Skin Research Laboratory, Faculty of Medicine, Technion - Israel Institute of Technology, Haifa, Israel.
Faculty of Medicine, The Hebrew University of Jerusalem, Jerusalem, Israel.
Immunology. 2019 Nov;158(3):171-193. doi: 10.1111/imm.13109.
Activated T cells are pathological in various autoimmune and inflammatory diseases including Psoriasis, and also in graft rejection and graft-versus-host-disease. In these pathological conditions, selective silencing of activated T cells through physiological receptors they express remains a clinical challenge. In our previous studies we found that activation of dopamine receptors (DRs) in resting human T cells activates these cells, and induces by itself many beneficial T cell functions. In this study, we found that normal human T cells express all types of DRs, and that expression of D1R, D4R and D5R increases profoundly after T cell receptor (TCR) activation. Interestingly, DR agonists shift the membrane potential (V ) of both resting and activated human T cells, and induces instantaneous T cell depolarization within 15 seconds only. Thus, activation of DRs in T cells depolarize these immune cells, alike activation of DRs in neural cells. The skin of Psoriasis patients contains 20-fold more D1R T cells than healthy human skin. In line with that, 25-fold more D1R T cells are present in Psoriasis humanized mouse model. Highly selective D1-like receptor agonists, primarily Fenoldopam (Corlopam) - a D1-like receptor agonist and a drug used in hypertension, induced the following suppressive effects on activated T cells of Psoriasis patients: reduced chemotactic migration towards the chemokine SDF-1/CXCL12; reduced dramatically the secretion of eight cytokines: tumor necrosis factor-α, interferon-γ, interleukin-1β (IL-1β), IL-2, IL-4, IL-6, IL-8 and IL-10; and reduced three T cell activation proteins/markers: CD69, CD28 and IL-2. Next, we invented a novel topical/dermal Fenoldopam formulation, allowing it to be spread on, and providing prolonged and regulated release in, diseased skin. Our novel topical/dermal Fenoldopam: reduced secretion of the eight cytokines by activated human T cells; reduced IL-1β and IL-6 secretion by human lipopolysaccharide-inflamed skin; eliminated preferentially >90% of live and large/proliferating human T cells. Together, our findings show for the first time that both resting and activated T cells are depolarized instantaneously via DRs, and that targeting D1-like receptors in activated T cells and inflamed human skin by Fenoldopam, in Psoriasis, and potentially in other T cell-mediated diseases, could be therapeutic. Validation in vivo is required.
活化的 T 细胞在各种自身免疫和炎症性疾病中是病理性的,包括银屑病,也存在于移植物排斥和移植物抗宿主病中。在这些病理条件下,通过它们表达的生理受体选择性地沉默活化的 T 细胞仍然是一个临床挑战。在我们之前的研究中,我们发现,在静息的人 T 细胞中激活多巴胺受体 (DRs) 会激活这些细胞,并自行诱导许多有益的 T 细胞功能。在这项研究中,我们发现正常的人 T 细胞表达所有类型的 DRs,并且在 T 细胞受体 (TCR) 激活后,D1R、D4R 和 D5R 的表达显著增加。有趣的是,DR 激动剂会使静息和活化的人 T 细胞的膜电位 (V) 发生偏移,并且仅在 15 秒内诱导瞬时 T 细胞去极化。因此,T 细胞中 DR 的激活使这些免疫细胞去极化,就像在神经细胞中激活 DR 一样。银屑病患者的皮肤中含有比健康人皮肤多 20 倍的 D1R T 细胞。与此一致的是,在银屑病人源化小鼠模型中,D1R T 细胞的数量增加了 25 倍。高度选择性的 D1 样受体激动剂,主要是 Fenoldopam (Corlopam) - D1 样受体激动剂和一种用于高血压的药物,对银屑病患者的活化 T 细胞产生了以下抑制作用:减少对趋化因子 SDF-1/CXCL12 的趋化性迁移;显著减少八种细胞因子的分泌:肿瘤坏死因子-α、干扰素-γ、白细胞介素-1β (IL-1β)、白细胞介素-2 (IL-2)、白细胞介素-4 (IL-4)、白细胞介素-6 (IL-6)、白细胞介素-8 (IL-8) 和白细胞介素-10 (IL-10);减少三种 T 细胞激活蛋白/标志物:CD69、CD28 和 IL-2。接下来,我们发明了一种新型的局部/皮肤 Fenoldopam 制剂,使其能够在患病皮肤上扩散,并提供延长和调节释放。我们的新型局部/皮肤 Fenoldopam:减少活化的人 T 细胞分泌的八种细胞因子;减少人脂多糖诱导的皮肤中 IL-1β 和 IL-6 的分泌;优先消除 >90%的活的和大/增殖的人 T 细胞。总的来说,我们的研究结果首次表明,静息和活化的 T 细胞都可以通过 DR 立即去极化,并且在银屑病中以及在其他 T 细胞介导的疾病中,通过 Fenoldopam 靶向活化的 T 细胞和炎症性人皮肤中的 D1 样受体,可能具有治疗作用。需要进行体内验证。
