Spondylodiscitis Clinical Trial
Official title:
Verification and Progress of Cytokine Profiles and suPAR for the Discrimination of Infectious and Non-infectious, Degenerative Diseases of the Spine
Spondylodiscitis is an infectious disease of the intervertebral discs and adjacent vertebral
bodies, which often has a protracted progression. Diagnosis is frequently delayed because of
the unspecific pathology and a lack of specific infection markers. However, an early
diagnosis is fundamental to prevent long periods with symptoms including extensive back pain
and progressive and destructive changes of the spine.
Cytokines can be helpful to extend the knowledge about diverse biological processes.
Furthermore, they are a promising category of biomarkers that are already present in the
early phases of developing diseases. Currently, little is known about the participation of
cytokines in Spondylodiscitis. The aim of this study is to establish a non-invasive method to
improve the diagnosis of spondylodiscitis. Therefore, blood and tissue samples will be
analyzed at different time points for the concentration of specific cytokines to select
potential marker cytokines via a Multiplex Assay and suPAR (soluble urokinase-type
plasminogen activator receptor) via ELISA. After successful identification of the biomarkers
cytokines and suPAR, verification of the results will be done by expression analysis of
cytokine-producing cells.
The potential of such a diagnostic method lies in reducing medical costs and preventing
extensive pain and structural changes of the spine.
Experimental research will be performed with the approval of the ethic committee of the
medical faculty of the University of Cologne.
Spondylodiscitis is a primary infection of the intervertebral discs with secondary infection
of the adjacent end-plates and vertebral bodies. It is relatively rare with an incidence of
2.4:100.000 and three times more common among men. The process of infection, which is
commonly creeping, leads to a destruction of the vertebral bodies and production of
abscesses, which can cause neurological deficits.
Clinical symptoms, especially in the early stages, are uncommon. Patients suffer from
unspecific back pain and fever occurs only in 50% of all cases. Currently, markers used
including leucocyte count, erythrocyte sedimentation rate (ESR) and C-reactive protein (CRP)
are also unspecific.For this reason of that several weeks may elapse between the first signs
of symptoms and the final diagnosis of spondylodiscitis. Therefore, the identification of the
pathogen is indispensable for an effective antibiotic therapy.
Spinal infections are generally monomicrobial, frequently with a haematogenous source.
Therefore, blood cultures can be used for identifying the pathogens. In case of negative
blood cultures, the pathogens can be identified by invasive methods such as percutaneous
punch biopsy or CT-guided fine needle aspiration. Despite biopsies, the pathogen can only be
identified in two out of three patients. Failures of pathogen identification are mainly due
to previous systemic antibiotic treatment. As a consequence, diagnosis is often based on
medical imaging methods (CT, MRT, PET, radiograph, skeletal scintigraphy). The disadvantage
of these methods is that structural changes of the spine must occur to become visible.
Treatment of an advanced spondylodiscitis consists of removal of the necrotic tissue,
stabilization of the affected vertebral bodies and concomitant antibiotic therapy. Randomized
studies for the duration of antibiotic treatments have not been published as yet. Current
recommendations are between 6 to 12 weeks. For evaluating the therapy response only the
clinical improvement and the CRP value are used. The mean period of stay in the hospital is
about 49 days.
The goal is to establish a non-invasive method which allows discrimination of infectious and
non-infectious diseases to improve the diagnosis of spondylodiscitis. For that purpose, blood
and tissue samples from patients with spondylodiscitis and erosive osteochondrosis will be
collected and analyzed for their cytokine and suPAR concentration. Erosive osteochondrosis is
a non-infectious, degenerative disease of the spine with similar surgical treatment. Thus, it
is an optimal reference group. Nevertheless, erosive osteochondrosis includes special types,
called modic type I-III. Because modic type I is associated with an immune response caused by
repeated traumata of the spine this modic type will be excluded from the study.
Cytokines are messengers, which are present in blood and all tissues, regulating the immune
response. In this study, the goal is to assess if cytokine profiles and suPAR contribute to
the discrimination of infectious and non-infectious spondylodiscitis and if this could be
verified by the characterization of the cytokine-producing cells. Furthermore, the
investigators want to analyze the therapy response by measuring the cytokine and suPAR
profiles.
Routine blood collection will be carried out directly before surgery and also during the
stationary hospitalization on day 4 and day 10. Additional blood collection will be done
after 6 weeks and 3 months during the follow-up. At each time point serum and plasma will be
used for the study to determine the cytokine and suPAR concentration and expression of the
cytokine-producing cells. Necrotic tissue, which is removed during the surgery, will be
analyzed microbiologically as well as pathologically. Parts of this tissue will also be used
for the determination of cytokines. Further blood samples will be collected when a patient
appears again in the Department of Orthopaedic Surgery and Traumatology because of treatment
and therapy of a re-infection. A minimum of 15 patients per group - control group (erosive
osteochondrosis modic type II-III) and spondylodiscitis - will be included in this study.
Both groups should be homogeneous in sex and age distribution.
There will be no additional pain or complications for the patients participating in this
study. All samples will be collected for a period of about one year and stored at -80°C.
Afterwards, the blood and tissue samples will be analyzed for potential marker suPAR via
ELISA and cytokines by using a Multiplex Assay. Furthermore, results will be linked to
anamnesis to detect potential correlations. Specific correlations can indicate a diagnostic
and perhaps a prognostic value of the measured cytokines and suPAR.
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