Sage Journals: Discover world-class research

Abstract

Background:

¹¹C-PBR28 positron emission tomography (PET), targeting the translocator protein, and paramagnetic rim lesions (PRL) have emerged as promising imaging markers of MS chronic inflammation. No consensus on which is the optimal marker exists.

Objectives:

To investigate the ability of ¹¹C-PBR28 PET and PRL assessment to identify chronic inflammation in white matter (WM) MS lesions and their relation to neurological impairment.

Methods:

Based on ¹¹C-PBR28 uptake, brain WM lesions from 30 MS patients were classified as PET active or inactive. The PRL presence was assessed on 7T phase reconstructions, T1/T2 ratio was calculated to measure WM microstructural integrity.

Results:

Less than half (44%) of non-PRL WM lesions were active on ¹¹C-PBR28 imaging either throughout the lesion (whole active) or at its periphery. PET peripherally active lesions and PRL did not differ in T1/T2 ratio and ¹¹C-PBR28 uptake. A positive correlation was observed between PRL and active PET lesion count. Whole active PET lesion volume was the strongest predictor (β = 0.97, p < 0.001) of increased Expanded Disability Status Scale scores.

Conclusion:

¹¹C-PBR28 imaging reveals more active WM lesions than 7T PRL assessment. Although PRL and PET active lesion counts are related, neurological disability is better explained by PET whole active lesion volume.

Keywords

Multiple sclerosis positron emission tomography TSPO 7T MRI smoldering lesions

Get full access to this article

View all access options for this article.

References

Popescu

Pirko

Lucchinetti

. Pathology of multiple sclerosis: Where do we stand? Continuum 2013; 19(4 Multiple Sclerosis): 901–921.

Kuhlmann

Ludwin

Prat

, et al. An updated histological classification system for multiple sclerosis lesions. Acta Neuropathol 2017; 133(1): 13–24.

Luchetti

Fransen

Van Eden

, et al. Progressive multiple sclerosis patients show substantial lesion activity that correlates with clinical disease severity and sex: A retrospective autopsy cohort analysis. Acta Neuropathol 2018; 135(4): 511–528.

Frischer

Weigand

Guo

, et al. Clinical and pathological insights into the dynamic nature of the white matter multiple sclerosis plaque. Ann Neurol 2015; 78(5): 710–721.

Dal-Bianco

Grabner

Kronnerwetter

, et al. Slow expansion of multiple sclerosis iron rim lesions: Pathology and 7 T magnetic resonance imaging. Acta Neuropathol 2017; 133(1): 25–42.

Absinta

Sati

Schindler

, et al. Persistent 7-tesla phase rim predicts poor outcome in new multiple sclerosis patient lesions. J Clin Invest 2016; 126(7): 2597–2609.

Absinta

Sati

Masuzzo

, et al. Association of chronic active multiple sclerosis lesions with disability in vivo. JAMA Neurol 2019; 76: 1474–1483.

Hamzaoui

Garcia

Boffa

, et al. Positron Emission Tomography with [¹⁸ F]-DPA-714 unveils a smoldering component in most multiple sclerosis lesions which drives disease progression. Ann Neurol 2023; 94(2): 366–383.

Nutma

Stephenson

Gorter

, et al. A quantitative neuropathological assessment of translocator protein expression in multiple sclerosis. Brain 2019; 142(11): 3440–3455.

10.

Kaunzner

Kang

Zhang

, et al. Quantitative susceptibility mapping identifies inflammation in a subset of chronic multiple sclerosis lesions. Brain 2019; 142(1): 133–145.

11.

Elliott

Rudko

Arnold

, et al. Lesion-level correspondence and longitudinal properties of paramagnetic rim and slowly expanding lesions in multiple sclerosis. Mult Scler 2023; 29(6): 680–690.

12.

Datta

Colasanti

Kalk

, et al. ¹¹C-PBR28 and ¹⁸F-PBR111 detect white matter inflammatory heterogeneity in multiple sclerosis. J Nucl Med 2017; 58(9): 1477–1482.

13.

Bodini

Poirion

Tonietto

, et al. Individual mapping of innate immune cell activation is a candidate marker of patient-specific trajectories of worsening disability in multiple sclerosis. J Nucl Med 2020; 61(7): 1043–1049.

14.

Nylund

Sucksdorff

Matilainen

, et al. Phenotyping of multiple sclerosis lesions according to innate immune cell activation using 18 kDa translocator protein-PET. Brain Commun 2022; 4(1): fcab301.

15.

