Integrated GWAS and mRNA Microarray Analysis Identified IFNG and CD40L as the Central Upstream Regulators in Primary Biliary Cholangitis

Genome‐wide association studies (GWASs) in European and East Asian populations have identified more than 40 disease‐susceptibility genes in primary biliary cholangitis (PBC). The aim of this study is to computationally identify disease pathways, upstream regulators, and therapeutic targets in PBC th...

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Autores principales: Ueno, Kazuko, Aiba, Yoshihiro, Hitomi, Yuki, Shimoda, Shinji, Nakamura, Hitomi, Gervais, Olivier, Kawai, Yosuke, Kawashima, Minae, Nishida, Nao, Kohn, Seik‐Soon, Kojima, Kaname, Katsushima, Shinji, Naganuma, Atsushi, Sugi, Kazuhiro, Komatsu, Tatsuji, Mannami, Tomohiko, Matsushita, Kouki, Yoshizawa, Kaname, Makita, Fujio, Nikami, Toshiki, Nishimura, Hideo, Kouno, Hiroshi, Kouno, Hirotaka, Ohta, Hajime, Komura, Takuya, Tsuruta, Satoru, Yamauchi, Kazuhiko, Kobata, Tatsuro, Kitasato, Amane, Kuroki, Tamotsu, Abiru, Seigo, Nagaoka, Shinya, Komori, Atsumasa, Yatsuhashi, Hiroshi, Migita, Kiyoshi, Ohira, Hiromasa, Tanaka, Atsushi, Takikawa, Hajime, Nagasaki, Masao, Tokunaga, Katsushi, Nakamura, Minoru
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2020
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7193132/
https://www.ncbi.nlm.nih.gov/pubmed/32363322
http://dx.doi.org/10.1002/hep4.1497
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author Ueno, Kazuko
Aiba, Yoshihiro
Hitomi, Yuki
Shimoda, Shinji
Nakamura, Hitomi
Gervais, Olivier
Kawai, Yosuke
Kawashima, Minae
Nishida, Nao
Kohn, Seik‐Soon
Kojima, Kaname
Katsushima, Shinji
Naganuma, Atsushi
Sugi, Kazuhiro
Komatsu, Tatsuji
Mannami, Tomohiko
Matsushita, Kouki
Yoshizawa, Kaname
Makita, Fujio
Nikami, Toshiki
Nishimura, Hideo
Kouno, Hiroshi
Kouno, Hirotaka
Ohta, Hajime
Komura, Takuya
Tsuruta, Satoru
Yamauchi, Kazuhiko
Kobata, Tatsuro
Kitasato, Amane
Kuroki, Tamotsu
Abiru, Seigo
Nagaoka, Shinya
Komori, Atsumasa
Yatsuhashi, Hiroshi
Migita, Kiyoshi
Ohira, Hiromasa
Tanaka, Atsushi
Takikawa, Hajime
Nagasaki, Masao
Tokunaga, Katsushi
Nakamura, Minoru
author_facet Ueno, Kazuko
Aiba, Yoshihiro
Hitomi, Yuki
Shimoda, Shinji
Nakamura, Hitomi
Gervais, Olivier
Kawai, Yosuke
Kawashima, Minae
Nishida, Nao
Kohn, Seik‐Soon
Kojima, Kaname
Katsushima, Shinji
Naganuma, Atsushi
Sugi, Kazuhiro
Komatsu, Tatsuji
Mannami, Tomohiko
Matsushita, Kouki
Yoshizawa, Kaname
Makita, Fujio
Nikami, Toshiki
Nishimura, Hideo
Kouno, Hiroshi
Kouno, Hirotaka
Ohta, Hajime
Komura, Takuya
Tsuruta, Satoru
Yamauchi, Kazuhiko
Kobata, Tatsuro
Kitasato, Amane
Kuroki, Tamotsu
Abiru, Seigo
Nagaoka, Shinya
Komori, Atsumasa
Yatsuhashi, Hiroshi
Migita, Kiyoshi
Ohira, Hiromasa
Tanaka, Atsushi
Takikawa, Hajime
Nagasaki, Masao
Tokunaga, Katsushi
Nakamura, Minoru
author_sort Ueno, Kazuko
collection PubMed
