteroids and cytostatics, which are then returned to the patient. Such targeted immunosuppression is much more effective then “pulse therapy” with minimum negative consequences for the body. At the same time a supporting drug therapy can be carried out with half smaller doses.
自身免疫性疾病的体外免疫药物治疗
本文旨在分析自身免疫性疾病的发病机制,包括细胞免疫和体液免疫的紊乱。皮质类固醇和细胞抑制剂的标准药物治疗会导致许多副作用,如脂质代谢紊乱(库欣综合征)、动脉高血压、糖尿病和骨质疏松症,每一种都需要额外治疗。嵌合单克隆抗体(利妥昔单抗、那他珠单抗等)也可引起并发症。因此,去除自身抗体、循环免疫复合物和其他病理代谢物的单采疗法在病理学上是合理的。然而,体外免疫药物治疗的效果最好,除了通过血浆置换去除抗体外,还可以选择淋巴细胞,并将其与皮质类固醇和细胞抑制剂一起暂时孵育,然后将其返回患者体内。这种有针对性的免疫抑制比“脉冲疗法”更有效,对身体的负面影响最小。同时,辅助药物治疗可以用小一半的剂量进行。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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