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Alternative splicing during chondrogenesis: Modulation of fibronectin exon EIIIA splicing by SR proteins

โœ Scribed by Bruce A. Kuo; Tatiana M. Uporova; Hongyan Liang; Vickie D. Bennett; Rocky S. Tuan; Pamela A. Norton


Publisher
John Wiley and Sons
Year
2002
Tongue
English
Weight
238 KB
Volume
86
Category
Article
ISSN
0730-2312

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โœฆ Synopsis


The alternative exon EIIIA of the fibronectin gene is included in mRNAs produced in undifferentiated mesenchymal cells but excluded from differentiated chondrocytes. As members of the SR protein family of splicing factors have been demonstrated to be involved in the alternative splicing of other mRNAs, the role of SR proteins in chondrogenesis-associated EIIIA splicing was investigated. SR proteins interacted with chick exon EIIIA sequences that are required for exon inclusion in a gel mobility shift assay. Addition of SR proteins to in vitro splicing reactions increased the rate and extent of exon EIIIA inclusion. Co-transfection studies employing cDNAs encoding individual SR proteins revealed that SRp20 decreased mRNA accumulation in HeLa cells, which make A+ mRNA, apparently by interfering with pre-mRNA splicing. Co-transfection studies also demonstrated that SRp40 increased exon EIIIA inclusion in chondrocytes, but not in HeLa cells, suggesting the importance of cellular context for SR protein activity. Immunoblot analysis did not reveal a relative depletion of SRp40 in chondrocytic cells. Possible mechanisms for regulation of EIIIA splicing in particular, and chondrogenesis associated splicing in general, are discussed.


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Alternative splicing during chondrogenes
โœ Tatyana M. Uporova; Pamela A. Norton; Rocky S. Tuan; Vickie D. Bennett ๐Ÿ“‚ Article ๐Ÿ“… 2000 ๐Ÿ› John Wiley and Sons ๐ŸŒ English โš– 172 KB

Primary chicken mesenchymal cells from limb buds and vertebral chondrocytes have been used to study the changes that occur in alternative mRNA splicing of fibronectin exon EIIIA during chondrogenesis. The mesenchymal cell phenotype (exon EIIIA included) and chondrocyte phenotype (exon EIIIA excluded

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## Abstract Type III homologies of human fibronectin are generally encoded by two exons, with the exception of the EDโ€A and EDโ€B repeats which are encoded by a single exon undergoing alternative splicing. We report that also the type IIIโ€9 homology is encoded by a single exon. Further more, RTโ€PCR