Early 7,8-Dihydroxyflavone Administration Ameliorates Synaptic and Behavioral Deficits in the Young FXS Animal Model by Acting on BDNF-TrkB Pathway

Chen, Yu‐Shan; Zhang, Siming; Tan, Wei; Zhu, Qiong; Yue, Chao-xiong; Xiang, Peng; Li, Jinquan; Wei, Zhen; Zeng, Yan

doi:10.1007/s12035-023-03226-w

“…The discovery of 7,8-DHF as a direct PDXP inhibitor was unexpected. Interestingly, numerous in vivo studies have reported the effectiveness of 7,8-DHF in brain disorder models, including rodent models of Alzheimer’s disease ( Zhang et al, 2014a ; Devi and Ohno, 2012 ; Bollen et al, 2013 ; Castello et al, 2014 ; Aytan et al, 2018 ; Gao et al, 2016 ; Akhtar et al, 2021 ; Hsiao et al, 2014 ), depression ( Blugeot et al, 2011 ; Zhang et al, 2014b ; Yao et al, 2016 ; Zhang et al, 2016 ; Li et al, 2022 ; Amin et al, 2020 ), schizophrenia ( Jaehne et al, 2021 ; Han et al, 2016 ; Yang et al, 2014 ; Han et al, 2017 ; Ren et al, 2013 ), epilepsy ( Becker et al, 2015 ; Guarino et al, 2022 ), and autism ( Johnson et al, 2012 ; Kang et al, 2017 ; Lee and Han, 2019 ; Chen et al, 2023 ). Although PLP deficiency is thought to contribute to the respective human conditions ( di Salvo et al, 2012 ; Majewski et al, 2016 ; Sorolla et al, 2016 ), PLP-dependent processes have not yet been considered in the context of 7,8-DHF-induced effects.…”

Section: Discussionmentioning

confidence: 99%

7,8-Dihydroxyflavone is a direct inhibitor of human and murine pyridoxal phosphatase

Brenner,

Zink,

Witzinger

et al. 2024

eLife

2

0

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Vitamin B6 deficiency has been linked to cognitive impairment in human brain disorders for decades. Still, the molecular mechanisms linking vitamin B6 to these pathologies remain poorly understood, and whether vitamin B6 supplementation improves cognition is unclear as well. Pyridoxal phosphatase (PDXP), an enzyme that controls levels of pyridoxal 5’-phosphate (PLP), the co-enzymatically active form of vitamin B6, may represent an alternative therapeutic entry point into vitamin B6-associated pathologies. However, pharmacological PDXP inhibitors to test this concept are lacking. We now identify a PDXP and age-dependent decline of PLP levels in the murine hippocampus that provides a rationale for the development of PDXP inhibitors. Using a combination of small molecule screening, protein crystallography and biolayer interferometry, we discover and analyze 7,8-dihydroxyflavone (7,8-DHF) as a direct and potent PDXP inhibitor. 7,8-DHF binds and reversibly inhibits PDXP with low micromolar affinity and sub-micromolar potency. In mouse hippocampal neurons, 7,8-DHF increases PLP in a PDXP-dependent manner. These findings validate PDXP as a druggable target. Of note, 7,8-DHF is a well-studied molecule in brain disorder models, although its mechanism of action is actively debated. Our discovery of 7,8-DHF as a PDXP inhibitor offers novel mechanistic insights into the controversy surrounding 7,8-DHF-mediated effects in the brain.

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“…The discovery of 7,8-DHF as a direct PDXP inhibitor was unexpected. Interestingly, numerous in vivo studies have reported the effectiveness of 7,8-DHF in brain disorder models, including rodent models of Alzheimer's disease (49)(50)(51)(52)(53)(54)(55)(56), depression (57)(58)(59)(60)(61)(62), schizophrenia (63)(64)(65)(66)(67), or epilepsy (68,69), as well as in rodent models of autism (70)(71)(72)(73).…”

Section: Discussionmentioning

confidence: 99%

“…The discovery of 7,8-DHF as a direct PDXP inhibitor was unexpected. Interestingly, numerous in vivo studies have reported the effectiveness of 7,8-DHF in brain disorder models, including rodent models of Alzheimer's disease (50)(51)(52)(53)(54)(55)(56)(57), depression (58)(59)(60)(61)(62)(63), schizophrenia (64)(65)(66)(67)(68), epilepsy (69,70) and autism (71)(72)(73)(74). Although PLP deficiency is thought to contribute to the respective human conditions (3,75,76), PLP-dependent processes have not yet been considered in the context of 7,8-DHF-induced effects.…”

