The Journal of Bone & Joint Surgery

The Journal of Bone & Joint Surgery, Volume 88, Issue suppl 2

Workshop Articles | April 01, 2006

Biologic Markers and Disc Degeneration

A. Robin Poole, PhD, DSc

In support of his research for or preparation of this manuscript, the author received grants or outside funding from the Shriners Hospitals for Children and the Canadian Arthritis Network. In addition, the author received payments or other benefits or a commitment or agreement to provide such benefits from a commercial entity (Dr. Poole is a consultant to IBEX Technologies). No commercial entity paid or directed, or agreed to pay or direct, any benefits to any research fund, foundation, educational institution, or other charitable or nonprofit organization with which the author is affiliated or associated.

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J Bone Joint Surg Am, 2006 Apr 01;88(suppl 2):72-75. doi: 10.2106/JBJS.E.01326

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Abstract

Biomarkers of skeletal turnover, such as the synthesis and degradation of extracellular matrix molecules in specific tissues, offer the opportunity to gain new insights into spinal pathology and treatment. The creation, use, and interpretation of these analytical body-fluid measures of process (rather than outcome) require a clear understanding of the nature of the molecules and events being measured. This review provides examples of how protein and carbohydrate assays of biomarkers can be used to measure the contribution from the intervertebral discs and vertebrae of the spine. With regard to spinal degeneration and ankylosing spondylitis, these investigations are providing important new information, in weeks rather than years, on the response of patients to treatment.

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Biologic markers are molecules, or the breakdown products thereof, that originate from the extracellular matrix of skeletal tissues¹. These molecules or breakdown products may include those from the intervertebral discs and bone of the axial skeleton. Biologic markers can be detected in body fluids such as blood and urine; their presence reflects a specific biologic process such as the degradation, synthesis, or turnover of a specific matrix molecule in a known tissue location. The measurement of these biologic markers of molecular processes involved in the maintenance or pathology of the skeleton (including the spine) should provide useful information concerning the state of the discs and the vertebrae. This review will address the research that is being done on the biologic markers that are of relevance to the study and treatment of disc and spinal degeneration.

The Intervertebral Disc and Spine: A Source of Biomarkers of Skeletal Turnover

The disc is composed of a cartilage-like nucleus and is contained laterally by the anulus fibrosus. The cartilaginous end plates act as an interface between the disc and the vertebrae. Analytic studies of the human disc that have made use of cartilage biomarkers have revealed that the disc contains mainly type-II collagen and the proteoglycan aggrecan². The same molecules are present in the end plates³. Type-I collagen is the most dominant collagen present in the anulus, where type-II collagen and aggrecan are also present. Type-I collagen is also present in subchondral bone, where specific deoxypyridinoline crosslinks enable the detection of fragments of type-I collagen originating from the resorption of bone. All hyaline cartilages or bones share these tissue-specific molecules. Therefore, the detection of biomarkers originating from the spine can only be done under conditions in which all cartilage and bones will contribute to the total pool of biomarkers present in body fluids. Preclinical and human studies of arthritis involving large joints such as the knee or hip^1,4 have demonstrated that concentrations of specific biomarkers differing from the normal range can be observed in arthritis involving only a single large joint and may also be predictive of disease progression. Thus, the measurement of spine biomarkers in body fluids has the potential to assist researchers and clinicians with the study and treatment of spinal pathology and physiology.

When making measurements of biomarkers, it is important to understand that the content of a biomarker in a body fluid (e.g., serum) depends on the rate of generation and clearance of that biomarker from a tissue and the rate of removal from the blood, such as by the liver or kidneys, depending on the biomarker. Generation of biomarkers in tissues can be potently influenced by inflammation, causing, for example, increased degradation whereby cytokines such as interleukin-1 or tumor necrosis factor-a may cause increased proteolysis of matrix molecules. Alternatively, such cytokines can produce inhibition of synthesis of these molecules. Newly synthesized molecules may also be primary targets for proteolysis. Biomarker levels can be influenced by age, gender, body mass index, menopause, circadian rhythms, ethnicity, growth, and surgery; corrections for these factors must be made where applicable.

