A Bispecific, Tetravalent Antibody Targeting Inflammatory and Pruritogenic Pathways in Atopic Dermatitis

Julia Tietz , Tea Gunde , Stefan Warmuth , Christopher Weinert , Matthias Brock , Alexandre Simonin , Christian Hess , Maria Johansson , Fabio Spiga , Simone Muntwiler , Belinda Wickihalder , Dana Mahler , Dania Diem , Julia Zeberer , Robin Heiz , Naomi Flückiger , Noriko Shiraishi , Yoshihide Miyake , Nobuaki Takahashi , Markus Fehrholz , Daniel Snell
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Abstract

Inhibition of IL-4/IL-13 signaling has dramatically improved the treatment of atopic dermatitis (AD). However, in many patients, clinical responses are slow to develop and remain modest. Indeed, some symptoms of AD are dependent on IL-31, which is only partially reduced by IL-4/IL-13 inhibition. Thus, there is an unmet need for AD treatments that concomitantly block IL-4/IL-13 and IL-31 pathways. We engineered NM26-2198, a bispecific tetravalent antibody designed to accomplish this task. In reporter cell lines, NM26-2198 concomitantly inhibited IL-4/IL-13 and IL-31 signaling with a potency comparable with that of the combination of an anti–IL-4Rα antibody (dupilumab) and an anti–IL-31 antibody (BMS-981164). In human PBMCs, NM26-2198 inhibited IL-4–induced upregulation of CD23, demonstrating functional binding to FcγRII (CD32). NM26-2198 also inhibited the secretion of the AD biomarker thymus and activation-regulated chemokine (TARC) in blood samples from healthy human donors. In male cynomolgus monkeys, NM26-2198 exhibited favorable pharmacokinetics and significantly inhibited IL-31–induced scratching at a dose of 30 mg/kg. In a repeat-dose, good laboratory practice toxicology study in cynomolgus monkeys, no adverse effects of NM26-2198 were observed at a weekly dose of 125 mg/kg. Together, these results justify the clinical investigation of NM26-2198 as a treatment for moderate-to-severe AD.

一种靶向特应性皮炎炎症和致瘙痒途径的双特异性四价抗体
抑制IL-4/IL-13信号传导大大改善了特应性皮炎(AD)的治疗效果。然而,许多患者的临床反应发展缓慢,而且仍然不明显。事实上,特应性皮炎的某些症状依赖于IL-31,而抑制IL-4/IL-13只能部分减少IL-31的作用。因此,对同时阻断IL-4/IL-13和IL-31通路的AD治疗方法的需求尚未得到满足。我们设计了一种双特异性四价抗体 NM26-2198 来完成这一任务。在报告细胞系中,NM26-2198 可同时抑制 IL-4/IL-13 和 IL-31 信号传导,其效力可与抗 IL-4Rα 抗体(dupilumab)和抗 IL-31 抗体(BMS-981164)的组合相媲美。在人PBMCs中,NM26-2198抑制了IL-4诱导的CD23上调,显示了与FcγRII(CD32)的功能性结合。NM26-2198 还能抑制健康人捐献者血液样本中胸腺和活化调节趋化因子(TARC)的分泌。在雄性猕猴体内,NM26-2198 表现出良好的药代动力学,在剂量为 30 毫克/千克时可显著抑制 IL-31 诱导的搔抓。在对绒猴进行的重复剂量、良好实验室规范毒理学研究中,每周 125 毫克/千克剂量的 NM26-2198 未观察到不良反应。总之,这些结果证明了将 NM26-2198 作为中度至重度 AD 治疗药物进行临床研究是正确的。
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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CiteScore
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