Long Yan, Lu Ke-Jia, Xia Chang-Sheng, Feng Jing-Hong, Li Wen-Yi, Ma Yin-Ting, Sun Yuan-Yuan, Fan Chun-Hong, Li Chun
Department of Clinical Laboratory, Peking University People's Hospital, Beijing, China.
Department of Biochemistry and Biophysics, School of Basic Medical Sciences, Beijing Key Laboratory of Protein Posttranslational Modifications and Cell Function, Peking University Health Science Center, Beijing, China.
Clin Exp Immunol. 2024 Apr 23;216(2):132-145. doi: 10.1093/cei/uxae016.
Natural killer (NK) cells were reported to be involved in the pathogenesis of primary antiphospholipid syndrome (pAPS). Immunosuppressive receptor T-cell immunoreceptor with Ig and ITIM domains (TIGIT) and activating receptor cluster of differentiation 226 (CD226) are specifically expressed on NK cells with competitive functions. This study aims to investigate the expression diversities of CD226/TIGIT on NK subsets and their associations with NK subsets activation phenotypes and potential clinical significance, furthermore, to explore potential cause for CD226/TIGIT expression diversities in pAPS. We comparatively assessed the changes of CD56brightNK, CD56dimNK, and NK-like cells in 70 pAPS patients compared with control groups, including systemic lupus erythematosus, asymptomatic antiphospholipid antibodies carriers (asymp-aPLs carriers), and healthy controls and their expression diversities of CD226/TIGIT by flow cytometry. CD25, CD69, CD107α expression, and interferon gamma (IFN-γ) secretion levels of NK subsets were detected to determine the potential association of CD226/TIGIT expression with NK subsets phenotypes. CD226/TIGIT expression levels were compared among different subgroups divided by aPLs status. Moreover, in vitro cultures were conducted to explore the potential mechanisms of CD226/TIGIT expression imbalance. CD56brightNK and CD3+CD56+NK-like cells were significantly increased while CD56dimNK cells were obviously decreased in pAPS, and CD56brightNK and NK-like cells exhibited significantly higher CD226 but lower TIGIT expressions. CD226+CD56brightNK and TIGIT-CD56brightNK cells show higher CD69 expression and IFN-γ secretion capacity, and CD226+NK-like and TIGIT-NK-like cells showed higher expressions of CD25 and CD69 but lower apoptosis rate than CD226- and TIGIT+CD56brightNK/NK-like cells, respectively. The imbalanced CD226/TIGIT expressions were most significant in aPLs triple-positive group. Imbalanced expressions of CD226/TIGIT on CD56brightNK and NK-like cells were aggravated after interleukin-4 (IL-4) stimulation and recovered after tofacitinib blocking. Our data revealed significant imbalanced CD226/TIGIT expressions on NK subsets in pAPS, which closely associated with NK subsets phenotypes and more complicated autoantibody status. CD226/TIGIT imbalanced may be affected by IL-4/Janus Kinase (JAK) pathway activation.
据报道,自然杀伤(NK)细胞参与了原发性抗磷脂综合征(pAPS)的发病机制。具有Ig和ITIM结构域的免疫抑制受体T细胞免疫受体(TIGIT)和激活受体分化簇226(CD226)在具有竞争功能的NK细胞上特异性表达。本研究旨在探讨CD226/TIGIT在NK亚群上的表达差异及其与NK亚群激活表型的关联和潜在临床意义,此外,还探讨pAPS中CD226/TIGIT表达差异的潜在原因。我们通过流式细胞术比较评估了70例pAPS患者与对照组(包括系统性红斑狼疮、无症状抗磷脂抗体携带者(无症状aPLs携带者)和健康对照)中CD56brightNK、CD56dimNK和NK样细胞的变化及其CD226/TIGIT的表达差异。检测NK亚群的CD25、CD69、CD107α表达及干扰素γ(IFN-γ)分泌水平,以确定CD226/TIGIT表达与NK亚群表型的潜在关联。比较不同aPLs状态分组的CD226/TIGIT表达水平。此外,进行体外培养以探讨CD226/TIGIT表达失衡的潜在机制。pAPS患者中CD56brightNK和CD3+CD56+NK样细胞显著增加,而CD56dimNK细胞明显减少,且CD56brightNK和NK样细胞表现出CD226表达显著更高但TIGIT表达更低。CD226+CD56brightNK和TIGIT-CD56brightNK细胞显示出更高的CD69表达和IFN-γ分泌能力,且CD226+NK样细胞和TIGIT-NK样细胞分别比CD226-和TIGIT+CD56brightNK/NK样细胞表现出更高的CD25和CD69表达但更低的凋亡率。CD226/TIGIT表达失衡在aPLs三阳性组中最为显著。CD56brightNK和NK样细胞上CD226/TIGIT的表达失衡在白细胞介素-4(IL-4)刺激后加剧,在托法替布阻断后恢复。我们的数据显示pAPS患者NK亚群上CD226/TIGIT表达存在显著失衡,这与NK亚群表型和更复杂的自身抗体状态密切相关。CD226/TIGIT失衡可能受IL-4/Janus激酶(JAK)途径激活的影响。
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