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Matrix metalloproteinase expression levels suggest distinct enzyme roles during lumbar disc herniation and degeneration

TLDR
Data on the gene and protein level is provided, which highlights the key role of MMP-3 in the degenerative cascade leading to symptomatic disc degeneration and herniation and Control of the proteolytic activity of M MP-3 may, therefore, come into the focus when aiming to develop new treatment options for earlyDisc degeneration.
Abstract
The disruption of the extracellular disc matrix is a major hallmark of disc degeneration. This has previously been shown to be associated with an up-regulation of major matrix metalloproteinase (MMP) expression and activity. However, until now hardly any data are available for MMP/TIMP regulation and thereby no concept exists as to which MMP/TIMP plays a major role in disc degeneration. The objective of this study was, therefore, to identify and quantify the putative up-regulation of MMPs/TIMPs on the mRNA and protein level and their activity in disc material in relation to clinical data and histological evidence for disc degeneration. A quantitative molecular analysis of the mRNA expression levels for the MMPs (MMPs-1, -2, -3, -7, -8, -9, -13) and the MMP inhibitors (TIMPs-1 and -2) was performed on 37 disc specimens obtained from symptomatic disc herniation or degeneration. In addition, disc specimens from patients without disc degeneration/herniation (=controls) were analyzed. Expression of MMPs-1, -2, -3, -7, -8, -9, -13 and TIMPs-1, -2 was analyzed using quantitative RT-PCR, normalized to the expression level of a house keeping gene (GAPDH). Gene expression patterns were correlated with MMP activity (in situ zymography), protein expression patterns (immunohistochemistry), degeneration score (routine histology) and clinical data. MMP-3 mRNA levels were consistently and substantially up-regulated in samples with histological evidence for disc degeneration. A similar but less pronounced up-regulation was observed for MMP-8. This up-regulation was paralleled by the expression of TIMP-1 and to a lesser extent TIMP-2. In general, these findings could be confirmed with regard to protein expression and enzyme activity. This study provides data on the gene and protein level, which highlights the key role of MMP-3 in the degenerative cascade leading to symptomatic disc degeneration and herniation. Control of the proteolytic activity of MMP-3 may, therefore, come into the focus when aiming to develop new treatment options for early disc degeneration.

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Role of cytokines in intervertebral disc degeneration: pain and disc content.

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TL;DR: Upregulation of MMP and ADAMTS expression and enzymatic activity is implicated in disc ECM destruction, leading to the development of IDD.
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Disc in flames: Roles of TNF-α and IL-1β in intervertebral disc degeneration.

TL;DR: The contributions of TNF-α and IL-1β to changes seen during disc degeneration at both cellular and tissue level are described, as well as new evidence suggesting a link between infection of the spine and low back pain, and the emerging therapeutic modalities aimed at combating these processes.
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Inflammatory mediators in intervertebral disk degeneration and discogenic pain.

TL;DR: This review provides information on the most relevant inflammatory mediators during different types of disk diseases and explains how these factors can induce disk degeneration and the development of discogenic and sciatic/radiculopathic pain.
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MMPs and ADAMTSs in intervertebral disc degeneration.

TL;DR: A greater understanding of the catabolic pathways involved in IDD will help to develop potential prophylactic or regenerative biological treatment for degenerative disc disease in the future.
References
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Journal ArticleDOI

Matrix metalloproteinases and tissue inhibitors of metalloproteinases: structure, function, and biochemistry.

TL;DR: This review describes the members of the matrixin family and discusses substrate specificity, domain structure and function, the activation of proMMPs, the regulation of matrixin activity by tissue inhibitors of metalloproteinases, and their pathophysiological implication.
Journal ArticleDOI

Structure and function of matrix metalloproteinases and TIMPs

TL;DR: The members of the MMP family are introduced and their domain structure and function, proenyme activation, the mechanism of inhibition by TIMPs and their significance in physiology and pathology are discussed.
Journal ArticleDOI

Classification of age-related changes in lumbar intervertebral discs: 2002 Volvo Award in basic science.

TL;DR: Histologic disc alterations can reliably be graded based on the proposed classification system providing a morphologic framework for more sophisticated molecular biologic analyses of factors leading to age-related disc changes.
Journal ArticleDOI

Histology and pathology of the human intervertebral disc

TL;DR: The intervertebral disc is a highly organized matrix laid down by relatively few cells in a specific manner that allows the discs to facilitate movement and flexibility within what would be an otherwise rigid spine.
Journal ArticleDOI

Matrix metalloproteinases and aggrecanase: Their role in disorders of the human intervertebral disc

TL;DR: In this paper, a comprehensive immunohistochemical study of matrix metalloproteinase activity in discs from patients with different disc diseases was conducted, and the most extensive staining was seen for matrix metallo-phrase 1, 2, 3, 7, 8, 9 and 13, with 91, 71, 65, and 72% of samples having some immunopositivity for the respective antibodies.
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