In the search for a specific biomarker, it is essential to have a clear understanding of the molecules or fragments being measured (especially the epitopes that are recognized by antibodies employed in immunoassays), the nature of the biologic event being measured (e.g., synthesis and/or degradation), the tissue origin of the biomarker, its half-life in a body fluid as well as the tissue of clearance from that fluid, and whether the biomarker reflects a product from a diseased or damaged tissue or a genetically determined difference in that individual. Without such knowledge, the interpretation of results obtained from biomarker studies is restricted and may lead to incorrect conclusions.

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Fig. 1: Cartilage biomarkers. (Reprinted from: Poole AR. Biochemical/immunochemical biomarkers of osteoarthritis: utility for prediction of incident or progressive osteoarthritis. Rheum Dis Clin North Am. 2003;29:806; with permission from Elsevier.)

Biomarkers have the potential to detect spinal disease, progression, and effects of therapy.

Cartilage Biomarkers

This discussion will be restricted to biomarkers of type-II collagen and aggrecan, as summarized in Figure 1. The collagen degradation markers can detect the C-telopeptide (CTx-II assay) or intrahelical cleavage neoepitopes generated by collagenases (C2C and C1, 2C assays). The carboxy propeptide (CPII assay) can be used to measure the synthesis of all type-II procollagen, and the amino propeptide of type-IIA procollagen can be used to measure type-IIA procollagen synthesis. The 846 assay detects an epitope of aggrecan present on chondroitin sulfate chains of intact molecules that are probably recently synthesized. The C2C, C1, 2C, CPII, and 846 epitopes detected by commercially available assays (IBEX, Montreal, Quebec, Canada) would all be present in developing and mature intervertebral discs, being most concentrated in the nucleus in the case of C2C, CPII, and the 846 epitope but also present in the anulus² and the end plate³. The CPII and 846 epitopes decrease in content with degeneration.

Contribution of Disc to Total Biomarker Pool

The contribution of disc was investigated by Garnero et al.⁵ in the case of the CTx-II biomarker (present in urine, the C-telopeptide of type-II collagen) in a group of 324 untreated postmenopausal women. Lateral radiographs of the thoracic and lumbar spine recorded disc-space narrowing and osteophytes. The authors used multivariate analyses to demonstrate that radiologic disc degeneration is associated with an increase in urinary CTx-II (Nordic Bioscience Diagnostics, Herlev, Denmark), independent of the presence of radiologic knee and clinical hand osteoarthritis. The contribution is from the lumbar rather than the thoracic spine; spinal osteophytes do not contribute.

Cartilage Biomarker Levels in Ankylosing Spondylitis

Patients with ankylosing spondylitis suffer disc degeneration that is associated with an underlying inflammatory arthritis. This disorder primarily involves the spine and may also involve the appendicular skeleton in about 25% of patients.

A recent study has revealed that the CPII and 846 epitope biomarkers of type-II procollagen synthesis and aggrecan synthesis-turnover, respectively, are significantly increased in patients with ankylosing spondylitis as compared with that seen in controls⁶. The 846 epitope is also increased in patients with axial and appendicular (peripheral) disease compared with axial disease only, as is CPII, although not significantly. This may be related to an increase from joints contributing to the circulating biomarkers (joint load).

Patients with ankylosing spondylitis have exhibited significant clinical improvement following a sixteen-week treatment period with etanercept, an inhibitor of tumor necrosis factor-a activity⁷. Treatment resulted in a significant reduction in the C2C neoepitope (type-II collagen cleavage) and an increase in the 846 biomarker. These changes may be predictive of a longer-term reduction in spinal damage. Because this usually requires a two-year period before effective treatment can be assessed (such as by magnetic resonance imaging), these early biomarker changes may be of value in determining the long-term effect of therapy.

