Selective Targeting of Non-nuclear Estrogen Receptors with PaPE-1 as a New Treatment Strategy for Alzheimer’s Disease

Wnuk, Agnieszka; Przepiórska, Karolina; Rzemieniec, Joanna; Pietrzak, Bernadeta Angelika; Kajta, Małgorzata

doi:10.1007/s12640-020-00289-8

Cited by 13 publications

(12 citation statements)

References 28 publications

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“…Furthermore, in the present study, PaPE-1-evoked neuroprotection was mediated through a reduction in ROS formation and enhancement of cellular metabolic activity that was dysregulated in the course of hypoxia and ischemia. Previously, we showed that PaPE-1 has the ability to reduce ROS formation and to prevent apoptosis through the restoration of the mitochondrial membrane potential and BAX/BCL2 ratio as well as the downregulation of Fas/ FAS expression (Wnuk et al 2020a), which concurs with the results of the present research. Interestingly, estrogen deficiency appeared to predispose brain neurons to apoptosis following cerebral ischemia (Guo et al 2017), which supports essential roles of estrogen-based compounds such as PaPE-1 in pharmacotherapy of stroke and perinatal asphyxia.…”

Section: Discussionsupporting

confidence: 93%

“…However, similar to E2, PaPE-1 strongly activates the MAPK and mTOR pathways. The neuroprotective capacity of PaPE-1 against Amyloid β (Aβ)-induced neurotoxicity and apoptosis has already been evidenced by our group (Wnuk et al 2020a). We showed that following 24 h of exposure, PaPE-1 inhibited Aβ-evoked effects, as shown by reduced parameters of neurotoxicity, oxidative stress, and apoptosis.…”

Section: Introductionmentioning

confidence: 84%

“…Newly synthesized PaPE-1 selectively activates membrane (nonnuclear/extranuclear) estrogen receptors (ERs), namely, mERα, and mERβ, and has been shown to evoke neuroprotection in a cellular model of AD and in a mouse model of stroke, specifically transient middle cerebral artery occlusion (tMCAO). PaPE-1 appeared to inhibit both Aβ-induced neurotoxicity in mouse primary neurons in in vitro cultures and tMCAO-evoked infarction and leukocyte infiltration into the ischemic mouse brain (Wnuk et al 2020a;Selvaraj et al 2018). However, until recently, PaPE-1's effectiveness in protecting brain tissue against hypoxia/ischemia has been verified only in a pretreatment paradigm, namely, PaPE-1 was administered 24 h before inducing brain lesions via tMCAO.…”

Section: Discussionmentioning

confidence: 99%

“…Primary neocortical cultures were prepared from CD-1 ® IGS Swiss mouse embryos at 15 days of gestation (Charles River, Germany) as previously described (Kajta et al 2006;Wnuk et al 2020a, b). The cortices were mechanically and then enzymatically fragmented with 0.1% trypsin for 15 min at 37 °C.…”

Section: Primary Neuronal Cell Culturementioning

confidence: 99%

“…During reoxygenation, cells were cultured in a humidified incubator (New Brunswick Scientific, NJ, USA). PaPE-1 was dissolved in DMSO, not exceeding a concentration of 0.1% in the culture medium, as previously described (Wnuk et al 2020a).…”

Section: Treatmentmentioning

confidence: 99%

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Posttreatment Strategy Against Hypoxia and Ischemia Based on Selective Targeting of Nonnuclear Estrogen Receptors with PaPE-1

et al. 2021

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Newly synthesized Pathway Preferential Estrogen-1 (PaPE-1) selectively activates membrane estrogen receptors (mERs), namely, mERα and mERβ, and has been shown to evoke neuroprotection; however, its effectiveness in protecting brain tissue against hypoxia and ischemia has not been verified in a posttreatment paradigm. This is the first study showing that a 6-h delayed posttreatment with PaPE-1 inhibited hypoxia/ischemia-induced neuronal death, as indicated by neutral red uptake in mouse primary cell cultures in vitro. The effect was accompanied by substantial decreases in neurotoxicity and neurodegeneration in terms of LDH release and Fluoro-Jade C staining of damaged cells, respectively. The mechanisms of the neuroprotective action of PaPE-1 also involved apoptosis inhibition demonstrated by normalization of both mitochondrial membrane potential and expression levels of apoptosis-related genes and proteins such as Fas, Fasl, Bcl2, FAS, FASL, BCL2, BAX, and GSK3β. Furthermore, PaPE-1-evoked neuroprotection was mediated through a reduction in ROS formation and restoration of cellular metabolic activity that had become dysregulated due to hypoxia and ischemia. These data provide evidence that targeting membrane non-GPER estrogen receptors with PaPE-1 is an effective therapy that protects brain neurons from hypoxic/ischemic damage, even when applied with a 6-h delay from injury onset.

