Listen on the go
CORRECT!
Next question
touchNEUROLOGY touchNEUROLOGY
Multiple Sclerosis
Read Time: 8 mins

Optical Coherence Tomography – A New Monitoring Tool for Multiple Sclerosis?

Copy Link
Published Online: Jun 4th 2011 European Neurological Review, 2010;5(1):73-77 DOI: http://doi.org/10.17925/ENR.2010.05.01.73
Authors: Patrick Vermersch, Olivier Outteryck, Axel Petzold
Quick Links:
Abstract
Article
Article Information
Abstract:
Overview

Optical coherence tomography (OCT) is a simple office-based measure that can be used to quantify changes in the retina in patients with multiple sclerosis (MS). Such retinal changes in some MS patient subgroups, as assessed by OCT, are associated with brain atrophy as detected by magnetic resonance imaging (MRI). There is also some evidence that changes detected by OCT are correlated with increasing levels of cognitive impairment. OCT in MS patients introduces a new tool to characterise the disease process and could prove beneficial in the assessment of new therapies. It may provide information additional to that produced by MRI. For example, the use of OCT to quantify the retinal nerve fibre layer may offer some advantages by detecting neural degeneration in the MS disease process more quickly, cheaply and specifically than MRI. The latest OCT equipment and software offer high reproducibility and improve accuracy due to eye-tracking and follow-up scan capabilities.

Keywords

Optical coherence tomography, retinal nerve fibre layer, multiple sclerosis, axonal loss, optic neuritis

Article:

Multiple sclerosis (MS) is an immune-mediated disease of the central nervous system (CNS) with inflammatory demyelinating lesions and neuronal loss that is clinically characterised by unpredictable clinical relapses, remissions and progression of disability over time.1–3 Damage occurs to the myelin sheath that surrounds and protects nerve cells; this slows down or blocks messages between the brain and the body, leading to the symptoms of MS. The disease usually begins with one or more clinically isolated syndrome (CIS) leading to a relapsing– remitting phase (RRMS) that is accompanied by a varying degree of impairment.2 After 10–15 years, approximately 50% of these patients advance to the secondary progressive form of the disease, which is characterised by a slow but progressive decline in performance with or without superimposed relapses.4,5 Approximately 10–15% of MS patients show progression from the onset (primary progressive MS [PPMS]).6,7 Symptoms are highly heterogeneous from one patient to another. More recently, our attention has been focused on the nonphysical symptoms such as fatigue and cognitive symptoms.8–11
Despite significant advances in treatment, MS remains a highly disabling disease, and in many cases significantly reduces life expectancy.12 Recent studies have shown that initiating treatment early with a disease-modifying drug, possibly during CIS, can provide significant advantages over delaying it until symptoms are more apparent. This has generated much interest and has modified treatment practices in MS.13,14 However, some neurologists have questioned the long-term benefit of treating everyone with CIS, suggesting that in some cases the disease will not progress and that greater investigation of patients is warranted before starting more appropriately tailored therapies.15
Acute idiopathic demyelinating optic neuritis (ON) is a frequent early manifestation of MS that is often indicative of early disease and can be predictive of later progressive stages.16 Optical coherence tomography (OCT) is an evolving technique that has the potential not only to diagnose ON but also to provide a valuable assessment of MS.17 This review will consider the evidence for using OCT in patients with ON and its potential role as a tool for routinely monitoring MS.

