The Effect of Alemtuzumab on the Blood-brain-barrier and the Brain's Metabolism in Multiple Sclerosis Patients

Study Description

Brief Summary

The development and progression of multiple sclerosis seem to be driven by concomitant inflammation and, to a less well-defined degree, disturbances in metabolism of individual cells of the human central nervous system as well as changes in the dynamical supply of blood to the brain. These alterations in normal physiology can be quantified by investigating the change in specific parameters over the time course of multiple sclerosis evolution. Amongst these specific parameters, the ability of the so-called blood-brain-barrier to selectively filter nutrients from the blood stream prior to passage into the nervous tissue, is disrupted in multiple sclerosis, and the severity of this deficiency seem to be related to the underlying disease burden. The present study utilises a novel imaging technology in order to monitor changes in the integrity of the blood-brain-barrier over the course of treatment with a biological disease modifying agent known as alemtuzumab. Alemtuzumab is a potent immunosuppressant drug. It is hypothesised that alemtuzumab reverts the deficiency in blood-brain-barrier integrity and, conversely, the severity of blood-brain-barrier disruption at several time points during alemtuzumab treatment can be utilised as prognostic marker for the requirement of additional administration of alemtuzumab beyond the regular treatment regimen. In addition, several other factors are investigated by advanced imaging techniques in combination with blood and urine samples in order to elucidate the possible underlying mechanism of alemtuzumab efficacy. It is hypothesized that alemtuzumab normalises metabolic alterations and changes in the blood supply through resolution of inflammation in the brains of multiple sclerosis patients.

Detailed Description

Traditional paraclinical measures of disease severity in multiple sclerosis (MS), such as T2 lesion load as measured by magnetic resonance imaging (MRI), are poorly correlated with long-term disability accumulation. Other surrogate markers of the current and future disease burden are therefore needed. The permeability of the blood-brain-barrier (BBB) seems to better reflect the substantial, subclinical disease activity underlying MS progression. Its useful role as a prognostic marker in MS has been clearly established by the recent observation that BBB permeability increase in optic neuritis patients is associated with conversion to definite MS. BBB permeability can be quantified, in a convenient manner to the patient, using Dynamic-Contrast-Enhanced Magnetic Resonance Imaging (DCE-MRI) by modelling the change in intrinsic MRI parameters of the human brain in response to the administration of a bolus contrast agent. Alemtuzumab is a disease modifying drug that depletes T- and B-cells. It is administered in two series separated by 12 months, as explained in the section "Groups and Interventions." The number of relapses are significantly reduced as compared to other efficacious treatments in MS, as demonstrated recently (study referred to by its ClinicalTrials.gov identifier NCT00050778). The efficacy of alemtuzumab in resolving the inflammatory burden underlying relapses is, thus, well-established. Its influence on subclinical inflammation, however, remains unknown. It is the aim of the present study to investigate whether or not the latter influence is of importance, and, consequently, can be used to evaluate the need for an intensified treatment, in the form of an additional series of alemtuzumab administration.

BBB permeability changes, as surrogate markers of subclinical inflammation, are measured every 6 months just prior to and during the course of alemtuzumab treatment. In order to elucidate other potential mechanisms involved in disability accumulation, biomarkers and MRI-derived parameters are evaluated concomitantly. Specifically, the role of metabolic changes are investigated using MRI methods that measures blood perfusion and oxygen consumption. Secondarily, the BBB permeability and metabolic changes are correlated to novel biomarkers of inflammation and neurodegeneration in serum and urine, as well as conventional measures of MS severity: annual relapse rate, Expanded Disability Severity Score, MRI-derived estimates of disease activity and brain atrophy.

35 patients are included in the study in order to achieve enough statistical power and accommodate drop-outs. Patients are MRI scanned at baseline, 6 months after alemtuzumab treatment, and, finally, prior to administration of the second series of alemtuzumab 12 months after the baseline MRI scanning. At each time point, the patient's disease status is evaluated by an experienced neurologist, and urine and serum samples are obtained. Repeated Measures Analysis Of Variance (ANOVA) will be used to evaluate changes of permeability of the BBB and metabolic parameters at different time points, and baseline characteristics, such as prednisolone treatment will be implemented as between-subjects covariates. Logistic regression will be applied to estimate the ability of BBB permeability changes to predict the need for additional series of alemtuzumab administration.

Study Design

Outcome Measures

Primary Outcome Measures

1. Blood-Brain-Barrier Permeability [1 year]

   Blood-Brain-Barrier Permeability as measured by Dynamic-Contrast-Enhanced MRI (DCE-MRI)

Secondary Outcome Measures

1. Oxygen Consumption [1 year]

   The Cerebral Metabolic Rate of Oxygen Consumption as measured by a novel MRI technique

2. Cerebral perfusion [1 year]

   Quantification of cerebral perfusion using DCE-MRI and Arterial-Spin-Labelling MRI

3. Diffusion Tensor MRI parameters and MR spectroscopy metabolite concentrations [1 year]

   Measurement of changes in microstructural organization as measured by Diffusion Tensor MRI

4. Brain atrophy [2 years]

   Voxel-Based-Morphometry of grey and white matter utilizing high-resolution MRI

5. Clinical Severity of Disease [1 year]

   Estimation of disease severity by the Expanded Disability Severity Scale (EDSS)

6. Relapse frequency [1 year]

   Number of relapses during follow-up and past history

7. Plasma markers of Blood-Brain-Barrier breakdown [1 year]

   Detection of markers associated with Blood-Brain-Barrier breakdown nervous system

8. Plasma markers of neuronal damage [1 year]

   Detection of markers associated with neuronal damage

9. Urinary markers of inflammation [1 year]

   Detection of markers associated with inflammatory activity specific to macrophages/microglia in the human central nervous system

Eligibility Criteria

Criteria

Inclusion Criteria:

• A diagnosis of Relapsing-Remitting Multiple Sclerosis

• Eligible for alemtuzumab treatment at Glostrup Hospital or The Danish Kingdom Hospital

• Subjects must be deemed physically and mentally able to participate in the study

Exclusion Criteria:

• Contraindications to MRI scanning (pregnancy, pacemakers, claustrophobia, extreme obesity)

• Contraindications to the use of MRI contrast agents (kidney disease, previous allergic reactions)

• Conflicting disorders (e.g. disorders with a systemic, inflammatory component)

Contacts and Locations

Locations

Sponsors and Collaborators

• Glostrup University Hospital, Copenhagen
• Genzyme, a Sanofi Company

Investigators

• Study Director: Henrik BW Larsson, MD, Prof., Functional Imaging Unit, Department of Clinical Physiology, Nuclear medicine and PET, Glostrup Hospital

Study Documents (Full-Text)

More Information

Publications

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