Characterization of Human Type III Collagen Expressed in a Baculovirus System

  • Lamberg A
  • Helaakoski T
  • Myllyharju J
  • et al.
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Abstract

An efficient expression system for recombinant collagens would have numerous scientific and practical applications. Nevertheless, most recombinant systems are not suitable for this purpose, as they do not have sufficient amounts of prolyl 4-hydroxylase activity. Pro-[alpha]1 chains of human type III collagen expressed in insect cells by a baculovirus vector are reported here to contain significant amounts of 4-hydroxyproline and to form triple-helical molecules, although the T[(m)] of the triple helices was only about 32-34 {degrees}C. Coexpression of the pro-[alpha]1(III) chains with the [alpha] and [beta] subunits of human prolyl 4-hydroxylase increased the T[(m)] to about 40 {degrees}C, provided that ascorbate was added to the culture medium. The level of expression of type III procollagen was also increased in the presence of the recombinant prolyl 4-hydroxylase, and the pro-[alpha]1(III) chains and [alpha]1(III) chains were found to be present in disulfide-bonded molecules. Most of the triple-helical collagen produced was retained within the insect cells and could be extracted from the cell pellet. The highest expression levels were obtained in High Five cells, which produced up to about 80 {micro}g of cellular type III collagen (120 {micro}g of procollagen) per 5 [times] 10[^6] cells in monolayer culture and up to 40 mg/liter of cellular type III collagen (60 mg/liter procollagen) in suspension. The 4-hydroxyproline content and T[(m)] of the purified recombinant type III collagen were very similar to those of the nonrecombinant protein, but the hydroxylysine content was slightly lower, being about 3 residues/1000 in the former and 5/1000 in the latter.

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Lamberg, A., Helaakoski, T., Myllyharju, J., Peltonen, S., Notbohm, H., Pihlajaniemi, T., & Kivirikko, K. I. (1996). Characterization of Human Type III Collagen Expressed in a Baculovirus System. Journal of Biological Chemistry, 271(20), 11988–11995. https://doi.org/10.1074/jbc.271.20.11988

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