Alpha-synuclein distribution and seeding activity in rectal biopsies in Parkinson’s disease

Author:

Kluge Annika,Kintrup Carmen,Kulcsarova Kristina,Schröder Katja,Welzel Julius,Heinzel Sebastian,Wedel Thilo,Böttner Martina,Lucius Ralph,Bonkat Sarah Kim,Pendziwiat Manuela,Schoch Stephan,Ellrichmann Mark,Berg Daniela,Schaeffer Eva,Cossais FrançoisORCID

Abstract

AbstractBackgroundParkinson’s disease (PD) is characterized by the accumulation of alpha-synuclein (aSyn) pathology, not only in the brain but also in the gastrointestinal (GI) tract. This study investigates the use of unique aSyn antibodies and an aSyn seed amplification assay (SAA) for detecting pathological aSyn in rectal biopsy samples from PD patients and healthy individuals. These samples were preserved using formalin-fixed paraffin-embedded (FFPE) methods.Materials and MethodsThe study analyzed the seeding capacity of FFPE submucosal rectal biopsies from 24 PD patients and 20 healthy controls using an aSyn-SAA. The distribution of aSyn was examined using immunohistochemistry with antibodies targeting specific conformations and phosphorylated forms of aSyn at S129 and Y39.ResultsPathological forms of aSyn were found in all FFPE biopsies from PD patients, as confirmed by SAA, and these were linked to the severity of motor symptoms (MDS-UPDRS-III). However, the immunoreactive patterns of conformation-specific or phosphorylated aSyn in rectal biopsies did not show notable differences between PD patients and healthy subjects.ConclusionPathological aSyn strains are detectable in FFPE rectal biopsies from PD patients with high accuracy using aSyn-SAA. However, the utility of immunohistochemical detection with current antibodies for identifying pathological aSyn forms appears limited. The findings advocate the use of aSyn-SAA as a diagnostic tool for PD, contributing to a deeper understanding of the gut-brain connection in the disease.

Publisher

Cold Spring Harbor Laboratory

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