The Role of Magnetic Resonance Imaging in Multiple Sclerosis

Magnetic resonance imaging (MRI) has revolutionised the diagnosis of MS and greatly facilitated our understanding of MS. Diagnostic criteria based on both clinical and MRI findings have been proposed and have been adopted by many treatment centres.18 The presence of MRI lesions at symptom onset was found to be correlated with the development of clinically definite MS (CDMS). In patients with one or more T2-weighted lesion at baseline, 56% developed MS within 10 years.19 Neurological damage starts before symptoms become apparent. The presence of gadolinium (Gd)-enhancing lesions generally indicates current disease activity and is used as one of the key criteria for the assessment of the effectiveness of a new drug. Other key MRI variables include T2 lesion load, indicating the global burden of the disease, and T1 lesion load (black holes). The Gd-enhancing lesions and T2 lesion load are considered to be related to the degree of inflammation and provide an approximation of the demyelinating component of the disease, whereas the black holes and brain and spinal cord atrophy are more related to the degenerative component of MS.20 However, MRI is an imperfect tool that measures the results of many types of tissue loss rather than specifically nerve damage itself. Furthermore, extensive lesions and brain shrinking occur relatively late in the progression of the disease and this can be confounded by inflammation in MS that may increase overall volume. MRI is therefore not a good tool for the detection of MS in its early stages. There is an urgent need for tools able to detect axonal loss early. In addition, MRI facilities are expensive and require expertise and considerable resources to operate, and are mostly confined to specialist centres. MRI investigation is thus not readily available to patients with MS in many locations, and for some people scanning can be an unpleasant procedure.

Optic Neuritis in Multiple Sclerosis

The visual system is often affected in MS and, as the retina is an integral part of the central nervous system (CNS), examination of the eye enables unmyelinated axons of the CNS to be visualised directly. ON is inflammation with accompanying demyelination in the optic nerve that may cause complete or partial loss of vision. It is frequently the initial clinical manifestation of MS and is reported in 94–96% of MS autopsy cases.21 Although there is a broad age range at onset, most patients with acute demyelinating ON are young (20–45 years of age).22,23 There is a gender difference: women are three times as likely as men to develop ON.22 A patient with typical demyelinating ON usually experiences a decline in vision over a seven- to 10-day period, often characterised by a decline in contrast sensitivity.24 The progression of visual loss beyond two weeks is distinctly unusual and visual acuity usually recovers well.
In the Optic Neuritis Treatment Trial (ONTT),25 which investigated the use of corticosteroids to treat a population of 448 patients with ON, the majority (92%) of patients had pain, particularly with eye movements. In a patient with typical ON, some recovery of vision should occur within 30 days of onset. Clinical features that suggest non-typical ON include the presence of retinal haemorrhages, a markedly swollen nerve, retinal exudates, the absence of pain and the presence of no light-perception vision at onset. These patients have a lower risk of developing MS, particularly when their baseline MRI scan is normal.19 Approximately 50–80% of patients with ON have periventricular white-matter abnormalities consistent with demyelination on an initial MRI scan.26
In the ONTT, 10 years after acute ON the presence or absence of MRI lesions was the main factor in determining the risk of MS:19 56% of patients with one or more white-matter lesion on their baseline brain MRI scan developed MS, whereas 22% of patients with a normal baseline MRI developed MS at 10 years. The presence of oligoclonal bands in the CSF is also an independent risk factor for MS.27 Subclinical or chronic forms of demyelinating ON in which the patient notices a gradual decline in vision instead of acute vision loss followed by improvement may also develop in MS. These patients may show abnormalities on neuro-ophthalmological examination, including field loss, pupillary abnormalities and disc pallor.28 Subclinical ON can be sensitively detected using lower-contrast letter acuity testing.29 ON and other visual defects contribute significantly to the reduction in quality of life of MS patients.30
In patients with acute ON, treatment with a three-day course of high-dose (1g/day) intravenous corticosteroids is usually recommended. The ONTT used three treatment groups: intravenous methylprednisolone for three days followed by an oral prednisone taper; oral prednisone; and oral placebo.31 The use of oral corticosteroids was associated with an increased risk of recurrent ON five years after an initial bout of ON; patients who received oral prednisone (1mg/kg) had the highest rate of recurrence (41%) compared with those who received methylprednisolone or placebo (25% for both groups). However, there was no significant difference in the long-term risk of MS.

