IL-24 在 NK 细胞活化中的作用及其在系统性红斑狼疮中的临床意义。
Role of IL-24 in NK cell activation and its clinical implication in systemic lupus erythematosus.
机构信息
Department of Rheumatology and Immunology, Peking University People's Hospital, 11 South Xizhimen Street, Beijing, 100044, China.
Department of Immunology, College of Basic Medical Science, Dalian Medical University, 465 Zhongshan Road, Liaoning, 116044, China.
出版信息
Clin Rheumatol. 2021 Jul;40(7):2707-2715. doi: 10.1007/s10067-021-05618-6. Epub 2021 Feb 3.
OBJECTIVES
Interleukin (IL)-24 has been considered as an inflammatory cytokine in autoimmune diseases. However, conflicting data exist and its biological function remains controversial. Additionally, little is known about its functional impact on natural killer (NK) cells. The aim of this study was to investigate the role of IL-24 in NK cell activation and its clinical implication in systemic lupus erythematosus (SLE).
METHODS
Serum cohort consisting of 299 SLE patients, 214 RA patients, and 159 healthy controls (HCs) and plasma cohort consisting of 70 SLE patients, 82 RA patients, and 123 HCs were included in evaluating IL-24 concentrations. Impact of IL-24 on NK cell activation was assessed in two NK cell subsets, i.e., CD56CD16 and CD56CD16 NK cells. Human NK-92 cell line was applied to evaluate functional potential of IL-24 on NK cell migration and invasion.
RESULTS
Serum and plasma levels of IL-24 were comparable between patients with SLE or RA and HCs. While recombinant human (rh) IL-2 consistently induced an increased expression of CD69 on both CD56CD16 and CD56CD16 cells derived from both healthy subjects and patients with SLE, IL-24 alone was insufficient to activate the CD56 and CD56 NK cells. Similarly, while the migratory NK-92 cell numbers were significantly increased with rhIL-2 stimulation, IL-24 alone was unable to enhance NK-92 cell migratory and invasive capacity.
CONCLUSION
Our data indicate that there were no significant differences in serum and plasma concentrations of IL-24 between SLE patients and healthy controls. Recombinant IL-24 has no effect on NK cell activation and migration. Key points • This is the first study to investigate functional potential of IL-24 on NK cell activation. • Recombinant IL-24 lacks functional capacity on NK cell activation in either CD56CD16 or CD56CD16 NK cell subsets derived from both healthy subjects and patients with SLE. • No significant differences in serum and plasma levels of IL-24 between SLE patients and healthy controls.
目的
白细胞介素 (IL)-24 被认为是自身免疫性疾病中的炎症细胞因子。然而,目前存在相互矛盾的数据,其生物学功能仍存在争议。此外,人们对其对自然杀伤 (NK) 细胞的功能影响知之甚少。本研究旨在探讨 IL-24 在 NK 细胞激活中的作用及其在系统性红斑狼疮 (SLE) 中的临床意义。
方法
纳入了血清队列(包含 299 例 SLE 患者、214 例 RA 患者和 159 例健康对照者)和血浆队列(包含 70 例 SLE 患者、82 例 RA 患者和 123 例健康对照者)来评估 IL-24 浓度。通过两个 NK 细胞亚群(即 CD56CD16 和 CD56CD16 NK 细胞)评估 IL-24 对 NK 细胞激活的影响。应用人 NK-92 细胞系评估 IL-24 对 NK 细胞迁移和侵袭的功能潜力。
结果
SLE 或 RA 患者与健康对照者的血清和血浆 IL-24 水平相当。虽然重组人 (rh) IL-2 始终能诱导来自健康受试者和 SLE 患者的 CD56CD16 和 CD56CD16 NK 细胞上 CD69 的表达增加,但 IL-24 本身不足以激活 CD56 和 CD56 NK 细胞。同样,虽然 rhIL-2 刺激可显著增加迁移的 NK-92 细胞数量,但 IL-24 本身不能增强 NK-92 细胞的迁移和侵袭能力。
结论
我们的数据表明,SLE 患者与健康对照者的血清和血浆 IL-24 浓度无显著差异。重组 IL-24 对 NK 细胞激活和迁移没有影响。关键点:
这是第一项研究 IL-24 对 NK 细胞激活的功能潜力的研究。
重组 IL-24 缺乏在源自健康受试者和 SLE 患者的 CD56CD16 或 CD56CD16 NK 细胞亚群中激活 NK 细胞的功能能力。
SLE 患者与健康对照者的血清和血浆 IL-24 水平无显著差异。
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