Alonso-Ortiz

Levesque

Pike

. MRI-based myelin water imaging: A technical review. Magn Reson Med 2015; 73(1): 70–81.

16.

Owen

Yeo

Gunn

, et al. An 18-kDa translocator protein (TSPO) polymorphism explains differences in binding affinity of the PET radioligand PBR28. J Cereb Blood Flow Metab 2012; 32(1): 1–5.

17.

Polman

Reingold

Banwell

, et al. Diagnostic criteria for multiple sclerosis: 2010 revisions to the McDonald criteria. Ann Neurol 2011; 69(2): 292–302.

18.

Catana

Van der Kouwe

Benner

, et al. Toward implementing an MRI-based PET attenuation-correction method for neurologic studies on the MR-PET brain prototype. J Nucl Med 2010; 51(9): 1431–1438.

19.

Van der Kouwe

AJW

Benner

Salat

, et al. Brain morphometry with multiecho MPRAGE. Neuroimage 2008; 40(2): 559–569.

20.

Bagnato

Sati

Hemond

, et al. Imaging chronic active lesions in multiple sclerosis: A consensus statement. Brain 2024; 147: 2913–2933.

21.

Treaba

Conti

Klawiter

, et al. Cortical and phase rim lesions on 7 T MRI as markers of multiple sclerosis disease progression. Brain Commun 2021; 3(3): fcab134.

22.

Ganzetti

Wenderoth

Mantini

. Whole brain myelin mapping using T1- and T2-weighted MR imaging data. Front Hum Neurosci 2014; 8: 671.

23.

Ganzetti

Wenderoth

Mantini

. Mapping pathological changes in brain structure by combining T1- and T2-weighted MR imaging data. Neuroradiology 2015; 57(9): 917–928.

24.

Herranz

Gianni

Louapre

, et al. Neuroinflammatory component of gray matter pathology in multiple sclerosis. Ann Neurol 2016; 80(5): 776–790.

25.

Herranz

Hooker

Izquierdo-Garcia

, et al. Reply. Ann Neurol 2017; 81: 324–325.

26.

Dal-Bianco

Grabner

Kronnerwetter

, et al. Long-term evolution of multiple sclerosis iron rim lesions in 7 T MRI. Brain 2021; 144: 833–847.

27.

Haacke

Mittal

, et al. Susceptibility-weighted imaging: Technical aspects and clinical applications, part 1. AJNR Am J Neuroradiol 2009; 30(1): 19–30.

28.

Popescu

Frischer

Webb

, et al. Pathogenic implications of distinct patterns of iron and zinc in chronic MS lesions. Acta Neuropathol 2017; 134(1): 45–64.

29.

Zhang

Shao

, et al. Recent developments on PET radiotracers for TSPO and their applications in neuroimaging. Acta Pharm Sin B 2021; 11(2): 373–393.

30.

Lavisse

Guillermier

Herard

, et al. Reactive astrocytes overexpress TSPO and are detected by TSPO positron emission tomography imaging. J Neurosci 2012; 32(32): 10809–10818.

31.

Sucksdorff

Matilainen

Tuisku

, et al. Brain TSPO-PET predicts later disease progression independent of relapses in multiple sclerosis. Brain 2020; 143(11): 3318–3330.

32.

Polvinen

Matilainen

Nylund

, et al. TSPO-detectable chronic active lesions predict disease progression in multiple sclerosis. Neurol Neuroimmunol Neuroinflamm 2023; 10(5): e200133.

33.

Nutma

Fancy

Weinert

, et al. Translocator protein is a marker of activated microglia in rodent models but not human neurodegenerative diseases. Nat Commun 2023; 14(1): 5247.

34.

Nutma

Gebro

Marzin

, et al. Activated microglia do not increase 18 kDa translocator protein (TSPO) expression in the multiple sclerosis brain. Glia 2021; 69(10): 2447–2458.

Supplementary Material

Please find the following supplemental material available below.

For Open Access articles published under a Creative Commons License, all supplemental material carries the same license as the article it is associated with.

For non-Open Access articles published, all supplemental material carries a non-exclusive license, and permission requests for re-use of supplemental material or any part of supplemental material shall be sent directly to the copyright owner as specified in the copyright notice associated with the article.

0.00 MB

0.02 MB

Phenotyping in vivo chronic inflammation in multiple sclerosis by combined 11 C-PBR28 MR-PET and 7T susceptibility-weighted imaging

Abstract

Background:

Objectives:

Methods:

Results:

Conclusion:

Keywords

Get full access to this article

References

Supplementary Material