Optical Coherence Tomography

One of the most exciting developments in ophthalmic imaging is arguably OCT, which was introduced in 199132 and has been a part of clinical practice since 1995.33 OCT is widely used to obtain high-resolution images of the retina and the anterior segment of the eye. Figure 1 provides a summary of the operation of OCT. OCT creates images by reflecting laser light on the retina to generate a cross-sectional image. The extent of the reflectivity differs between cell types in retinal layers. OCT measures retinal nerve fibre layer (RNFL) thickness utilising interferometry – the technique of determining the properties of two waves by analysing the pattern of interference created by their superposition.34 The light source is a super-luminescent diode. OCT captures cross-sectional images from a series of lateral adjacent depth-scans. OCT therefore determines overall thickness and quadrant thicknesses in different pathological conditions including ON or MS and compared with normative values (see Figure 2). OCT has the advantages of being non-invasive, easy to use and quantitative. Its sensitivity allows direct visualisation and measurement of RNFL thickness and macular volume with micron-scale resolution (see Figure 3).35,36 The latest technical improvements, such as higher resolution (between 2 and 3μm) and dual laser beams to overcome eye movements, have enabled these instruments to gain a high clinical utility in predicting MS disease course and determining treatment response.33,37

Optical Coherence Tomography Studies in Optic Neuritis and Multiple Sclerosis

Among patients with ON, optic nerve atrophy has often been detected by MRI.38–40 In a study in the UK including 10 patients with a history of ON, a correlation was found between the mean loss of cross-sectional area of the optic nerve and changes in the amplitude of visual-evoked potential (VEP), implicating axonal loss in this progressive atrophy.39 In ON and MS, axonal loss is an early pathological feature despite clinical recovery and lack of clinical symptoms. Even in the absence of a history of ON, the eyes of patients with MS have reduced numbers of retinal ganglion cell axons in pathological studies.21
Axonal degeneration in the RNFL of patients with MS, as observed in ophthalmoscopic studies, is detectable in some patients before any visual signs or symptoms of ON have appeared, and has been associated with electrophysiological abnormalities as measured with visual-evoked response testing.41 More recent evidence also supports axonal loss as an early event in the clinical course of MS,42 and optic nerve atrophy is detectable with MRI within months after a single episode of ON. Recent studies using OCT provide direct evidence that patients with only partial recovery from a single ON episode were found to have significantly reduced RNFL thickness compared with healthy controls. This reduction correlated with the loss of visual acuity. Thinning of the RNFL in these patients was also shown to be significantly correlated with optic nerve atrophy, detected by MRI as reduced optic nerve cross-sectional area.40,43 Even patients with MS but without a history of ON have been shown to have reduced RNFL thickness compared with healthy controls.44 Visual function correlated well with RNFL thickness in patients with MS: every one-line decrease in low-contrast letter acuity and contrast sensitivity test score was associated with an average 4μm thinning of the RNFL.44
Some correlations have been shown between RNLF thickness and disease characteristics. In one study RRMS patients who experienced relapses or a disability progression had a significantly thinner average RNLF compared with patients who remained relapse-free over a two-year period.45 Lower average RNFL thickness was correlated with patients with more active disease and greater Expanded Disability Status Scale (EDSS) at baseline and greater increase of EDSS over two years. The correlations are better in the temporal quadrant.46 Correlations have also been found between RNFL thickness and performance on some tests of cognitive function in MS patients, particularly the symbol digit modality test.45 Despite some conflicting results, longitudinal studies have shown a progressive thinning of RNLF thickness over time, with lower values in progressive MS than in RRMS.47 In patients with CIS who had no history of ON, our group in Lille failed to find significant differences in RNLF thickness, and changes did not increase the risk of conversion to MS after a six-month period of follow-up.48 However, our analysis was not performed using the latest technical methods. Since RNLF thickness may be associated with the degenerative component of MS, OCT measurements and atrophy of the brain, assessed using the brain parenchymal fraction (BPF), were compared. This identified a partial but significant correlation between BPF and minimum RNLF thickness, and the correlation was stronger in RRMS than in PPMS patients.49,50 Determination of axonal thickness in the retina by OCT can therefore provide concurrent information about MRI brain abnormality in MS.
The reliability of OCT in MS was demonstrated in a study in the US. A total of 396 patients with MS and 153 healthy controls were assessed using OCT at three different medical centres; the results showed excellent inter- and intra-rater reproducibility (intra-class correlation [ICC] 0.89 and 0.98, respectively).51 In addition, there was excellent inter-visit correlation (ICC 0.91). These results indicated that OCT can be reliably performed at different centres to assess MS patients and can be performed by different operators at different times, with the results remaining comparable.
The feasibility of using OCT as an alternative to MRI scanning for monitoring the effects of glatiramer acetate versus placebo treatment on the condition of the optic nerve is being assessed in a study in The Netherlands.52 This study will involve a target 60 patients with clinically diagnosed MS with or without ON, and will also determine the mean change in RNFL in both eyes and other ophthalmological parameters. Another study is investigating the correlation between cognition and RNFL thickness determined by OCT in a group of 20 patients with MS who are receiving either natalizumab or an active comparator.53 These small studies may provide additional evidence justifying the use of OCT as a lower-cost alternative for monitoring MS patients in both clinical trials and clinical practice.