description Genome‐wide association studies (GWASs) in European and East Asian populations have identified more than 40 disease‐susceptibility genes in primary biliary cholangitis (PBC). The aim of this study is to computationally identify disease pathways, upstream regulators, and therapeutic targets in PBC through integrated GWAS and messenger RNA (mRNA) microarray analysis. Disease pathways and upstream regulators were analyzed with ingenuity pathway analysis in data set 1 for GWASs (1,920 patients with PBC and 1,770 controls), which included 261 annotated genes derived from 6,760 single‐nucleotide polymorphisms (P < 0.00001), and data set 2 for mRNA microarray analysis of liver biopsy specimens (36 patients with PBC and 5 normal controls), which included 1,574 genes with fold change >2 versus controls (P < 0.05). Hierarchical cluster analysis and categorization of cell type–specific genes were performed for data set 2. There were 27 genes, 10 pathways, and 149 upstream regulators that overlapped between data sets 1 and 2. All 10 pathways were immune‐related. The most significant common upstream regulators associated with PBC disease susceptibility identified were interferon‐gamma (IFNG) and CD40 ligand (CD40L). Hierarchical cluster analysis of data set 2 revealed two distinct groups of patients with PBC by disease activity. The most significant upstream regulators associated with disease activity were IFNG and CD40L. Several molecules expressed in B cells, T cells, Kupffer cells, and natural killer–like cells were identified as potential therapeutic targets in PBC with reference to a recently reported list of cell type–specific gene expression in the liver. Conclusion: Our integrated analysis using GWAS and mRNA microarray data sets predicted that IFNG and CD40L are the central upstream regulators in both disease susceptibility and activity of PBC and identified potential downstream therapeutic targets.
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spelling pubmed-71931322020-05-01 Integrated GWAS and mRNA Microarray Analysis Identified IFNG and CD40L as the Central Upstream Regulators in Primary Biliary Cholangitis Ueno, Kazuko Aiba, Yoshihiro Hitomi, Yuki Shimoda, Shinji Nakamura, Hitomi Gervais, Olivier Kawai, Yosuke Kawashima, Minae Nishida, Nao Kohn, Seik‐Soon Kojima, Kaname Katsushima, Shinji Naganuma, Atsushi Sugi, Kazuhiro Komatsu, Tatsuji Mannami, Tomohiko Matsushita, Kouki Yoshizawa, Kaname Makita, Fujio Nikami, Toshiki Nishimura, Hideo Kouno, Hiroshi Kouno, Hirotaka Ohta, Hajime Komura, Takuya Tsuruta, Satoru Yamauchi, Kazuhiko Kobata, Tatsuro Kitasato, Amane Kuroki, Tamotsu Abiru, Seigo Nagaoka, Shinya Komori, Atsumasa Yatsuhashi, Hiroshi Migita, Kiyoshi Ohira, Hiromasa Tanaka, Atsushi Takikawa, Hajime Nagasaki, Masao Tokunaga, Katsushi Nakamura, Minoru Hepatol Commun Original Articles Genome‐wide association studies (GWASs) in European and East Asian populations have identified more than 40 disease‐susceptibility genes in primary biliary cholangitis (PBC). The aim of this study is to computationally identify disease pathways, upstream regulators, and therapeutic targets in PBC through integrated GWAS and messenger RNA (mRNA) microarray analysis. Disease pathways and upstream regulators were analyzed with ingenuity pathway analysis in data set 1 for GWASs (1,920 patients with PBC and 1,770 controls), which included 261 annotated genes derived from 6,760 single‐nucleotide polymorphisms (P < 0.00001), and data set 2 for mRNA microarray analysis of liver biopsy specimens (36 patients with PBC and 5 normal controls), which included 1,574 genes with fold change >2 versus controls (P < 0.05). Hierarchical cluster analysis and categorization of cell type–specific genes were performed for data set 