Sensitivity of contrast enhanced MRI in multiple sclerosis - Effects of gadolinium dose, magnetization transfer contrast and delayed imaging

被引:150
|
作者
Silver, NC
Good, CD
Barker, GJ
MacManus, DG
Thompson, AJ
Moseley, IF
McDonald, WI
Miller, DH
机构
[1] INST NEUROL, NMR RES UNIT, LONDON WC1N 3BG, ENGLAND
[2] UCL NATL HOSP NEUROL & NEUROSURG, LONDON WC1N 3BG, ENGLAND
关键词
multiple sclerosis; magnetic resonance imaging; gadolinium enhancement; magnetization transfer contrast;
D O I
10.1093/brain/120.7.1149
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
Although clinical end points remain the definitive measure of therapeutic efficacy in multiple sclerosis, more sensitive markers of disease activity are required to screen potential disease-modifying agents. The use of gadolinium contrast-media in MRI studies increases both the reliability and sensitivity of detecting active lesions in multiple sclerosis. We studied three potential methods for further improving sensitivity; the use of 0.3 mmol/kg (triple-dose) gadolinium-diethylenetriaminepenta-acetic acid (Gd-DTPA), magnetization transfer (MT) contrast imaging and the introduction of a delay between contrast-medium injection and imaging. Fifty patients were studied (seven with benign, 14 with relapsing-remitting 10 with secondary progressive, 16 with primary progressive and three with transitional multiple sclerosis). Imaging was performed on two occasions, 24-72 h apart, with triple- and single-dose Gd-DTPA. Pairs of contrast-enhanced T-1-weighted studies, with and without MI: were obtained at three different times, i.e. within early (0-20 min), short-delay (20-40 min) and long-delay (40-60 min) time-windows. Nineteen patients did not have the full complement of studies. Seven patients suffered minor self-limiting adverse events possibly related to triple-dose Gd-DTPA. Overall, triple-dose Gd-DTPA resulted in a 75% increase in the number of enhancing lesions detected compared with the single dose (P < 0.002). The use of MT or delay alone did not significantly increase the sensitivity of either single- or triple-dose studies. The combination of MT and short delay increased the number of enhancing lesions detected with single-dose Gd-DTPA by 47% (P < 0.05) and with triple-dose Gd-DTPA by 27% (P < 0.01). Detection was not significantly further improved by a long delay. The most sensitive modality was MT imaging with a long delay following triple-dose Gd-DTPA, resulting in the detection of 126% more enhancing lesions than in standard single-dose imaging (P < 0.05). This applies to all subgroups except for primary progressive multiple sclerosis, in which none of these methods alone or in combination improved the sensitivity. We conclude that for relapsing-remitting and secondary progressive multiple sclerosis, the combination of triple-dose Gd-DTPA and delayed MT imaging more than doubles the sensitivity to contrast-enhancing lesions.
引用
收藏
页码:1149 / 1161
页数:13
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