Neuroinflammation predicts disease progression in progressive supranuclear palsy

Author:

Malpetti MauraORCID,Passamonti Luca,Jones Peter Simon,Street Duncan,Rittman TimothyORCID,Fryer Timothy D,Hong Young T,Vàsquez Rodriguez Patricia,Bevan-Jones William Richard,Aigbirhio Franklin I,O'Brien John TiernanORCID,Rowe James BenedictORCID

Abstract

IntroductionIn addition to tau pathology and neuronal loss, neuroinflammation occurs in progressive supranuclear palsy (PSP). However, the prognostic value of the in vivo imaging markers for these processes in PSP remains unclear. We test the primary hypothesis that baseline in vivo imaging assessment of neuroinflammation in subcortical regions predicts clinical progression in patients with PSP.MethodsSeventeen patients with PSP–Richardson’s syndrome underwent a baseline multimodal imaging assessment, including [11C]PK11195 positron emission tomography (PET) to index microglial activation, [18F]AV-1451 PET for tau pathology and structural MRI. Disease severity was measured at baseline and serially up to 4 years with the Progressive Supranuclear Palsy Rating Scale (PSPRS) (average interval of 5 months). Regional grey-matter volumes and PET ligand binding potentials were summarised by three principal component analyses (PCAs). A linear mixed-effects model was applied to the longitudinal PSPRS scores. Single-modality imaging predictors were regressed against the individuals’ estimated rate of progression to identify the prognostic value of baseline imaging markers.ResultsPCA components reflecting neuroinflammation and tau burden in the brainstem and cerebellum correlated with the subsequent annual rate of change in the PSPRS. PCA-derived PET markers of neuroinflammation and tau pathology correlated with regional brain volume in the same regions. However, MRI volumes alone did not predict the rate of clinical progression.ConclusionsMolecular imaging with PET for microglial activation and tau pathology can predict clinical progression in PSP. These data encourage the evaluation of immunomodulatory approaches to disease-modifying therapies in PSP and the potential for PET to stratify patients in early phase clinical trials.

Funder

National Institute for Health Research Cambridge Biomedical Research Centre

Cambridge Centre for Parkinson-Plus

PSP Association

Medical Research Council

Wellcome Trust

Publisher

BMJ

Subject

Psychiatry and Mental health,Neurology (clinical),Surgery

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