Anti-apoptotic Genes and Non-coding RNAs Are Potential Outcome Predictors for Ulcerative Colitis

Overview

Journal Funct Integr Genomics

Publisher Springer

Specialties Genetics
Molecular Biology

Date 2023 May 18

PMID 37199828

Authors

Wei Meng

Kay-Martin Johnsen

Christopher G Fenton

Jon Florholmen

Ruth H Paulssen

Affiliations

Soon will be listed here.

Abstract

Due to the lack of clinical, immunologic, genetic, and laboratory markers to predict remission in ulcerative colitis (UC) without relapse, there is no clear recommendation regarding withdrawal of therapy. Therefore, this study was to investigate if transcriptional analysis together with Cox survival analysis might be able to reveal molecular markers that are specific for remission duration and outcome. Mucosal biopsies from patients in remission with active treatment-naïve UC and healthy control subjects underwent whole-transcriptome RNA-seq. Principal component analysis (PCA) and Cox proportional hazards regression analysis were applied to the remission data concerning duration and status of patients. A randomly chosen remission sample set was used for validation of the applied methods and results. The analyses distinguished two different UC remission patient groups with respect to remission duration and outcome (relapse). Both groups showed that altered states of UC with quiescent microscopic disease activity are still present. The patient group with the longest remission duration and no relapse revealed specific and increased expression of antiapoptotic factors belonging to the MTRNR2-like gene family and non-coding RNAs. In summary, the expression of anti-apoptotic factors and non-coding RNAs may contribute to personalized medicine approaches in UC by improving patient stratification for different treatment regimens.

Citing Articles

DNA methylation fine-tunes pro-and anti-inflammatory signalling pathways in inactive ulcerative colitis tissue biopsies.

Meng W, Fenton C, Johnsen K, Taman H, Florholmen J, Paulssen R Sci Rep. 2024; 14(1):6789.

PMID: 38514698 PMC: 10957912. DOI: 10.1038/s41598-024-57440-0.

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