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Merck

NFIA and GATA3 are crucial regulators of embryonic articular cartilage differentiation.

Development (Cambridge, England) (2017-12-17)
Pratik Narendra Pratap Singh, Upendra Singh Yadav, Kimi Azad, Pooja Goswami, Veena Kinare, Amitabha Bandyopadhyay
ABSTRAKT

During appendicular skeletal development, the bi-potential cartilage anlagen gives rise to transient cartilage, which is eventually replaced by bone, and to articular cartilage that caps the ends of individual skeletal elements. While the molecular mechanism that regulates transient cartilage differentiation is relatively well understood, the mechanism of articular cartilage differentiation has only begun to be unraveled. Furthermore, the molecules that coordinate the articular and transient cartilage differentiation processes are poorly understood. Here, we have characterized in chick the regulatory roles of two transcription factors, NFIA and GATA3, in articular cartilage differentiation, maintenance and the coordinated differentiation of articular and transient cartilage. Both NFIA and GATA3 block hypertrophic differentiation. Our results suggest that NFIA is not sufficient but necessary for articular cartilage differentiation. Ectopic activation of GATA3 promotes articular cartilage differentiation, whereas inhibition of GATA3 activity promotes transient cartilage differentiation at the expense of articular cartilage. We propose a novel transcriptional circuitry involved in embryonic articular cartilage differentiation, maintenance and its crosstalk with the transient cartilage differentiation program.

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Sigma-Aldrich
Anti-β-Catenin−Cy3 antibody, Mouse monoclonal, clone 15B8, purified from hybridoma cell culture
Sigma-Aldrich
Anti-phospho-Histone H3 (pSer10) antibody produced in rabbit, IgG fraction of antiserum, buffered aqueous solution