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Section: Discussionsupporting

confidence: 93%

Section: Introductionmentioning

confidence: 84%

Section: Discussionmentioning

confidence: 99%

Section: Primary Neuronal Cell Culturementioning

confidence: 99%

Section: Treatmentmentioning

confidence: 99%

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Posttreatment Strategy Against Hypoxia and Ischemia Based on Selective Targeting of Nonnuclear Estrogen Receptors with PaPE-1

et al. 2021

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Estrogenic hormones receptors in Alzheimer’s disease

2021

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Posttreatment with PaPE-1 Protects from Aβ-Induced Neurodegeneration Through Inhibiting the Expression of Alzheimer’s Disease-Related Genes and Apoptosis Process That Involves Enhanced DNA Methylation of Specific Genes

Pietrzak-Wawrzyńska,

Wnuk,

Przepiórska-Drońska

et al. 2023

Mol Neurobiol

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Targeting the non-nuclear estrogen receptor (ER) signaling has been postulated as novel therapeutic strategy for central nervous system pathologies. Recently, we showed that newly designed PaPE-1 (Pathway Preferential Estrogen-1), which selectively activates ER non-nuclear signaling pathways, elicited neuroprotection in a cellular model of Alzheimer’s disease (AD) when it was applied at the same time as amyloid-β (Aβ). Since delayed treatment reflects clinical settings better than cotreatment does, current basic study proposes a novel therapeutic approach for AD that relies on a posttreatment with PaPE-1. In this study, mouse neuronal cell cultures treated with preaggregated Aβ1-42 (10 µM) showed the presence of extracellular Aβ1-42, confirming the adequacy of the AD model used. We are the first to demonstrate that a 24-h delayed posttreatment with PaPE-1 decreased the degree of Aβ-induced neurodegeneration, restored neurite outgrowth, and inhibited the expression of AD-related genes, i.e., Rbfox, Apoe, Bace2, App, and Ngrn, except for Chat, which was stimulated. In addition, PaPE-1 elicited anti-apoptotic effects by inhibiting Aβ-induced caspase activities as well as attenuating apoptotic chromatin condensation, and in these ways, PaPE-1 prevented neuronal cell death. Posttreatment with PaPE-1 also downregulated the Aβ-affected mRNA expression of apoptosis-specific factors, such as Bax, Gsk3b, Fas, and Fasl, except for Bcl2, which was upregulated by PaPE-1. In parallel, PaPE-1 decreased the protein levels of BAX, FAS, and FASL, which were elevated in response to Aβ. PaPE-1 elicited a decrease in the BAX/BCL2 ratio that corresponds to increased methylation of the Bax gene. However, the PaPE-1-evoked Bcl2 gene hypermethylation suggests other PaPE-1-dependent mechanisms to control Aβ-induced apoptosis.

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Selective Targeting of Non-nuclear Estrogen Receptors with PaPE-1 as a New Treatment Strategy for Alzheimer’s Disease

Cited by 13 publications

References 28 publications

Posttreatment Strategy Against Hypoxia and Ischemia Based on Selective Targeting of Nonnuclear Estrogen Receptors with PaPE-1

Posttreatment Strategy Against Hypoxia and Ischemia Based on Selective Targeting of Nonnuclear Estrogen Receptors with PaPE-1

Estrogenic hormones receptors in Alzheimer’s disease

Posttreatment with PaPE-1 Protects from Aβ-Induced Neurodegeneration Through Inhibiting the Expression of Alzheimer’s Disease-Related Genes and Apoptosis Process That Involves Enhanced DNA Methylation of Specific Genes

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