iPSC modeling of young-onset Parkinson’s disease reveals a molecular signature of disease and novel therapeutic candidates

A. H. Laperle; S. Sances; N. Yucer; V. J. Dardov; V. J. Garcia; R. Ho; A. N. Fulton; M. R. Jones; K. M. Roxas; P. Avalos; D. West; M. G. Banuelos; Z. Shu; R. Murali; N. T. Maidment; J. E. Van Eyk; M. Tagliati; C. N. Svendsen

doi:10.1038/s41591-019-0739-1

iPSC modeling of young-onset Parkinson’s disease reveals a molecular signature of disease and novel therapeutic candidates

A. H. Laperle
, S. Sances
, N. Yucer
, V. J. Dardov
, V. J. Garcia
, R. Ho
, A. N. Fulton
, M. R. Jones
, K. M. Roxas
, P. Avalos
, D. West
, M. G. Banuelos
, Z. Shu
, R. Murali
, N. T. Maidment
, J. E. Van Eyk
, M. Tagliati
, C. N. Svendsen

Research output: Contribution to journal › Article › peer-review

108 Scopus citations

Abstract

Young-onset Parkinson’s disease (YOPD), defined by onset at <50 years, accounts for approximately 10% of all Parkinson’s disease cases and, while some cases are associated with known genetic mutations, most are not. Here induced pluripotent stem cells were generated from control individuals and from patients with YOPD with no known mutations. Following differentiation into cultures containing dopamine neurons, induced pluripotent stem cells from patients with YOPD showed increased accumulation of soluble α-synuclein protein and phosphorylated protein kinase Cα, as well as reduced abundance of lysosomal membrane proteins such as LAMP1. Testing activators of lysosomal function showed that specific phorbol esters, such as PEP005, reduced α-synuclein and phosphorylated protein kinase Cα levels while increasing LAMP1 abundance. Interestingly, the reduction in α-synuclein occurred through proteasomal degradation. PEP005 delivery to mouse striatum also decreased α-synuclein production in vivo. Induced pluripotent stem cell-derived dopaminergic cultures reveal a signature in patients with YOPD who have no known Parkinson’s disease-related mutations, suggesting that there might be other genetic contributions to this disorder. This signature was normalized by specific phorbol esters, making them promising therapeutic candidates.

Original language	English (US)
Pages (from-to)	289-299
Number of pages	11
Journal	Nature Medicine
Volume	26
Issue number	2
DOIs	https://doi.org/10.1038/s41591-019-0739-1
State	Published - Feb 1 2020
Externally published	Yes

ASJC Scopus subject areas

General Medicine
General Biochemistry, Genetics and Molecular Biology

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Laperle, A. H., Sances, S., Yucer, N., Dardov, V. J., Garcia, V. J., Ho, R., Fulton, A. N., Jones, M. R., Roxas, K. M., Avalos, P., West, D., Banuelos, M. G., Shu, Z., Murali, R., Maidment, N. T., Van Eyk, J. E., Tagliati, M., & Svendsen, C. N. (2020). iPSC modeling of young-onset Parkinson’s disease reveals a molecular signature of disease and novel therapeutic candidates. Nature Medicine, 26(2), 289-299. https://doi.org/10.1038/s41591-019-0739-1

Laperle, AH, Sances, S, Yucer, N, Dardov, VJ, Garcia, VJ, Ho, R, Fulton, AN, Jones, MR, Roxas, KM, Avalos, P, West, D, Banuelos, MG, Shu, Z, Murali, R, Maidment, NT, Van Eyk, JE, Tagliati, M & Svendsen, CN 2020, 'iPSC modeling of young-onset Parkinson’s disease reveals a molecular signature of disease and novel therapeutic candidates', Nature Medicine, vol. 26, no. 2, pp. 289-299. https://doi.org/10.1038/s41591-019-0739-1