Future Perspectives

Data from longitudinal and multicentre studies comparing OCT scans in patients with different MS subtypes and treatment regimens are limited. In addition, correlations of up-to-date OCT measurements with MRI and other clinical tests (physical evaluations, cognitive tests) have been mostly obtained in small patient populations assessed during short follow-up periods and correlated with single parameters.54 There is consequently a need for more extensive studies that demonstrate the value of OCT in MS in larger populations than used to date. Future perspectives should therefore include: prospective and long-term studies including patients with different types of MS; confirmation of the relationship between MRI markers of disease activity, including RNLF, and clinical outcomes; and assessment of RNLF thickness in response to treatment. These studies need to be performed with the more advanced OCT instruments with facilities that include a realtime eye-tracking system. ■

Article Information:
Disclosure

The authors have no conflicts of interest to declare.

Correspondence

Patrick Vermersch, Pôle de Neurologie, Hôpital R Salengro, Université de Lille Nord de France, 59037 Lille cedex, France. E: patrick.vermersch@chru-lille.fr

Received

2010-05-25T00:00:00

References

  1. Confavreux C, Compston A, McAlpine Multiple Sclerosis: The natural history of multiple sclerosis, Elsevier, 2005;183–269.
  2. Ebers GC, Natural history of multiple sclerosis, J Neurol Neurosurg Psychiatry, 2001;71(Suppl. 2):ii16–19.
  3. Pugliatti M, Rosati G, Carton H, et al., The epidemiology of multiple sclerosis in Europe, Eur J Neurol, 2006;13:700–722.
  4. Polman CH, Uitdehaag BM, Drug treatment of multiple sclerosis, BMJ, 2000;321:490–94.
  5. Weinshenker BG, Bass B, Rice GP, et al., The natural history of multiple sclerosis: a geographically based study. I. Clinical course and disability, Brain, 1989;112(Pt 1):133–46.
  6. Koch M, Kingwell E, Rieckmann P, et al., The natural history of primary progressive multiple sclerosis, Neurology, 2009;73:1996–2002.
  7. Miller DH, Leary SM, Primary-progressive multiple sclerosis, Lancet Neurol, 2007;6:903–12.
  8. Benedict RH, Wahlig E, Bakshi R, et al., Predicting quality of life in multiple sclerosis: accounting for physical disability, fatigue, cognition, mood disorder, personality, and behavior change, J Neurol Sci, 2005;231:29–34.
  9. Diamond BJ, Johnson SK, Kaufman M, et al., Relationships between information processing, depression, fatigue and cognition in multiple sclerosis, Arch Clin Neuropsychol, 2008;23:189–99.
  10. Oken BS, Flegal K, Zajdel D, et al., Cognition and fatigue in multiple sclerosis: Potential effects of medications with central nervous system activity, J Rehabil Res Dev, 2006;43: 83–90.
  11. Simioni S, Ruffieux C, Bruggimann L, et al., Cognition, mood and fatigue in patients in the early stage of multiple sclerosis, Swiss Med Wkly, 2007;137:496–501.
  12. Grytten Torkildsen N, Lie SA, Aarseth JH, et al., Survival and cause of death in multiple sclerosis: results from a 50-year follow-up in Western Norway, Mult Scler, 2008;14: 1191–8.
  13. Doggrell SA, Good results for early treatment of clinically isolated syndrome prior to multiple sclerosis with interferon beta-1b and glatiramer group, Expert Opin Pharmacother, 2010;11:1225–30.
  14. Tintore M, New options for early treatment of multiple sclerosis, J Neurol Sci, 2009;277(Suppl. 1):S9–S11.
