Quantitative T1 brain mapping in early relapsing-remitting multiple sclerosis: longitudinal changes, lesion heterogeneity and disability

James G Harper,Michael J Thrippleton,Gwen Kennedy,Amit Akula,Matt Justin,Belinda Weller,Angus Grossart,Alan Maclean,Anna Williams,Katarzyna Hafezi,Yingdi Chen,David Hunt,Niall Macdougall,Baljean Dhillon,Don Mahad,Aidan Hutchison,Daisy Mollison,Siddharthan Chandran,Haane Haagenrud,Lesley Macfarlane,Tracy Brunton,Patrick K A Kearns,Scott Semple,Lynn Mcmahon,Michaela Kleynhans,Annette Cooper,Tracey Hopkins,Adil Harroud,Dawn Lyle,Conni Mccarthy,Rozanna Meijboom,Rachel Dakin,Peter Connick,Adam Scotson,Jessie Chang,Christine Weaver,Agniete Kampaite,Jonathan O’Riordan,Emily Beswick,Stuart Webb,Shuna Colville,Judith Newton,Peter Foley,Julian Ng Kee Kwong,Chris Batchelor,Katherine Love,Liz Elliott,James Macdonald,Juan Larraz,Fraser Brown,Mary Monaghan,Charlotte Jardine,Denise Cranley,Katy Murray,Amy Stenson,Javier Carod Artal,Suzanne Quigley,Sara Hathorn,Kiran Jayprakash,David Perry,Stewart Wiseman,Lee Murphy,Charis Wong,Nicole White,Adam Waldman ,Sergio E Baranzini ,F Barret ,Sarah‐Jane Martin ,Neil Macleod ,Melissa K Stuart ,Lucy Joanne Kessler ,Elizabeth York ,Jg Macfarlane ,Beverly Maclennan ,Ian L Megson ,Michael L Wong ,Mark E Bastin ,Mary Joan Macleod ,James K Finlayson ,María Del C Valdés Hernández ,Eleanor Harrison ,Stella Glasmacher ,Rosemary Woodward

doi:10.1007/s00330-023-10351-6

Abstract

ObjectivesTo quantify brain microstructural changes in recently diagnosed relapsing-remitting multiple sclerosis (RRMS) using longitudinal T1 measures, and determine their associations with clinical disability.MethodsSeventy-nine people with recently diagnosed (< 6 months) RRMS were recruited from a single-centre cohort sub-study, and underwent baseline and 1-year brain MRI, including variable flip angle T1 mapping. Median T1 was measured in white matter lesions (WML), normal-appearing white matter (NAWM), cortical/deep grey matter (GM), thalami, basal ganglia and medial temporal regions. Prolonged T1 (≥ 2.00 s) and supramedian T1 (relative to cohort WML values) WML voxel counts were also measured. Longitudinal change was assessed with paired t-tests and compared with Bland-Altman limits of agreement from healthy control test-retest data. Regression analyses determined relationships with Expanded Disability Status Scale (EDSS) score and dichotomised EDSS outcomes (worsening or stable/improving).ResultsSixty-two people with RRMS (mean age 37.2 ± 10.9 [standard deviation], 48 female) and 11 healthy controls (age 44 ± 11, 7 female) contributed data. Prolonged and supramedian T1 WML components increased longitudinally (176 and 463 voxels, respectively; p < .001), and were associated with EDSS score at baseline (p < .05) and follow-up (supramedian: p < .01; prolonged: p < .05). No cohort-wide median T1 changes were found; however, increasing T1 in WML, NAWM, cortical/deep GM, basal ganglia and thalami was positively associated with EDSS worsening (p < .05).ConclusionT1 is sensitive to brain microstructure changes in early RRMS. Prolonged WML T1 components and subtle changes in NAWM and GM structures are associated with disability.Clinical relevance statementMRI T1 brain mapping quantifies disability-associated white matter lesion heterogeneity and subtle microstructural damage in normal-appearing brain parenchyma in recently diagnosed RRMS, and shows promise for early objective disease characterisation and stratification.Key Points• Quantitative T1 mapping detects brain microstructural damage and lesion heterogeneity in recently diagnosed relapsing-remitting multiple sclerosis.• T1 increases in lesions and normal-appearing parenchyma, indicating microstructural damage, are associated with worsening disability.• Brain T1 measures are objective markers of disability-relevant pathology in early multiple sclerosis.Graphical abstract

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