Common functional alterations identified in blood transcriptome of autoimmune cholestatic liver and inflammatory bowel diseases

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作者
Jerzy Ostrowski
Krzysztof Goryca
Izabella Lazowska
Agnieszka Rogowska
Agnieszka Paziewska
Michalina Dabrowska
Filip Ambrozkiewicz
Jakub Karczmarski
Aneta Balabas
Anna Kluska
Magdalena Piatkowska
Natalia Zeber-Lubecka
Maria Kulecka
Andrzej Habior
Michal Mikula
机构
[1] Maria Sklodowska-Curie Institute – Oncology Centre,Department of Genetics
[2] Medical Center for Postgraduate Education,Department of Gastroenterology and Hepatology
[3] Medical University of Warsaw,Department of Pediatric Gastroenterology and Nutrition
[4] Faculty of Health Sciences,Department of Public Health
[5] Medical University of Warsaw,Department of General, Transplant and Liver Surgery
[6] Medical University of Warsaw,Department of Gastroenterology
[7] Medical University,Department of General
[8] Liver and Internal Medicine Unit,Department of Clinical and Molecular Biochemistry
[9] Transplant and Liver Surgery,Department of Immunology
[10] Medical University of Warsaw,Department of Gastroenterology and Hepatology
[11] Pomeranian Medical University,Department of Gastroenterology and Infectious Diseases
[12] Transplantology and Internal Medicine,Department of Gastroenterology
[13] Medical University of Warsaw,Department of Gastroenterology and Hepatology
[14] Institute of Biochemistry and Biophysics,Department of Internal and Metabolic Diseases and Dietetics
[15] Polish Academy of Sciences,Department of Gastroenterology
[16] Medical University of Silesia,Department of Gastroenterology
[17] Collegium Medicum Jagiellonian University,Department of Internal Medicine and Gastroenterology with IBD Subdivision
[18] Provincial Hospital,Department of Pediatrics
[19] Medical University of Gdansk,Department of Pediatrics
[20] Poznan University of Medical Sciences,Department of Pediatric Gastroenterology &Metabolic Diseases
[21] Provincial Hospital,Department of Gastroenterology
[22] Hepatology and Feeding Disorders,Department of Pediatrics
[23] Children’s Memorial Health Institute,Medical College
[24] Central Clinical Hospital of the Ministry of the Interior,Department of Gastroenterology
[25] Vascular Diseases and Internal Medicine,undefined
[26] Nicolaus Copernicus University in Torun,undefined
[27] Collegium Medicum,undefined
[28] Gastroenterology and Nutrition,undefined
[29] Wroclaw Medical University,undefined
[30] School of Medicine with the Division of Dentistry in Zabrze,undefined
[31] Medical University of Silesia,undefined
[32] Poznan University of Medical Sciences,undefined
[33] Medical University of Lublin,undefined
[34] School of Medicine in Katowice,undefined
[35] Medical University of Silesia,undefined
[36] University of Rzeszow,undefined
[37] Pomeranian Medical University,undefined
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摘要
Primary biliary cholangitis (PBC), primary sclerosing cholangitis (PSC), and inflammatory bowel diseases (IBDs), including Crohn’s disease (CD) and ulcerative colitis (UC), are heterogeneous chronic autoimmune diseases that may share underlying pathogenic mechanisms. Herein, we compared simultaneously analyzed blood transcriptomes from patients with PBC, PSC, and IBD. Microarray-based measurements were conducted using RNA isolated from whole blood samples from 90, 45, 95 and 93 patients with PBC, PSC, CD, and UC, respectively, and 47 healthy controls. Expression levels of selected transcripts were analyzed by quantitative reverse-transcribed PCR using an independent cohort of 292, 71 and 727 patients with PBC, PSC, and IBD, respectively. Of 4026, 2650 and 4967 probe sets differentially expressed (adjusted p-value < 0.05) in samples from patients with PBC, PSC, and IBD, respectively, compared with healthy controls, 1946 were common to all three comparisons. Functional analyses indicated that most terms enriched for genes differentially expressed in PBC, PSC, and IBD patients compared with healthy controls were related to mitochondrial function, the vesicle endomembrane system, and GTPase-mediated processes. This study indicates that microarray-based profiling of blood gene expression supports research into the molecular mechanisms underlying disease, rather than being useful for selection of diagnostic biomarkers for use in clinical practice.
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