  15. Gilmore C, Cottrell D, Scolding N, et al., A window of opportunity for no treatment in early multiple sclerosis?, Mult Scler, 2010;16:756–9.
  16. Burton EV, Greenberg BM, Frohman EM, Optic neuritis: A mechanistic view, Pathophysiology, 2010 May 14 (Epub ahead of print).
  17. Oreja-Guevara C, Noval S, Manzano B, et al., Optic neuritis, multiple sclerosis-related or not: structural and functional study, Neurologia, 2010;25:78–82.
  18. Polman CH, Reingold SC, Edan G, et al., Diagnostic criteria for multiple sclerosis: 2005 revisions to the “McDonald Criteria”, Ann Neurol, 2005;58:840–46.
  19. Beck RW, Trobe JD, Moke PS, et al., High- and low-risk profiles for the development of multiple sclerosis within 10 years after optic neuritis: experience of the optic neuritis treatment trial, Arch Ophthalmol, 2003;121:944–9.
  20. Meier DS, Weiner HL, Khoury SJ, et al., Magnetic resonance imaging surrogates of multiple sclerosis pathology and their relationship to central nervous system atrophy, J Neuroimaging, 2004;14:46S–53S.
  21. Evangelou N, Konz D, Esiri MM, et al., Size-selective neuronal changes in the anterior optic pathways suggest a differential susceptibility to injury in multiple sclerosis, Brain, 2001;124:1813–20.
  22. Balcer LJ, Clinical practice. Optic neuritis, N Engl J Med, 2006;354:1273–80.
  23. Shams PN, Plant GT, Optic neuritis: a review, Int MS J, 2009;16:82–9.
  24. Beck RW, Cleary PA, Anderson MM, Jr., et al., A randomized, controlled trial of corticosteroids in the treatment of acute optic neuritis. The Optic Neuritis Study Group, N Engl J Med, 1992;326:581–8.
  25. Optic Neuritis Study Group, The clinical profile of optic neuritis. Experience of the Optic Neuritis Treatment Trial. Optic Neuritis Study Group, Arch Ophthalmol, 1991;109: 1673–8.
  26. Morrissey SP, Miller DH, Kendall BE, et al., The significance of brain magnetic resonance imaging abnormalities at presentation with clinically isolated syndromes suggestive of multiple sclerosis. A 5-year follow-up study, Brain, 1993;116(Pt 1):135–46.
  27. Tintore M, Rovira A, Rio J, et al., Do oligoclonal bands add information to MRI in first attacks of multiple sclerosis?, Neurology, 2008;70:1079–83.
  28. Newman NJ, Multiple sclerosis and related demyelinating diseases. In: Miller NR, Newman NJ (eds.), Walsh and Hoyt’s Clinical Neuro-Ophthalmology, Baltimore: Williams and Wilkins, 1998;5539–76.
  29. Baier ML, Cutter GR, Rudick RA, et al., Low-contrast letter acuity testing captures visual dysfunction in patients with multiple sclerosis, Neurology, 2005;64:992–5.
  30. Mowry EM, Loguidice MJ, Daniels AB, et al., Vision related quality of life in multiple sclerosis: correlation with new measures of low and high contrast letter acuity, J Neurol Neurosurg Psychiatry, 2009;80:767–72.
  31. The Optic Neuritis Study Group, Visual function 5 years after optic neuritis: experience of the Optic Neuritis Treatment Trial. The Optic Neuritis Study Group, Arch Ophthalmol, 1997;115:1545–52.
  32. Huang D, Swanson EA, Lin CP, et al., Optical coherence tomography, Science, 1991;254:1178–81.
  33. van Velthoven ME, Faber DJ, Verbraak FD, et al., Recent developments in optical coherence tomography for imaging the retina, Prog Retin Eye Res, 2007;26:57–77.
  34. Frohman EM, Fujimoto JG, Frohman TC, et al., Optical coherence tomography: a window into the mechanisms of multiple sclerosis, Nat Clin Pract Neurol, 2008;4:664–75.
  35. Monteiro ML, Leal BC, Rosa AA, et al., Optical coherence tomography analysis of axonal loss in band atrophy of the optic nerve, Br J Ophthalmol, 2004;88:896–9.