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title = "iPSC modeling of young-onset Parkinson{\textquoteright}s disease reveals a molecular signature of disease and novel therapeutic candidates",

abstract = "Young-onset Parkinson{\textquoteright}s disease (YOPD), defined by onset at <50 years, accounts for approximately 10\% of all Parkinson{\textquoteright}s disease cases and, while some cases are associated with known genetic mutations, most are not. Here induced pluripotent stem cells were generated from control individuals and from patients with YOPD with no known mutations. Following differentiation into cultures containing dopamine neurons, induced pluripotent stem cells from patients with YOPD showed increased accumulation of soluble α-synuclein protein and phosphorylated protein kinase Cα, as well as reduced abundance of lysosomal membrane proteins such as LAMP1. Testing activators of lysosomal function showed that specific phorbol esters, such as PEP005, reduced α-synuclein and phosphorylated protein kinase Cα levels while increasing LAMP1 abundance. Interestingly, the reduction in α-synuclein occurred through proteasomal degradation. PEP005 delivery to mouse striatum also decreased α-synuclein production in vivo. Induced pluripotent stem cell-derived dopaminergic cultures reveal a signature in patients with YOPD who have no known Parkinson{\textquoteright}s disease-related mutations, suggesting that there might be other genetic contributions to this disorder. This signature was normalized by specific phorbol esters, making them promising therapeutic candidates.",

author = "Laperle, \{A. H.\} and S. Sances and N. Yucer and Dardov, \{V. J.\} and Garcia, \{V. J.\} and R. Ho and Fulton, \{A. N.\} and Jones, \{M. R.\} and Roxas, \{K. M.\} and P. Avalos and D. West and Banuelos, \{M. G.\} and Z. Shu and R. Murali and Maidment, \{N. T.\} and \{Van Eyk\}, \{J. E.\} and M. Tagliati and Svendsen, \{C. N.\}",

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AU - Laperle, A. H.

AU - Sances, S.

AU - Yucer, N.

AU - Dardov, V. J.

AU - Garcia, V. J.

AU - Ho, R.

AU - Fulton, A. N.

AU - Jones, M. R.

AU - Roxas, K. M.

AU - Avalos, P.

AU - West, D.

AU - Banuelos, M. G.

AU - Shu, Z.

AU - Murali, R.

AU - Maidment, N. T.

AU - Van Eyk, J. E.

AU - Tagliati, M.

AU - Svendsen, C. N.

PY - 2020/2/1

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N2 - Young-onset Parkinson’s disease (YOPD), defined by onset at <50 years, accounts for approximately 10% of all Parkinson’s disease cases and, while some cases are associated with known genetic mutations, most are not. Here induced pluripotent stem cells were generated from control individuals and from patients with YOPD with no known mutations. Following differentiation into cultures containing dopamine neurons, induced pluripotent stem cells from patients with YOPD showed increased accumulation of soluble α-synuclein protein and phosphorylated protein kinase Cα, as well as reduced abundance of lysosomal membrane proteins such as LAMP1. Testing activators of lysosomal function showed that specific phorbol esters, such as PEP005, reduced α-synuclein and phosphorylated protein kinase Cα levels while increasing LAMP1 abundance. Interestingly, the reduction in α-synuclein occurred through proteasomal degradation. PEP005 delivery to mouse striatum also decreased α-synuclein production in vivo. Induced pluripotent stem cell-derived dopaminergic cultures reveal a signature in patients with YOPD who have no known Parkinson’s disease-related mutations, suggesting that there might be other genetic contributions to this disorder. This signature was normalized by specific phorbol esters, making them promising therapeutic candidates.

AB - Young-onset Parkinson’s disease (YOPD), defined by onset at <50 years, accounts for approximately 10% of all Parkinson’s disease cases and, while some cases are associated with known genetic mutations, most are not. Here induced pluripotent stem cells were generated from control individuals and from patients with YOPD with no known mutations. Following differentiation into cultures containing dopamine neurons, induced pluripotent stem cells from patients with YOPD showed increased accumulation of soluble α-synuclein protein and phosphorylated protein kinase Cα, as well as reduced abundance of lysosomal membrane proteins such as LAMP1. Testing activators of lysosomal function showed that specific phorbol esters, such as PEP005, reduced α-synuclein and phosphorylated protein kinase Cα levels while increasing LAMP1 abundance. Interestingly, the reduction in α-synuclein occurred through proteasomal degradation. PEP005 delivery to mouse striatum also decreased α-synuclein production in vivo. Induced pluripotent stem cell-derived dopaminergic cultures reveal a signature in patients with YOPD who have no known Parkinson’s disease-related mutations, suggesting that there might be other genetic contributions to this disorder. This signature was normalized by specific phorbol esters, making them promising therapeutic candidates.

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iPSC modeling of young-onset Parkinson’s disease reveals a molecular signature of disease and novel therapeutic candidates

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