Parkinson’s Disease Genes VPS35 and EIF4G1 Interact Genetically and Converge on α-Synuclein

Dhungel, Nripesh; Eleuteri, Simona; Li, Ling Bo; Kramer, Nicholas J.; Chartron, J.W.; Spencer, Brian; Kosberg, Kori; Fields, Jerel Adam; Stafa, Klodjan; Adame, Anthony; Lashuel, Hilal A.; Frydman, Judith; Shen, Kang; Masliah, Eliezer; Gitler, Aaron D.

doi:10.1016/j.neuron.2014.11.027

Cited by 154 publications

(181 citation statements)

References 75 publications

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“…13 Rather, the resultant pathologies are protein-specific: 1) improper folding or maintenance of structure can lead to a protein's improper degradation, such as occurs in cystic fibrosis (cystic fibrosis transmembrane conductance regulator protein) and Gaucher disease (β-glucosidase), 14,15 ; 2) a dominant negative mutation that leads to a hypo-functional peptide, which occurs in epidermolysis bullosa simplex (keratin), 16 ; 3) a gain of toxicity function, such as occurs with certain variants of APOE4 in Alzheimer disease (AD), 17 ; and 4) the accumulation of multiple, misfolded species resulting in formation of toxic polypeptides and aggregates, such as occurs with many of the neurodegenerative diseases. 18,19 …”

Section: Introduction: Proteotoxicitymentioning

confidence: 99%

Proteotoxicity and Cardiac Dysfunction

McLendon

Robbins

2015

Circulation Research

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Baseline physiological function of the mammalian heart is under the constant threat of environmental or intrinsic pathological insults. Cardiomyocyte proteins are thus subject to unremitting pressure to function optimally and this depends upon them assuming and maintaining proper conformation. This review explores the multiple defenses a cell may employ for its proteins to assume and maintain correct protein folding and conformation. There are multiple quality control mechanisms to ensure that nascent polypeptides are properly folded and mature proteins maintain their functional conformation. When proteins do misfold, either in the face of normal or pathologic stimuli or because of intrinsic mutations or post-translational modifications, they must either be refolded correctly or recycled. In the absence of these corrective processes, they may become toxic to the cell. Herein, we explore some of the underlying mechanisms that lead to proteotoxicity. The continued presence and chronic accumulation of misfolded or unfolded proteins can be disastrous in cardiomyocytes as these misfolded proteins can lead to aggregation or the formation of soluble peptides that are proteotoxic. This in turn leads to compromised protein quality control and precipitating a downward spiral of the cell's ability to maintain protein homeostasis. Some underlying mechanisms are discussed and the therapeutic potential of interfering with proteotoxicity in the heart is explored.

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Section: Introduction: Proteotoxicitymentioning

confidence: 99%

Proteotoxicity and Cardiac Dysfunction

McLendon

Robbins

2015

Circulation Research

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“…Interestingly, functional studies of trafficking proteins implicate their role in α-syn-mediated cell death (11)(12)(13). Whereas these studies imply that vesicle trafficking deficits may lead to α-syn accumulation, no studies have demonstrated a mechanistic linkage between these processes.…”

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confidence: 99%

α-Synuclein–induced lysosomal dysfunction occurs through disruptions in protein trafficking in human midbrain synucleinopathy models

Mazzulli

Zunke

Isacson

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

297

321

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Parkinson's disease (PD) is an age-related neurodegenerative disorder characterized by the accumulation of protein aggregates comprised of α-synuclein (α-syn). A major barrier in treatment discovery for PD is the lack of identifiable therapeutic pathways capable of reducing aggregates in human neuronal model systems. Mutations in key components of protein trafficking and cellular degradation machinery represent important risk factors for PD; however, their precise role in disease progression and interaction with α-syn remains unclear. Here, we find that α-syn accumulation reduced lysosomal degradation capacity in human midbrain dopamine models of synucleinopathies through disrupting hydrolase trafficking. Accumulation of α-syn at the cell body resulted in aberrant association with cis-Golgi-tethering factor GM130 and disrupted the endoplasmic reticulum-Golgi localization of rab1a, a key mediator of vesicular transport. Overexpression of rab1a restored Golgi structure, improved hydrolase trafficking and activity, and reduced pathological α-syn in patient neurons. Our work suggests that enhancement of lysosomal hydrolase trafficking may prove beneficial in synucleinopathies and indicates that human midbrain disease models may be useful for identifying critical therapeutic pathways in PD and related disorders.

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“…TIF4631 and TIF4632, of which TIF4631 is the most closely related to the human EIF4G1. To investigate the function of these genes in more detail, Dhungel et al (2015) performed two genetic screens with respectively vps35∆ and tif4631∆ yeast strains. As expected, the major functional groups, identified from the vps35∆ screen, included protein targeting and vacuolar transport while transcription and translation groups were identified by means of the tif4631∆ screen.…”

Section: Yeast Models To Study Parkinson's Disease Associated Genesmentioning

confidence: 99%