  36. Sergott RC, Optical coherence tomography: measuring in-vivo axonal survival and neuroprotection in multiple sclerosis and optic neuritis, Curr Opin Ophthalmol, 2005;16:346–50.
  37. Sakata LM, Deleon-Ortega J, Sakata V, et al., Optical coherence tomography of the retina and optic nerve – a review, Clin Experiment Ophthalmol, 2009;37:90–99.
  38. Hickman SJ, Optic nerve imaging in multiple sclerosis, J Neuroimaging, 2007;17(Suppl. 1):42S–5S.
  39. Hickman SJ, Brierley CM, Brex PA, et al., Continuing optic nerve atrophy following optic neuritis: a serial MRI study, Mult Scler, 2002;8:339–42.
  40. Trip SA, Schlottmann PG, Jones SJ, et al., Optic nerve atrophy and retinal nerve fibre layer thinning following optic neuritis: evidence that axonal loss is a substrate of MRI-detected atrophy, Neuroimage, 2006;31:286–93.
  41. Feinsod M, Hoyt WF, Subclinical optic neuropathy in multiple sclerosis. How early VER components reflect axon loss and conduction defects in optic pathways, J Neurol Neurosurg Psychiatry, 1975;38:1109–14.
  42. Filippi M, Bozzali M, Rovaris M, et al., Evidence for widespread axonal damage at the earliest clinical stage of multiple sclerosis, Brain, 2003;126:433–7.
  43. Trip SA, Schlottmann PG, Jones SJ, et al., Retinal nerve fiber layer axonal loss and visual dysfunction in optic neuritis, Ann Neurol, 2005;58:383–91.
  44. Fisher JB, Jacobs DA, Markowitz CE, et al., Relation of visual function to retinal nerve fiber layer thickness in multiple sclerosis, Ophthalmology, 2006;113:324–32.
  45. Toledo J, Sepulcre J, Salinas-Alaman A, et al., Retinal nerve fiber layer atrophy is associated with physical and cognitive disability in multiple sclerosis, Mult Scler, 2008;14:906–12.
  46. Sepulcre J, Murie-Fernandez M, Salinas-Alaman A, et al., Diagnostic accuracy of retinal abnormalities in predicting disease activity in MS, Neurology, 2007;68:1488–94.
  47. Costello F, Hodge W, Pan YI, et al., Differences in retinal nerve fiber layer atrophy between multiple sclerosis subtypes, J Neurol Sci, 2009;281:74–9.
  48. Outteryck O, Zephir H, Defoort S, et al., Optical coherence tomography in clinically isolated syndrome: no evidence of subclinical retinal axonal loss, Arch Neurol, 2009;66:1373–7.
  49. Gordon-Lipkin E, Chodkowski B, Reich DS, et al., Retinal nerve fiber layer is associated with brain atrophy in multiple sclerosis, Neurology, 2007;69:1603–9.
  50. Grazioli E, Zivadinov R, Weinstock-Guttman B, et al., Retinal nerve fiber layer thickness is associated with brain MRI outcomes in multiple sclerosis, J Neurol Sci, 2008;268:12–17.
  51. Cettomai D, Pulicken M, Gordon-Lipkin E, et al., Reproducibility of optical coherence tomography in multiple sclerosis, Arch Neurol, 2008;65:1218–22.
  52. NCT00910598, Optical Coherence Tomography: Glatiramer in Clinically Isolated Syndrome or Early Relapsing Remitting Multiple Sclerosis (MS) (OCTIMS), 2009. Available at: clinicaltrials.gov/ct2/show/NCT00910598? term=OCTIMS&rank=1 (accessed October 2009).
  53. NCT01071512, Tysabri Effects on Cognition and Neurodegeneration in Multiple Sclerosis, 2010. Available at: clinicaltrials.gov/ct2/show/NCT01071512? term=optical+coherence+tomography+AND+multiple+ sclerosis&rank=3 (accessed February 2010).
  54. Henderson AP, Trip SA, Schlottmann PG, et al., A preliminary longitudinal study of the retinal nerve fiber layer in progressive multiple sclerosis, J Neurol, 2010;257:1083–91.

