C/EBPβ Promotes Transition from Proliferation to Hypertrophic Differentiation of Chondrocytes through Transactivation of p57Kip2

Hirata, Makoto; Kugimiya, Fumitaka; Fukai, Atsushi; Ohba, Shinsuke; Kawamura, Naohiro; Ogasawara, Toru; Kawasaki, Yosuke; Saito, Taku; Yano, Fumiko; Ikeda, Toshiyuki; Nakamura, Kozo; Chung, Ung‐il; Kawaguchi, Hiroshi

doi:10.1371/journal.pone.0004543

Cited by 85 publications

(97 citation statements)

References 61 publications

(73 reference statements)

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“…Tissue sections were deparaffinized in xylene and rehydrated through an ethanol series. IHC was performed, as described previously (8,37), using the primary antibodies goat polyclonal anti-GADD45␤ (catalog number sc-8776, Santa Cruz Biotechnology, Inc.; 1:400 dilution, 0.5 g/ml final concentration) and rabbit polyclonal anti-C/EBP␤ (sc-150X, Santa Cruz Biostechnology, Inc.; 1:2000 dilution). Rabbit polyclonal antibody to collagen type X (1:1000 dilution) was kindly supplied by Prof. Ray Boot-Handford (Wellcome Trust Centre for Cell-Matrix Research, Manchester, UK).…”

Section: Methodsmentioning

confidence: 99%

“…The Gadd45␤ and C/ebp␤ knock-out mice display similar phenotypic changes in the embryonic growth plate, characterized by a delay in terminal chondrocyte differentiation along with decreased expression of genes linked to this process, including Col10a1 and Mmp13 (8,37,69). In addition, the embryonic limbs of C/ebp␤ knock-out mice display impaired osteogenesis (53).…”

Section: Gadd45␤ Regulation Of Genes Involved In Terminal Chondrocytementioning

confidence: 99%

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GADD45β Enhances Col10a1 Transcription via the MTK1/MKK3/6/p38 Axis and Activation of C/EBPβ-TAD4 in Terminally Differentiating Chondrocytes

Tsuchimochi

Otero

Dragomir

et al. 2010

Journal of Biological Chemistry

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GADD45␤ (growth arrest-and DNA damage-inducible) interacts with upstream regulators of the JNK and p38 stress response kinases. Previously, we reported that the hypertrophic zone of the Gadd45␤ ؊/؊ mouse embryonic growth plate is compressed, and expression of type X collagen (Col10a1) and matrix metalloproteinase 13 (Mmp13) genes is decreased. Herein, we report that GADD45␤ enhances activity of the proximal Col10a1 promoter, which contains evolutionarily conserved AP-1, cAMP-response element, and C/EBP half-sites, in synergism with C/EBP family members, whereas the MMP13 promoter responds to GADD45␤ together with AP-1, ATF, or C/EBP family members. C/EBP␤ expression also predominantly co-localizes with GADD45␤ in the embryonic growth plate. Moreover, GADD45␤ enhances C/EBP␤ activation via MTK1, MKK3, and MKK6, and dominant-negative p38␣apf, but not JNKapf, disrupts the combined trans-activating effect of GADD45␤ and C/EBP␤ on the Col10a1 promoter. Importantly, GADD45␤ knockdown prevents p38 phosphorylation while decreasing Col10a1 mRNA levels but does not affect C/EBP␤ binding to the Col10a1 promoter in vivo, indicating that GADD45␤ influences the transactivation function of DNA-bound C/EBP␤. In support of this conclusion, we show that the evolutionarily conserved TAD4 domain of C/EBP␤ is the target of the GADD45␤-dependent signaling. Collectively, we have uncovered a novel molecular mechanism linking GADD45␤ via the MTK1/MKK3/6/p38 axis to C/EBP␤-TAD4 activation of Col10a1 transcription in terminally differentiating chondrocytes.

