A Stearoyl–Coenzyme A Desaturase Inhibitor Prevents Multiple Parkinson Disease Phenotypes in <scp>α</scp>‐Synuclein Mice

Nuber, Silke; Nam, Alice Y; Rajsombath, Molly M; Cirka, Haley; Hronowski, Xiaoping; Wang, Junmin; Hodgetts, Kevin J.; Kalinichenko, L. S.; Müller, Christian P.; Lambrecht, Vera; Winkler, Jürgen; Weihofen, Andreas; Imberdis, Thibaut; Dettmer, Ulf; Fanning, Saranna; Selkoe, Dennis J.

doi:10.1002/ana.25920

Cited by 54 publications

(82 citation statements)

References 68 publications

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“…These yeast models have proven to be powerful platforms that have enabled the discovery of several important genetic and small-molecule modifiers of disease protein aggregation and toxicity. Importantly, these modifiers have translated to more complex model systems including worm, fly, mouse, and neuronal models of neurodegenerative disease ( Armakola et al, 2012 ; Barmada et al, 2015 ; Becker et al, 2017 ; Caraveo et al, 2014 ; Caraveo et al, 2017 ; Chung et al, 2013 ; Cooper et al, 2006 ; Dhungel et al, 2015 ; Elden et al, 2010 ; Fanning et al, 2019 ; Gitler et al, 2009 ; Jackrel et al, 2014 ; Jackson et al, 2015 ; Ju et al, 2011 ; Khurana et al, 2017 ; Kim et al, 2014a ; Nuber et al, 2020 ; Su et al, 2010 ; Tardiff et al, 2013 ; Tardiff et al, 2012 ; Vincent et al, 2018 ). Indeed, potential therapeutics for ALS (e.g.…”

Section: Resultsmentioning

confidence: 99%

Therapeutic genetic variation revealed in diverse Hsp104 homologs

March

Sweeney

Kim

et al. 2020

eLife

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The AAA+ protein disaggregase, Hsp104, increases fitness under stress by reversing stress-induced protein aggregation. Natural Hsp104 variants might exist with enhanced, selective activity against neurodegenerative disease substrates. However, natural Hsp104 variation remains largely unexplored. Here, we screened a cross-kingdom collection of Hsp104 homologs in yeast proteotoxicity models. Prokaryotic ClpG reduced TDP-43, FUS, and α-synuclein toxicity, whereas prokaryotic ClpB and hyperactive variants were ineffective. We uncovered therapeutic genetic variation among eukaryotic Hsp104 homologs that specifically antagonized TDP-43 condensation and toxicity in yeast and TDP-43 aggregation in human cells. We also uncovered distinct eukaryotic Hsp104 homologs that selectively antagonized α-synuclein condensation and toxicity in yeast and dopaminergic neurodegeneration in C. elegans. Surprisingly, this therapeutic variation did not manifest as enhanced disaggregase activity, but rather as increased passive inhibition of aggregation of specific substrates. By exploring natural tuning of this passive Hsp104 activity, we elucidated enhanced, substrate-specific agents that counter proteotoxicity underlying neurodegeneration.

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Section: Resultsmentioning

confidence: 99%

Therapeutic genetic variation revealed in diverse Hsp104 homologs

March

Sweeney

Kim

et al. 2020

eLife

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show abstract

Section: Resultsmentioning

confidence: 99%

“…Recently, transgenic mice that expressed a PD-associated form of αS were treated with SCD inhibitor by oral administration and were characterized [ 65 ]. Inhibition of SCD protected these mice from gait defects, resting tremor, and progressive motor decline; however, they also exhibited hair loss and dry eyes [ 65 ]. Mice heterozygous for Scd1 and expressing a PD-associated form of αS displayed less lipid-rich αS aggregates and performed better on rotarod tests [ 65 ].…”

Section: Resultsmentioning

confidence: 99%

“…Inhibition of SCD protected these mice from gait defects, resting tremor, and progressive motor decline; however, they also exhibited hair loss and dry eyes [ 65 ]. Mice heterozygous for Scd1 and expressing a PD-associated form of αS displayed less lipid-rich αS aggregates and performed better on rotarod tests [ 65 ]. As SCD inhibitors generally target all SCD isoforms and Scd1 haploinsufficiency is effective in reducing PD phenotypes, specifically inhibiting either SCD2 or hSCD5 in the brain may also be a viable method for combating αS-induced neurotoxicity without unwanted side effects.…”

