Gogesch Patricia, Ortega Iannazzo Samira, Zimmermann Tamara, Villenave Remi, Sewald Katherina, Waibler Zoe
Paul-Ehrlich-Institut, Division of Immunology, Langen, Germany.
Innovation Center, Roche Pharma Research and Early Development, Basel, Switzerland.
J Immunotoxicol. 2024 Oct;21(sup1):S79-S88. doi: 10.1080/1547691X.2024.2369123. Epub 2024 Dec 10.
Immune-related adverse outcome pathways (irAOPs) are a toxicological tool for the structuring of complex immunological mechanisms. The EU-funded IMI-project imSAVAR analyses the applicability of irAOPs in pre-clinical safety assessment of immunotherapies. Here, we use immunotherapy with interleukin (IL)-2 as a use case to develop an irAOP for IL-2-mediated vascular leakage (VL). Despite severe side effects observed upon high-dose treatment, IL-2 remains a promising candidate for cancer- and autoimmune therapy. The secondary systemic capillary leakage syndrome is described by a high mortality and a lethality rate of 20 - 30%. However, due to its non-specific symptoms, it remains a serious but under-diagnosed pathology. VL as general phenomenon is associated with several pro-inflammatory scenarios or observed as severe side effect of immunotherapies. In such situations, the physiological condition, in which endothelial cells (ECs) form the semipermeable seal of the vasculature, can escalate into pathological vascular permeability and finally VL. Although EC-biology and mechanisms underlying VL are ongoing subjects of research since many years, exact understanding of VL pathophysiology remains unclear. With this review, we provide an overview of the development of VL from an immunological perspective in the context of high-dose IL-2 immunotherapy. We structured the corresponding knowledge and generated an irAOP for IL-2-mediated VL with the aim to identify gaps and possible biomarkers. Gained insights from this theoretical approach facilitate the identification of relevant scientific questions as a basis for concrete experimental work. Integration of novel experiment-based knowledge into the existing irAOP could close a 'feedback-loop' by enabling irAOP-refinement and the identification of new questions. At the same time this could give rise to important information to improve test systems for IL-2-based immunotherapy safety-assessment and overall the approach to understand, prevent, or predict VL as critical side effect of other clinical conditions.
免疫相关不良结局途径(irAOPs)是一种用于构建复杂免疫机制的毒理学工具。欧盟资助的IMI项目imSAVAR分析了irAOPs在免疫疗法临床前安全性评估中的适用性。在此,我们以白细胞介素(IL)-2免疫疗法为例,开发一种针对IL-2介导的血管渗漏(VL)的irAOP。尽管高剂量治疗时会观察到严重的副作用,但IL-2仍是癌症和自身免疫治疗的有前景的候选药物。继发性系统性毛细血管渗漏综合征的死亡率和致死率高达20%-30%。然而,由于其症状不具特异性,它仍然是一种严重但诊断不足的病理状况。VL作为一种普遍现象,与多种促炎情况相关,或被视为免疫疗法的严重副作用。在这种情况下,内皮细胞(ECs)形成血管系统半透性密封的生理状态可能会升级为病理性血管通透性,最终导致VL。尽管多年来EC生物学和VL的潜在机制一直是研究的主题,但对VL病理生理学的确切理解仍不清楚。通过本综述,我们从免疫角度概述了高剂量IL-2免疫疗法背景下VL的发展。我们梳理了相应知识,并生成了针对IL-2介导的VL的irAOP,旨在识别差距和可能的生物标志物。从这种理论方法中获得的见解有助于识别相关科学问题,作为具体实验工作的基础。将基于新实验的知识整合到现有的irAOP中,可以通过完善irAOP和识别新问题来形成一个“反馈回路”。同时,这可能会产生重要信息,以改进基于IL-2的免疫疗法安全性评估的测试系统,并总体上改进理解、预防或预测VL作为其他临床状况关键副作用的方法。
