The transcriptional network that controls growth arrest and differentiation in a human myeloid leukemia cell line

Suzuki, Harukazu; Forrest, Alistair R.R.; Nimwegen, Erik van; Daub, Carsten O.; Balwierz, Piotr J.; Irvine, Katharine M.; Lassmann, Timo; Ravasi, Timothy; Hasegawa, Yuki; Hoon, Michiel de; Katayama, Shintaro; Schroder, Kate; Carninci, Piero; Tomaru, Yuji; Kanamori-Katayama, Mutsumi; Kubosaki, Atsutaka; Akalin, Altuna; Ando, Yoshinari; Arner, Erik; Asada, Maki; Asahara, Hiroshi; Bailey, Timothy L.; Bajic, Vladimir B.; Bauer, Denis C.; Beckhouse, Anthony G; Bertin, Nicolas; Björkegren, Johan; Brombacher, Frank; Bulger, Erika; Chalk, Alistair M.; Chiba, Joe; Cloonan, Nicole; Dawe, Adam; Dostie, Josée; Engström, Pär G.; Essack, Magbubah; Faulkner, Geoffrey J.; Fink, J. Lynn; Fredman, David; Fujimori, Ko; Furuno, Masaaki; Gojobori, Takashi; Gough, Julian; Grimmond, Sean M.; Gustafsson, Mika; Hashimoto, Megumi; Hashimoto, Takehiro; Hatakeyama, Mariko; Heinzel, Susanne; Hide, Winston; Hofmann, Oliver; Hörnquist, Michael; Huminiecki, Łukasz; Ikeo, Kazuho; Imamoto, Naoko; Inoue, Satoshi; Inoue, Yusuke; Ishihara, Ryoko; Iwayanagi, Takao; Jacobsen, Anders; Kaur, Mandeep; Kawaji, Hideya; Kerr, Markus C.; Kimura, Ryuichiro; Kimura, Syuhei; Kimura, Yasumasa; Kitano, Hiroaki; Koga, Hisashi; Kojima, Toshio; Kondo, Shinji; Konno, Tomohiro; Krogh, Anders; Kruger, Adéle; Kumar, Ajit; Lenhard, Boris; Lennartsson, Andreas; Lindow, Morten; Lizio, Marina; MacPherson, Cameron Ross; Maeda, Norihiro; Maher, Christopher A.; Maqungo, Monique; Mar, Jessica C.; Matigian, Nicholas; Matsuda, Hideo; Mattick, John S.; Meier, Stuart; Miyamoto, Sei; Miyamoto‐Sato, Etsuko; Nakabayashi, Kazuhiko; Nakachi, Yutaka; Nakano, Mika; Nygaard, Sanne; Okayama, Toshitsugu; Okazaki, Yasushi; Okuda-Yabukami, Haruka; Orlando, Valerio; Otomo, Jun; Pachkov, Mikhail; Petrovsky, Nikolai; Plessy, Charles; Quackenbush, John; Radovanović, Aleksandar; Rehli, Michael; Saito, Rintaro; Sandelin, Albin; Schmeier, Sebastian; Schönbach, Christian; Schwartz, Ariel; Semple, Colin A.; Sera, M.; Severin, Jessica; Shirahige, Katsuhiko; Simons, Cas; Laurent, George St.; Suzuki, Masanori; Suzuki, Tsuyoshi; Sweet, Matthew J.; Taft, Ryan J.; Takeda, Satomi; Takenaka, Yasuhiro; Tan, Kai Soo; Taylor, Martin S.; Teasdale, Rohan D.; Tegnér, Jesper; Teichmann, Sarah A.; Valen, Eivind; Wahlestedt, Claes; Waki, Kazunori; Waterhouse, Andrew; Wells, Christine A.; Winther, Ole; Wu, Linda Lin-yan; Yamaguchi, Kazumi; Yanagawa, Hiroshi; Yasuda, Jun; Zavolan, Mihaela; Hume, David; Arakawa, Takahiro; Fukuda, Shiro; Imamura, Kengo; Cui, Kai; Kaiho, Ai; Kawashima, Tsugumi; Kawazu, Chika; Kitazume, Yayoi; Kojima, Miki; Miura, Hisashi; Murakami, Kayoko; Murata, Mitsuyoshi; Ninomiya, Noriko; Nishiyori, Hiromi; Noma, Shohei; Ogawa, Chihiro; Sano, Takuma; Simon, Christophe; Tagami, Michihira; Takahashi, Yukari; Kawai, Jun; Hayashizaki, Yoshihide

doi:10.1038/ng.375

Cited by 395 publications

(370 citation statements)

References 47 publications

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“…bone marrow progenitors develop into monocytes, and extravasate into various tissues, where they differentiate into resident macrophages [15]. The monocyte-macrophage lineage is diverse and plastic, attributed to a complex transcriptome [30]. To facilitate immune function and maintain tissue homeostasis, macrophages adopt a wide range of activation states that can be classified within the classic activated M1 and alternative activated M2 models of macrophage polarization by interaction with the tumor-microenvironment milieu [31].…”

