Mozart Therapeutics, Seattle, WA, United States.
Front Immunol. 2024 Nov 4;15:1452537. doi: 10.3389/fimmu.2024.1452537. eCollection 2024.
Regulatory CD8 T cells (CD8 Treg) are responsible for the selective killing of self-reactive and pathogenic CD4 T cells. In autoimmune disease, CD8 Treg may accumulate in the peripheral blood but fail to control the expansion of pathogenic CD4 T cells that subsequently cause tissue destruction. This CD8 Treg dysfunction is due in part to the expression of inhibitory killer immunoglobulin-like receptors (KIR; KIR2DL isoforms [KIR2DL1, KIR2DL2, and KIR2DL3]); these molecules serve as autoimmune checkpoints and limit CD8 Treg activation.
Here we describe the pre-clinical characterization of MTX-101, a bispecific antibody targeting inhibitory KIR and CD8. Using human peripheral blood mononuculear cells (PBMC) derived from healthy donors and autoimmune patients, humanized mouse models, and human derived tissue organoids, we evaluated the molecular mechanisms and functional effects of MTX-101.
By binding to KIR, MTX-101 inhibited KIR signaling that can restore CD8 Treg ability to eliminate pathogenic CD4 T cells. MTX-101 bound and activated CD8 Treg in human peripheral blood mononuclear cells (PBMC), resulting in increased CD8 Treg cytolytic capacity, activation, and prevalence. Enhancing CD8 Treg function with MTX-101 reduced pathogenic CD4 T cell expansion and inflammation, without increasing pro-inflammatory cytokines or activating immune cells that express either target alone. MTX-101 reduced antigen induced epithelial cell death in disease affected tissues, including in tissue biopsies from individuals with autoimmune disease (i.e., celiac disease, Crohn's disease). The effects of MTX-101 were specific to autoreactive CD4 T cells and did not suppress responses to viral and bacterial antigens. In a human PBMC engrafted Graft versus Host Disease (GvHD) mouse model of acute inflammation, MTX-101 bound CD8 Treg and delayed onset of disease. MTX-101 induced dose dependent binding, increased prevalence and cytolytic capacity of CD8 Treg, as well as increased CD4 T cell death. MTX-101 selectively bound CD8 Treg without unwanted immune cell activation or increase of pro-inflammatory serum cytokines and exhibited an antibody-like half-life in pharmacokinetic and exploratory tolerability studies performed using IL-15 transgenic humanized mice with engrafted human lymphocytes, including CD8 Treg at physiologic ratios.
Collectively, these data support the development of MTX-101 for the treatment of autoimmune diseases.
调节性 CD8 T 细胞(CD8 Treg)负责选择性杀伤自身反应性和致病性 CD4 T 细胞。在自身免疫性疾病中,CD8 Treg 可能在外周血中积累,但未能控制随后导致组织破坏的致病性 CD4 T 细胞的扩增。这种 CD8 Treg 功能障碍部分归因于抑制性杀伤细胞免疫球蛋白样受体(KIR;KIR2DL 同工型 [KIR2DL1、KIR2DL2 和 KIR2DL3])的表达;这些分子充当自身免疫检查点并限制 CD8 Treg 的激活。
在这里,我们描述了针对抑制性 KIR 和 CD8 的双特异性抗体 MTX-101 的临床前特征。使用来自健康供体和自身免疫性疾病患者的人外周血单核细胞(PBMC)、人源化小鼠模型和人衍生的组织类器官,我们评估了 MTX-101 的分子机制和功能影响。
通过与 KIR 结合,MTX-101 抑制了 KIR 信号传导,从而恢复了 CD8 Treg 消除致病性 CD4 T 细胞的能力。MTX-101 结合并激活人外周血单核细胞(PBMC)中的 CD8 Treg,导致 CD8 Treg 的细胞毒性、激活和流行度增加。用 MTX-101 增强 CD8 Treg 功能可减少致病性 CD4 T 细胞的扩增和炎症,而不会增加表达任一靶标的促炎细胞因子或激活免疫细胞。MTX-101 减少了疾病影响组织中抗原诱导的上皮细胞死亡,包括来自自身免疫性疾病(例如乳糜泻、克罗恩病)个体的组织活检。MTX-101 的作用特异性针对自身反应性 CD4 T 细胞,并且不抑制对病毒和细菌抗原的反应。在急性炎症的人 PBMC 移植移植物抗宿主病(GvHD)小鼠模型中,MTX-101 结合 CD8 Treg 并延迟疾病发作。MTX-101 诱导剂量依赖性结合,增加 CD8 Treg 的流行度和细胞毒性,并增加 CD4 T 细胞死亡。MTX-101 选择性地结合 CD8 Treg,而不会引起不必要的免疫细胞激活或增加促炎血清细胞因子,并在使用 IL-15 转基因人源化小鼠进行的药代动力学和探索性耐受性研究中表现出抗体样半衰期,其中包括生理比例的嵌合人淋巴细胞,包括 CD8 Treg。
综上所述,这些数据支持 MTX-101 用于治疗自身免疫性疾病。
