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Differential roles of epigenetic changes and Foxp3 expression in regulatory T cell-specific transcriptional regulation

Authors :
Morikawa, H
Ohkura, N
Vandenbon, A
Itoh, M
Nagao Sato, S
Kawaji, H
Lassmann, T
Carninci, P
Hayashizaki, Y
Forrest, Ar
Standley, Dm
Date, H
Sakaguchi, S
FANTOM Consortium (Forrest AR
Rehli, M
Baillie, Jk
de Hoon MJ
Haberle, V
Kulakovskiy, Iv
Lizio, M
Andersson, R
Mungall, Cj
Meehan, Tf
Schmeier, S
Bertin, N
Jørgensen, M
Dimont, E
Arner, E
Schmidl, C
Schaefer, U
Medvedeva, Ya
Plessy, C
Vitezic, M
Severin, J
Semple, Ca
Ishizu, Y
Francescatto, M
Alam, I
Albanese, D
Altschuler, Gm
Archer, Ja
Arner, P
Babina, M
Baker, S
Balwierz, Pj
Beckhouse, Ag
Pradhan Bhatt, S
Blake, Ja
Blumenthal, A
Bodega, B
Bonetti, A
Briggs, J
Brombacher, F
Burroughs, Am
Califano, A
Cannistraci, Cv
Carbajo, D
Chen, Y
Chierici, M
Ciani, Y
Clevers, Hc
Dalla, E
Davis, Ca
Deplancke, B
Detmar, M
Diehl, Ad
Dohi, T
Drabløs, F
Edge, As
Edinger, M
Ekwall, K
Endoh, M
Enomoto, H
Fagiolini, M
Fairbairn, L
Fang, H
Farach Carson MC
Faulkner, Gj
Favorov, Av
Fisher, Me
Frith, Mc
Fujita, R
Fukuda, S
Furlanello, C
Furuno, M
Furusawa, J
Geijtenbeek, Tb
Gibson, A
Gingeras, T
Goldowitz, D
Gough, J
Guhl, S
Guler, R
Gustincich, Stefano
Ha, Tj
Hamaguchi, M
Hara, M
Harbers, M
Harshbarger, J
Hasegawa, A
Hasegawa, Y
Hashimoto, T
Herlyn, M
Hitchens, Kj
Ho Sui SJ
Hofmann, Om
Hoof, I
Hori, F
Huminiecki, L
Iida, K
Ikawa, T
Jankovic, Br
Jia, H
Joshi, A
Jurman, G
Kaczkowski, B
Kai, C
Kaida, K
Kaiho, A
Kajiyama, K
Kanamori Katayama, M
Kasianov, As
Kasukawa, T
Katayama, S
Kato, S
Kawaguchi, S
Kawamoto, H
Kawamura, Yi
Kawashima, T
Kempfle, Js
Kenna, Tj
Kere, J
Khachigian, Lm
Kitamura, T
Klinken, Sp
Knox, Aj
Kojima, M
Kojima, S
Kondo, N
Koseki, H
Koyasu, S
Krampitz, S
Kubosaki, A
Kwon, At
Laros, Jf
Lee, W
Lennartsson, A
Li, K
Lilje, B
Lipovich, L
Mackay Sim, A
Manabe, R
Mar, Jc
Marchand, B
Mathelier, A
Mejhert, N
Meynert, A
Mizuno, Y
Morais, Da
Morimoto, M
Moro, K
Motakis, E
Motohashi, H
Mummery, Cl
Murata, M
Nakachi, Y
Nakahara, F
Nakamura, T
Nakamura, Y
Nakazato, K
van Nimwegen, E
Ninomiya, N
Nishiyori, H
Noma, S
Nozaki, T
Ogishima, S
Ohmiya, H
Ohno, H
Ohshima, M
Okada Hatakeyama, M
Okazaki, Y
Orlando, V
Ovchinnikov, Da
Pain, A
Passier, R
Patrikakis, M
Persson, H
Piazza, S
Prendergast, Jg
Rackham, Oj
Ramilowski, Ja
Rashid, M
Ravasi, T
Rizzu, P
Roncador, M
Roy, S
Rye, Mb
Saijyo, E
Sajantila, A
Saka, A
Sakai, M
Sato, H
Satoh, H
Savvi, S
Saxena, A
Schneider, C
Schultes, Ea
Schulze Tanzil GG
Schwegmann, A
Sengstag, T
Sheng, G
Shimoji, H
Shimoni, Y
Shin, Jw
Simon, C
Sugiyama, D
Sugiyama, T
Suzuki, M
Swoboda, Rk
't Hoen PA
Tagami, M
Takahashi, N
Takai, J
Tanaka, H
Tatsukawa, H
Tatum, Z
Thompson, M
Toyoda, H
Toyoda, T
Valen, E
van de Wetering, M
van den Berg LM
Verardo, R
Vijayan, D
Vorontsov, Ie
Wasserman, Ww
Watanabe, S
Wells, Ca
Winteringham, Ln
Wolvetang, E
Wood, Ej
Yamaguchi, Y
Yamamoto, M
Yoneda, M
Yonekura, Y
Yoshida, S
Zabierowski, Se
Zhang, Pg
Zhao, X
Zucchelli, S
Summers, Km
Suzuki, H
Daub, Co
Kawai, J
Heutink, P
Hide, W
Freeman, Tc
Lenhard, B
Bajic, Vb
Taylor, Ms
Makeev, Vj
Sandelin, A
Hume, Da
Hayashizaki, Y.
AII - Amsterdam institute for Infection and Immunity
Infectious diseases
Experimental Immunology
Hubrecht Institute for Developmental Biology and Stem Cell Research
Source :
Proceedings of the National Academy of Sciences of the United States of America, 111(14), 5289-5294. National Academy of Sciences, University of Western Australia, Proceedings of the National Academy of Sciences, 111(14), 5289-5294, Proceedings of the National Academy of Sciences of the United States of America, 111(14), 5289-94. National Academy of Sciences
Publication Year :
2014

Abstract

Naturally occurring regulatory T (Treg) cells, which specifically express the transcription factor forkhead box P3 (Foxp3), are engaged in the maintenance of immunological self-tolerance and homeostasis. By transcriptional start site cluster analysis, we assessed here how genome-wide patterns of DNA methylation or Foxp3 binding sites were associated with Treg-specific gene expression. We found that Treg-specific DNA hypomethylated regions were closely associated with Treg up-regulated transcriptional start site clusters, whereas Foxp3 binding regions had no significant correlation with either up- or down-regulated clusters in nonactivated Treg cells. However, in activated Treg cells, Foxp3 binding regions showed a strong correlation with down-regulated clusters. In accordance with these findings, the above two features of activation-dependent gene regulation in Treg cells tend to occur at different locations in the genome. The results collectively indicate that Treg-specific DNA hypomethylation is instrumental in gene up-regulation in steady state Treg cells, whereas Foxp3 down-regulates the expression of its target genes in activated Treg cells. Thus, the two events seem to play distinct but complementary roles in Treg-specific gene expression.

Details

Language :
English
ISSN :
00278424
Database :
OpenAIRE
Journal :
Proceedings of the National Academy of Sciences of the United States of America, 111(14), 5289-5294. National Academy of Sciences, University of Western Australia, Proceedings of the National Academy of Sciences, 111(14), 5289-5294, Proceedings of the National Academy of Sciences of the United States of America, 111(14), 5289-94. National Academy of Sciences
Accession number :
edsair.doi.dedup.....e36c21559e09eded6c21af9387e9344a
Full Text :
https://doi.org/10.1073/pnas.1312717110