Bone Biomarkers, Axial Disease, and Disc Degeneration

Significant remodeling of vertebral bone usually occurs in association with spinal disease that involves disc degeneration. The amino (NTx) and carboxy (CTx-I) telopeptides crosslink biomarkers of type-I collagen resorption have proved useful in detecting changes in bone turnover that involve increases in bone resorption. The small (6 KDa) bone-matrix protein osteocalcin, which contains ?-carboxyglutamic acid residues and binds hydroxyapatite with high affinity, is the second most abundant protein in bone after type-I collagen. Its release into serum is observed during both bone resorption and assembly. These assays reveal circadian rhythms involving these biomarkers, peaking overnight.

A study of a small group of patients with ankylosing spondylitis⁸ revealed that markers of bone resorption—NTx, free deoxypyridinoline (bone-specific), and pyridinoline crosslinks—are elevated in ankylosing spondylitis, pointing to increased bone resorption.

Summary and Conclusions

The axial skeleton, including the discs, contains extracellular matrix molecules and degradation products thereof that can be detected using commercially available assays in peripheral blood and urine. These include cartilage and bone-specific molecules. The whole skeleton, as well as all hyaline cartilages, contributes these biomarkers, which can be detected in body fluids. However, degeneration and alterations in turnover of the axial skeleton associated with aging, spondylitis, and disc degeneration are reflected in changes in these biomarkers in body fluids. Therefore, the opportunity exists to use these extracellular biomarkers to study spinal degeneration of the axial skeleton and possible treatment methods for the same.

Several general references^1,4,9,10 and other, more specific references^11-22 should be consulted for a better understanding of this topic. ?

References

Poole AR. Biochemical/immunochemical biomarkers of osteoarthritis: utility for prediction of incident or progressive osteoarthritis. Rheum Dis Clin North Am. 2003;29: 803-18.29803 2003 [PubMed][CrossRef]

Antoniou J, Steffen T, Nelson F, Winterbottom N, Hollander AP, Poole AR, Aebi M, Alini M. The human lumbar intervertebral disc: evidence for changes in the biosynthesis and denaturation of the extracellular matrix with growth, maturation, ageing, and degeneration. J Clin Invest. 1996;98: 996-1003.98996 1996 [PubMed][CrossRef]

Antoniou J, Goudsouzian NM, Heathfield TF, Winterbottom N, Steffen T, Poole AR, Aebi M, Alini M. The human lumbar end-plate. Evidence of changes in biosynthesis and denaturation of the extracellular matrix with growth, maturation, aging, and degeneration. Spine. 1996;21: 1153-61.211153 1996 [PubMed][CrossRef]

Lohmander LS, Poole AR. Defining and validating the clinical role of molecular markers in osteoarthritis. In: Brandt KD, Doherty M, Lohmander LS, editors. Osteoarthritis. New York: Oxford University Press; 2003. p 468-77.468 2003

Garnero P, Sornay-Rendu E, Arlot M, Christiansen C, Delmas PD. Association between spine disc degeneration and type II collagen degradation in postmenopausal women: the OFELY study. Arthritis Rheum. 2004;50: 3137-44.503137 2004 [PubMed][CrossRef]

Kim TH, Stone M, Payne U, Zhang X, Ionescu M, Lobanok T, King L, Poole AR, Inman RD. Cartilage biomarkers in ankylosing spondylitis: relationship to clinical variables and treatment response. Arthritis Rheum. 2005;52: 885-91.52885 2005 [PubMed][CrossRef]

Maksymowych WP, Poole AR, Hiebert L, Webb A, Ionescu M, Lobanok T, King L, Davis JC Jr. Etanercept exerts beneficial effects on articular cartilage biomarkers of degradation and turnover in patients with ankylosing spondylitis. J Rheumatol. 2005;32: 1911-7.321911 2005 [PubMed]

Acebes C, de la Piedra C, Traba ML, Seibel MJ, Garcia Martin C, Armas J, Herrero-Beaumont G. Biochemical markers of bone remodeling and bone sialo-protein in ankylosing spondylitis. Clin Chim Acta. 1999;289: 99-110.28999 1999 [PubMed][CrossRef]

Garnero P, Delmas PD. Biomarkers in osteoarthritis. Curr Opin Rheumatol. 2003;15: 641-6.15641 2003 [PubMed][CrossRef]

