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Macrophage-Targeted Therapy: CD64-Based Immunotoxins for Treatment of Chronic Inflammatory Diseases

机译:巨噬细胞靶向治疗:基于CD64的免疫毒素治疗慢性炎症性疾病

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Diseases caused by chronic inflammation (e.g., arthritis, multiple sclerosis and diabetic ulcers) are multicausal, thus making treatment difficult and inefficient. Due to the age-associated nature of most of these disorders and the demographic transition towards an overall older population, efficient therapeutic intervention strategies will need to be developed in the near future. Over the past decades, elimination of activated macrophages using CD64-targeting immunotoxins has proven to be a promising way of resolving inflammation in animal models. More recent data have shown that the M1-polarized population of activated macrophages in particular is critically involved in the chronic phase. We recapitulate the latest progress in the development of IT. These have advanced from full-length antibodies, chemically coupled to bacterial toxins, into single chain variants of antibodies, genetically fused with fully human enzymes. These improvements have increased the range of possible target diseases, which now include chronic inflammatory diseases. At present there are no therapeutic strategies focusing on macrophages to treat chronic disorders. In this review, we focus on the role of different polarized macrophages and the potential of CD64-based IT to intervene in the process of chronic inflammation.
机译:由慢性炎症引起的疾病(例如关节炎,多发性硬化症和糖尿病性溃疡)是多因的,因此使治疗困难且效率低下。由于大多数此类疾病的年龄相关性质以及人口向总体老年人口的过渡,因此在不久的将来将需要开发有效的治疗干预策略。在过去的几十年中,使用靶向CD64的免疫毒素消除活化的巨噬细胞已被证明是解决动物模型炎症的一种有前途的方法。最近的数据表明,活化阶段的巨噬细胞的M1极化群体特别参与了慢性期。我们概述了IT开发的最新进展。这些技术已从与细菌毒素化学偶联的全长抗体发展成为与全人类酶基因融合的抗体单链变体。这些改善增加了可能的目标疾病的范围,其中包括慢性炎症性疾病。当前,没有针对巨噬细胞的治疗策略来治疗慢性疾病。在这篇综述中,我们关注于不同极化的巨噬细胞的作用以及基于CD64的IT干预慢性炎症过程的潜力。

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