Protein aggregation and calcium dysregulation are hallmarks of familial Parkinson’s disease in midbrain dopaminergic neurons

By Gurvir Virdi, MSc, Minee Choi, PhD, James Evans, MSc, Anna Wernick, BSc, Dario Alessi, PhD, Tilo Kunath, Sonia Gandhi, PhD, Zhi Yao, Dilan Athauda, Stephanie Strohbuecker, Raja S. Nirujogi, Noelia Pelegrina-Hidalgo, Craig Leighton, Rebecca S. Saleeb, Olga Kopach, Haya Alrashidi, Daniela Melandri, MSc, Jimana Perez-Lloret, Plamena R. Angelova, Sergiy Sylantyev, Simon Eaton, Simon Heales, Dmitri A. Rusakov, Mathew H. Horrocks, Andrey Y. Abramov and Rickie Patani

Published November 24, 2022

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Description

Mutations in the SNCA gene cause autosomal dominant Parkinson’s disease (PD), with loss of dopaminergic neurons in the substantia nigra, and aggregation of α-synuclein. The sequence of molecular events that proceed from an SNCA mutation during development, to end-stage pathology is unknown. Utilising human-induced pluripotent stem cells (hiPSCs), we resolved the temporal sequence of SNCA-induced pathophysiological events in order to discover early, and likely causative, events. Our small molecule-based protocol generates highly enriched midbrain dopaminergic (mDA) neurons: molecular identity was confirmed using single-cell RNA sequencing and proteomics, and functional identity was established through dopamine synthesis, and measures of electrophysiological activity. At the earliest stage of differentiation, prior to maturation to mDA neurons, we demonstrate the formation of small β-sheet-rich oligomeric aggregates, in SNCA-mutant cultures. Aggregation persists and progresses, ultimately resulting in the accumulation of phosphorylated α-synuclein aggregates. Impaired intracellular calcium signalling, increased basal calcium, and impairments in mitochondrial calcium handling occurred early at day 34–41 post differentiation. Once midbrain identity fully developed, at day 48–62 post differentiation, SNCA-mutant neurons exhibited mitochondrial dysfunction, oxidative stress, lysosomal swelling and increased autophagy. Ultimately these multiple cellular stresses lead to abnormal excitability, altered neuronal activity, and cell death. Our differentiation paradigm generates an efficient model for studying disease mechanisms in PD and highlights that protein misfolding to generate intraneuronal oligomers is one of the earliest critical events driving disease in human neurons, rather than a late-stage hallmark of the disease.

Identifier (DOI)

10.1038/s41531-022-00423-7

Tags

hiPSCs (Human induced pluripotent stem cells)
Original Research

Team

Team Wood

Program

Collaborative Research Network

Theme

PD Functional Genomics

Meet the Authors

Gurvir Virdi, MSc

Key Personnel: Team Wood,

The Francis Crick Institute
Minee Choi, PhD

Key Personnel: Team Wood,

The Francis Crick Institute
James Evans, MSc

Key Personnel: Team Wood,

University College London
Anna Wernick, BSc

Key Personnel: Team Hardy, Team Wood,

University College London
Dario Alessi, PhD

Lead PI (Core Leadership): Team Alessi,

University of Dundee
Tilo Kunath
Sonia Gandhi, PhD

Co-PI (Core Leadership): Team Wood,

University College London
Zhi Yao
Dilan Athauda
Stephanie Strohbuecker
Raja S. Nirujogi
Noelia Pelegrina-Hidalgo
Craig Leighton
Rebecca S. Saleeb
Olga Kopach
Haya Alrashidi
Daniela Melandri, MSc

Key Personnel: Team Hardy, Team Wood,

University College London
Jimana Perez-Lloret
Plamena R. Angelova
Sergiy Sylantyev
Simon Eaton
Simon Heales
Dmitri A. Rusakov
Mathew H. Horrocks
Andrey Y. Abramov
Rickie Patani