Activation of Janus kinase 2 contributes to the autoimmune pathology in the salivary glands of patients with Sjögren's syndrome

IF 0.6 Q4 DENTISTRY, ORAL SURGERY & MEDICINE Oral Science International Pub Date : 2024-04-18 DOI:10.1002/osi2.1241
K. Aota, Koichi Kani, Shinji Ono, Kohei Naniwa, Y. Momota, Makoto Fukui, Naozumi Ishimaru, Masayuki Azuma
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Abstract

Primary Sjögren's syndrome (pSS) is a chronic autoimmune disease that affects exocrine glands. CXCL10 production from salivary gland ductal cells via the Janus kinase (JAK)/signal transducer and activator of transcription (STAT) pathway has been suggested to be involved in glandular inflammation in pSS. We aimed to investigate JAK1, JAK2, phosphorylated JAK1, and phosphorylated JAK2 expression in labial salivary gland (LSG) tissues from patients with pSS to evaluate the potential of JAK inhibitors as therapeutic agents for pSS.Immunohistochemical analysis was performed using LSG tissues of patients with pSS (n = 10), non‐SS patients (n = 5), and healthy controls (n = 5). The LSG sections were scored to determine the expression levels of JAK1, JAK2, phosphorylated JAK1, and phosphorylated JAK2 in the ductal and acinar epithelium.In acinar epithelial cells of LSG tissues, JAK1, JAK2, and phosphorylated JAK1 expression was significantly lower in patients with pSS than in the controls. Significantly high expression of phosphorylated JAK1 and phosphorylated JAK2 was observed in the ductal epithelial cells of patients with pSS. However, there was no significant association between phosphorylated JAK1 or JAK2 expression levels and inflammation degree. Furthermore, immunofluorescence analysis revealed JAK2 phosphorylation in many CD3+ T cells infiltrating the LSG tissues.The results suggest JAK2 activation in both ductal epithelial cells and infiltrating CD3+ T cells in LSG tissues of patients with pSS. JAK inhibitors may be effective therapeutic agents for pSS by regulating both chemokine production from salivary gland cells and effector T cell activation.
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Janus 激酶 2 的活化导致了斯约格伦综合征患者唾液腺的自身免疫性病变
原发性斯约格伦综合征(pSS)是一种影响外分泌腺的慢性自身免疫性疾病。唾液腺导管细胞通过Janus激酶(JAK)/信号转导和激活转录(STAT)途径产生的CXCL10被认为参与了pSS的腺体炎症。我们的研究目的是调查pSS患者唇唾液腺(LSG)组织中JAK1、JAK2、磷酸化JAK1和磷酸化JAK2的表达情况,以评估JAK抑制剂作为pSS治疗药物的潜力。对LSG切片进行评分,以确定JAK1、JAK2、磷酸化JAK1和磷酸化JAK2在导管和尖状上皮细胞中的表达水平。在LSG组织的尖状上皮细胞中,PSS患者的JAK1、JAK2和磷酸化JAK1表达明显低于对照组。在 pSS 患者的导管上皮细胞中,磷酸化 JAK1 和磷酸化 JAK2 的表达明显较高。然而,磷酸化 JAK1 或 JAK2 的表达水平与炎症程度无明显关联。此外,免疫荧光分析显示,浸润LSG组织的许多CD3+ T细胞中都存在JAK2磷酸化。通过调节唾液腺细胞趋化因子的产生和效应T细胞的活化,JAK抑制剂可能是治疗pSS的有效药物。
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来源期刊
Oral Science International
Oral Science International DENTISTRY, ORAL SURGERY & MEDICINE-
CiteScore
1.00
自引率
20.00%
发文量
43
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