Section: Discussionmentioning

confidence: 99%

7,8-Dihydroxyflavone is a direct inhibitor of pyridoxal phosphatase

Brenner,

Zink,

Witzinger

et al. 2023

Preprint

0

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Vitamin B6 deficiency has been linked to cognitive impairment in human brain disorders for decades. Still, the molecular mechanisms linking vitamin B6 to these pathologies remain poorly understood, and whether vitamin B6 supplementation improves cognition is unclear as well. Pyridoxal phosphatase (PDXP), an enzyme that controls levels of pyridoxal 5’-phosphate (PLP), the co-enzymatically active form of vitamin B6, may represent an alternative therapeutic entry point into vitamin B6-associated pathologies. However, pharmacological PDXP inhibitors to test this concept are lacking. We now identify a PDXP and age-dependent decline of PLP levels in the murine hippocampus that provides a rationale for the development of PDXP inhibitors. Using a combination of small molecule screening, protein crystallography and biolayer interferometry, we discover and analyze 7,8-dihydroxyflavone (7,8-DHF) as a direct and potent PDXP inhibitor. 7,8-DHF binds and reversibly inhibits PDXP with low micromolar affinity and sub-micromolar potency. In mouse hippocampal neurons, 7,8-DHF increases PLP in a PDXP-dependent manner. These findings validate PDXP as a druggable target. Of note, 7,8-DHF is a well-studied molecule in brain disorder models, although its mechanism of action is actively debated. Our discovery of 7,8-DHF as a PDXP inhibitor offers novel mechanistic insights into the controversy surrounding 7,8-DHF-mediated effects in the brain.

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“…Brain-derived neurotrophic factor (BDNF) plays an important role in the survival, growth and differentiation of neuronal cells, while tyrosine kinase receptor B (TrkB) is the main receptor of BDNF which performs a regulatory role in downstream signaling pathways after binding to BDNF and activating its biological effects. Studies have shown alterations in the expressions of BDNF and TrkB in the hippocampus of autism mouse model, indicating that these proteins are associated with autism [6]. In addition, it was found that simvastatin improved the behavioral performance of VPA-induced autism model in mice [7].…”

Section: Introductionmentioning

confidence: 95%

Effect of simvastatin on brain-derived neurotrophic factor (BDNF)/TrkB pathway in hippocampus of autism rat model

Chen¹,

Cai²,

Xu³

2023

Trop. J. Pharm Res

0

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Purpose: To study the effect of simvastatin on behavioral performance in a rat model of autism, and its effect on hippocampal brain-derived BDNF-TrkB pathway. Methods: Twelve rats with valproic acid (VPA)-induced autism were randomly divided into model group and simvastatin group, while six healthy rats served as normal control group. Rats in the simvastatin group received the drug (5 mg/kg) via i.p. route, while rats in model group and normal control group were injected with equivalent volume of normal saline in place of simvastatin. Capacity for interaction and repetitive stereotyped behavior, as well as results of Morris water maze test were determined for each group. The expressions of BDNF-TrkB proteins were assayed with immunoblotting. Results: The frequencies of sniffing normal saline, alcohol and rat urine were significantly higher in model and simvastatin rats than in normal rats, but they were significantly lower in simvastatin-treated rats than in model rats (p < 0.05). There was higher duration of turning, jumping and grooming in the model group and simvastatin group than in the normal rats, but the duration was significantly reduced in simvastatin rats, relative to model rats. Escape latency times was significantly longer in model and simvastatin rats than in controls, but number of target quadrant crossings was significantly reduced. However, escape latency time was lower in simvastatin rats than in model rats, but number of target quadrant crossings was significantly higher. The model and simvastatin rats had down-regulated levels of BDNF and TrkB protein, relative to control rats, but there were markedly higher levels of these proteins in simvastatin-treated rats than in model rats. Conclusion: Simvastatin improves the behavioral performance of autistic rats by regulating BDNF/TrkB signal axis. This finding may be useful in the development of new drugs for treating autism.

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Early 7,8-Dihydroxyflavone Administration Ameliorates Synaptic and Behavioral Deficits in the Young FXS Animal Model by Acting on BDNF-TrkB Pathway

Cited by 14 publications

References 60 publications

7,8-Dihydroxyflavone is a direct inhibitor of human and murine pyridoxal phosphatase

7,8-Dihydroxyflavone is a direct inhibitor of human and murine pyridoxal phosphatase

7,8-Dihydroxyflavone is a direct inhibitor of pyridoxal phosphatase

Effect of simvastatin on brain-derived neurotrophic factor (BDNF)/TrkB pathway in hippocampus of autism rat model

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