Clonal Hematopoiesis of Indeterminate Potential in Crohn′s Disease and Ulcerative Colitis

Myvizhi Esai Selvan, Daniel I Nathan, Daniela Guisado, Giulia Collatuzzo, Sushruta Iruvanti, Paolo Boffetta, John Mascarenhas, Ronald Hoffman, Louis J Cohen, Bridget K Marcellino, Zeynep H Gümüş
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Abstract

Background Clonal hematopoiesis of indeterminate potential (CHIP) is the presence of somatic mutations in myeloid and lymphoid malignancy genes in the blood cells of individuals without a hematologic malignancy. Inflammation is hypothesized to be a key mediator in the progression of CHIP to hematologic malignancy and patients with CHIP have a high prevalence of inflammatory diseases. This study aimed to identify the prevalence and characteristics of CHIP in patients with inflammatory bowel disease (IBD). Methods We analyzed whole exome sequencing data from 587 Crohn′s disease (CD), 441 ulcerative colitis (UC), and 293 non-IBD controls to assess CHIP prevalence and used logistic regression to study associations with clinical outcomes. Results Older UC patients (age>45) harbored increased myeloid-CHIP mutations compared to younger patients (age≤45) (p=0.01). Lymphoid-CHIP was more prevalent in older IBD patients (p=0.007). Young CD patients were found to have myeloid-CHIP with high-risk features. IBD patients with CHIP exhibited unique mutational profiles compared to controls. Steroid use was associated with increased CHIP (p=0.05), while anti-TNF therapy was associated with decreased myeloid-CHIP (p=0.03). Pathway enrichment analyses indicated overlap between CHIP genes, IBD phenotypes, and inflammatory pathways. Conclusions Our findings underscore a connection between IBD and CHIP pathophysiology. Patients with IBD and CHIP had unique risk profiles especially among older UC patients and younger CD patients. These findings suggest distinct evolutionary pathways for CHIP in IBD and necessitate awareness among IBD providers and hematologists to identify patients potentially at risk for CHIP-related complications including malignancy, cardiovascular disease and acceleration of their inflammatory disease.
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克罗恩病和溃疡性结肠炎中潜能不确定的克隆性造血
背景不确定潜能克隆性造血(CHIP)是指未患血液系统恶性肿瘤的人的血细胞中存在髓系和淋巴系恶性肿瘤基因的体细胞突变。据推测,炎症是CHIP发展为血液恶性肿瘤的关键介质,而CHIP患者的炎症性疾病发病率很高。本研究旨在确定CHIP在炎症性肠病(IBD)患者中的患病率和特征。方法我们分析了587名克罗恩病(CD)患者、441名溃疡性结肠炎(UC)患者和293名非IBD对照者的全外显子组测序数据,以评估CHIP的患病率,并使用逻辑回归法研究其与临床结果的关联。结果与年轻患者(年龄小于45岁)相比,年龄较大的UC患者(年龄>45岁)携带的骨髓-CHIP突变增多(p=0.01)。淋巴细胞-CHIP在年龄较大的IBD患者中更为普遍(P=0.007)。年轻的 CD 患者被发现患有具有高风险特征的骨髓-CHIP。与对照组相比,患有CHIP的IBD患者表现出独特的突变特征。使用类固醇与CHIP增加有关(p=0.05),而抗TNF治疗与骨髓-CHIP减少有关(p=0.03)。通路富集分析表明,CHIP 基因、IBD 表型和炎症通路之间存在重叠。结论我们的发现强调了 IBD 与 CHIP 病理生理学之间的联系。IBD 和 CHIP 患者具有独特的风险特征,尤其是老年 UC 患者和年轻的 CD 患者。这些研究结果表明,IBD 中的 CHIP 有不同的进化途径,因此 IBD 提供者和血液科医生有必要提高认识,以识别可能面临 CHIP 相关并发症(包括恶性肿瘤、心血管疾病和炎症性疾病加速)风险的患者。
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