Identification and Characterization of a Novel Follistatin-like Protein as a Binding Protein for the TGF-β Family

Tsuchida, Kunihiro; Arai, Koji Y.; Kuramoto, Yoji; Yamakawa, Noriko; Hasegawa, Yoshihisa; Sugino, Hiromu

doi:10.1074/jbc.m006114200

Cited by 181 publications

(168 citation statements)

References 43 publications

(65 reference statements)

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“…These factors have not been linked to tendon formation and their abundance in adult tendon has therefore not been tested previously. Fstl1 encodes a secreted glycoprotein that binds members of the TGF-b superfamily of growth/differentiation factors and is able to interfere with BMP2-induced transcriptional responses in a dose-dependent manner [14]. Its expression might be one of the reasons for the low osteogenic properties of tenogenic C3H10T½-BMP2/Smad8ca cells [5] and for tenogenic tissue in general [15].…”

Section: Discussionmentioning

confidence: 99%

“…cDNA synthesis and reverse transcriptionpolymerase chain reaction Five micrograms of total RNA from cell cultures was reverse transcribed with the cDNA synthesis kit (MMLV-RT; Life Technologies) and with oligo-dT (12)(13)(14)(15)(16)(17)(18) -primer. For tendon and muscle tissue, the entire material was used for cDNA synthesis, which was carried out after DNase treatment to remove genomic DNA according to the protocol of the supplier (Revert Aid First Strand cDNA synthesis Kit; Fermentas) using random hexamer primers.…”

Section: Isolation Of Rnamentioning

confidence: 99%

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Periostin Secreted by Mesenchymal Stem Cells Supports Tendon Formation in an Ectopic Mouse Model

Noack

Seiffart

Willbold

et al. 2014

Stem Cells and Development

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True tendon regeneration in human patients remains a vision of musculoskeletal therapies. In comparison to other mesenchymal lineages the biology of tenogenic differentiation is barely understood. Specifically, easy and efficient protocols are lacking that might enable tendon cell and tissue differentiation based on adult (stem) cell sources. In the murine mesenchymal progenitor cell line C3H10T½, overexpression of the growth factor bone morphogenetic protein 2 (BMP2) and a constitutively active transcription factor, Smad8 L + MH2, mediates tendon cell differentiation in vitro and the formation of tendon-like tissue in vivo. We hypothesized that during this differentiation secreted factors involved in extracellular matrix formation exert a major impact on tendon development. Gene expression analyses revealed four genes encoding secreted factors that are notably upregulated: periostin, C-type lectin domain family 3 (member b), RNase A4, and follistatin-like 1. These factors have not previously been implicated in tendon biology. Among these, periostin showed a specific expression in tenocytes of adult mouse Achilles tendon and in chondrocytes within the nonmineralized fibrocartilage zone of the enthesis with the calcaneus. Overexpression of periostin alone or in combination with constitutively active BMP receptor type in human mesenchymal stem cells and subsequent implantation into ectopic sites in mice demonstrated a reproducible moderate tenogenic capacity that has not been described before. Therefore, periostin may belong to the factors contributing to the development of tenogenic tissue.

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Section: Discussionmentioning

confidence: 99%

Section: Isolation Of Rnamentioning

confidence: 99%

Periostin Secreted by Mesenchymal Stem Cells Supports Tendon Formation in an Ectopic Mouse Model

Noack

Seiffart

Willbold

et al. 2014

Stem Cells and Development

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“…Follistatin, through its binding to activin, modulates its biological activity in a broad range of cells. This suggests that FLRG may constitute another partner in the regulation of the biological activity of activin (Tsuchida et al, 2000). TGFb increases the expression of both activin ligands, FLRG and follistatin (Maguer-Satta et al, 2001).…”

