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Literature DB >> 29427098

Mitochondrial Dysfunction in Huntington's Disease.

Catarina Carmo¹, Luana Naia^1,2, Carla Lopes^1,2, A Cristina Rego^3,4.

Abstract

Mitochondrial dysfunction has been described as an early pathological mechanism delineating the selective neurodegeneration that occurs in Huntington's disease (HD), a polyglutamine-expansion disorder that largely affects the striatum and the cerebral cortex. Over the years, mitochondria roles in eukaryotic cells (e.g. in neurons) have largely diverged from the classically attributed cell power source; indeed, mitochondria not only contribute for synthesis of several metabolites, but are also dynamic organelles that fragment and fuse to achieve a maximal bioenergetic performance, are transported along microtubules, regulate intracellular calcium homeostasis through the interaction with the endoplasmic reticulum, produce free radicals and participate in cell death processes. Indeed, most of these activities have been demonstrated to be affected in HD, potentially contributing for the neuronal dysfunction in pre-symptomatic stages. This chapter resumes some of the evidences that pose mitochondria as a main regulatory organelle in HD-affected neurons, uncovering some potentially therapeutic mitochondrial-based relevant targets.

Entities: Chemical Disease Gene

Keywords: Calcium dyshomeostasis; Cell death; Metabolic deficits; Mitochondrial dynamics; Oxidative stress

Mesh：

Year: 2018 PMID： 29427098 DOI： 10.1007/978-3-319-71779-1_3

Source DB: PubMed Journal: Adv Exp Med Biol ISSN： 0065-2598 Impact factor: 2.622

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Cited

37 in total

1. Sodium selenite protects from 3-nitropropionic acid-induced oxidative stress in cultured primary cortical neurons.

Authors: Dirleise Colle; Danúbia Bonfanti Santos; Viviane de Souza; Mark William Lopes; Rodrigo Bainy Leal; Patricia de Souza Brocardo; Marcelo Farina
Journal: Mol Biol Rep Date: 2018-12-03 Impact factor: 2.316

2. Circadian dysfunction in the Q175 model of Huntington's disease: Network analysis.

Authors: Benjamin Smarr; Tamara Cutler; Dawn H Loh; Takashi Kudo; Dika Kuljis; Lance Kriegsfeld; Cristina A Ghiani; Christopher S Colwell
Journal: J Neurosci Res Date: 2019-07-29 Impact factor: 4.164

Review 3. Mitochondrial Genetic Disorders: Cell Signaling and Pharmacological Therapies.

Authors: Fatima Djouadi; Jean Bastin
Journal: Cells Date: 2019-03-28 Impact factor: 6.600

4. Ursodeoxycholic acid as a potential alternative therapeutic approach for neurodegenerative disorders: Effects on cell apoptosis, oxidative stress and inflammation in the brain.

Authors: Fei Huang
Journal: Brain Behav Immun Health Date: 2021-09-21

5. Inhibition of Drp1 hyperactivation reduces neuropathology and behavioral deficits in zQ175 knock-in mouse model of Huntington's disease.

Authors: Yuanyuan Zhao; Xiaoyan Sun; Xin Qi
Journal: Biochem Biophys Res Commun Date: 2018-11-16 Impact factor: 3.575

6. Huntington's disease mice and human brain tissue exhibit increased G3BP1 granules and TDP43 mislocalization.

Authors: Isabella I Sanchez; Thai B Nguyen; Whitney E England; Ryan G Lim; Anthony Q Vu; Ricardo Miramontes; Lauren M Byrne; Sebastian Markmiller; Alice L Lau; Iliana Orellana; Maurice A Curtis; Richard Lewis Maxwell Faull; Gene W Yeo; Christie D Fowler; Jack C Reidling; Edward J Wild; Robert C Spitale; Leslie M Thompson
Journal: J Clin Invest Date: 2021-06-15 Impact factor: 14.808

Mitochondrial Dysfunction in Huntington's Disease.

1. Sodium selenite protects from 3-nitropropionic acid-induced oxidative stress in cultured primary cortical neurons.

2. Circadian dysfunction in the Q175 model of Huntington's disease: Network analysis.

Review 3. Mitochondrial Genetic Disorders: Cell Signaling and Pharmacological Therapies.

4. Ursodeoxycholic acid as a potential alternative therapeutic approach for neurodegenerative disorders: Effects on cell apoptosis, oxidative stress and inflammation in the brain.

5. Inhibition of Drp1 hyperactivation reduces neuropathology and behavioral deficits in zQ175 knock-in mouse model of Huntington's disease.

6. Huntington's disease mice and human brain tissue exhibit increased G3BP1 granules and TDP43 mislocalization.

Review 7. Cellular functions of the protein kinase ATM and their relevance to human disease.

Review 8. Purinergic Signaling in the Pathophysiology and Treatment of Huntington's Disease.

Review 9. Mitochondrial Ca²⁺ Signaling in Health, Disease and Therapy.

10. Accelerated expansion of pathogenic mitochondrial DNA heteroplasmies in Huntington's disease.

Mitochondrial Dysfunction in Huntington's Disease.

1. Sodium selenite protects from 3-nitropropionic acid-induced oxidative stress in cultured primary cortical neurons.

2. Circadian dysfunction in the Q175 model of Huntington's disease: Network analysis.

Review 3. Mitochondrial Genetic Disorders: Cell Signaling and Pharmacological Therapies.

4. Ursodeoxycholic acid as a potential alternative therapeutic approach for neurodegenerative disorders: Effects on cell apoptosis, oxidative stress and inflammation in the brain.

5. Inhibition of Drp1 hyperactivation reduces neuropathology and behavioral deficits in zQ175 knock-in mouse model of Huntington's disease.

6. Huntington's disease mice and human brain tissue exhibit increased G3BP1 granules and TDP43 mislocalization.

Review 7. Cellular functions of the protein kinase ATM and their relevance to human disease.

Review 8. Purinergic Signaling in the Pathophysiology and Treatment of Huntington's Disease.

Review 9. Mitochondrial Ca2+ Signaling in Health, Disease and Therapy.

10. Accelerated expansion of pathogenic mitochondrial DNA heteroplasmies in Huntington's disease.

Review 9. Mitochondrial Ca²⁺ Signaling in Health, Disease and Therapy.