SHR-1819(一种用于治疗2型炎症性疾病的强效人源化IL-4Rα抗体)的临床前开发
Preclinical Development of SHR-1819, a Potent Humanized IL-4Rα Antibody for Treating Type 2 Inflammatory Diseases.
作者信息
Zhao Guolin, Wang Zhijun, Zhang Jun, Lin Yuan, Zhou Tang, Liu Kaili, Yang Changyong, Liao Cheng
机构信息
Department of Preclinical Research and Development, Jiangsu Hengrui Pharmaceuticals Co., Ltd., Lianyungang, Jiangsu, People's Republic of China.
Department of Preclinical Research and Development, Shanghai Shengdi Pharmaceutical Co., Ltd., Shanghai, People's Republic of China.
出版信息
J Inflamm Res. 2024 Sep 14;17:6375-6388. doi: 10.2147/JIR.S471963. eCollection 2024.
BACKGROUND
Interleukin (IL)-4 and IL-13 are critical pathogenic factors for type 2 inflammation-related allergic diseases, sharing the mutual receptor subunit IL-4Rα. However, it was ineffective for certain type 2 inflammation diseases by targeting IL-4, IL-13 ligand alone or both in clinical studies. The work presented herein aimed to evaluate the preclinical efficacy and pharmacokinetics profile of a novel monoclonal antibody against IL-4Rα, SHR-1819, as a promising therapy for type 2 inflammation diseases.
METHODS
SHR-1819 was generated through immunization by C57BL/6 mice with recombinant hIL-4Rα protein, followed by humanization and affinity maturation. Then, its binding properties with IL-4Rα were determined using surface plasmon resonance (SPR) and ELISA. In vitro inhibitory effects of SHR-1819 were assessed on hIL-4-/hIL-13-induced cell proliferation and signal transducer and activator of transcription 6 (STAT6) signaling activation. In vivo efficacy of SHR-1819 was evaluated in several type 2 inflammatory diseases models, including asthma, atopic dermatitis (AD), and allergic rhinitis (AR) by using hIL-4/hIL-4Rα transgenic mice. Furthermore, the pharmacokinetic (PK) profiles of SHR-1819 were characterized.
RESULTS
SHR-1819 showed high binding affinity to human IL-4Rα and effectively blocked IL-4Rα at sub-nanomolar concentration. In vitro assays indicated that SHR-1819 significantly inhibited TF-1 cell proliferation and STAT6 activation induced by hIL-4/hIL-13. In the asthma model, SHR-1819 could reduce airway hyperresponsiveness, decrease serum IgE levels, and alleviated inflammatory lung cell infiltration. In the AD model, SHR-1819 could significantly alleviate inflammatory and skin symptoms. In the AR model, it could remarkably decrease the frequencies of nasal rubbing and sneezing, and inflammatory cell infiltration in nasal tissues. These in vivo efficacy studies demonstrated the therapeutic potential of SHR-1819 in preclinical disease models. Moreover, subcutaneous administration of SHR-1819 exhibited favorable bioavailability in mice.
CONCLUSION
The results supported SHR-1819 as a promising preclinical candidate for the treatment of type 2 inflammatory diseases, including asthma, AD and AR.
背景
白细胞介素(IL)-4和IL-13是2型炎症相关过敏性疾病的关键致病因素,共享共同的受体亚基IL-4Rα。然而,在临床研究中,单独靶向IL-4、IL-13配体或两者对某些2型炎症疾病无效。本文介绍的工作旨在评估一种新型抗IL-4Rα单克隆抗体SHR-1819作为2型炎症疾病的一种有前景的治疗方法的临床前疗效和药代动力学特征。
方法
通过用重组人IL-4Rα蛋白免疫C57BL/6小鼠,然后进行人源化和亲和力成熟来制备SHR-1819。然后,使用表面等离子体共振(SPR)和酶联免疫吸附测定(ELISA)确定其与IL-4Rα的结合特性。评估SHR-1819对人IL-4/人IL-13诱导的细胞增殖以及信号转导和转录激活因子6(STAT6)信号激活的体外抑制作用。通过使用人IL-4/人IL-4Rα转基因小鼠,在几种2型炎症疾病模型中评估SHR-1819的体内疗效,包括哮喘、特应性皮炎(AD)和过敏性鼻炎(AR)。此外,还对SHR-1819的药代动力学(PK)特征进行了表征。
结果
SHR-1819对人IL-4Rα显示出高结合亲和力,并在亚纳摩尔浓度下有效阻断IL-4Rα。体外试验表明,SHR-1819显著抑制人IL-4/人IL-13诱导的TF-1细胞增殖和STAT6激活。在哮喘模型中,SHR-1819可降低气道高反应性,降低血清IgE水平,并减轻肺部炎症细胞浸润。在AD模型中,SHR-1819可显著减轻炎症和皮肤症状。在AR模型中,它可显著降低鼻擦和打喷嚏的频率以及鼻组织中的炎症细胞浸润。这些体内疗效研究证明了SHR-1819在临床前疾病模型中的治疗潜力。此外,皮下注射SHR-1819在小鼠中表现出良好的生物利用度。
结论
结果支持SHR-1819作为治疗2型炎症疾病(包括哮喘、AD和AR)的一种有前景的临床前候选药物。
Zotero 插件