Human Recombinant Type I Collagen Produced in Plants

Shoseyov, Oded; Posen, Yehudit; Grynspan, Frida

doi:10.1089/ten.tea.2012.0347

Cited by 54 publications

(49 citation statements)

References 63 publications

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“…7 However, the yields obtained may not be sufficient for widespread commercial use, although recent production of mammalian collagens in plants looks more promising as a commercial production direction. 8 More recently, the collagen like (CL) domain Scl2 from Streptococcus pyogenes has been proposed as a potential biomedical material 9 that is non-cytotoxic and non-immunogenic. 10 This protein can be readily prepared in good yields, up to around 19 g/L in 2 L fermentation studies 11 and can be purified using a simple precipitation and proteolysis approach.…”

Section: Introductionmentioning

confidence: 99%

Preparation and characterization of monomers to tetramers of a collagen-like domain fromStreptococcus pyogenes

et al. 2014

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Abbreviations: V, non-collagenous N-terminal domain of the S. pyogenes collagen-like protein; CL, collagenous domain of the S.pyogenes collagen-like protein; VCL, full collagen-like protein structureThe collagen like domain Scl2 from Streptococcus pyogenes has been proposed as a potential biomedical material. It is non-cytotoxic and non-immunogenic and can be prepared in good yield in fermentation. The Scl2 collagen domain is about a quarter of the length, 234 residues, of the main collagen type, mammalian type I collagen (1014 residues) that is currently used in biomedical devices. In the present study we have made constructs comprising 1 to 4 copies of the Scl2 collagen domain, plus these same constructs with a CysCys sequence at the C-terminal, analogous to that found in mammalian type III collagens. The yields of these constructs were examined from 2 L fermentation studies. The yields of both series declined with increasing size. Circular dichroism showed that the addition of further collagen domains did not lead to a change in the melting temperature compared to the monomer domain. Addition of the CysCys sequence led to a small additional stabilization of about 2-3 C for the monomer construct when the folding (V) domain was present.

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Section: Introductionmentioning

confidence: 99%

Preparation and characterization of monomers to tetramers of a collagen-like domain fromStreptococcus pyogenes

et al. 2014

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“…It is worthwhile to check whether this system is a viable alternative to oocytes for assaying AQPs even from animal sources (that functional animal proteins can be expressed in plant cells has been already demonstrated 17 ).…”

Section: Discussionmentioning

confidence: 99%

Measuring the Osmotic Water Permeability Coefficient (P<sub>f</sub>) of Spherical Cells: Isolated Plant Protoplasts as an Example

Shatil‐Cohen

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Chaumont

et al. 2014

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“…Notable progress has been made on commercial, recombinant production of human collagens. 7,[10][11][12][13][14][15][16][17] However, the rapidly emerging technologies that have characterized and produced recombinant non-animal (bacterial) collagens in E. coli [23][24][25]27,28 have introduced an exciting new collagen option that can be readily customized for specific biomedical applications. 28,33 These customized collagens will pave the way for more diverse applications in medical devices, implantable materials and potentially as scaffolds for stem cells, to name but a few examples of uses for these recombinant bacterial collagens.…”

Section: Conclusion and Future Trendsmentioning

confidence: 99%

“…Most recently, heterotrimeric collagen has been produced with P4H also present, giving excellent protein yields, which can be commercialized. 17 There may be further advantages of recombinant systems that possibly work only at a laboratory level. For example a range of constructs have been made for type II collagen, where specific "D-period" repeats, about 234 amino acids each, have been removed or substituted into the structure, allowing a better understanding of collagen structure and function.…”

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confidence: 99%