Delmas PD. Biological markers of bone turnover in osteoporosis. In: Stevenson JC, Lindsay R, editors. Osteoporosis. New York: Chapman and Hall; 1998. p 29-47.29 1998

Aoshima H, Kushida K, Takahashi M, Ohishi T, Hoshino H. Circadian variation of urinary type I collagen crosslinked C-telopeptide and free and peptide-bound forms of pyridinium crosslinks. Bone. 1998;22: 73-8.2273 1998 [PubMed][CrossRef]

Bollen AM, Martin MD, Leroux BG, Eyre DR. Circadian variation in urinary excretion of bone collagen cross-links. J Bone Miner Res. 1995;10: 1885-90.101885 1995 [PubMed][CrossRef]

Bonde M, Qvist P, Fledelius C, Riis BJ, Christiansen C. Immunoassay for quantifying type I collagen degradation products in urine evaluated. Clin Chem. 1994;40: 2022-5.402022 1994 [PubMed]

Charni N, Juillet F, Garnero P. Urinary type II collagen helical peptide (HELIX-II) as a new biochemical marker of cartilage degradation in patients with osteoarthritis and rheumatoid arthritis. Arthritis Rheum. 2005;52: 1081-90.521081 2005 [PubMed][CrossRef]

Christgau S, Garnero P, Fledelius C, Moniz C, Ensig M, Gineyts E, Rosenquist C, Qvist P. Collagen type II C-telopeptide fragments as an index of cartilage degradation. Bone. 2001;29: 209-15.29209 2001 [PubMed][CrossRef]

Hanson PA, Weis MA, Bollen AM, Maslan SL, Singer FR, Eyre DR. A specific immunoassay for monitoring human bone resorption: quantitation of type I collagen cross-linked N-telopeptides in urine. J Bone Miner Res. 1992;7: 1251-8.71251 1992 [PubMed][CrossRef]

Ivaska KK, Hentunen TA, Vaaraniemi J, Ylipahkala H, Pettersson K, Vaananen HK. Release of intact and fragmented osteocalcin molecules from bone matrix during bone resorption in vitro. J Biol Chem. 2004;279: 18361-9.27918361 2004 [PubMed][CrossRef]

Lohmander LS, Atley LM, Pietka TA, Eyre DR. The release of crosslinked peptides from type II collagen into human synovial fluid is increased soon after joint injury and in osteoarthritis. Arthritis Rheum. 2003;48: 3130-9.483130 2003 [PubMed][CrossRef]

Nelson F, Dahlberg L, Laverty S, Reiner A, Pidoux I, Ionescu M, Fraser GL, Brooks E, Tanzer M, Rosenberg LC, Dieppe P, Poole AR. Evidence for altered synthesis of type II collagen in patients with osteoarthritis. J Clin Invest. 1998;102: 2115-25.1022115 1998 [PubMed][CrossRef]

Poole AR, Ionescu M, Fitzcharles MA, Billinghurst RC. The assessment of cartilage degradation in vivo: development of an immunoassay for the measurement in body fluids of type II collagen cleaved by collagenases. J Immunol Methods. 2004;294: 145-53.294145 2004 [PubMed][CrossRef]

Rizkalla G, Reiner A, Bogoch E, Poole AR. Studies of the articular cartilage proteoglycan aggrecan in health and osteoarthritis. Evidence for molecular heterogeneity and extensive molecular changes in disease. J Clin Invest. 1992;90: 2268-77.902268 1992 [PubMed][CrossRef]

Rousseau JC, Zhu Y, Miossec P, Vignon E, Sandell LJ, Garnero P, Delmas PD. Serum levels of type IIA procollagen amino terminal propeptide (PIIANP) are decreased in patients with knee osteoarthritis and rheumatoid arthritis. Osteoarthritis Cartilage. 2004;12: 440-7.12440 2004 [CrossRef]

Topics

ankylosing spondylitis ; cartilage ; personnel turnover ; spine ; vertebrae ; degenerative disc disease

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A. Robin Poole; Biologic Markers and Disc Degeneration. The Journal of Bone & Joint Surgery. 2006 Apr;88(suppl_2):72-75.

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