Literature DB >> 16773379

Senescence in human intervertebral discs.

S Roberts1, E H Evans, D Kletsas, D C Jaffray, S M Eisenstein.   

Abstract

Intervertebral discs demonstrate degenerative changes relatively early in life. Disc degeneration, in turn, is associated with back pain and disc herniation, both of which cause considerable clinical problems in the western world. Cell senescence has been linked to degenerative diseases of other connective tissues such as osteoarthritis. Thus we investigated the degree of cell senescence in different regions of discs from patients with different disc disorders. Discs were obtained from 25 patients with disc herniations; from 27 patients undergoing anterior surgery for either back pain due to degenerative disc disease (n = 25) or spondylolisthesis (n = 2) and from six patients with scoliosis. In addition, four discs were obtained post-mortem. Samples were classified as annulus fibrosus or nucleus pulposus and tissue sections were assessed for the degree of cell senescence (using the marker senescence-associated-beta-galactosidase (SA-beta-Gal)) and the number of cells present in clusters. There were significantly more SA-beta-Gal positive cells in herniated discs (8.5% of cells) than those with degenerative disc disease, spondylolisthesis, scoliosis, or cadaveric discs (0.5% of cells; P < 0.001). There was more senescence of cells of the nucleus pulposus compared to those of the annulus fibrosus and in herniated discs a higher proportion of cells in cell clusters (defined as groups of three or more cells) were SA-beta-Gal positive (25.5%) compared to cells not in clusters (4.2%, P < 0.0001). This study demonstrates an increased degree of cell senescence in herniated discs, particularly in the nucleus where cell clusters occur. These clusters have been shown previously to form via cell proliferation, which is likely to explain the increased senescence. These findings could have two important clinical implications: firstly, that since senescent cells are known to behave abnormally in other locations, they may lead to deleterious effects on the disc matrix and so contribute to the pathogenesis and secondly, cells from such tissue may not be ideal for cell therapy and repair via tissue engineering.

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Year:  2006        PMID: 16773379      PMCID: PMC2335374          DOI: 10.1007/s00586-006-0126-8

Source DB:  PubMed          Journal:  Eur Spine J        ISSN: 0940-6719            Impact factor:   3.134


  20 in total

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3.  The origin and fate of herniated lumbar intervertebral disc tissue.

Authors:  R J Moore; B Vernon-Roberts; R D Fraser; O L Osti; M Schembri
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Review 5.  A biological approach to treating disc degeneration: not for today, but maybe for tomorrow.

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Journal:  Eur Spine J       Date:  2002-08-30       Impact factor: 3.134

6.  Replicative senescence of human skin fibroblasts correlates with a loss of regulation and overexpression of collagenase activity.

Authors:  M D West; O M Pereira-Smith; J R Smith
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7.  Chondrocyte senescence, joint loading and osteoarthritis.

Authors:  James A Martin; Thomas D Brown; Anneliese D Heiner; Joseph A Buckwalter
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8.  The role of chondrocyte senescence in the pathogenesis of osteoarthritis and in limiting cartilage repair.

Authors:  James A Martin; Joseph A Buckwalter
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Authors:  Jo S Price; Jasmine G Waters; Clare Darrah; Caroline Pennington; Dylan R Edwards; Simon T Donell; Ian M Clark
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10.  Histological changes in aging lumbar intervertebral discs. Their role in protrusions and prolapses.

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Journal:  J Bone Joint Surg Am       Date:  1990-02       Impact factor: 5.284

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  118 in total

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Review 2.  Inflammatory networks during cellular senescence: causes and consequences.

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Journal:  Trends Mol Med       Date:  2010-05-03       Impact factor: 11.951

3.  Age-related changes in human cervical, thoracal and lumbar intervertebral disc exhibit a strong intra-individual correlation.

Authors:  C Weiler; M Schietzsch; T Kirchner; A G Nerlich; N Boos; K Wuertz
Journal:  Eur Spine J       Date:  2011-08-12       Impact factor: 3.134

Review 4.  A survey of the "surgical and research" articles in the European Spine Journal, 2006.

Authors:  Robert C Mulholland
Journal:  Eur Spine J       Date:  2006-12-08       Impact factor: 3.134

5.  Three-dimensional morphology of the pericellular matrix of intervertebral disc cells in the rat.

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Journal:  J Anat       Date:  2007-08-02       Impact factor: 2.610

Review 6.  Cellular senescence: putting the paradoxes in perspective.

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Journal:  Curr Opin Genet Dev       Date:  2010-11-17       Impact factor: 5.578

7.  Development of an intact intervertebral disc organ culture system in which degeneration can be induced as a prelude to studying repair potential.

Authors:  Bernice Jim; Thomas Steffen; Janet Moir; Peter Roughley; Lisbet Haglund
Journal:  Eur Spine J       Date:  2011-02-19       Impact factor: 3.134

Review 8.  Senescent cells: an emerging target for diseases of ageing.

Authors:  Bennett G Childs; Martina Gluscevic; Darren J Baker; Remi-Martin Laberge; Dan Marquess; Jamie Dananberg; Jan M van Deursen
Journal:  Nat Rev Drug Discov       Date:  2017-07-21       Impact factor: 84.694

Review 9.  An understanding of intervertebral disc development, maturation and cell phenotype provides clues to direct cell-based tissue regeneration therapies for disc degeneration.

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10.  Disc cell clusters in pathological human intervertebral discs are associated with increased stress protein immunostaining.

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Journal:  Eur Spine J       Date:  2009-06-11       Impact factor: 3.134

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