Section: Resultsmentioning

confidence: 99%

“…Drugs targeting SCD1 have shown promising effects in mice to prevent Parkinson′s disease, blunt weight gain, improve glucose tolerance, promote sebaceous gland atrophy, protect against fatty liver disease, and inhibit cancer cells [ 65 , 72 ]. Despite this, topical and intraperitoneally injected SCD inhibitors produce unwanted side effects, such as dry eyes, partial eye closure, dry skin, and alopecia [ 45 , 65 , 72 , 73 ]. These side effects do not occur in SCD2KO mice, and therefore SCD2 may be a more suitable drug target than SCD1.…”

Section: Discussionmentioning

confidence: 99%

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Stearoyl-CoA Desaturase-2 in Murine Development, Metabolism, and Disease

O’Neill

Guo

Ding

et al. 2020

IJMS

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Stearoyl-CoA Desaturase-2 (SCD2) is a member of the Stearoyl-CoA Desaturase (SCD) family of enzymes that catalyze the rate-limiting step in monounsaturated fatty acid (MUFA) synthesis. The MUFAs palmitoleoyl-CoA (16:1n7) and oleoyl-CoA (18:1n9) are the major products of SCD2. Palmitoleoyl-CoA and oleoyl-CoA have various roles, from being a source of energy to signaling molecules. Under normal feeding conditions, SCD2 is ubiquitously expressed and is the predominant SCD isoform in the brain. However, obesogenic diets highly induce SCD2 in adipose tissue, lung, and kidney. Here we provide a comprehensive review of SCD2 in mouse development, metabolism, and various diseases, such as obesity, chronic kidney disease, Alzheimer′s disease, multiple sclerosis, and Parkinson′s disease. In addition, we show that bone mineral density is decreased in SCD2KO mice under high-fat feeding conditions and that SCD2 is not required for preadipocyte differentiation or the expression of PPARγ in vivo despite being required in vitro.

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Brain region-specific susceptibility of Lewy body pathology in synucleinopathies is governed by α-synuclein conformations

et al. 2022

Self Cite

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The protein α-synuclein, a key player in Parkinson’s disease (PD) and other synucleinopathies, exists in different physiological conformations: cytosolic unfolded aggregation-prone monomers and helical aggregation-resistant multimers. It has been shown that familial PD-associated missense mutations within the α-synuclein gene destabilize the conformer equilibrium of physiologic α-synuclein in favor of unfolded monomers. Here, we characterized the relative levels of unfolded and helical forms of cytosolic α-synuclein in post-mortem human brain tissue and showed that the equilibrium of α-synuclein conformations is destabilized in sporadic PD and DLB patients. This disturbed equilibrium is decreased in a brain region-specific manner in patient samples pointing toward a possible “prion-like” propagation of the underlying pathology and forms distinct disease-specific patterns in the two different synucleinopathies. We are also able to show that a destabilization of multimers mechanistically leads to increased levels of insoluble, pathological α-synuclein, while pharmacological stabilization of multimers leads to a “prion-like” aggregation resistance. Together, our findings suggest that these disease-specific patterns of α-synuclein multimer destabilization in sporadic PD and DLB are caused by both regional neuronal vulnerability and “prion-like” aggregation transmission enabled by the destabilization of local endogenous α-synuclein protein.

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A Stearoyl–Coenzyme A Desaturase Inhibitor Prevents Multiple Parkinson Disease Phenotypes in α‐Synuclein Mice

Cited by 54 publications

References 68 publications

Therapeutic genetic variation revealed in diverse Hsp104 homologs

Therapeutic genetic variation revealed in diverse Hsp104 homologs

Stearoyl-CoA Desaturase-2 in Murine Development, Metabolism, and Disease

Brain region-specific susceptibility of Lewy body pathology in synucleinopathies is governed by α-synuclein conformations

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