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Section: Methodsmentioning

confidence: 99%

Section: Gadd45␤ Regulation Of Genes Involved In Terminal Chondrocytementioning

confidence: 99%

GADD45β Enhances Col10a1 Transcription via the MTK1/MKK3/6/p38 Axis and Activation of C/EBPβ-TAD4 in Terminally Differentiating Chondrocytes

Tsuchimochi

Otero

Dragomir

et al. 2010

Journal of Biological Chemistry

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“…In particular, CKI is able to stabilize MyoD, a transcription factor that is highly specific for muscle involved in myogenic differentiation. p57 Kip2 is also involved in the differentiation of several other cell phenotypes, including podocytes (79), placental cells (65,80,81), keratinocytes (82), pancreatic cells (83), hepatocytes (84,85), T-lymphocytes (86), spermatozoa (87,88), Leydig cells (88), chondrocytes (89)(90)(91), and adrenal cortex cells (92).…”

Section: P57 Kip2 Metabolismmentioning

confidence: 99%

p57Kip2 and Cancer: Time for a Critical Appraisal

Borriello

Caldarelli

Bencivenga

et al. 2011

Molecular Cancer Research

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p57Kip2 is a cyclin-dependent kinase inhibitor belonging to the Cip/Kip family, which also includes p21Cip1 and p27Kip1. So far, p57Kip2 is the least-studied Cip/Kip protein, and for a long time its relevance has been related mainly to its unique role in embryogenesis. Moreover, genetic and molecular studies on animal models and patients with Beckwith-Wiedemann syndrome have shown that alterations in CDKN1C (the p57Kip2 encoding gene) have functional relevance in the pathogenesis of this disease. Recently, a number of investigations have identified and characterized heretofore unexpected roles for p57Kip2. The protein appears to be critically involved in initial steps of cell and tissue differentiation, and particularly in neuronal development and erythropoiesis. Intriguingly, p27Kip1, the Cip/Kip member that is most homologous to p57Kip2, is primarily involved in the process of cell cycle exit. p57Kip2 also plays a critical role in controlling cytoskeletal organization and cell migration through its interaction with LIMK-1. Furthermore, p57Kip2 appears to modulate genome expression. Finally, accumulating evidence indicates that p57Kip2 protein is frequently downregulated in different types of human epithelial and nonepithelial cancers as a consequence of genetic and epigenetic events. In summary, the emerging picture is that several aspects of p57Kip2's functions are only poorly clarified. This review represents an appraisal of the data available on the p57Kip2 gene and protein structure, and its role in human physiology and pathology. We particularly focus our attention on p57Kip2 changes in cancers and pharmacological approaches for modulating p57Kip2 levels. Mol Cancer Res; 9(10); 1269–84. ©2011 AACR.

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“…C/EBP␤ induced by pro-inflammatory cytokines such as IL-1␤ and TNF-␣ directly binds to the MMP13 and MMP3 promoter regions and stimulates their expression in chondrocytes, resulting in degradation of cartilage in arthritis (21,22). Furthermore, it was reported that hypertrophic differentiation of chondrocytes was delayed in C/EBP␤ knock-out mice through transactivation of cell cycle factor p57 (23). This was associated with decreased expression of Col10a1 (24) and suggested that C/EBP␤ plays an important role in promoting hypertrophic differentiation of chondrocytes.…”

mentioning

confidence: 99%

CCAAT/Enhancer-binding Protein β Regulates the Repression of Type II Collagen Expression during the Differentiation from Proliferative to Hypertrophic Chondrocytes

Ushijima

Okazaki

Tsushima

et al. 2014

Journal of Biological Chemistry

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Background: CCAAT/enhancer-binding protein ␤ (C/EBP␤) promotes hypertrophic differentiation of chondrocytes. Results: C/EBP␤ directly represses the expression of type II collagen by interacting with its intronic enhancer. Conclusion: C/EBP␤ biphasically functions to repress genes characteristic of proliferative chondrocytes while stimulating genes expressed by hypertrophic chondrocytes. Significance: C/EBP␤ is a key regulator to trigger phenotypic conversion from proliferative to hypertrophic chondrocytes.

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C/EBPβ Promotes Transition from Proliferation to Hypertrophic Differentiation of Chondrocytes through Transactivation of p57Kip2

Cited by 85 publications

References 61 publications

GADD45β Enhances Col10a1 Transcription via the MTK1/MKK3/6/p38 Axis and Activation of C/EBPβ-TAD4 in Terminally Differentiating Chondrocytes

GADD45β Enhances Col10a1 Transcription via the MTK1/MKK3/6/p38 Axis and Activation of C/EBPβ-TAD4 in Terminally Differentiating Chondrocytes

p57Kip2 and Cancer: Time for a Critical Appraisal

CCAAT/Enhancer-binding Protein β Regulates the Repression of Type II Collagen Expression during the Differentiation from Proliferative to Hypertrophic Chondrocytes

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