2. There were 27 genes, 10 pathways, and 149 upstream regulators that overlapped between data sets 1 and 2. All 10 pathways were immune‐related. The most significant common upstream regulators associated with PBC disease susceptibility identified were interferon‐gamma (IFNG) and CD40 ligand (CD40L). Hierarchical cluster analysis of data set 2 revealed two distinct groups of patients with PBC by disease activity. The most significant upstream regulators associated with disease activity were IFNG and CD40L. Several molecules expressed in B cells, T cells, Kupffer cells, and natural killer–like cells were identified as potential therapeutic targets in PBC with reference to a recently reported list of cell type–specific gene expression in the liver. Conclusion: Our integrated analysis using GWAS and mRNA microarray data sets predicted that IFNG and CD40L are the central upstream regulators in both disease susceptibility and activity of PBC and identified potential downstream therapeutic targets. John Wiley and Sons Inc. 2020-03-15 /pmc/articles/PMC7193132/ /pubmed/32363322 http://dx.doi.org/10.1002/hep4.1497 Text en © 2020 The Authors. Hepatology Communications published by Wiley Periodicals, Inc., on behalf of the American Association for the Study of Liver Diseases. This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc-nd/4.0/ License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Original Articles
Ueno, Kazuko
Aiba, Yoshihiro
Hitomi, Yuki
Shimoda, Shinji
Nakamura, Hitomi
Gervais, Olivier
Kawai, Yosuke
Kawashima, Minae
Nishida, Nao
Kohn, Seik‐Soon
Kojima, Kaname
Katsushima, Shinji
Naganuma, Atsushi
Sugi, Kazuhiro
Komatsu, Tatsuji
Mannami, Tomohiko
Matsushita, Kouki
Yoshizawa, Kaname
Makita, Fujio
Nikami, Toshiki
Nishimura, Hideo
Kouno, Hiroshi
Kouno, Hirotaka
Ohta, Hajime
Komura, Takuya
Tsuruta, Satoru
Yamauchi, Kazuhiko
Kobata, Tatsuro
Kitasato, Amane
Kuroki, Tamotsu
Abiru, Seigo
Nagaoka, Shinya
Komori, Atsumasa
Yatsuhashi, Hiroshi
Migita, Kiyoshi
Ohira, Hiromasa
Tanaka, Atsushi
Takikawa, Hajime
Nagasaki, Masao
Tokunaga, Katsushi
Nakamura, Minoru
Integrated GWAS and mRNA Microarray Analysis Identified IFNG and CD40L as the Central Upstream Regulators in Primary Biliary Cholangitis
title Integrated GWAS and mRNA Microarray Analysis Identified IFNG and CD40L as the Central Upstream Regulators in Primary Biliary Cholangitis
title_full Integrated GWAS and mRNA Microarray Analysis Identified IFNG and CD40L as the Central Upstream Regulators in Primary Biliary Cholangitis
title_fullStr Integrated GWAS and mRNA Microarray Analysis Identified IFNG and CD40L as the Central Upstream Regulators in Primary Biliary Cholangitis
title_full_unstemmed Integrated GWAS and mRNA Microarray Analysis Identified IFNG and CD40L as the Central Upstream Regulators in Primary Biliary Cholangitis
title_short Integrated GWAS and mRNA Microarray Analysis Identified IFNG and CD40L as the Central Upstream Regulators in Primary Biliary Cholangitis
title_sort integrated gwas and mrna microarray analysis identified ifng and cd40l as the central upstream regulators in primary biliary cholangitis
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7193132/
https://www.ncbi.nlm.nih.gov/pubmed/32363322
http://dx.doi.org/10.1002/hep4.1497
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