Magnetic resonance imaging in the evaluation of treatment in multiple sclerosis

Kappos, Ludwig; Städt, D.; Ratzka, M.; Keil, W.; Schneiderbanger-Grygier, Sigrid; Heitzer, Thomas; Poser, S.; Nadjmi, M

doi:10.1007/bf00328179

Cited by 57 publications

(22 citation statements)

References 13 publications

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“…1. It can be broadly divided into: (1) pulse sequence design for improving the LTC; ( 2 ) generation of flow images for minimizing flow-related false classifications; (3) segmentation based on fast FLAIR/MTC (referred to simply as "FLAIR/MTC" throughout the remainder of this manuscript), fast spin-echo (FSE), and flow images; and (4) volumetric analysis for tissue quantitation. A brief description of these individual steps is given below.…”

Section: Methodsmentioning

confidence: 99%

A dual approach for minimizing false lesion classifications on magnetic resonance images

Bedell¹,

Narayana²,

Wolinsky³

1997

Magnetic Resonance in Med

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Segmentation methods based on dual-echo MR images are generally prone to significant false lesion classifications. We have minimized these false classifications by (1) improving the lesion-to-tissue contrast on MR images by developing a fast spin-echo sequence that incorporates both cerebrospinal fluid signal attenuation and magnetization transfer contrast and (2) including information from MR flow images. Studies on patients with multiple sclerosis indicate that this dual approach to tissue segmentation reduces the volume of false lesion classifications by an average of 87%.

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Section: Methodsmentioning

confidence: 99%

A dual approach for minimizing false lesion classifications on magnetic resonance images

Bedell¹,

Narayana²,

Wolinsky³

1997

Magnetic Resonance in Med

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“…New silent lesions appear 5 to 10 times more frequently than do lesions associated with clinical relapses. [29][30][31] Between 50% and 80% of patients with CIS have 1 or more clinically silent T2-bright abnormalities on their baseline brain MRI. 5,6,32,33 Both the presence and the number of clinically silent lesions reflect older subclinical disease activity and are predictive of development of MS in the next 5 to 14 years.…”

Section: Radiology In the Diagnosis Of Cismentioning

confidence: 99%

Updates on Clinically Isolated Syndrome and Diagnostic Criteria for Multiple Sclerosis

Marcus

Waubant

2012

The Neurohospitalist

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Clinically isolated syndrome (CIS) is a central nervous system demyelinating event isolated in time that is compatible with the possible future development of multiple sclerosis (MS). Early risk stratification for conversion to MS helps with treatment decisions. Magnetic resonance imaging (MRI) is currently the most useful tool to evaluate risk. Cerebrospinal fluid studies and evoked potentials may also be used to assess the likelihood of MS. Four clinical trials evaluating the benefits of either interferon b (IFN-b) or glatiramer acetate (GA) within the first 3 months after a high-risk CIS demonstrate decreased rates of conversion to clinically definite MS (CDMS) and a lesser degree of MRI progression with early treatment. In the 3-, 5-, and 10-year extension studies of 2 formulations of IFN-b, the decreased conversion rate to CDMS remained meaningful when comparing early treatment of CIS to treatment delayed by a median of 2 to 3 years. Diagnostic criteria have been developed based on the clinical and MRI follow-up of large cohorts with CIS and provide guidance on how to utilize clinical activity in combination with radiographic information to diagnose MS. The most recent 2010 McDonald criteria simplify requirements for dissemination in time and space and allow for diagnosis of MS from a baseline brain MRI if there are both silent gadolinium-enhancing lesions and nonenhancing lesions on the same imaging study. The diagnostic criteria for MS require special consideration in children at risk for acute disseminated encephalomyelitis (ADEM), in older adults who may have small vessel ischemic disease, and in ethnic groups that more commonly develop neuromyelitis optica (NMO).

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“…Quantitation of hyperintensities seen on T 2 -weighted imaging, in particular the number of visible lesions and total lesion volume, has been utilized in demonstrating the effects of treatment in both relapsing-remitting and secondary progressive MS (Molyneux et al, 2001;Paty and Li, 1993;Ge et al, 2000;Paolillo, et al, 1999;Kappos et al, 1988). Clinical MRI correlations were demonstrated between relapse rate and number of lesions seen on T 2 -weighted images, suggesting a role for MRI in monitoring disease progression, and between lesion number and volume and the presence or absence of treatment (Molyneux et al, 2001;Li, 1993 IFNB MS Study Group, 1995;Miller et al, 1999).…”

Section: Multiple Sclerosismentioning

confidence: 99%

T ₂ : The Transverse Relaxation Time

Boulby

Rugg‐Gunn

2003

Quantitative MRI of the Brain

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Magnetic resonance imaging in the evaluation of treatment in multiple sclerosis

Cited by 57 publications

References 13 publications

A dual approach for minimizing false lesion classifications on magnetic resonance images

A dual approach for minimizing false lesion classifications on magnetic resonance images

Updates on Clinically Isolated Syndrome and Diagnostic Criteria for Multiple Sclerosis

T ₂ : The Transverse Relaxation Time

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Magnetic resonance imaging in the evaluation of treatment in multiple sclerosis

Cited by 57 publications

References 13 publications

A dual approach for minimizing false lesion classifications on magnetic resonance images

A dual approach for minimizing false lesion classifications on magnetic resonance images

Updates on Clinically Isolated Syndrome and Diagnostic Criteria for Multiple Sclerosis

T 2 : The Transverse Relaxation Time

Contact Info

Product

Resources

About

T ₂ : The Transverse Relaxation Time