Immunotherapy-related colitis (irC) frequently emerges as an immune-related adverse event during immune checkpoint inhibitor therapy and is presumably influenced by the gut microbiota. We longitudinally studied microbiomes from 38 ICI-treated cancer patients. We compared 13 ICI-treated subjects who developed irC against 25 ICI-treated subjects who remained irC-free, along with a validation cohort. Leveraging a preclinical mouse model, predisease stools from irC subjects induced greater colitigenicity upon transfer to mice. The microbiota during the first 10 days of irC closely resembled inflammatory bowel disease microbiomes, with reduced diversity, increased Proteobacteria and Veillonella, and decreased Faecalibacterium, which normalized before irC remission. These findings highlight the irC gut microbiota as functionally distinct but phylogenetically similar to non-irC and healthy microbiomes, with the exception of an acute, transient disruption early in irC. We underscore the significance of longitudinal microbiome profiling in developing clinical avenues to detect, monitor, and mitigate irC in ICI therapy cancer patients.
Baseline colitogenicity and acute perturbations of gut microbiota in immunotherapy-related colitis.
免疫治疗相关性结肠炎中肠道菌群的基线致结肠炎性和急性扰动
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作者:Shang Joan, Del Valle Diane Marie, Britton Graham J, Mead K R, Rajpal Urvija, Chen-Liaw Alice, Mogno Ilaria, Li Zhihua, Menon Rajita, Gonzalez-Kozlova Edgar, Elkrief Arielle, Peled Jonathan U, Gonsalves Tina Ruth, Shah Neil J, Postow Michael, Colombel Jean-Frederic, Gnjatic Sacha, Faleck David M, Faith Jeremiah J
| 期刊: | Journal of Experimental Medicine | 影响因子: | 10.600 |
| 时间: | 2025 | 起止号: | 2025 Jan 6; 222(1):e20232079 |
| doi: | 10.1084/jem.20232079 | 研究方向: | 炎症/感染 |
| 疾病类型: | 肠炎 | ||
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