靶向 C3 的牙周病治疗:向临床应用更近一步。
C3-targeted therapy in periodontal disease: moving closer to the clinic.
机构信息
University of Pennsylvania, Penn Dental Medicine, Department of Basic and Translational Sciences, Philadelphia, PA, USA.
The Forsyth Institute, Center for Clinical and Translational Research, Cambridge, MA, USA.
出版信息
Trends Immunol. 2021 Oct;42(10):856-864. doi: 10.1016/j.it.2021.08.001. Epub 2021 Sep 2.
Abstract
Complement plays a key role in immunosurveillance and homeostasis. When dysregulated or overactivated, complement can become a pathological effector, as seen in several inflammatory disorders, including periodontal disease. Recently, clinical correlative studies and preclinical mechanistic investigations have collectively demonstrated that complement is hyperactivated during periodontitis and that targeting its central component (C3) provides therapeutic benefit in nonhuman primates (NHPs). The preclinical efficacy of a C3-targeted drug candidate combined with excellent safety and pharmacokinetic profiles supported its use in a recent Phase IIa clinical study in which C3 inhibition resolved gingival inflammation in patients with periodontal disease. We posit that C3-targeted intervention might represent a novel and transformative host-modulation therapy meriting further investigation in Phase III clinical trials for the treatment of periodontitis.
摘要
补体在免疫监视和稳态中起着关键作用。当失调或过度激活时,补体可能成为一种病理性效应因子,如在几种炎症性疾病中,包括牙周病。最近,临床相关性研究和临床前机制研究共同表明,补体在牙周炎中过度激活,靶向其中心成分(C3)可在非人类灵长类动物(NHPs)中提供治疗益处。一种靶向 C3 的药物候选物的临床前疗效具有出色的安全性和药代动力学特征,支持其在最近的一项 IIa 期临床试验中使用,该试验表明 C3 抑制可缓解牙周病患者的牙龈炎症。我们认为,靶向 C3 的干预可能代表一种新的、变革性的宿主调节治疗方法,值得在 III 期临床试验中进一步研究,以治疗牙周炎。
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