格雷夫斯病中与 T 细胞耗竭相关的基因:一项全面的基因组图谱分析。
T-cell exhaustion-related genes in Graves' disease: a comprehensive genome mapping analysis.
机构信息
Department of Endocrinology, Second Affiliated Hospital of Fujian Medical University, Quanzhou, Fujian, China.
Department of Internal Medicine, Gutian County Hospital of Ningde City, Ningde, Fujian, China.
出版信息
Front Endocrinol (Lausanne). 2024 Aug 22;15:1364782. doi: 10.3389/fendo.2024.1364782. eCollection 2024.
BACKGROUND
T-cell exhaustion (Tex) can be beneficial in autoimmune diseases, but its role in Graves' disease (GD), an autoimmune disorder of the thyroid, remains unknown. This study investigated Tex-related gene expression in GD patients to discern the potential contributions of these genes to GD pathogenesis and immune regulation.
METHODS
Through gene landscape analysis, a protein-protein interaction network of 40 Tex-related genes was constructed. mRNA expression levels were compared between GD patients and healthy control (HCs). Unsupervised clustering categorized GD cases into subtypes, revealing distinctions in gene expression, immune cell infiltration, and immune responses. Weighted gene co-expression network analysis and differential gene expression profiling identified potential therapeutic targets. RT-qPCR validation of candidate gene expression was performed using blood samples from 112 GD patients. Correlations between Tex-related gene expression and clinical indicators were analyzed.
RESULTS
Extensive Tex-related gene interactions were observed, with six genes displaying aberrant expression in GD patients. This was associated with atypical immune cell infiltration and regulation. Cluster analysis delineated two GD subtypes, revealing notable variations in gene expression and immune responses. Screening efforts identified diverse drug candidates for GD treatment. The Tex-related gene was identified for further validation and showed reduced mRNA expression in GD patients, especially in cases of relapse. mRNA expression was significantly lower in patients with moderate-to-severe thyroid enlargement than in those without such enlargement. Additionally, mRNA expression was negatively correlated with the disease-specific indicator thyrotropin receptor antibodies.
CONCLUSION
Tex-related genes modulate GD pathogenesis, and their grouping aids subtype differentiation and exploration of therapeutic targets. represents a potential marker for GD recurrence.
背景
T 细胞耗竭(Tex)在自身免疫性疾病中可能有益,但它在 Graves 病(GD)中的作用,一种甲状腺自身免疫性疾病,尚不清楚。本研究通过检测 GD 患者 Tex 相关基因的表达,探讨这些基因在 GD 发病机制和免疫调节中的潜在作用。
方法
通过基因图谱分析,构建了 40 个 Tex 相关基因的蛋白质-蛋白质相互作用网络。比较 GD 患者和健康对照(HC)之间的 mRNA 表达水平。无监督聚类将 GD 病例分为亚类,揭示了基因表达、免疫细胞浸润和免疫反应的差异。加权基因共表达网络分析和差异基因表达谱分析确定了潜在的治疗靶点。使用 112 例 GD 患者的血液样本进行候选基因表达的 RT-qPCR 验证。分析 Tex 相关基因表达与临床指标的相关性。
结果
观察到广泛的 Tex 相关基因相互作用,其中 6 个基因在 GD 患者中表达异常。这与非典型免疫细胞浸润和调节有关。聚类分析描绘了两种 GD 亚型,揭示了基因表达和免疫反应的显著差异。筛选工作确定了用于 GD 治疗的多种药物候选物。Tex 相关基因 进一步验证,发现 GD 患者的 mRNA 表达降低,尤其是在复发患者中。mRNA 表达在甲状腺肿大程度为中重度的患者中明显低于无甲状腺肿大的患者。此外,mRNA 表达与疾病特异性指标促甲状腺素受体抗体呈负相关。
结论
Tex 相关基因调节 GD 的发病机制,其分组有助于亚类分化和治疗靶点的探索。 代表 GD 复发的潜在标志物。
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