Literature DB >> 16023419

Hypoxia induces chondrocyte-specific gene expression in mesenchymal cells in association with transcriptional activation of Sox9.

Jared C Robins1, Nagako Akeno, Aditi Mukherjee, Ravi R Dalal, Bruce J Aronow, Peter Koopman, Thomas L Clemens.   

Abstract

Endochondral bone is formed during an avascular period in an environment of low oxygen. Under these conditions, pluripotential mesenchymal stromal cells preferentially differentiate into chondrocytes and form cartilage. In this study, we investigated the hypothesis that oxygen tension modulates bone mesenchymal cell fate by altering the expression of genes that function to promote chondrogenesis. Microarray of RNA samples from ST2 cells revealed significant changes in 728 array elements (P < 0.01) in response to hypoxia. Real-time PCR on these RNA samples, and separate samples from C3H10T1/2 cells, revealed hypoxia-induced changes in the expression of additional genes known to be expressed by chondrocytes including Sox9 and its downstream targets aggrecan and Col2a. These changes were accompanied by the accumulation of mucopolysacharide as detected by alcian blue staining. To investigate the mechanisms responsible for upregulation of Sox9 by hypoxia, we determined the effect of hypoxia on HIF-1alpha levels and Sox9 promoter activity in ST2 cells. Hypoxia increased nuclear accumulation of HIF-1alpha and activated the Sox9 promoter. The ability of hypoxia to transactivate the Sox9 promoter was virtually abolished by deletion of HIF-1alpha consensus sites within the proximal promoter. These findings suggest that hypoxia promotes the differentiation of mesenchymal cells along a chondrocyte pathway in part by activating Sox-9 via a HIF-1alpha-dependent mechanism.

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Year:  2005        PMID: 16023419     DOI: 10.1016/j.bone.2005.04.040

Source DB:  PubMed          Journal:  Bone        ISSN: 1873-2763            Impact factor:   4.398


  100 in total

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2.  Hypoxic adipocytes pattern early heterotopic bone formation.

Authors:  Elizabeth Olmsted-Davis; Francis H Gannon; Mustafa Ozen; Michael M Ittmann; Zbigniew Gugala; John A Hipp; Kevin M Moran; Christine M Fouletier-Dilling; Shannon Schumara-Martin; Ronald W Lindsey; Michael H Heggeness; Malcolm K Brenner; Alan R Davis
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Review 4.  Metabolic regulation of skeletal cell fate and function in physiology and disease.

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Review 5.  Environmental preconditioning rejuvenates adult stem cells' proliferation and chondrogenic potential.

Authors:  Ming Pei
Journal:  Biomaterials       Date:  2016-11-25       Impact factor: 12.479

6.  Nanofibrous spongy microspheres to deliver rabbit mesenchymal stem cells and anti-miR-199a to regenerate nucleus pulposus and prevent calcification.

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7.  HIF-1-PHD2 axis controls expression of syndecan 4 in nucleus pulposus cells.

Authors:  Nobuyuki Fujita; Yuichiro Hirose; Cassie M Tran; Kazuhiro Chiba; Takeshi Miyamoto; Yoshiaki Toyama; Irving M Shapiro; Makarand V Risbud
Journal:  FASEB J       Date:  2014-02-20       Impact factor: 5.191

Review 8.  Hypoxia. HIF-mediated articular chondrocyte function: prospects for cartilage repair.

Authors:  Christopher L Murphy; Brendan L Thoms; Rasilaben J Vaghjiani; Jérôme E Lafont
Journal:  Arthritis Res Ther       Date:  2009-02-05       Impact factor: 5.156

Review 9.  Cartilage homeostasis in health and rheumatic diseases.

Authors:  Mary B Goldring; Kenneth B Marcu
Journal:  Arthritis Res Ther       Date:  2009-05-19       Impact factor: 5.156

10.  Oxygen and Cell Fate Decisions.

Authors:  Qun Lin; Yuri Kim; Rodolfo M Alarcon; Zhong Yun
Journal:  Gene Regul Syst Bio       Date:  2008-02-10
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