Dyclonine rescues frataxin deficiency in animal models and buccal cells of patients with Friedreich's ataxia

Sahdeo, Sunil; Scott, Brian D.; McMackin, Marissa Z.; Jasoliya, Mittal; Brown, Brandon M.; Wulff, Heike; Perlman, Susan; Pook, Mark A.; Cortopassi, Gino A

doi:10.1093/hmg/ddu408

Cited by 67 publications

(71 citation statements)

References 70 publications

(86 reference statements)

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“…The lack of a compensatory pathway to acetyl-CoA from fatty acid β-oxidation suggests that decreased histone acetylation could occur in FRDA through decreased cofactor availability similar to our recent observation in tumor cells [40]. This finding is also consistent with epigenetic silencing of frataxin expression that occurs in FRDA [41] as a result of the GAA expansion [4,42], which results in increased DNA [43,44] and histone methylation [45] at the expense of histone acetylation. Decreased glucose utilization in FRDA platelets also results in decreased labeling of succinyl-CoA, suggesting that without some compensatory metabolic change there could be down-regulation of protein succinylation in FRDA through decreased cofactor availability.…”

Section: Discussionsupporting

confidence: 81%

“…One pathway of epigenetic silencing arises through upregulation of histone lysine methyltransferases resulting in increased methylation of specific lysine residues on histone tails (e.g., H3K9) and inhibition of frataxin gene transcription [45]. Cosilencing of the nrf-2 gene in FRDA could potentially result from a similar pathway.…”

Section: Discussionmentioning

confidence: 99%

“…Cosilencing of the nrf-2 gene in FRDA could potentially result from a similar pathway. This would then explain the paradoxical finding that nrf-2 expression is reduced in FRDA [45]. The reduction in nrf-2 protein expression in FRDA suggests that there would be a reduced ability to mount an antioxidant response.…”

Section: Discussionmentioning

confidence: 99%

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Stable Isotopes and LC–MS for Monitoring Metabolic Disturbances in Friedreich’s Ataxia Platelets

et al. 2015

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Background Friedreich’s ataxia (FRDA) is an autosomal recessive disease with metabolic abnormalities that have been proposed to play an important role in the resulting neurodegeneration and cardiomyopathy. The inability to access the highly affected neuronal and cardiac tissues has hampered metabolic evaluation and biomarker development. Methods Employment of a LC–MS-based method to determine whether platelets isolated from patients with FRDA exhibit differentiable metabolism compared with healthy controls. Results Isotopologue analysis showed a marked decrease in glucose incorporation with a concomitant increase in palmitate-derived acyl-CoA thioesters in FRDA platelets compared with controls. Conclusion Our findings demonstrate that platelets can be used as a surrogate tissue for in vivo biomarker studies to monitor new therapeutic approaches for the treatment of FRDA.

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Section: Discussionsupporting

confidence: 81%

Section: Discussionmentioning

confidence: 99%

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Stable Isotopes and LC–MS for Monitoring Metabolic Disturbances in Friedreich’s Ataxia Platelets

et al. 2015

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“…) is currently in a Phase 2 clinical trial in FRDA patients (ClinicalTrials.gov). Interestingly, Nrf2 binds an upstream response element in the frataxin locus, and the anesthetic dyclonine has been shown to activate Nrf2, increase the mRNA and protein levels of frataxin and rescue frataxin‐dependent enzyme deficiencies in the iron‐sulfur enzymes aconitase and succinate dehydrogenase .…”

Section: Role Of Nrf2 In Mitochondrial Functionmentioning

confidence: 99%

The role of Nrf2 signaling in counteracting neurodegenerative diseases

2018

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The transcription factor Nrf2 (nuclear factor‐erythroid 2 p45‐related factor 2) functions at the interface of cellular redox and intermediary metabolism. Nrf2 target genes encode antioxidant enzymes, and proteins involved in xenobiotic detoxification, repair and removal of damaged proteins and organelles, inflammation, and mitochondrial bioenergetics. The function of Nrf2 is altered in many neurodegenerative disorders, such as Huntington's disease, Alzheimer's disease, amyotrophic lateral sclerosis, and Friedreich's ataxia. Nrf2 activation mitigates multiple pathogenic processes involved in these neurodegenerative disorders through upregulation of antioxidant defenses, inhibition of inflammation, improvement of mitochondrial function, and maintenance of protein homeostasis. Small molecule pharmacological activators of Nrf2 have shown protective effects in numerous animal models of neurodegenerative diseases, and in cultures of human cells expressing mutant proteins. Targeting Nrf2 signaling may provide a therapeutic option to delay onset, slow progression, and ameliorate symptoms of neurodegenerative disorders.

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“…A number of laboratories have reported identification of small molecule activators of FXN mRNA synthesis or frataxin protein in patient cells. These include histone deacetylase inhibitors [3, 20], erythropoietin alpha [21], dyclonine [22], gamma-interferon [23], SRC inhibitors [24], short oligonucleotides [25], and inhibitors of frataxin degradation [26]. With the exception of HDAC inhibitors and frataxin stabilizers, the mechanism of action of these compounds has yet to be elucidated.…”

Section: Introductionmentioning

confidence: 99%

Translating HDAC inhibitors in Friedreich’s ataxia

Soragni

Gottesfeld

2016

Expert Opinion on Orphan Drugs

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Introduction Friedreich's ataxia (FRDA) is an autosomal recessive neurodegenerative disease caused by expansion of a GAA·TTC triplet in the first intron of the FXN gene, encoding the essential mitochondrial protein frataxin. Repeat expansion results in transcriptional silencing through an epigenetic mechanism, resulting in significant decreases in frataxin protein in affected individuals. Since the FXN protein coding sequence is unchanged in FRDA, an attractive therapeutic approach for this disease would be to increase transcription of pathogenic alleles with small molecules that target the silencing mechanism. Areas covered We review the evidence that histone postsynthetic modifications and heterochromatin formation are responsible for FXN gene silencing in FRDA, along with efforts to reverse silencing with drugs that target histone modifying enzymes. Chemical and pharmacological properties of histone deacetylase (HDAC) inhibitors, which reverse silencing, together with enzyme target profiles and kinetics of inhibition, are discussed. Two HDAC inhibitors have been studied in human clinical trials and the properties of these compounds are compared and contrasted. Efforts to improve on bioavailability, metabolic stability, and target activity are reviewed. Expert opinion 2-aminobenzamide class I HDAC inhibitors are attractive therapeutic small molecules for FRDA. These molecules increase FXN gene expression in human neuronal cells derived from patient induced pluripotent stem cells, and in two mouse models for the disease, as well as in circulating lymphocytes in patients treated in a phase Ib clinical trial. Medicinal chemistry efforts have identified compounds with improved brain penetration, metabolic stability and efficacy in the human neuronal cell model. A clinical candidate will soon be identified for further human testing.

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Dyclonine rescues frataxin deficiency in animal models and buccal cells of patients with Friedreich's ataxia

Cited by 67 publications

References 70 publications

Stable Isotopes and LC–MS for Monitoring Metabolic Disturbances in Friedreich’s Ataxia Platelets

Stable Isotopes and LC–MS for Monitoring Metabolic Disturbances in Friedreich’s Ataxia Platelets

The role of Nrf2 signaling in counteracting neurodegenerative diseases

Translating HDAC inhibitors in Friedreich’s ataxia

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