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The authors characterized lesion changes on quantitative susceptibility mapping and R2* at various gadolinium enhancement stages (nodular, shell-like, nonenhancing) in 64 patients with 203 lesions. They found that: 1) active MS lesions with nodular enhancement show R2* decrease but no quantitative susceptibility mapping change; 2) late active lesions with peripheral enhancement show R2* decrease and quantitative susceptibility mapping increase in the lesion center; and 3) nonenhancing lesions show both quantitative susceptibility mapping and R2* increase, reflecting iron accumulation.

Abstract

Figure 1 from paper — Example of ROIs of an MS lesion and reference at normal-appearing WM in a 44-year-old woman with MS. A, T2WI 8 months before the appearance of the enhancing lesion. B, T2WI, and C, T1WI + Gd image of 1 enhancing MS lesion. D, T2WI, E, QSM, and F, R2* images with ROIs of the enhancing lesion (left side) and the normal-appearing WM (right side). The vein inside the selected normal-appearing WM is excluded.

BACKGROUND AND PURPOSE

Quantitative susceptibility mapping and R2* are sensitive to myelin and iron changes in multiple sclerosis lesions. This study was designed to characterize lesion changes on quantitative susceptibility mapping and R2* at various gadolinium-enhancement stages.

MATERIALS AND METHODS

This study included 64 patients with MS with different enhancing patterns in white matter lesions: nodular, shell-like, nonenhancing < 1 year old, and nonenhancing 1–3 years old. These represent acute, late acute, early chronic, and late chronic lesions, respectively. Susceptibility values measured on quantitative susceptibility mapping and R2* values were compared among the 4 lesion types. Their differences were assessed with a generalized estimating equation, controlling for Expanded Disability Status Scale score, age, and disease duration.

RESULTS

We analyzed 203 lesions: 80 were nodular-enhancing, of which 77 (96.2%) were isointense on quantitative susceptibility mapping; 33 were shell-enhancing, of which 30 (90.9%) were hyperintense on quantitative susceptibility mapping; and 49 were nonenhancing lesions < 1 year old and 41 were nonenhancing lesions 1–3 years old, all of which were hyperintense on quantitative susceptibility mapping. Their relative susceptibility/R2* values were 0.5 ± 4.4 parts per billion/−5.6 ± 2.9 Hz, 10.2 ± 5.4 parts per billion/−8.0 ± 2.6 Hz, 20.2 ± 7.8 parts per billion/−3.1 ± 2.3 Hz, and 33.2 ± 8.2 parts per billion/−2.0 ± 2.6 Hz, respectively, and were significantly different (P < .005).

CONCLUSIONS

Early active MS lesions with nodular enhancement show R2* decrease but no quantitative susceptibility mapping change, reflecting myelin breakdown; late active lesions with peripheral enhancement show R2* decrease and quantitative susceptibility mapping increase in the lesion center, reflecting further degradation and removal of myelin debris; and early or late chronic nonenhancing lesions show both quantitative susceptibility mapping and R2* increase, reflecting iron accumulation.

Read this article: http://bit.ly/2dpYOFb

Quantitative Susceptibility Mapping and R2* Measured Changes during White Matter Lesion Development in Multiple Sclerosis: Myelin Breakdown, Myelin Debris Degradation and Removal, and Iron Accumulation

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