Section: Binding Of Smad3 and Smad4 To The Sbe Sitementioning

confidence: 99%

FLRG, an activin-binding protein, is a new target of TGFβ transcription activation through Smad proteins

et al. 2001

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The FLRG gene encodes a secreted glycoprotein that binds to activin and is highly homologous to follistatin, an activin ligand. We cloned the promoter region of the human FLRG gene, and de®ned the minimal region necessary for transcription activation in a reportersystem assay. We showed that the fragment between positions 7130 and +6, which consists of multiple consensus Sp1-binding sites, is required for the constitutive expression of the FLRG gene. We demonstrate here that FLRG mRNA expression is rapidly induced by TGFb or by transfection with Smad protein expression vectors in human HepG2 cells. We investigated the transcription-regulation mechanism of FLRG expression in HepG2 cells following treatment with TGFb. By deletion and point-mutation analysis of the FLRG promoter, we identi®ed a Smad-binding element involved in the TGFb-inducible expression of the FLRG gene. Moreover, transactivation of the FLRG promoter by TGFb was compromised by dominant-negative mutants of Smad3 and Smad4 proteins. In addition, gel electrophoresis mobility-shift assays demonstrated the speci®c interaction of Smad3 and Smad4 proteins with the Smad-binding element consensus motif found in the FLRG promoter. Taken together, our data imply that Smad proteins participate in the regulation of expression of FLRG, a new target of TGFb transcription activation. Oncogene (2001) 20, 5409 ± 5419.

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“…Recently, a new protein that shares the characteristic 10-cysteine structures of follistatin domains was cloned from a B cell leukemia line based on its overexpression in response to a chromosomal translocation (10). Referred to as follistatin-related gene (FLRG) on the basis of the striking sequence homology with follistatin (11), it also shares a similar Nterminal domain with follistatin, a region that is crucial for the binding to activin (12) and, like follistatin, it binds strongly to activin (11,13,14).…”

Section: Introductionmentioning

confidence: 99%

Follistatin-related gene expression, but not follistatin expression, is decreased in human endometrial adenocarcinoma

Ciarmela

Florio²,

Sigurðardóttir³

et al. 2004

European Journal of Endocrinology

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P Ciarmela and P Florio contributed equally to this work AbstractObjective: Activin A is a multifunctional growth and cell differentiation factor produced by normal endometrium, and secreted in high amounts by endometrial adenocarcinoma. In the present study we evaluated the expression of two inhibitory activin A ligands, follistatin and follistatin-related gene (FLRG), in endometrial adenocarcinoma and in age-matched healthy human endometrium. Design and methods: Atropic menopausal (n ¼ 13) and tumoral (n ¼ 9 adenocarcinoma) tissues were processed to evaluate mRNA expression levels (by semiquantitative RT-PCR) and peptide localization (by immunohistochemistry). Differences were evaluated by the unpaired t-test and assumed to be statistically significant when P , 0.05. Results: Both control and tumoral endometrial samples express and localize follistatin and FLRG. However, whereas follistatin mRNA expression did not differ significantly, FLRG was significantly lower in endometrial adenocarcinoma than in healthy endometrial specimens (P , 0.0001). With respect to the localization of proteins, follistatin was immunolocalized in endometrial epithelial and vascular cells both in tumoral and healthy endometrium without any significant difference in intensity. Nuclear and cytoplasmic FLRG immunolocalization was seen in glands, and only nuclear immunolocalization was found in stroma and vessels of healthy endometrium. FLRG was weakly immunostained in endometrial adenocarcinoma. Conclusions: Whilst follistatin expression is unchanged, FLRG is down-regulated in endometrial carcinoma. As activin A is a differentiation factor of human endometrium, the present findings support an imbalance between increased activin A and decreased FLRG expression in endometrial cancer, so that the failure of the activin A pathway through FLRG may be pivotal in endometrial tumorigenesis.

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Identification and Characterization of a Novel Follistatin-like Protein as a Binding Protein for the TGF-β Family

Cited by 181 publications

References 43 publications

Periostin Secreted by Mesenchymal Stem Cells Supports Tendon Formation in an Ectopic Mouse Model

Periostin Secreted by Mesenchymal Stem Cells Supports Tendon Formation in an Ectopic Mouse Model

FLRG, an activin-binding protein, is a new target of TGFβ transcription activation through Smad proteins

Follistatin-related gene expression, but not follistatin expression, is decreased in human endometrial adenocarcinoma

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