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XOMA052,一种强效、高亲和力的单克隆抗体,用于治疗白细胞介素-1β介导的疾病。

XOMA 052, a potent, high-affinity monoclonal antibody for the treatment of IL-1β-mediated diseases.

机构信息

XOMA (US) LLC, Preclinical Department, Berkeley, CA, USA.

出版信息

MAbs. 2011 Jan-Feb;3(1):49-60. doi: 10.4161/mabs.3.1.13989. Epub 2011 Jan 1.

Abstract

Interleukin-1β (IL-1β) is a potent mediator of inflammatory responses and plays a role in the differentiation of a number of lymphoid cells. In several inflammatory and autoimmune diseases, serum levels of IL-1β are elevated and correlate with disease development and severity. The central role of the IL-1 pathway in several diseases has been validated by inhibitors currently in clinical development or approved by the FDA. However, the need to effectively modulate IL-1β-mediated local inflammation with the systemic delivery of an efficacious, safe and convenient drug still exists. To meet these challenges, we developed XOMA 052 (gevokizumab), a potent anti-IL-1β neutralizing antibody that was designed in silico and humanized using Human Engineering™ technology. XOMA 052 has a 300 femtomolar binding affinity for human IL-1β and an in vitro potency in the low picomolar range. XOMA 052 binds to a unique IL-1β epitope where residues critical for binding have been identified. We have previously reported that XOMA 052 is efficacious in vivo in a diet-induced obesity mouse model thought to be driven by low levels of chronic inflammation. We report here that XOMA 052 also reduces acute inflammation in vivo, neutralizing the effect of exogenously administered human IL-1β and blocking peritonitis in a mouse model of acute gout. Based on its high potency, novel mechanism of action, long half-life, and high affinity, XOMA 052 provides a new strategy for the treatment of a number of inflammatory, autoimmune and metabolic diseases in which the role of IL-1β is central to pathogenesis.

摘要

白细胞介素-1β(IL-1β)是炎症反应的有力介质,在多种淋巴样细胞的分化中发挥作用。在几种炎症性和自身免疫性疾病中,血清中 IL-1β 的水平升高,与疾病的发展和严重程度相关。IL-1 途径在几种疾病中的核心作用已被目前正在临床开发或 FDA 批准的抑制剂所验证。然而,仍需要通过有效的全身递送有效的、安全的和方便的药物来调节 IL-1β 介导的局部炎症。为了满足这些挑战,我们开发了 XOMA 052(gevokizumab),一种有效的抗 IL-1β 中和抗体,它是通过计算机设计和使用 Human Engineering™ 技术进行人源化的。XOMA 052 对人 IL-1β 的结合亲和力为 300 飞摩尔,体外效力在低皮摩尔范围内。XOMA 052 结合到一个独特的 IL-1β 表位,其中已确定了对结合至关重要的残基。我们之前报道过,XOMA 052 在一种饮食诱导的肥胖小鼠模型中具有体内疗效,该模型被认为是由低水平的慢性炎症驱动的。我们在这里报告,XOMA 052 还能减轻体内的急性炎症,中和外源性给予的人 IL-1β 的作用,并阻断急性痛风小鼠模型中的腹膜炎。基于其高效力、新颖的作用机制、长半衰期和高亲和力,XOMA 052 为治疗多种炎症性、自身免疫性和代谢性疾病提供了一种新策略,其中 IL-1β 的作用是发病机制的核心。

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