Further Resources

Share this Article
Related Content In Multiple Sclerosis
Multiple Sclerosis
What Fluid Biomarkers Tell Us at Different Stages of Multiple Sclerosis
Georgina Arrambide Read Time: 5 mins

touchREVIEWS in Neurology. 2024;20(1):Online ahead of journal publication

Multiple sclerosis (MS) is a complex disease that can pose significant challenges in diagnosis, monitoring and treatment. Over the years, the quest for more precise and accessible diagnostic tools has led to the exploration of different fluid biomarkers in cerebrospinal fluid (CSF) or serum. Fluid biomarkers can offer insights into the diagnosis, prognosis and treatment […]

Multiple Sclerosis
Foreword: touchREVIEWS in Neurology, Volume 19, Issue 2, 2023
Read Time: 2 mins

In the latest edition of touchREVIEWS in Neurology, we are pleased to present a collection of insightful articles that highlight the current landscape and future directions in neurological research and treatment. Firstly, Rajvinder Karda opens this issue with a compelling expert interview on the future of SCN1A gene-targeting research for the treatment of Dravet syndrome. […]

Multiple Sclerosis
Paradoxical Tumefactive Worsening of Multiple Sclerosis After Natalizumab Initiation: A Case Report
Cathal Ahern Read Time: 7 mins

touchREVIEWS in Neurology. 2023;19(2):19-22

Multiple sclerosis (MS) is a chronic, immune-mediated disorder of the central nervous system characterized by inflammation, demyelination and neurodegeneration. Natalizumab is a widely used anti-α4 integrin inhibitor for treating highly active MS. In the pivotal trials of natalizumab for MS, the SENTINEL and AFFIRM trials, natalizumab was established to reduce the rate of clinical relapses and […]

Trending In Multiple Sclerosis:

