Fibrosis-related transcriptome unveils a distinctive remodeling matrix pattern in penetrating ileal Crohn's disease

Helena Tavares de Sousa, Marta Ferreira, Irene Gullo, Ana Mafalda Rocha, Ana Pedro, Dina Leitão, Carla Oliveira, Fátima Carneiro, Fernando Magro
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Abstract

Background and aims Stricturing (B2) and penetrating (B3) ileal Crohn’s disease have been reported to present similar levels of histopathological transmural fibrosis. This study aimed to compare the fibrosis-related transcriptomic profiles of penetrating and stricturing ileal Crohn’s disease. Methods Using Nanostring technology and comparative bioinformatics, we analyzed the expression of 787 fibrosis-related genes in 36 ileal surgical specimens, 12 B2 and 24 B3, the latter including 12 cases with associated stricture(s) (B3s) and 12 without (B3o). Quality control of extracted RNA was performed according to Nanostring parameters and principal component analysis for the distribution analysis. For the selection of the differentially expressed genes a p-adjusted <0.05 and Fold Change ≤-1.5 or ≥ 1.5 was adopted. qPCR and immunohistochemistry analyses were used to validate selected differentially expressed genes. Results We included 34 patients with B2 and B3 phenotypes, balanced for age at diagnosis, age at surgery, gender, Crohn’s disease localization, perianal disease and therapy. Inflammation and fibrosis histopathological scoring were similar in all cases. B2 and B3 groups showed a very good clustering regarding 30 significantly differentially expressed genes, all being remarkably upregulated in B3. More than half of these genes were involved in Crohn’s disease fibrogenesis, while eight differentially expressed genes were so in other organs. The most significantly active biologic processes and pathways in penetrating disease were response to TGFβand matrix organization and degradation, as validated by immunohistochemistry. Conclusions Despite the histopathological similarities in fibrosis between stricturing and penetrating ileal Crohn’s disease, their fibrosis-related transcriptomic profiles are distinct. Penetrating disease exhibits a distinctive transcriptomic landscape related to enhanced matrix remodeling.
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纤维化相关转录组揭示了穿透性回肠克罗恩病的独特重塑基质模式
背景和目的 据报道,狭窄性(B2)和穿透性(B3)回肠克罗恩病表现出相似程度的组织病理学跨壁纤维化。本研究旨在比较穿透型和严格型回肠克罗恩病纤维化相关的转录组学特征。方法 我们使用 Nanostring 技术和比较生物信息学分析了 36 例回肠手术标本中 787 个纤维化相关基因的表达,其中 12 例为 B2,24 例为 B3,后者包括 12 例伴有狭窄(B3s)的病例和 12 例没有狭窄(B3o)的病例。根据 Nanostring 参数对提取的 RNA 进行了质量控制,并对分布分析进行了主成分分析。在选择差异表达基因时,采用了 p 调整<0.05 和折叠变化≤-1.5 或≥1.5。结果 我们纳入了 34 例 B2 和 B3 表型的患者,他们的诊断年龄、手术年龄、性别、克罗恩病定位、肛周疾病和治疗方法均相同。所有病例的炎症和纤维化组织病理学评分相似。B2 和 B3 组中有 30 个基因的表达存在显著差异,B3 组中所有基因的表达都明显升高。其中半数以上的基因参与了克罗恩病的纤维化过程,而 8 个差异表达基因则参与了其他器官的纤维化过程。经免疫组化验证,穿透性疾病中最活跃的生物过程和途径是对 TGFβ 的反应以及基质的组织和降解。结论 尽管紧缩性和穿透性回肠克罗恩病的纤维化在组织病理学上有相似之处,但它们的纤维化相关转录组学特征却截然不同。穿透性疾病表现出与基质重塑增强相关的独特转录组图谱。
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