Section: Discussionmentioning

confidence: 99%

Infiltration of diametrically polarized macrophages predicts overall survival of patients with gastric cancer after surgical resection

et al. 2014

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Background Tumor-associated macrophages (TAMs), the most predominant tumor-infiltrating immune cells, are emerging prognostic factors and therapeutic targets for personalized therapy against malignant neoplasms. We aimed to evaluate the prognostic significance of diametrically polarized TAMs in gastric cancer and generate a predictive nomogram to refine a risk stratification system. Methods We evaluated polarized functional status of infiltrated TAMs by immunohistochemical staining of CD68, CD11c, and CD206 in 180 consecutive gastric cancer patients from Zhongshan Hospital, Shanghai, China. Prognostic values were assessed in these patients. We created a predictive nomogram by integrating polarized TAMs with the TNM staging system for overall survival of gastric cancer patients.Results CD68 ? TAMs display polarized programs comprising CD11c ? proinflammatory macrophages (M1) and CD206 ? immunosuppressive macrophages (M2) that configure versatile infiltration files in gastric cancer. CD11c ? TAMs negatively correlated with lymph node metastasis (p = 0.012), whereas CD206 ? TAMs correlated with the Lauren classification (p = 0.031). No prognostic difference was observed for overall survival for CD68 density (high vs low, p = 0.1031), whereas high versus low CD11c density (p \ 0.0001) and low vs high CD206 density (p = 0.0105) indicate better overall survival. Multivariate Cox regression analysis identified CD11c and CD206 as independent prognostic factors (p \ 0.001 and p = 0.030, respectively), which could be integrated with the TNM staging system to generate a predictive nomogram for patient outcomes. Conclusion Infiltration of polarized TAMs, a novel identified independent prognostic factor, could be combined with the TNM stage to refine a risk stratification system and better stratify patients with different prognosis. Tipping TAMs to an antitumoral phenotype might be a promising therapeutic target for postoperative treatment.

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Section: Discussionmentioning

confidence: 99%

Infiltration of diametrically polarized macrophages predicts overall survival of patients with gastric cancer after surgical resection

et al. 2014

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“…Thus, CAGE provides information on two aspects of the capped transcriptome: 1) genome-wide single basepair resolution map of transcription start sites, and 2) relative levels of transcripts initiated at each CTSS. This information can be used for various analyses, from 5' end centred expression profiling [30,31] to studying promoter architecture [12,25].…”

Section: Cap Analysis Of Gene Expression (Cage)mentioning

confidence: 99%

“…This has led to the discovery of distinct classes of promoters with respect to TSS distribution that correlates with both underlying sequence features and gene function [12], and implies distinct modes of their regulation (reviewed in [34]). Quantitative nature of CAGE has been used to model expression dynamics and to reconstruct the regulatory networks driving the differentiation [30] and maintaining identity of numerous human and mouse cell and tissue types [27], by identifying key transcription factors binding at promoters. Moreover, CAGE signal has been shown to be enriched at enhancers [35] and has been used to construct an atlas of active enhancers over cells and tissues across the whole human body [36].…”

Section: Cap Analysis Of Gene Expression (Cage)mentioning

confidence: 99%

Promoter architectures and developmental gene regulation

Haberle

Lenhard

2016

Seminars in Cell & Developmental Biology

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Core promoters are minimal regions sufficient to direct accurate initiation of transcription and are crucial for regulation of gene expression. They are highly diverse in terms of associated core promoter motifs, underlying sequence composition and patterns of transcription initiation.Distinctive features of promoters are also seen at the chromatin level, including nucleosome positioning patterns and presence of specific histone modifications. Recent advances in identifying and characterizing promoters using next-generation sequencing-based technologies have provided the basis for their classification into functional groups and have shed light on their modes of regulation, with important implications for transcriptional regulation in development.This review discusses the methodology and the results of genome-wide studies that provided insight into the diversity of RNA polymerase II promoter architectures in vertebrates and other Metazoa, and the association of these architectures with distinct modes of regulation in embryonic development and differentiation.

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“…Bioinformatic analysis of motif activity and motif target predictions were performed as described previously. 28 All genes represented on the microarray, which had been allocated a RefSeq (12752 in total), were classified as being either among the 205 genes of the Fbn1-associated cluster or not within the set. The proportion of genes with a z(p, m) score of greater than 1 for each transcription factor binding motif m was calculated for the two groups and a z-value for this difference was determined.…”

Section: Location and Function Of Cluster Genesmentioning

confidence: 99%

“…28 Table 2 lists the 15 transcription factors that had the highest positive correlations with the expression pattern of cluster genes. Comparison was also carried out between genes within the cluster and the remaining genes of the data set.…”

Section: P E R I T O N E a L M A C R O P H A G E S M Y E L O I D D E mentioning

confidence: 99%

Co-expression of FBN1 with mesenchyme-specific genes in mouse cell lines: implications for phenotypic variability in Marfan syndrome

et al. 2010

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Mutations in the human FBN1 gene cause Marfan syndrome, a complex disease affecting connective tissues but with a highly variable phenotype. To identify genes that might participate in epistatic interactions with FBN1, and could therefore explain the observed phenotypic variability, we have looked for genes that are co-expressed with Fbn1 in the mouse. Microarray expression data derived from a range of primary mouse cells and cell lines were analysed using the network analysis tool BioLayout Express 3D . A cluster of 205 genes, including Fbn1, were selectively expressed by mouse cell lines of different mesenchymal lineages and by mouse primary mesenchymal cells (preadipocytes, myoblasts, fibroblasts, osteoblasts). Promoter analysis of this gene set identified several candidate transcriptional regulators. Genes within this co-expressed cluster are candidate genetic modifiers for Marfan syndrome and for other connective tissue diseases.

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The transcriptional network that controls growth arrest and differentiation in a human myeloid leukemia cell line

Cited by 395 publications

References 47 publications

Infiltration of diametrically polarized macrophages predicts overall survival of patients with gastric cancer after surgical resection

Infiltration of diametrically polarized macrophages predicts overall survival of patients with gastric cancer after surgical resection

Promoter architectures and developmental gene regulation

Co-expression of FBN1 with mesenchyme-specific genes in mouse cell lines: implications for phenotypic variability in Marfan syndrome

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