What Fluid Biomarkers Tell Us at Different Stages of Multiple Sclerosis
Multiple Sclerosis
    • Download PDF More Actions
    Copied to clipboard!
    accredited arrow-down-editablearrow-downarrow_leftarrow-right-bluearrow-right-dark-bluearrow-right-greenarrow-right-greyarrow-right-orangearrow-right-whitearrow-right-bluearrow-up-orangeavatarcalendarchevron-down consultant-pathologist-nurseconsultant-pathologistcrosscrossdownloademailexclaimationfeedbackfiltergraph-arrowinterviewslinkmdt_iconmenumore_dots nurse-consultantpadlock patient-advocate-pathologistpatient-consultantpatientperson pharmacist-nurseplay_buttonplay-colour-tmcplay-colourAsset 1podcastprinter scenerysearch share single-doctor social_facebooksocial_googleplussocial_instagramsocial_linkedin_altsocial_linkedin_altsocial_pinterestlogo-twitter-glyph-32social_youtubeshape-star (1)tick-bluetick-orangetick-red tick-whiteticktimetranscriptup-arrowwebinar Sponsored Department Location NEW TMM Corporate Services Icons-07NEW TMM Corporate Services Icons-08NEW TMM Corporate Services Icons-09NEW TMM Corporate Services Icons-10NEW TMM Corporate Services Icons-11NEW TMM Corporate Services Icons-12Salary £ TMM-Corp-Site-Icons-01TMM-Corp-Site-Icons-02TMM-Corp-Site-Icons-03TMM-Corp-Site-Icons-04TMM-Corp-Site-Icons-05TMM-Corp-Site-Icons-06TMM-Corp-Site-Icons-07TMM-Corp-Site-Icons-08TMM-Corp-Site-Icons-09TMM-Corp-Site-Icons-10TMM-Corp-Site-Icons-11TMM-Corp-Site-Icons-12TMM-Corp-Site-Icons-13TMM-Corp-Site-Icons-14TMM-Corp-Site-Icons-15TMM-Corp-Site-Icons-16TMM-Corp-Site-Icons-17TMM-Corp-Site-Icons-18TMM-Corp-Site-Icons-19TMM-Corp-Site-Icons-20TMM-Corp-Site-Icons-21TMM-Corp-Site-Icons-22TMM-Corp-Site-Icons-23TMM-Corp-Site-Icons-24TMM-Corp-Site-Icons-25TMM-Corp-Site-Icons-26TMM-Corp-Site-Icons-27TMM-Corp-Site-Icons-28TMM-Corp-Site-Icons-29TMM-Corp-Site-Icons-30TMM-Corp-Site-Icons-31TMM-Corp-Site-Icons-32TMM-Corp-Site-Icons-33TMM-Corp-Site-Icons-34TMM-Corp-Site-Icons-35TMM-Corp-Site-Icons-36TMM-Corp-Site-Icons-37TMM-Corp-Site-Icons-38TMM-Corp-Site-Icons-39TMM-Corp-Site-Icons-40TMM-Corp-Site-Icons-41TMM-Corp-Site-Icons-42TMM-Corp-Site-Icons-43TMM-Corp-Site-Icons-44TMM-Corp-Site-Icons-45TMM-Corp-Site-Icons-46TMM-Corp-Site-Icons-47TMM-Corp-Site-Icons-48TMM-Corp-Site-Icons-49TMM-Corp-Site-Icons-50TMM-Corp-Site-Icons-51TMM-Corp-Site-Icons-52TMM-Corp-Site-Icons-53TMM-Corp-Site-Icons-54TMM-Corp-Site-Icons-55TMM-Corp-Site-Icons-56TMM-Corp-Site-Icons-57TMM-Corp-Site-Icons-58TMM-Corp-Site-Icons-59TMM-Corp-Site-Icons-60TMM-Corp-Site-Icons-61TMM-Corp-Site-Icons-62TMM-Corp-Site-Icons-63TMM-Corp-Site-Icons-64TMM-Corp-Site-Icons-65TMM-Corp-Site-Icons-66TMM-Corp-Site-Icons-67TMM-Corp-Site-Icons-68TMM-Corp-Site-Icons-69TMM-Corp-Site-Icons-70TMM-Corp-Site-Icons-71TMM-Corp-Site-Icons-72