Biofluid Markers and Tissue Biopsies Analyses for the Prodromal and Earliest Phase of Parkinson's Disease

Overview

Journal J Parkinsons Dis

Publisher Sage Publications

Specialty Neurology

Date 2024 Sep 27

PMID 39331105

Authors

Andrea Pilotto

Gianluigi Zanusso

Elena Antelmi

Ayami Okuzumi

Cinzia Zatti

Alessandro Lupini

Matilde Bongianni

Alessandro Padovani

Nobutaka Hattori

Affiliations

Soon will be listed here.

Abstract

The recent development of new methods to detect misfolded α-synuclein (αSyn) aggregates in biofluids and tissue biopsies in the earliest Parkinson's disease (PD) phases is dramatically challenging the biological definition of PD. The αSyn seed amplification methods in cerebrospinal fluid (CSF) showed high sensitivity and specificity for early diagnosis of PD and Lewy bodies disorders. Several studies in isolated REM sleep behavior disorders and other at-risk populations also demonstrated a high prevalence of CSF αSyn positivity and its potential value in predicting the phenoconversion to clinically manifested diseases. Growing evidence exists for αSyn aggregates in olfactory mucosa, skin, and other tissues in subjects with PD or at-risk subjects. DOPA decarboxylase and numerous other candidates have been additionally proposed for either diagnostic or prognostic purposes in earliest PD phases. The newly described αSyn detection in blood, through its quantification in neuronally-derived exosome vesicles, represents a technical challenge that could open a new scenario for the biological diagnosis of PD. Despite this growing evidence in the field, most of method of αSyn detection and markers still need to be validated in ongoing longitudinal studies through an accurate assessment of different prodromal disease subtypes and scenarios before being definitively implemented in clinical settings.

Citing Articles

Introduction: The Earliest Phase of Parkinson's Disease: Possibilities for Detection and Intervention.

Berg D, Bloem B, Kalia L, Postuma R J Parkinsons Dis. 2024; 14(s2):S253-S255.

PMID: 39331112 PMC: 11492101. DOI: 10.3233/JPD-249011.

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