A cross-sectional study reveals a chronic low-grade inflammation in achalasia

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  • 作者:Li-Yun Ma, Zu-Qiang Liu, Wei-Feng Chen, Lu Yao, Yun-Shi Zhong, Yi-Qun Zhang, Li-Li Ma, Wen-Zhen Qin, Jian-Wei Hu, Ming-Yan Cai, Zhen Zhang, Sheng-Li Lin, Hao Hu, Ping-Hong Zhou, Quan-Lin Li
  • 期刊:JOURNAL OF GASTROENTEROLOGY AND HEPATOLOGY
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Background and aim:Immune-mediated neuroinflammation has been proposed to underlie the loss of lower esophageal sphincter (LES) myenteric neurons in achalasia. However, the immune status and key pathogenic immune subpopulations remain unclear. This study aims to evaluate the inflammatory status of patients with achalasia and their correlation with clinical characteristics, and further explore the key pathogenic subpopulations.

Methods:We investigated the complete blood cell count and inflammatory markers in a large population of patients with achalasia (n = 341) and healthy controls (n = 80). The subpopulations of lymphocytes were analyzed by flow cytometry. Immunofluorescence was used to determine immune cell infiltration in the LES. Transcriptome changes of the key subpopulation were determined by RNA sequencing analysis.

Results:NLR, MLR, CRP, globulin, IL-6 and IL-10 were significantly elevated in patients with achalasia. MLR and globulin were positively correlated with disease duration. The absolute count and percentage of CD8+ T cells in peripheral blood and its infiltration around ganglion in the LES were significantly increased in achalasia. Transcriptome analysis indicated that CD8+ T cells were activated and proliferative. In addition to multiple inflammatory pathways, regulation of neuroinflammatory response pathway was also significantly up-regulated in achalasia. GSEA analysis revealed a close association with autoimmune diseases.

Conclusions:Patients with achalasia suffered from chronic low-grade inflammation with dysregulated immune cells and mediators associated with disease duration. CD8+ T cells might be the key pathogenic subpopulation of achalasia. Our results provide an important immune cell signature of the pathogenesis of achalasia.

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