header advert
Orthopaedic Proceedings Logo

Receive monthly Table of Contents alerts from Orthopaedic Proceedings

Comprehensive article alerts can be set up and managed through your account settings

View my account settings

Visit Orthopaedic Proceedings at:

Facebook
X (Twitter)
LinkedIn
Article alerts Social media
Current issue
Full Access

CHARACTERIZATION OF INTERVERTEBRAL DISC CELLS BEHAVIOR IN A MOUSE SUBCUTANEOUS MODEL

Abstract

Although the etiology of low back pain is unclear, it is believed that intervertebral disc (IVD) degeneration plays a major role. In the present study, we sought to determine if bovine IVD cells maintain their phenotype in a mouse subcutaneous injection model, while embedded or not in biocompatible matrices.

Nucleus pulposus (NP) cells were isolated from adult bovine tails. Ten million cells were resuspended either in 500 ƒÝl of DMEM or in a negatively (alginate) or positively (chitosan) charged matrix. The mixtures were then injected subcutaneously in Balc/c nude mice. After two weeks, the mice were sacrificed and the implants harvested. The implants were examined histologically with a hematoxylin and eosin stain. The implant size was measured and the cells were counted. Proteoglycan was assessed by the GAG assay. The expression of type I and II collagens, aggrecan, and CD24 genes was analyzed by reverse transcription ¡V polymerase chain reaction (RT-PCR).

Histologic evaluation confirms the presence of cells in all NP implants. The presence of alginate increased the implant size, the number of cells in the implants, and to a lesser extent, the proteoglycan content, compared to implants formed with cells injected alone. However, chitosan had no effect on the implant size, the number of cells and the aggrecan content. NP implants expressed the same pattern of genes as the native NP tissue (i.e. type I and II collagens, aggrecan, and CD24). The presence of alginate did not affect this expression pattern whereas chitosan decreased slightly their expression.

After injection in mice, bovine NP cells appeared to retain their native phenotype. The RT-PCR analysis revealed that NP cells expressed aggrecan, type I and type II collagens as well as CD24, a specific marker for the NP phenotype. Also, NP cells can be embedded in matrices to produce NP-like features in vivo. In conclusion, we have developed a simple mouse subcutaneous injection model that recreates the features of the native IVD and avoids the need to use a disc degeneration model.

Correspondence should be addressed to: Cynthia Vezina, Communications Manager, COA, 4150-360 Ste. Catherine St. West, Westmount, QC H3Z 2Y5, Canada

Information

Journal

Orthopaedic Proceedings

Volume

91-B No.SUPP_II | Pages 226 - 226

Published

01 May 2009

Expand all

Lady Davis Institute for Medical Research, 3755, chemin de la Cote-ste-Catherine, Montreal, QC H3T 1E2

Search for more articles by this author

Lady Davis Institute for Medical Research, 3755, chemin de la Cote-ste-Catherine, Montreal, QC H3T 1E2

Search for more articles by this author

Lady Davis Institute for Medical Research, 3755, chemin de la Cote-ste-Catherine, Montreal, QC H3T 1E2

Search for more articles by this author

Lady Davis Institute for Medical Research, 3755, chemin de la Cote-ste-Catherine, Montreal, QC H3T 1E2

Search for more articles by this author

Lady Davis Institute for Medical Research, 3755, chemin de la Cote-ste-Catherine, Montreal, QC H3T 1E2

Search for more articles by this author

Lady Davis Institute for Medical Research, 3755, chemin de la Cote-ste-Catherine, Montreal, QC H3T 1E2

Search for more articles by this author

Share

Share article on social media
Facebook
X (Twitter)
LinkedIn
Email

Figures

Metrics

References