Literature DB >> 21150669

Comparative expression of matrix-associated genes and inflammatory cytokines-associated genes according to disc degeneration: analysis of living human nucleus pulposus.

Jeong Yoon Park1, Sung Uk Kuh, Hyo Suk Park, Keun Su Kim.   

Abstract

STUDY
DESIGN: The 2 groups of living human nucleus pulposus were prospectively compared according to disc degeneration.
OBJECTIVES: This study was conducted to investigate the expressions of various genes associated with matrix synthesis and expressions of inflammatory cytokines-associated genes according to degrees of disc degeneration in human discs. SUMMARY OF BACKGROUND DATA: Degenerated discs were obtained from 18 patients who underwent discectomy for lumbar disc herniation. Disc degeneration was graded by T2-weighted magnetic resonance imaging using Pfirrmann's grading system. Discs were allocated to 2 groups: group I (9 patients)-mildly degenerated discs (grades II and III) and group II (9 patients)-severely degenerated discs (grades IV and V).
METHODS: Cells from the nucleus pulposus were isolated and then cultured as monolayers. The mRNA expressions of aggrecan, type II collagen, Sox9, type I collagen, alkaline phosphatase, osteocalcin, tumor necrosis factor-α, and interleukin-1β in the 2 groups were compared by real-time polymerase chain reaction, and production of matrix-associate proteins (aggrecan, type II collagen, Sox9, type I collagen, alkaline phosphatase, and osteocalcin) were compared by Western blotting.
RESULTS: mRNA expressions in group I were upregulated versus group II to the following extents: 1.83 times for aggrecan, 1.82 times for type II collagen, 1.80 times for Sox9, 1.41 times for type I collagen, 1.38 times for alkaline phosphatase, and 1.80 times for osteocalcin. Furthermore, Western blotting showed that aggrecan, type II collagen, Sox9, type I collagen, alkaline phosphatase, and osteocalcin were higher in group I. However, the mRNA levels of tumor necrosis factor-α and interleukin-1β were 1.26 and 1.11-fold, respectively, upregulated in group II.
CONCLUSIONS: Mildly degenerated discs showed greater matrix, chondrogenic, and osteoblastic gene expressions than severely degenerated discs, indicating that the ability to produce matrix-associated proteins is greater for cells in mildly degenerated than in severely degenerated discs. However, inflammatory cytokine genes associated with disc degeneration were expressed at higher levels in the severely degenerated group. This study shows that a reduction in matrix synthesis and an increase of inflammatory cytokine levels occurs during disc degeneration at the same time.

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Year:  2011        PMID: 21150669     DOI: 10.1097/BSD.0b013e3181fee4df

Source DB:  PubMed          Journal:  J Spinal Disord Tech        ISSN: 1536-0652


  15 in total

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5.  Inflammatory cytokines induce caveolin-1/β-catenin signalling in rat nucleus pulposus cell apoptosis through the p38 MAPK pathway.

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6.  Bone morphogenic protein-2 signaling in human disc degeneration and correlation to the Pfirrmann MRI grading system.

Authors:  Alex M Hollenberg; Noorullah Maqsoodi; Amy Phan; Aric Huber; Ayodeji Jubril; Avionna L Baldwin; Noriaki Yokogawa; Roman A Eliseev; Addisu Mesfin
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7.  MicroRNA-494 promotes apoptosis and extracellular matrix degradation in degenerative human nucleus pulposus cells.

Authors:  Liang Kang; Cao Yang; Yu Song; Kangcheng Zhao; Wei Liu; Wenbin Hua; Kun Wang; Ji Tu; Shuai Li; Huipeng Yin; Yukun Zhang
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Review 8.  Inflammatory mediators in intervertebral disk degeneration and discogenic pain.

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9.  Correlation Between Expression of High Temperature Requirement Serine Protease A1 (HtrA1) in Nucleus Pulposus and T2 Value of Magnetic Resonance Imaging.

Authors:  Dapeng Li; Jiawei Yue; Lu Jiang; Yonghui Huang; Jifu Sun; Yan Wu
Journal:  Med Sci Monit       Date:  2017-04-22

10.  Inhibiting tumor necrosis factor-alpha at time of induced intervertebral disc injury limits long-term pain and degeneration in a rat model.

Authors:  Thomas W Evashwick-Rogler; Alon Lai; Hironobu Watanabe; Jonathan M Salandra; Beth A Winkelstein; Samuel K Cho; Andrew C Hecht; James C Iatridis
Journal:  JOR Spine       Date:  2018-05-21
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