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IL-12 as a therapeutic target for pharmacological modulation in immune-mediated and inflammatory diseases: regulation of T helper 1/T helper 2 responses

机译:IL-12作为免疫介导的炎症性疾病药理调节的治疗靶点:调节T辅助1 / T辅助2反应

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摘要

Interleukin-12 (IL-12) is a pivotal cytokine in driving the immune system towards a T helper (Th)1 type response and preventing a Th2 type immune profile. Therefore, IL-12 is indispensable in the defense against certain, mainly intracellular pathogens, but overproduction of this cytokine is crucially involved in the etiology of several inflammatory and autoimmune diseases.Hence, IL-12 is an ideal target for pharmacological intervention in the therapy of autoimmune and inflammatory diseases.The production of IL-12 and a resultant Th1 type immune response can be suppressed with several pharmacological approaches including modulation of intracellular cyclic AMP levels, glucocorticoids and nuclear factor-κB inhibition. IL-12 responsiveness may be inhibited using anti-IL-12 antibodies, soluble IL-12 receptors or the IL-12 p40 homodimer.Exploitation of these approaches may provide novel means for the experimental therapy of a variety of pathophysiological states.
机译:白细胞介素12(IL-12)是驱动免疫系统向T辅助(Th)1型应答和防止Th2型免疫谱的关键细胞因子。因此,IL-12在抵抗某些主要是细胞内病原体的防御中必不可少,但这种细胞因子的过度生产与多种炎性和自身免疫性疾病的病因至关重要。因此,IL-12是药物治疗中理想的靶标IL-12的产生和由此产生的Th1型免疫反应可以通过几种药理学方法来抑制,包括调节细胞内环AMP的水平,糖皮质激素和核因子-κB的抑制。使用抗IL-12抗体,可溶性IL-12受体或IL-12 p40同型二聚体可抑制IL-12的应答性。这些方法的开发可为多种病理生理状态的实验治疗提供新颖的手段。

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