DocumentCode :
3047754
Title :
Early Gene Expression of Immune Proteins in Chondrocytes Differentiation from Rat Bone Marrow Stromal Cells
Author :
Jia Tanghong ; Sun Yuping ; Wang Yunshan ; Ma Xiaoli ; Cao Yilin
Author_Institution :
Jinan Central Hosp., Shandong Univ., Jinan
fYear :
2007
fDate :
6-8 July 2007
Firstpage :
226
Lastpage :
229
Abstract :
To study an effective differentiation condition of chondrocytes(Ch) from rat bone marrow stromal cells(MSC) in vitro by immunohistochemistry, in situ hybridization and RT- PCR, and identify gene expression pattern of immune proteins in this process via cDNA microarray analysis. The results suggested that Dexamethasone (Dex) had an ability to promote cell proliferation. The group of TGF-beta could highly express collagen II while its cell proliferation was weaker than that of Dex group. These indicated that TGF-beta had the ability to differentiate MSC into Ch.The group of combination of TGF-beta and Dex could both express collagen II and maintain proliferation. Analysis by cDNA microarray revealed that 7 genes of immune proteins out of the 2242 rat genes had differential expression during this process, including membrane-spanning 4-domainssubfamily A; T-cell receptor active alpha-chain C-region, TRA29; MHC class I-related protein; pepti dylprolyl isomerase C-associated protein; C8b; complement component 4 binding protein a and beta.This study showed that combination cultural condition in which MSC were induced into Ch lineage was effective to repair of articular cartilage. Various immune genes were involved in Ch differentiation. This would provide foundation for repair of articular cartilage defect with Ch.
Keywords :
DNA; cellular biophysics; genetics; patient treatment; proteins; MHC class I-related protein; T-cell receptor active alpha-chain C-region; articular cartilage; cDNA microarray analysis; cell proliferation; chondrocytes differentiation; collagen II while; dexamethasone; gene expression; immune genes; immune proteins; immunohistochemistry; in situ hybridization; membrane-spanning 4-domainssubfamily A; pepti dylprolyl isomerase C-associated protein; rat bone marrow stromal cells; Bones; DNA; Gene expression; Immune system; In vitro; Manufacturing; Probes; Protein engineering; Protocols; RNA;
fLanguage :
English
Publisher :
ieee
Conference_Titel :
Bioinformatics and Biomedical Engineering, 2007. ICBBE 2007. The 1st International Conference on
Conference_Location :
Wuhan
Print_ISBN :
1-4244-1120-3
Type :
conf
DOI :
10.1109/ICBBE.2007.61
Filename :
4272545
Link To Document :
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