Gene expression profile of endoscopically active and inactive ulcerative colitis: preliminary data

Gene expression profile of endoscopically active and inactive ulcerative colitis: preliminary data

Multiple cytokines and chemokines related to immune response, apoptosis and inflammation have been identified as molecules implicated in ulcerative colitis (UC) pathogenesis. The aim of this study was to identify the differences at gene expression level of a panel of candidate genes in mucosa from p...

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Bibliographic Details
Published in:Romanian journal of morphology and embryology Vol. 58; no. 4; pp. 1301 - 1307
Main Authors: Ţieranu, Cristian George, Dobre, Maria, Mănuc, Teodora Ecaterina, Milanesi, Elena, Pleşea, Iancu Emil, Popa, Caterina, Mănuc, Mircea, Ţieranu, Ioana, Preda, Carmen Monica, Diculescu, Mihai Mircea, Ionescu, Elena Mirela, Becheanu, Gabriel
Format: Journal Article
Language:English
Published: Romania 2017
Subjects:
Adult
Colitis, Ulcerative - diagnostic imaging
Colitis, Ulcerative - pathology
Endoscopy - legislation & jurisprudence
Endoscopy - methods
Female
Humans
Male
Transcriptome - genetics
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Summary:Multiple cytokines and chemokines related to immune response, apoptosis and inflammation have been identified as molecules implicated in ulcerative colitis (UC) pathogenesis. The aim of this study was to identify the differences at gene expression level of a panel of candidate genes in mucosa from patients with active UC (UCA), patients in remission (UCR), and normal controls. Eleven individuals were enrolled in the study: eight UC patients (four with active lesions, four with mucosal healing) and three controls without inflammatory bowel disease (IBD) seen on endoscopy. All the individuals underwent mucosal biopsy during colonoscopy. Gene expression profile was evaluated by polymerase chain reaction (PCR) array, investigating 84 genes implicated in apoptosis, inflammation, immune response, cellular adhesion, tissue remodeling and mucous secretion. Seventeen and three genes out of 84 were found significantly differentially expressed in UCA and UCR compared to controls, respectively. In particular, REG1A and CHI3L1 genes reported an up-regulation in UCA with a fold difference above 200. In UCR patients, the levels of CASP1, LYZ and ISG15 were different compared to controls. However, since a significant up-regulation of both CASP1 and LYZ was observed also in the UCA group, only ISG15 levels remained associated to the remission state. ISG15, that plays a key role in the innate immune response, seemed to be specifically associated to the UC remission state. These preliminary data represent a starting point for defining the gene profile of UC in different stages in Romanian population. Identification of genes implicated in UC pathogenesis could be useful to select new therapeutic targets.
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ISSN:1220-0522