Copathology in Progressive Supranuclear Palsy: Does It Matter?

Milica Jecmenica Lukic,Barcelona Brain Bank Collaborative Group, The Mds‐Endorsed Psp Study Group ,Günter Höglinger,Armin Giese,John C Van Swieten,Oriol Grau‐Rivera,Ellen Gelpi,Claire Troakes,Carolin Kurz,Yaroslau Compta,Gesine Respondek,Thomas Arzberger,Sigrun Roeber

doi:10.1002/mds.28011

Abstract

The influence of concomitant brain pathologies on the progression rate in PSP is unclear. To analyze the frequency and severity of copathologies and their impact on the progression in PSP. We analyzed clinic-pathological features of 101 PSP patients. Diagnoses and stages of copathologies were established according to standardized criteria, including Alzheimer's disease-related pathology, argyrophilic grains, Lewy-related pathology, transactive response DNA-binding protein 43 pathology, fused in sarcoma pathology, cerebral amyloid angiopathy, and small vessel disease. Demographic data and major clinical milestones (frequency and latency to onset) were extracted from patients' files. Only 8% of 101 patients presented with pure PSP pathology without any copathology. Alzheimer's disease-related pathology was the most frequent (84%), followed by argyrophilic grains (58%), both occurring as single copathology or in combination with other proteinopathies or cerebrovascular disease. Lewy-related and transactive response DNA-binding protein 43 copathology occurred rarely (8% and 6%, respectively). Fused in sarcoma-positive cases were not found. While being common, copathology was mostly mild in severity, with the exception of frequently widespread argyrophilic grains. Small vessel disease was also frequent (65%). Cerebral amyloid angiopathy occurred only in the presence of Alzheimer's disease-related changes (25%). The copathologies did not have major impact on prevalence and time frame of major disease milestones. In PSP, concomitant neurodegenerative proteinopathies or cerebrovascular diseases are frequent, but generally mild in severity. Our data confirmed that four repeat tau is still the most relevant target for PSP, whereas the impact of copathologies on progression rate appears to be of less importance. This is relevant information for the development of disease-modifying therapies. © 2020 The Authors. Movement Disorders published by Wiley Periodicals, Inc. on behalf of International Parkinson and Movement Disorder Society.

Highlights

Our data confirmed that four repeat tau is still the most relevant target for PSP, whereas the impact of copathologies on progression rate appears to be of less importance
Correct clinical diagnoses of PSP were made in 9.9% at first clinical visit and in 72.3% the final examination (Table 1)
Given that Apolipoprotein E (APOE) ε4 was found to be the major genetic risk factor for Alzheimer;s disease (AD)-related pathology,18 we further investigated the influence of APOE status on the occurrence of such pathology in PSP

Summary

Objectives

To analyze the frequency and severity of copathologies and their impact on the progression in PSP. Given that the tempo of disease progression is mainly highlighted through the latency to reach major clinical milestones of PSP, we aimed to analyze the possible influence of concomitant brain pathology on occurrence of such milestones, in a well-characterized clinicopathological cohort of 101 autopsy-confirmed PSP patients. The main aim of our study was to analyze the possible effects of copathologies on the frequency and temporal evolution

Methods

Results

Discussion

Conclusion