Bach1 derepression is neuroprotective in a mouse model of Parkinson’s disease

Ahuja, Manuj; Kaidery, Navneet Ammal; Attucks, Otis C.; McDade, Erin; Hushpulian, Dmitry M.; Gaisin, Arsen; Gaisina, Irina N.; Ahn, Young Hoon; Никулин, С. В.; Полозников, А. А.; Gazaryan, Irina G.; Yamamoto, Masayuki; Matsumoto, Mitsuyo; Igarashi, Kazuhiko; Sharma, Sudarshana M.; Thomas, Bobby

doi:10.1073/pnas.2111643118

Cited by 31 publications

(34 citation statements)

References 59 publications

(100 reference statements)

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“…It is thought that microgliosis occurs early in disease progression and is sustained over its course [229]. This observed increased in microglial occupation could also explain a recent report of increased BACH1 expression in the PD post-mortem midbrain [230]. As we show in Figure 2b, microglia are enriched with Bach1, a transcriptional repressor of ARE-containing genes [4], so they would be a likely contributor.…”

Section: The Role Of Non-neuronal Cells In Responses To Oxidative Stresssupporting

confidence: 70%

“…As we show in Figure 2 b, microglia are enriched with Bach1 , a transcriptional repressor of ARE-containing genes [ 4 ], so they would be a likely contributor. This study goes on to show that BACH1 KO animals are more resilient to MPTP treatments, that and BACH1 inhibitors in wild-type animals attenuate MPTP-mediated toxicity [ 230 ]. These data suggest that the knockdown of BACH1 could be a viable strategy for promoting the neuroprotection of DAergic neurons in the context of PD.…”

Section: Oxidative Stress and The Transcriptional Regulation Of Antioxidant Defense Enzymes In Disease Statesmentioning

confidence: 99%

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The NRF2-Dependent Transcriptional Regulation of Antioxidant Defense Pathways: Relevance for Cell Type-Specific Vulnerability to Neurodegeneration and Therapeutic Intervention

2021

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Oxidative stress has been implicated in the etiology and pathobiology of various neurodegenerative diseases. At baseline, the cells of the nervous system have the capability to regulate the genes for antioxidant defenses by engaging nuclear factor erythroid 2 (NFE2/NRF)-dependent transcriptional mechanisms, and a number of strategies have been proposed to activate these pathways to promote neuroprotection. Here, we briefly review the biology of the transcription factors of the NFE2/NRF family in the brain and provide evidence for the differential cellular localization of NFE2/NRF family members in the cells of the nervous system. We then discuss these findings in the context of the oxidative stress observed in two neurodegenerative diseases, Parkinson’s disease (PD) and amyotrophic lateral sclerosis (ALS), and present current strategies for activating NFE2/NRF-dependent transcription. Based on the expression of the NFE2/NRF family members in restricted populations of neurons and glia, we propose that, when designing strategies to engage these pathways for neuroprotection, the relative contributions of neuronal and non-neuronal cell types to the overall oxidative state of tissue should be considered, as well as the cell types which have the greatest intrinsic capacity for producing antioxidant enzymes.

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Section: The Role Of Non-neuronal Cells In Responses To Oxidative Stresssupporting

confidence: 70%

Section: Oxidative Stress and The Transcriptional Regulation Of Antioxidant Defense Enzymes In Disease Statesmentioning

confidence: 99%

The NRF2-Dependent Transcriptional Regulation of Antioxidant Defense Pathways: Relevance for Cell Type-Specific Vulnerability to Neurodegeneration and Therapeutic Intervention

2021

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“…BACH1 has recently gained visibility as a potential therapeutic target against a variety of conditions ranging from Parkinson's disease [ 18 ], bone destructive diseases [ 24 ], non-alcoholic steatohepatitis [ 30 ], atherosclerosis [ 31 ], insulin resistance [ 28 ], coronary artery disease [ 51 ] and aging related conditions [ 25 ]. In addition, BACH1 is a promising therapeutic target against tumour metastasis in various tumour types [ 40 , 43 , [52] , [53] , [54] , [55] , [56] ].…”

Section: Discussionmentioning

confidence: 99%

“…Despite their therapeutic potential for a variety of conditions, including Huntington's and Parkinson's disease [ 18 , 19 ], spinal cord injury [ 20 , 21 ], ischemia/reperfusion injury [ 22 ], pulmonary fibrosis [ 23 ], and cancer [ [24] , [25] , [26] , [27] , [28] , [29] , [30] , [31] ], only a few BACH1 inhibitors/degraders have been identified so far. The most widely used BACH1 degrader is hemin, a heme derivative.…”

Section: Introductionmentioning

confidence: 99%

“…Based on the differential effect of BACH1 versus KEAP1 inhibitors, we expect drugs with dual activity, targeting both transcription factors, to have broader and stronger anti-inflammatory and antioxidant properties with potentially greater therapeutic value than drugs targeting either protein individually. In that regard, we have reported a chemical derivative of cannabidiol with dual activity and protective effects in a cellular model of Huntington's disease [ 19 ] and a recent work characterised a novel dual BACH1/KEAP1 inhibitor with protective effects in a Parkinson's model [ 18 ].…”

Section: Introductionmentioning

confidence: 99%

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The synthetic triterpenoids CDDO-TFEA and CDDO-Me, but not CDDO, promote nuclear exclusion of BACH1 impairing its activity

Casares

Moreno²,

Ali³

et al. 2022

Redox Biology

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Selective activation of cellular stress response pathways by fumaric acid esters

Erler,

Krafczyk,

Steinbrenner

et al. 2024

FEBS Open Bio

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The cellular response to oxidants or xenobiotics comprises two key pathways, resulting in modulation of NRF2 and FOXO transcription factors, respectively. Both mount a cytoprotective response, and their activation relies on crucial protein thiol moieties. Using fumaric acid esters (FAEs), known thiol‐reactive compounds, we tested for activation of NRF2 and FOXO pathways in cultured human hepatoma cells by dimethyl/diethyl as well as monomethyl/monoethyl fumarate. Whereas only the diesters caused acute glutathione depletion and activation of the stress kinase p38MAPK, all four FAEs stimulated NRF2 stabilization and upregulation of NRF2 target genes. However, no significant FAE‐induced activation of FOXO‐dependent target gene expression was observed. Therefore, while both NRF2 and FOXO pathways are responsive to oxidants and xenobiotics, FAEs selectively activate NRF2 signaling.

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Bach1 derepression is neuroprotective in a mouse model of Parkinson’s disease

Cited by 31 publications

References 59 publications

The NRF2-Dependent Transcriptional Regulation of Antioxidant Defense Pathways: Relevance for Cell Type-Specific Vulnerability to Neurodegeneration and Therapeutic Intervention

The NRF2-Dependent Transcriptional Regulation of Antioxidant Defense Pathways: Relevance for Cell Type-Specific Vulnerability to Neurodegeneration and Therapeutic Intervention

The synthetic triterpenoids CDDO-TFEA and CDDO-Me, but not CDDO, promote nuclear exclusion of BACH1 impairing its activity

Selective activation of cellular stress response pathways by fumaric acid esters

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